These are my notes from the 13^th European Nutrition Conference, arranged in Dublin, Ireland, October 15-18 2019.

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Main take-home messages

Nutrition policy is key to reach the sustainable development goals
The interaction between the MTHFR 677TT genotype, riboflavin and hypertension offers the potential for personalized nutritional prevention and treatment of hypertension in a high-risk subgroup of the population. Talks here and here.
Liver fat is a stronger predictor of insulin resistance compared to visceral adipose tissue
Low-carb/High-fat diets increases liver fat more than low-fat/high-carb diets, and in the context of similar weight gain, saturated fat induces more harm than simple sugars.
Insulin resistant people should consider lower carbohydrate diets, due to them being more satiating in this subgroup
Obesity is not driven by genetic changes, but changes in the food environment
Don’t forget GI physiology when considering the microbiome-health associations
Low-calorie sweeteners are safe, and a tool to reduce sugar intake. New report
Tissue-specific insulin resistance elicit different metabolic effects
The intake of ultra-processed foods are increasing, and is associated with negative health outcomes
Many environmental and political aspects contribute to the obesity epidemic
The omega-3/6 ratio is not a good parameter of PUFA intake or healthiness of a diet
Eating times and regularity have an impact on the risk of developing obesity

Tuesday

Plenary session 1

Drivers across the lifecycle of malnutrition in an obese world - European perspectives

Joäo Breda, WHO

Notes

Acting on nutrition is key to reach many of the sustainable development goals, e.g. 2 (zero hunger) and 3 (good health and well-being)
Europe
- Not a single country is on track to reach the global targets on alcohol, tobacco, adult obesity and salt reduction.
- Gender differences in premature mortality, especially in eastern Europe where premature mortality is more common in men
- Childhood overweight prevalence ~25%
European Food and Nutrition Action plan 2015-2020, main pillars
1. Create healthy food and drink environments
  - Sugar content of soft drinks highly variable between countries, which may help explain different rates of childhood obesity
  - We are not making progress in reducing salt intake to the recommended levels
2. Life course
  - Before and during pregnancy
  - In terms of exclusive breastfeeding, Europe is not doing good
  - The quality of complimentary food products is an arena for improvements, with high amounts of added sugar, as well as many products carrying health claims
3. Reinforce healthy systems to promote healthy diets
  - Much work need to be done to communicate infomation on healthy diets
4. Support surveillance, monitoring, evaluation and research
  - We need better data on dietary intake
5. Strengthen governance, alliances and networks to ensure a health-in-all-policies approach
  - We need more research on the implementation of selected interventions

Session 1A

The associations between genetics, salt taste perception and salt intake in young adults

Leta Pilic

Abstract

Hypertension is a major cause of cardiovascular disease and overall mortality. High dietary salt intake is one of the key risk factors for hypertension and in 2017, it was one of the three leading dietary risk factors for death and disability adjusted life years globally. Despite the efforts to change this behaviour, salt consumption still exceeds the recommendations. One of the main determinants of food intake, and potentially salt, is taste. Taste perception may be genetically determined, however research exploring the associations between genetics, salt taste perception and salt intake is scarce. This may be of special importance in younger adult populations where increased preference for salt is suggested. Therefore, the aim of this study was to explore the associations between genetics, salt taste perception (taste threshold and preference) and salt intake in young adults.

This study was approved by the St Mary’s University Ethics Sub-Committee. Forty-two participants (18-35 years, 67% female and 33% male) completed the study. Salt taste thresholds were identified using the British Standards Institution sensory analysis method (BS ISO 3972:2011) and preference for salty taste by asking participants how salty they usually prefer to eat their food using a Likert scale. Salt intake, expressed as mg sodium/1000 kcal, was measured using a five-step multiple pass 24-hour recall for one day of the week and one weekend day. Participants were genotyped for two genetic variants in the SCNN1B and TRPV1 genes, which code for ion channels expressed in taste cells. Multiple regression analysis was performed including SCNN1B and TRPV1 variants, salt taste threshold and preference as predictor variables and sodium intake (mg/1000 kcal) as the dependent variable. Statistical significance was set at p<0.05.

Participants were normal weight (Body Mass Index 23.8±3.7 kg/m2), predominantly Caucasian with salt intake 7.5±2.7g per day, reflecting current intakes in the UK. Regression model including genetics, thresholds and preference for salty taste explained 54% of the variance (p=0.028). In this model, TRPV1 variant rs8065080 [β=422, confidence interval (50, 794), p=0.030] and salt preference [β=618, confidence interval (258, 978), p=0.004] were indicated as predictors of sodium intake. These findings suggest that genetics and preference for salty taste may be drivers of salt intake in younger populations. If replicated, this information may in the future be used in designing more personalised approaches in changing this behaviour.

Notes

-High salt intake is the #1 dietary risk factor, and we eat too much. But what is driving our high intakes? - Lower salt taste sensitivity = higher threshold for salt intake - Salt taste preference - Genetic predisposition to salt taste perception paper - Salt taste preference was associated with salt intake, those preferring salty foods also eats more salt - Genetics, salt taste perception (threshold and preference) and habits explains 16 % of the variation in salt intake

Central blood pressure in adults screened for a genetic polymorphism in folate metabolism

Martina Rooney

Abstract

As the primary risk factor for cardiovascular disease (CVD), hypertension is the leading cause of preventable, premature mortality globally. Hypertension, or elevated blood pressure (BP), has a number of well-established risk factors, including genetics. A common C677T polymorphism in the gene encoding the folate metabolising enzyme methylenetetrahydrofolate reductase (MTHFR) affects 10-12% of UK and Irish populations and has been linked with 24-87% increased risk of hypertension globally. Evidence from randomised controlled trials (RCTs) conducted at this Centre has shown BP to be highly responsive (by 5-13 mmHg) to supplementation with riboflavin (MTHFR co-factor), an effect confined to homozygous individuals (TT genotype). To date, our trials have focused on peripheral BP; however, additional measures of vascular health such as central pressure are reported to be more closely correlated with CVD risk. Investigation of central BP, augmentation index (AIx) and pulse pressure amplification (PPA) may thus offer further insight into the role of this gene-nutrient interaction in blood pressure. The present study aims to investigate BP, and measures of vascular health in healthy adults stratified by MTHFR 677 genotype. Apparently healthy adults aged 18-60 years were recruited from workplaces across Northern Ireland and screened for MTHFR genotype via buccal swab. Clinic BP, anthropometry and blood sample were measured in TT individuals (n 209) and age and sex-matched CC (n 98) and CT (n 102) controls. AIx and central BP were assessed using SphygmoCor® (AtCor Medical, Australia). Preliminary results demonstrate higher BP in individuals with the MTHFR 677TT genotype compared to non-TT controls (systolic BP 134.7 ± 13.8 mmHg vs 129.7 ± 12.4 mmHg, P<0.001; diastolic BP 81.6 ± 9.5 mmHg vs 79.7 mmHg ± 8.9 mmHg, P=0.023, respectively). The MTHFR 677TT genotype group had significantly higher central systolic BP (119.4 ± 11.8 vs 116.7 ± 10.9 mmHg, P=0.018), central pulse pressure (P=0.006) and central mean pressure (P=0.011) compared to the non-TT group. No significant differences for central diastolic BP, pulse pressure amplification, pulse pressure ratio and augmentation index were observed. This study confirms the phenotype of elevated BP in individuals with the C677T polymorphism in the gene encoding MTHFR. For the first time, this study reports that individuals with the MTHFR 677TT genotype have higher central systolic BP, central mean pressure and pulse pressure. Further investigations through RCTs investigating the effect of the MTHFR cofactor, riboflavin, on central blood pressure in these genetically at-risk adults are warranted.

Notes

Genes are commonly thought of as non-modifiable risk factors
Gene-nutrient interactions challenge this notion
Previous research focused on peripheral blood pressure, this study expand the findings to central measures of hypertension.

Intakes and status of riboflavin in a representative sample of Irish adults aged 18-90 years screened for MTHFR C677T polymorphism

Emma O’Sullivan

Abstract

Meta-analyses of epidemiological data report that adults who carry a common polymorphism, the MTHFR 677C→T, in the gene encoding the folate-metabolising enzyme methylenetetrahydrofolate reductase (MTHFR) have a 40% increased risk of CVD and an 87% increased risk of hypertension. Riboflavin (vitamin B2), in its co-enzymatic form flavin adenine nucleotide (FAD), is required as a co-factor by MTHFR and previous trials in hypertensive patients have shown a blood pressure lowering response to riboflavin supplementation that is specific to individuals homozygous for this polymorphism (TT genotype). Low folate status is commonly reported in adults with the TT genotype however the effect of this genetic variant on riboflavin status has not previously been investigated. The aim of this study, therefore, was to investigate dietary intake and biomarker status of riboflavin by MTHFR genotype in Irish adults using data from the National Adult Nutrition Survey (2008-2010) (www.iuna.net).

A 4-day semi-weighed food record was used to collect food and beverage intake data from a representative sample of 1500 Irish adults (18–90 years). Dietary intake data were analysed using WISP© based on UK food composition tables (modified to include recipes of composite dishes, nutritional supplements, fortified foods and generic Irish foods that were commonly consumed). Usual intakes were calculated via the NCI-method using SAS© Enterprise Guide. Blood samples (n=1126) were collected by venepuncture by a trained professional and were processed and analysed using standard operating procedures. Biomarker status of riboflavin was determined by erthyrocyte gluthathione reductase activation coefficient (EGRac), a functional assay that measures the activity of the enzyme glutathione reductase before and after in vitro activation with its prosthetic group FAD; a lower value indicates better status.

It was found that 12% of the population had the TT genotype. As expected, there was no significant difference in riboflavin intake across the genotype (CC, CT or TT) groups. Similarly, no significant genotype differences in riboflavin status (EGRac) were observed (1.36 vs 1.37 vs 1.38 respectively). Overall, 61% of the total population had EGRac values >1.3, indicative of low/deficient status with no significant difference observed between the genotype groups (60%,61% and 61%, respectively).

These data suggest that riboflavin status is not influenced by the C677T polymorphism in MTHFR in this cohort of nationally representative Irish adults. Further research is needed to see the impact of riboflavin status on blood pressure across the genotype groups in this nationally representative cohort of Irish adults.

Notes

Riboflavin status is similar across the MTHFR 677-genotypes, suggesting that this genotype does not interfere with riboflavin status.
In Ireland, the average riboflavin intake is 3 mg/day,
14 % of irish men and 22 % of women have riboflavin intake below the EAR
There is a poor correlation between riboflavin intake and biomarker status, the DERiVE project aim to improve measures of riboflavin status.

Session 2B: Metabolic obesity

Symposium abstract

A body mass index (BMI) of 30 or above is universally accepted as the definition of obesity, and as a measure of excess body fatness that increases the risk of cardiovascular diseases (CVD). However, BMI is only a weak proxy for the strong link between excess body fat and metabolic dysfunction that increases CVD risk. This link can be attributed more specifically to the presence of excess visceral fat (visceral adipose tissue or VAT) in the abdominal cavity, and ectopic fat in key metabolic tissues such as the liver, pancreas and skeletal muscle. Excess VAT is a common finding in classic obesity (BMI>30), but also in non-obese individuals (BMI less than 30), who can be described as having an unhealthy form of metabolic ‘obesity’. In contrast, a relative lack of VAT, but excess of subcutaneous adipose tissue (SAT), that may protect against metabolic dysfunction and accumulation of ectopic fat, creates a form of obesity which in comparison to its classic and metabolic counterparts, is relatively benign or metabolically ‘healthy’. This symposium brings together three world leading experts in the field of human body composition, metabolic disease and nutrition to address the causes and consequences of metabolically healthy and unhealthy obesity, the various techniques for measuring metabolic ‘obesity’, and its dietary determinants and treatment.

Definition and clinical Impact of metabolically healthy and unhealthy Obesity

Norbert Stefan

Abstract

The prevalence of overweight and obese individuals has increased globally during the last few decades. An elevated fat mass in subjects with a BMI > 25 kg/m2 is thought to promote morbidity and mortality. However, the research into the causes and consequences of metabolically healthy obesity (MHO) has indicated that for a certain BMI, the risk of cardiometablic disease and death can vary substantially among subjects. In this respect, compared to metabolically healthy people in the normal weight range, subjects with MHO only have a moderately (~+25%) elevated risk of all-cause mortality and/or cardiovascular events. In contrast for a similar BMI, the same risk is substantially increased (~+150%) in subject with metabolically unhealthy obesity (MUHO). Among the mechanisms increasing this risk in subjects with MUHO nonalcoholic fatty liver disease (NAFLD) and dysregulated hepatokine release from NAFLD were identified. On the other spectrum of the BMI, a strongly elevated risk of all-cause mortality and/or cardiovascular events (~+180%) is being observed in about 20% of the subjects with a BMI <25 kg/m2. Here a lipodystrophy-like phenotype with a low amount of gluteofemoral or leg fat mass is the dominating parameter characterizing this phenotype. These findings may have several implications, not only for drug development, but also for clinical interventions. In particular the question of how much weight loss might be necessary to protect from cardiometabolic diseases in people with obesity; in effect, how much weight loss is necessary to move from a state of MUHO to MHO. Furthermore, risk stratification, also in subjects with normal weight, will help to accomplish the goal of providing personalized medicine to our patients.

Notes

Diabetes, pre-diabetes and risk
- Before 2010, those with diabetew had much higher CVD risk compared to pre-diabetes, but due to better treatment of diabetes the risk is now similar
Liver fat is highly correlated with insulin resistance, much stronger than the association with visceral fat
A problem with the metabolic syndrome is the criteria of at least 3 risk factors, because you can have 2 risk factors and be categorized as low-risk.
Metabolically healthy obesity - < 2 metabolic risk factors (hypertension, high TG, low HDL, low fasting glucose, high waist circumference)
Lasalle C 2017
- Metabolically healthy obese 28% increased risk, metabolically unhealthy obese 154% increased risk.
- Metabolically unhealthy normal weight 115% increased risk!

How can we measure or predict visceral fat - omics, big data and tea leaves

Louise Thomas

Abstract

Most countries across the world are reporting an increasing epidemic of obesity and obesity related co-morbidity, with type II diabetes rising to over 20% of the adult population in some places. At the same time, we are seeing report of substantial numbers of children and adolescents with marked metabolic dysfunction, including type II diabetes.

The associating between these conditions and body composition has for a long time used BMI, as a surrogate for body adiposity. With the advent of imaging methodologies, especially magnetic resonance imaging (MRI), it is now possible to determine the contribution of individual fat depots, such as visceral adipose tissue, liver, skeletal muscle and pancreatic fat content to the development and maintenance of these co-morbidities. Thus, accurate and reproducible measurements of individual fat depots can be obtained in minutes, allowing a more in-depth understanding of environmental and genetic factors associated with their deposition, retention and removal. Indeed, large scale studies, including the UK BioBank have now imaged >40,000 volunteers scanned so far, for the first time enabling studies of body composition and its impact on metabolic health to be investigated at a population level.

Despite this, and the increasing availability of MRI system across the globe, it is impractical and costly to undertake scanning of large numbers of volunteers and patients on a routine basis, even in some smaller cohorts. Thus, alternatives to MRI, that can give robust, accurate and reproducible estimates of these fat deports has been an ongoing challenge for the scientific community. In this talk, I will present the current advances in this area and discussed the new machine-learning approaches being utilised in order to provide novel tool for this work.

Notes

MRI is not for everyone (too big, metal implants, pregnancy etc)
DEXA can be used as an alternative, but cannot be compared to the MRI data as it measures a different area.
- MRI measures fat volume, including water, while DEXA measures fat mass.
Scaling factor, associations probably similar
Waist circumference as a proxy for visceral fat
- Overall good correlation, but large variation within person with the same WC. Can be used on the group level.
MRI is the gold standard, and should be used when you need to detect small changes. Simpler methods such as predictive algorithms perform less well, but are more accessible, and combined with machine learning it can be a promising approach

Effects of overfeeding different diets on the human liver

Hannele Yki-Järvinen

Notes

In Finland, diabetes and obesity is the most important risk factors for acute liver events, at any level of alcohol intake.
Metabolic NAFLD is dominated by saturated triglycerides, while genetically (PNPLA3) related NAFLD is dominated by polyunsaturated triglycerides.
Metabolic NAFLD associated the risk of insulin resistance, genetically NAFLD does not!
Low-carb/high-fat diets increase liver fat more than low-fat/high carb diets.
Saturated fat increases liver fat more than polyunsaturated fat
Simple sugard also contributes to metabolically determined NAFLD, through increasing de novo lipogenesis
In the context of similar weight gain, saturated fat induces greater metabolic harm compared to simple sugars

Session 1D: What advice does the public believe? – Challenges for researchers, policy makers and practitioners - safefood

1500-1630 Liffey Hall 1 ##### Symposium abstract > The public are becoming increasingly aware of the link between diet and health. Nutrition information is available from numerous sources including the media, internet, health professionals, social influencers and peers. The accuracy and credibility of information varies considerably. Research findings are also reported in the media and not always in the context of existing knowledge. These multiple and often apparently conflicting messages creates confusion for the public and can potentially lead to negative health impacts. A recent survey carried out by the British Dietetic Association in the United Kingdom (UK) found that the public don’t know who to trust for diet and nutrition advice while 58% of people trust nutrition advice from their personal trainer and fitness instructor and in the 18-24 year-old age group, 41% trusting the advice of a healthy eating blogger. The level of risk associated with following non-evidence based nutrition advice varies. For example, an individual temporarily following a low-carbohydrate diet promoted by a celebrity is relatively low risk, however a cancer patient following a ketogenic diet promoted by a nutrition therapist is high risk and potentially very harmful to the patient. This session will focus on the challenges faced by health communicators (including researchers, policy makers and practitioners) in promoting evidence based advice in a world where so many nutrition messages exist.

What’s driving the nutritional problem in cancer?

Robert O’Connor

Abstract

This talk will aim to discuss some of the major factors contributing to a growing challenge in communicating accurate and empowering information about the role of nutrition and cancer, both to patients, their loved ones and the wider public.

There has been a major shift in how nutritional matters are communicated, and nowhere is this more evident than in the public discourse over diet and nutrition and their relationships to health, disease and especially cancer.

There has been a huge explosion of information about diet and nutrition and monetisation of the sector has triggered a vast array of new streams of nutritional communication which bypass traditional means. Conepts such as “healthy” and “wellness” have become much more confusing to interpret and we are now starting to recognise the potential consequences for those impacted by cancer.

We will expolore some of the underlying personal, societal and media trends contributing to the current situation and try to identify some evolutions and opportunities for the communication of accurate and helpful information to the public and patients.

Notes

“Food is not medicine for a healthy person”
The dr.Google phenomenon is very real today
- Science is increasingly available, but scientific understanding is not
Meat and cancer is a good example of how the public are presented with confusing messages regarding the role of nutrition, as examplified by the recent headlines regarding the publication in Annals of Internal Medicine.

The Nutrition Maelstrom for Cancer Patients

Eileen O’Sullivan

Abstract

This presentation will outline a cancer patients experience of the abundance of misleading nutritional advice and pseudoscience that is actively targeted at cancer patients by those without the requisite qualifications and expertise, zoning in on their vulnerability and heightened emotions. There have always been snake oil salespeople but what has changed is the incredible reach those who promote their services and products have, made possible by a number of modern innovations, e.g. internet, social media, leading to a more acceptable face of an integrative or functional ‘wellness industry’ and the interpretation that healthcare practice can be democratised by popular demand rather than evidenced based science. It can be challenging for patients to discern evidenced based nutritional information from pseudoscience and potentially dangerous cancer fad diets. This is all the more difficult for patients due to the lack of oncology dietitians that should ideally be embedded within the cancer patients’ clinical team. Nutritional support is crucially important in respect of both patients’ tolerability of treatment and outcomes, but cancer patients are getting little or no appropriate professional nutritional support and therefore may seek support from non reputable sources. Cancer patients can also be influenced on nutritional decisions by well meaning but ill informed relatives and friends, all of which can be confusing and overwhelming for cancer patients.

Notes

As a cancer patient, O’Sullivan did not receive any specific nutritional advice from the hospital
Not only patients, but also their relatives, are targeted by “snake-oil salesmen”
NOt only amateurs, also doctors and nutritionists

Journalism and the proliferation of nutribabble

Philip Boucher-Hayes

Abstract

Journalist and presenter of many RTÉ television programmes on food, Philip Boucher-Hayes, takes a look at the role his own profession has played in the spread of fake food news, bad science and vested interests.

Notes

Occupy the same space as the charlatans, we need to talk to people about our research
Offer your expertise to the media!

Full disclosure - on food and nutrition

Gabriel Scally

Abstract

The opportunity to inform people about the provenance and content of what they are eating and drinking has never been better. Ready access to on-line scientific information and requirements to inform consumers of basic content and nutritional information in processed foodstuffs should be leading to greater consumer confidence. However, the growth of intensive agricultural methods and the widespread use of high volumes of industrially produced chemicals, including antibiotics and pesticides, creates a situation where it is increasingly difficult for the public to know exactly what they are putting in their bodies. Strategies to improve assurance to the public on food are needed and include better public information requirements and robust certification methods that will provide confidence to everyone that purchases food in an increasingly diverse marketplace

The Nutrition Society Postgraduate Competition - UK

1700-1830 Wicklow Hall 1 (level 2)

Low-carbohydrate diets: challenges for diabetes management and prevention?

ChaitongC huruangsuk

Abstract

Low-carbohydrate, high-fat diets (LCHF) have been promoted for type 2 diabetes (T2DM) management and prevention. In the context of weight management, a systematic review of published meta-analyses(1) demonstrated inconsistent findings regarding the effectiveness of LCHF and low-fat diets for weight loss, explained by differences in methodological quality. Definitions of LCHF varied 40g/d to <45%E carbohydrate(CHO). Interestingly, only two ‘high-quality’ meta-analyses (n=2/10) reported no weight loss difference, while ‘critically-low quality’ meta-analyses (n=5/10) reported LCHF superiority over low-fat diet for weight loss upto 4 kg difference. Meta-analyses favoring LCHF but low-quality also had higher citations, suggesting that public and scientific communities might be responding to findings generated through poor methodology.

While weight is often the main outcome, negative impacts of LCHF on micronutrients has been neglected. Avoidance of wholegrains, fruits and starchy vegetables could reduce vitamins and minerals. A systematic review(2) of LCHF reported reductions in thiamine, folate, vitamin C, magnesium, calcium, iron, and iodine intakes, and increased subclinical iodine deficiency upto 70%. Extreme avoidance could have clinical consequences sush as severe thiamine deficiency, or increased risk of poor fetal outcomes in women of child-bearing age.

LCHF could have physiological benefit on HbA1c reduction by lowering postprandial glucose and may prevent T2DM, but large prospective studies showed increased T2DM risk in men, with no benefit on reduced risk in women(3,4). It is still unclear whether amount of CHO and LCHF pattern relate to HbA1c concentration without weight loss. A cross-sectional analysis of the National Diet and Nutrition Survey(under review) showed that lower CHO intake and LCHF pattern were associated with higher HbA1c (+0.16 mmol/mol, p=0.012, per 5%E decrease in CHO; +0.10 mmol/mol, p=0.001, per 2-point increase in LCHF adherence score). This indicates that lower CHO content per se could not lower HbA1c. Other mechanisms (e.g. oxidative stress, peripheral insulin resistance) could contribute to HbA1c elevation.

LCHF is not superior to other weight-loss diets, potentially risking micronutrient deficiencies. In the context of T2DM prevention, solely lowering CHO intake does not reduce HbA1c, as multi-mechanisms may interplay. Long-term, high-quality RCTs of LCHF, either iso- or restricted-calorie, for T2DM management and prevention are needed, and micronutrients in foods/supplements should be considered.

Notes

Most meta-analyses suggests small differences (<1 kg) between low-carb and low-fat diets
Meta-analyses of lower quality and larger effect estimates are more cited, and given more attention
Low-carbohydrate diets may lower HbA1c if providing weight loss
Higher adherence to low-carb diets associated with increased HbA1c, while adherence to dietary recommendations are associated with lower HbA1c

Wednesday

Plenary session

Personalized dietary obesity weight management determined by glucose metabolism and microbiota

Arne Astrup

Abstract

About 5 years ago we discovered that the individual weight loss on a high fibre diet depended on pre-treatment glucose metabolic status i.e. that obese individuals with higher fasting glucose level lost more weight than those with normal glucose levels. This instigated re-analysis of several randomized controlled dietary intervention trials (RTC) to cross-validate the findings. Analyses of more than 10 trials provided robust evidence to support that insulin sensitive obese individuals (type A) achieve optimal satiety and weight loss on a low-fat, high carbohydrate and high-protein diet, whereas obese type 2 diabetics (type C) need the opposite, i.e. a lower-carbohydrate, high-fat and high-protein diet. The hypothesis that can explain these findings mechanistically suggests that carbohydrate tolerance is essential for meal-induced satiety during ingestion of carbohydrate-rich meals, as glucose must enter into the CNS (and probably other tissue and organs) in order to suppress hunger and induce sufficient satiety and fullness to terminate the eating episode. With increasing insulin resistance the satiety effect of carbohydrates is attenuated and the risk of overconsumption of calories is increased, unless a high secretory insulin capacity is present. The intermediate phenotype, pre-diabetics (type B), characterized by increased fasting plasma glucose, is very sensitive to the type of carbohydrate, and we found these patients gain weight rapidly on a diet with low fibre and whole grain, and on high glycemic index (GI) diets, whereas weight loss and weight control can effectively be achieved on a low GI diet with high fibre and whole grain. This dietary sensitivity among type B obese individuals might be linked to the gut microbiota, but it remains to be shown.

We found that the responsiveness to high-fibre diets also seems to depend on microbiota, e.g. the ratio of Prevotella to Bacteroides (P/B ratio), which suggests that the production of short-chain fatty acids such as butyrate, propionate and succinate by certain bacteria may stimulate satiety, potentially through an insulin sensitizing mechanism. The predictive power of P/B-ratio has been confirmed in 5 independent trials. Smaller prospective RCT’s are currently ongoing and major trials are being planned to disentangle the mechanistic interplay between diet, microbiota and appetite regulatory pathways involving peripheral tissues, gastrointestinal hormone and the brain, including the role of the glucostatic CNS sensing in appetite control. However, the use of pre-treatment fasting glucose level can be used clinically to optimize dietary management, whereas the use of microbiota biomarkers need more research.

Notes

Individual responses to weight loss diets
Multiple hormonal signals influence hunger and satiety
Glucose uptake in brain is blunted in diabetics, suggesting that carbohydrate have a satiating effect in insulin sensitive, but less so in insulin resistant individuals
NUGENOB study, low-carb (~40%) vs high-carb (~60%) diet
- Reanalysis divided by glycemig status, showed that diabetic patients lost more weight on the low-carb diet.
(Hjort 2017)
- Reanalysis of DiOGenes demonstrated that prediabetic patients following an ad libitum lower-carbohydrate diet achieved better weight loss maintenance
- Reanalysis of SHUPOS revealed that prediabetic patients responded particularly well to high-fiber diets
The Prevotella/Bacteroides ratio seem to predict the response to dietary fiber and whole grain
- Prevotella enterotype lose weight, while the bacteroides enterotype does not
- Those with the prevotella enterotype have a particular strong effect when combined with low amylase copynumbers.

Session 2A: The Nutrigenomics Journey- are we there yet? - NuGo- The Nutrigenomics Organisation

1045-1215 Wicklow Hall 2B (level 2) (ALTERNATIVE 1) ##### Symposium Abstract >Over the last 10 years there has been a rapid rise in the application of nutrigenomics techniques to Nutrition studies. It is therefore timely to examine the impact and map the way forward. We welcome a broad range of speakers who have employed nutrigenomics tools in their research to discuss the past, present and future.

The Nutrigenomics Journey- are we there yet?

Sander Kersten

Abstract

In the late 1990’s, a novel subdomain in nutritional sciences came to life called nutrigenomics. Nutrigenomics can be defined as the application of high throughput OMICS tools in nutrition research, including high throughput genotyping, transcriptomics, epigenomics, proteomics, and metabolomics. The emergence of nutrigenomics was largely technology-driven and benefitted from the characterization of the Human Genome. In the early days of nutrigenomics, many large national and international projects were initiated to explore the power of nutrigenomics and launch a new era in nutritional research. Significant expectations were raised that nutrigenomics would potentially revolutionize nutritional science, and have a lasting impact on human health. Today, about 20 years after the field erupted, the time has come to look back and reflect on what nutrigenomics has delivered. In my presentation, I will discuss to what extent nutrigenomics contributed to a more accurate prediction of the beneficial or adverse health effects of dietary components and whether nutrigenomics led to more personalized dietary recommendations on the basis of genotype. Furthermore, I will address whether nutrigenomics managed to provide genomic or metabolic signatures that allow the discrimination of healthy versus unhealthy individuals to enable early dietary intervention. In addition, I will reflect on the promise of nutrigenomics to improve our understanding of the molecular mechanism of action of dietary components. Finally, I will discuss what choices should be made to assure that nutrigenomics can continue to thrive over the next 20 years.

Notes

2 perspectives on gene-nutrient interactions
- Nutrigenomics - Food impacts genes and epigenetics
- Nutrigenetics - how our genes influences the response to food
Gene-nutrient interactions can be mono or polygenic
General problem of polygenic diseases
- We all carry ~160 risk alleles
- By following an unhealthy diet, the number of risk alleles required to develop the disease may be less
- By following a healthy diet, you can prevent or delay disease development relative to your genetic risk predisposition. This can be achieced by general or personalized recommendations.
Diet also influence gene expression, e.g. via PPARα-activation by fatty acids
Risk cannot be individually monitored, biomarkers can.
- In the future: Wearables
- Can be used to identify individuals for dietary interventions

The causes and consequences of obesity

Stephen O’Rahilly

Abstract

concern for global public health. The rising incidence of these disorders is clearly attributable to changes in the environment that promote caloric consumption and decrease energy expenditure. However we need to understand why some individuals are susceptible to obesogenic influences while others remain resistant. Similarly, it would be helpful to have a better insight into the mechanises whereby some seriously obese people completely avoid the metabolic consequences of over-nutrition while others succumb to the disabling complications of metabolic derangement despite being only modestly obese. In this lecture I will describe how human genetics has helped to enhance our understanding of our susceptibility or resistance to obesity and its adverse metabolic consequences. The findings have broad-ranging implications for the management of individual patients, for drug development and for public health strategies.

Notes

GDF is a hormone which is produced by more or less all cells as a response to stress
Circulating GDF15 goes up in many different contexts (cancer,cardiac failure, cytotoxic drugs, hypoxia…)
GDF signals to the brain in situations of stress, and facilitate aversion to that stimuli
- Has been used to make mice avoid sacharin
A role of GDF15 in body weight regulation
- Animals lacking GDF15 are more likely to become obese
- GDF15 is not postprandially regulated like glucose, insulin etc (Physiological nutrition stimuli)
- Prolonged overfeeding increases circulating GFD15 in mice (chronic nutrition stress)
- Metformin increases GDF15, and the larger the increase, the larger the weight loss
GDF15 is produced by concer cells, and contribute to cancer cachexia
In pregnancy, GDF15 increases during the first trimester, and is implicated in hyperemesis. This provides a potential target for treatment.

Nutritional Phenotyping- what does it mean

Hannelore Daniel

Abstract

We are all different! This applies not only to our physical appearance but also our metabolism and how we respond to the diet. Our metabolic phenotype is the expression of a (meta)genome x environment interaction and is closely linked to the individual health-disease trajectory. Differences between individuals are these days mainly explored via GWAS or MGWAS (meta-genome-wide association studies) that link genetic (host) and fecal microbial heterogeneity to disease susceptibility and risks. These studies have produced an enormous number of prestigious papers – but taken together they all explain as little as 10 to 15% of the variability found in human cohorts. Whereas genotyping/sequencing of the entire metagenome is easy to perform and becomes cheaper, proper phenotyping is most critical for any analysis of the metagenome-phenome relationship and this is tedious and demanding – and thus in most cases insufficient. Moreover, almost all intervention studies conducted in the life and/or biomedical sciences try to recruit their patient or volunteer cohorts as homogenous as possible to have the least variation in outcome and a normal distribution with little extremes. And, even extremes – called outliers – are frequently eliminated by statistical means for having more homogenous data. This means that the most interesting phenotypes are likely not found in scientific literature. So, we lack proper data on phenotypical variance. I shall present data from literature as well as from own studies on phenotypic differences in diet-responses (mainly acute challenge tests) that show how different but also how reproducible these metabolic responses are. Given these examples I argue that we need to define and standardize a set of phenotyping approaches for future human nutrition research and that we need new methods to describe and quantify the outcomes

Notes

Definition: “Assessing and quantifying the acute and chronic resonses of the organism to the individual food items or diet”
Phenotype = genotype * environment
Darwin: Not the strongest, not the most intelligent, but the most adaptive to change
We constantly switch between anabolic and catabolic state, but is the anabolic and catabolic space different between people?
HuMet study
- 36 hours of fasting, liquid diet etc
- Extensive phenotyping
NutriTECH study

Session 2A: The role of ‘big data’ in nutrition research - FENS 2019 Scientific Committee

Did not attend this session

Symposium Abstract

The expectation is high in some areas of research such as precision and personalized medicine that with a “Big Data” approach important research questions could be answered. Similar expectation can be assumed for precision and personalized nutrition. Further, in those nutritional research fields that address complex entities such as the microbiome/virom enormous amounts of data had to be collected and utilized. Finally, the for the elucidation of pathways it is often useful to combine data collection on different levels ranging from sequence genetic data to large molecules.

The “big data” approach requires new technologies in terms of data generation, novel and complex statistical algorithms including artificial intelligence for data treatment and the interaction with other research fields such as system biology.

In this session, examples of using the “Big Data” approach will be presented.

From Stratified Medicine to Personalised Nutrition: Can Systems Biology Help Integrate the Data?

J. Bernadette Moore

Abstract

With advances in genomics came a key concept underpinning stratified medicine and personalised nutrition. In particular, that with a better understanding of individual characteristics, e.g. genotype, could come better tailoring of pharmaceutical and nutritional therapy. Whether applied to the disciplines of medicine or nutrition, the overlapping terms of ‘stratified’, ‘personalised’, and the most ambitious ‘precision’, refer to this aim of providing targeted therapies or nutritional advice for the optimisation of individual health outcomes. Subsequent developments in the ‘omics’ fields, particularly metabolomics and proteomics; in addition to wearable technologies for tracking parameters such as blood glucose, heart rate, physical activity and even food intake, have further driven this idea. Specifically, that in following over time a virtual cloud of data from any one individual, will come personal insights into their health and, importantly, better nutrition and lifestyle strategies for reducing their risk of disease. Alongside this and the decreasing costs of nucleic acid sequencing, has come a rapid rise in companies offering direct-to-consumer genetic, and more recently gut microbiome, testing in combination with offering personalised nutrition services. While pertinent ethical questions involve who can access such services and how commercial companies are storing, using and/or re-mining consumer data; key scientific questions include how disparate datasets are integrated and how accurate predictions currently are, or may be in the future. In this regard, lessons from systems biology, which aims both to integrate data from different levels of organization (e.g. genomic, proteomic and metabolomic) and predict the emergent behaviours of biological systems or organisms as a whole, are instructive. Using examples from the application of systems approaches to non-alcoholic fatty liver disease (NAFLD), this talk will review recent advances in predictive modelling of human metabolism. Closely associated with obesity and type 2 diabetes, NAFLD is now a major public health concern worldwide. The complex pathogenesis of these ‘lifestyle diseases’ is driven by multiple dietary, lifestyle and genetic factors, and involves crosstalk between several organs and the intestinal microbiome. They are therefore ideal both for the application of systems analyses and personalised nutrition interventions. Lessons learned to date are that while human metabolism can now be computationally simulated at genome scale, current approaches to data integration and dynamic, multi-scale modelling are still evolving. Nonetheless, available models are capable of offering mechanistic insights and informing stratified medicine and personalised nutrition strategies for improving health outcomes.

Predicting personal metabolic responses to food integrating multi-omics and machine learning: The PREDICT Studies

Sarah Berry

Abstract

Developments in personalised approaches to nutrition are hindered by a lack of large-scale data integrating multiple dietary, lifestyle, physiological, genetic and metagenomic data. Understanding the role of the integrated multiple regulatory systems involved during the dynamic postprandial phase is key to unravelling inter-individual variations within a healthy phenotype and advancing precision nutrition. In the largest and most detailed studies of metabolic responses to food, the Personalized Responses to Dietary Composition studies (PREDICT) assess the genetic, metagenomic, metabolomic and meal-context drivers of postprandial metabolic responses to predict individual responses to food using a machine learning algorithm.

The PREDICT 1 multi-center postprandial study of 1,000 individuals from the UK (unrelated, identical and non-identical twins) and 100 unrelated individuals from the US, assessed postprandial (0-6h) metabolic responses to sequential mixed-nutrient dietary challenges in a clinic setting. Glycemic and lipaemic responses to multiple duplicate isocaloric meals of different macronutrient content and self-selected meals (>100,000), were tested at home using a continuous glucose monitor (CGM) and dry blood spots. Baseline factors included metabolomics, genomics, gut metagenomics and body composition. Dietary data was collected using the Zoe app and dashboard combining weighed food records, photographs, bar coding and live nutritional support. Sleep and activity were monitored using wearable devices. The ‘Big Data’ collected in PREDICT included 2 million glucose responses, 28,000 triacylglycerol (TG) measurements and 132,000 weighed meal logs.

Inter-individual variability in postprandial responses (glucose, insulin and TG) was high in the clinic setting, even between identical twins. Genetic contributions, determined by classical twin methods, for glucose, insulin and TG responses was less than 50%, 30% and 20% respectively. Identical twins shared 37% of their gut species, compared to 35% for unrelated individuals. Interim machine learning algorithm predicted 46% of the variation in glycemic responses based on meal content, meal context and participant’s baseline characteristics, excluding genetic and microbiome features. Only 29% of variation could be explained by the proportion of macronutrients in the meal.

The large and potentially modifiable variation in metabolic responses to identical meals in healthy people explains why ‘one size fits all’ nutritional guidelines are problematic. The ongoing PREDICT 1 and 2 studies, collecting more information on glucose and TG responses to thousands of meals, alongside environmental, genetic and microbiome variables, give excellent power to use machine learning to optimise and predict individual responses to foods and provide personalised nutrition advice.

The virome as a new target of research, enhancing the complexity of microbiota health relationships

Mohammad Tariq

Abstract

The gut microbiota plays a central role in human health, supporting nutrition, immune function and resistance to environmental pathogens. Diet/nutrition has been shown to impact the gut microbiota by means of shifting the abundance of bacteria, to act as primary degrader of resistant starch. The microbiota has also been shown to influences insulin sensitivity in obese individuals.

The human gut microbiota comprises all kingdoms of life including viruses, often termed the ‘virome’. Viruses outnumber prokaryotes by on average 10:1 yet despite their numerical dominance we still know very little about the virome and its contribution to health and disease states. This is in part due to insufficient reference viral genomes leading to the term ’viral dark matter’ to refer to the majority of unidentified gut viruses.

Despite these constraints recent studies suggest that the intestinal virome is dominated by bacteriophages (viruses that infect bacteria) and there is no ‘core’ gut virome amongst healthy individuals. In addition, changes in intestinal virome may be a cause of bacterial dysbiosis and chronic gastrointestinal inflammation that are a feature of inflammatory bowel disease, and type I diabetes.

New advances in ‘omic’ technologies have reduced the cost of DNA-based sequencing and increased data throughput. Current challenges with looking at the virome involve positively identifying viral genomes as they lack a universal viral marker, like 16S in bacteria. Genes associated with viruses are largely putative and thus many identifiable viral genomes are unclassified. Therefore supporting ‘omic’ data using culture-based technique to screen, identify and classify viruses is needed in order to resolve the ‘viral dark matter’ and evaluate its impact on the microbiota in health and disease.

Currently we have an established protocol looking to isolate and characterise viral DNA in ME patients. One of the limitations of these protocol is that you omit RNA viruses. We aim to characterise the virome by simultaneously isolating both single stranded and double stranded DNA and RNA viruses. Bioinformatic pipelines for the identification and analysis of viral metagenomic data remains challenging. We aim to positively identify as many of the viral contigs using multiple publicly available viral databases and thus improve the capacity to characterise the gut virome.

Session 5A: Personalised Nutrition for Health - UCD Institute of Food and Health

Symposium abstract

Personalised Nutrition or Precision Nutrition represents a new challenge for the nutrition community in a field where dietary fads come and go. The area is made further difficult not only by human complexity within a constantly changing environment, but also by the microbiome. This symposium seeks to address the hype versus hope, fact versus fallacy, that is anticipated from Personalised Nutrition research and to understand whether the Personalised Nutrition paradigm is relevant to all health/ age contexts. We anticipate a candid and provocative discussion in relation to the pros and cons of this field and to help to understand what can it deliver on, in a robust, reliable and reproducible way.

Precision nutrition for the prevention and management of cardiometabolic diseases: Hype or hope?

Frank Hu

Abstract

Recent advances in powerful tools such as genomics, metabolomics, and gut microbiome have offered new opportunities as well as challenges in the application of precision nutrition for the prevention and management of metabolic diseases such as type 2 diabetes (T2D). The integration of such technologies into epidemiological studies referred to as ‘‘systems epidemiology’’, can enhance our understanding of biological mechanisms underlying diet and human health. This approach can also enable us to achieve a better assessment of diet and nutritional status in free-living populations by identifying novel biomarkers of dietary intakes. Nutritional genomics has identified genetic variants that influence intakes and metabolism of specific nutrients and predict individuals’ variability in response to dietary interventions. Metabolomics has revealed metabolomic fingerprints of food and nutrient consumption and has uncovered new metabolic pathways that are potentially modified by diet. In addition, dietary interventions have been shown to alter abundance, composition, and activity of gut microbiota that are relevant for food metabolism and glycemic control. By integrating these technologies with big data analytics, precision nutrition has the potential to provide personalized nutrition guidance to achieve more effective T2D prevention and management. Despite recent advances, major challenges still exist, including non-replication of study results, difficulty in the translation of research findings into practice, and high cost. Although commercial companies have promoted personalized nutrition assessment and genetic testing, there is little evidence on the benefits of these approaches for improving diet and preventing disease. Therefore, it is essential to balance the investment in precision nutrition, which targets individual characteristics, with public health nutrition, which aims to improve the health of populations.

Notes

Nutritional epidemiology have shifted from focusing on single foods/nutrients to focus on larger dietary patterns and diet scores
Not all plant based diets are healthy
Dietary instruments Yuan AJE 2018
- 2 week dietary records is most accurate, and repeated measures of any method improves accuracy
Predimed
- Metabolic signature predicting adherence to Med Diet, associated with decreased CVD risk. Stronger effects were observed compared to self-reported adherence.
Metabolic networks can indicate metabolic pathways implicated in disease risk. Applying this approach to PREDIMED, identified ceramides among other as linked to increased risk, and unsaturated phospholipids as linked to reduced risk.
Obesity is not driven by genetic changes, but changes in the food environment. Therefore precision nutrition must be integrated with public health nutrition.

Personalised nutrition for the metagenome: host versus microbiome

Hannelore Daniel

Abstract

Personalized Nutrition approaches in the past created recommendations or provided products based on a small set of individual input data such as average food and nutrient intake (including likes and dislikes), a few biomarkers measured in blood and selected gene variants. Only recently has the gut microbiome as a” new entity” become part of the input panel by the ease to profile the fecal microbiome. With a number of key publications that linked fecal microbiome patterns with phenotypic parameters such as glycemic responses to defined foods, a number of start-ups have taken on this to provide “more specified” diet recommendations. However, despite around 23.000 entries in PubMed with “gut microbiota” and fecal profiling in hundreds of cohorts/populations worldwide and covering almost all possible individual genetic and lifestyle parameters, only around 12% of human fecal microbiota diversity can currently be explained. And, the contribution of the individual diet to fecal microbiota diversity and population densities of individual microbial species is in essence unknown. There can be no doubt that diets and individual ingredients affect the microbiota and its biochemical capacity to handle endogenous (during fasting and starvation) but also diet-derived constituents. The individual diversity of metabolic products derived from these processes of degrading/fermenting diet constituents is remarkable – yet their effect on the composition of the fecal microbiome seems generally overstated. Even with large quantities of fermentable fibers (that initially may even cause intestinal discomfort) fed for weeks to volunteers changed only around 0.9 % the microbiome composition. And, when taking into account that alterations of the microbiome by harsh antibiotic treatment in humans did not at all alter insulin-sensitivity or postprandial responses – it remains currently a mystery how gut microbiota and metabolic health are mechanistically linked. Personalized Nutrition of the metagenome is in the current state thus nothing more than “feeding shadows”.

Notes

Almost everything you eat have a statistically significant effect on the microbiome
Geographical location is 10 times more important than anything else with regard to microbiome.
- He 2018
- Dietary effects on microbiome is hard to replicate
The estimate that we have 10 times more bacteria than cells is wrong, but has never been questioned. It is traced back to a publication from 1972. Sender 2016
We excrete 60-80g of bacteria daily, requiring 200-250 kcal to be replaced, which is more than the amount of energy the bacteria provides to the host.
Don’t forget GI physiology when attributing everything to the microbiome
- Any changes in intestinal transit time changes the amount and diversity of the microbiome by affecting excretion of bacteria
- Altering transit times by medication influences blood glucose response.

Potential of Precision Nutrition to improve Health – Insights from biomarker approaches

Lorraine Brennan

Abstract

Metabolic profiling has great potential for aiding the delivery of Precision/Personalised Nutrition. Use of the metabolomics to track what people are eating has the potential to deliver a more objective assessment of intake which can then be used to guide improvements in a personalised manner. In this context, the use of dietary biomarkers and biomarker signatures have great potential. Dietary biomarkers have emerged as a complementary approach to the traditional methods and in recent years, metabolomics has developed as a key technology for the identification of new dietary biomarkers. Over the years a number of strategies have emerged for the discovery of dietary biomarkers including acute and medium-term interventions and cross-sectional/cohort study approaches. While each approach has advantages and disadvantages the key aspect is that the putative biomarkers are tested in different scenarios and demonstration of dose-response relationships is essential for validation. An overview of well-validated biomarkers will be presented. In this talk, I will review recent achievements in this area and the role of metabolomics derived biomarkers to assess dietary intake and to classify individuals into dietary patterns.

Furthermore, the use of metabolomics to define metabolic phenotypes which can then be used to deliver personalised nutrition has been explored. Work in our laboratory used a metabotyping approach to identify three distinct metabotypes in an Irish population. A framework was developed to deliver personalised dietary advice dependent on the metabotype characteristics. Importantly, there was good agreement between this approach and an individualised approach. Expansion of this work into a pan European population demonstrated that the approach could be used in a diverse population group and worked well in terms of delivery of personalised nutrition advice. Development of this approach further has the potential to deliver dietary advice based on the metabolic phenotype.

Notes

Precision nutrition is different from giving different advice to different subgroups.
Giving personalized nutrition advice yields higher adherence than general advice
Food intake biomarkers (NutriTECH study)
- Proline betaine is a good marker of citrus intake (r > 0.9 when true intake is known)
- When compared to self-reported intake (4-day record) of citrus, proline betaine did a good job predicting the intakes.
Combining biomarkers + self-reported data to make calibration equation used to correct selfreported data in D’Angelo 2019
Metabotypes combined with decision threes is an approach for automating the delivery of targeted advice to population segments.
- Identify metabotypes, develop the decision threes and the advice given in each situation
Precision nutrition to individuals must include response to dietary interventions

Session 1D: Low calorie sweeteners in the human diet: Scientific evidence and recommendations about their use and benefits

Symposium abstract

The aim of a scientific symposium on low calorie sweeteners, their benefits and use in the human diet is to present latest and science-based evidence on a topic of high scientific and public health interest.

Since 2015, when the last FENS European Nutrition Conference took place in Berlin, and the ISA-supported scientific symposium on that occasion, a wealth of new scientific research has been conducted and published in peer-reviewed scientific journals providing further evidence about the role of low calorie sweeteners in sugar reduction as well as in weight and diabetes management. Therefore, we believe that an ISA symposium at FENS 2019 with the participation of well renowned academic experts and researchers on this scientific area will be of high interest and relevance to the FENS audience.

Recommendations about the use of low calorie sweeteners: where evidence meets policy. Report from a 2018 Expert Consensus Workshop

Margaret Ashwell

Abstract

A consensus workshop on low calorie sweeteners (LCS) was held in November 2018 where seventeen experts (the panel) discussed three themes identified as key to the science and policy of LCS: (1) weight management and glucose control; (2) consumption, safety and perception; (3) nutrition policy. The aims were to identify the reliable facts on LCS, suggest research gaps and propose future actions.

The panel agreed that the safety of LCS is demonstrated by a substantial body of evidence reviewed by regulatory experts and current levels of consumption, even for high users, are within agreed safety margins. However, better risk communication is needed. More emphasis is required on the role of LCS in helping people reduce their sugar and energy intake, which is a public health priority. Based on reviews of clinical evidence to date, the panel concluded that LCS can be beneficial for weight management when they are used to replace sugar in products consumed in the diet (without calorie substitution). The available evidence suggests no grounds for concerns about adverse effects of LCS on sweet preference, appetite or glucose control; indeed, LCS may improve diabetic control and dietary compliance. Limited data does not provide adequate evidence that LCS affects gut health at doses relevant to human use.

The panel identified research priorities, including collation of the totality of evidence on LCS and body weight control, monitoring and modelling of LCS intakes, impacts on sugar reduction and diet quality and developing effective communication strategies to foster informed choice. There is also a need to reconcile policy discrepancies between organisations and reduce regulatory hurdles that impede low energy product development and reformulation.

Notes

Everyone agree that sugar intake should be reduced, but disagree whether LCS is a good alternative.
Themes
1. Weight management and glucose control
- facts
  - LCS can reduce net energy intake
  - The effect on appetite and energy intake is similar to water
  - No advese effects on blood glucose or insulin regulation
  - Associations to CVD probably due to confounding by adiposity
- research gaps
  - Long-term effects?
  - Individual variations in response?
  - Is the effect different in different contexts?
- Actions
  - Designing RCTs
  - Cohort studies to model changes in risk factors
1. Safety and consumer perception
- facts
  - Safety demonstrated by a substantial body of evidence
  - Major sources beverages and table sweeteners
  - Some consumers have concerns regarding safety
- Research gaps
  - What influence consumer perception?
  - Lack of in-depth dat on consumption patterns, as well as reliable intake measures
- Actions
  - Develop methods to communicate the facts
  - Develop biomarkers
1. Role of LCS in relation to policy
- Facts
  - Reduction in sugar intake is recommended
  - LCS can be used, but there is some distrust among policy makers
- Gaps
  - Can sweeteners help individuals to reach recommendations for sugar intake?
  - What is the effect on dietary quality?
- Actions
  - Model the potential for LCS to reduce sugar
  - Review policies related to LCS and find out why they differ, and can they be reconciled?

Low calorie sweeteners as a means for weight and glycaemic control: outcomes of systematic reviews and meta-analyses

Anne Raben

Abstract

Non or low calorie sweeteners (LCS) may be a useful tool to reduce caloric intake and control glucose response when consuming sweet foods and drinks. Still, several theories about untoward health effects of LCS acutely or in the long term exist, many of which are based on poor, little or no scientific documentation. A number of intervention studies in the past 3 decades have, however, shown that LCS do not stimulate appetite or increase BW, rather on the contrary. Thus, comprehensive meta-analyses from recent years have reported that the use of LCS may lead to reduced body weight relative to sugar (1). Lately, randomised controlled trials (RCTs) have also compared intake of LCS with water and changes in BW. Convincingly, a study in 303 overweight and obese individuals showed that subjects drinking LCS beverages maintained more than twice the weight loss than individuals drinking water after a 1-year behaviroual treatment programme, ie an improvement of weight control with LCS compared with water (2).

Another systematic review and meta-analyses of 29 randomised controlled trials investigated the role of aspartame, saccharin, steviosides and sucralose on glycemia. No rise in glucose was observed after LCS. Instead, glucose declined after LCS consumption (3). These findings have been confirmed by more recent short- and long term clinical studies (4, 5).

Currently, a new systematic review and meta-analysis of acute postprandial glycaemic and insulinemic response after acute exposure of LCS in randomised, controlled human intervention trials is being conducted (PROSPERO 2018 CRD42018099608). The results are expected to be presented at FENS 2019.

In a new Horizon-2020 project “SWEET” (www.sweetproject.eu, 2018 – 2023) we aim to dig further into the potential risks and benefits of sweeteners and sweetness enhancers (S&SEs). The focus in on health, obesity, safety and sustainability, while using a multidisciplinary approach. A main part of SWEET is a 2-y RCT, which will investigate the effect of prolonged use of S&SEs in a whole healthy diet approach (foods & drinks) on diet compliance, weight control and obesity related risk factors (eg glycemia, lipidemia) and safety (eg microbiota).

Notes

The composition and biological fate of sweeteners are different. Aspartame is completely degraded, andnot excreted, while sucralose is not degraded and therefore excreted.
Raben 2002: Body weight reduced with low calorie sweeteners compared to sugar ad libitum
LCS have been shown to yield more weight loss compared to water, possibly due to increased palatability increasing adherence to the diet.
Toews 2019 show that LCS reduced body weight in overweight individuals, but not in normal-weight

Psychological and behavioural factors influencing consumers’ views and intakes of low calorie sweeteners

Jason Halford

Abstract

Consumption of alternative sweeteners is increasing but there are concerns that sweeteners stimulate appetite, promote preference for sweet-tasting foods and lead to weight gain. Chronic dieters juggle two conflicting goals, hedonic goal of enjoyment of nice-tasting foods/beverages verses diet/weight control. Low Calorie Sweetened (LCS) beverages deliver sweetness (i.e. palatability) but without calories. Do LCS beverages help people to align conflicting goals (hedonic eating and successful weight control)? Our data show restrained eating patterns, body weight concerns, and positive beliefs about palatability and appetite control are key determinants of LCS beverage consumption. Consumption of LCS beverages may help consumers to align conflicting goals (hedonic eating and successful weight control). Frequent consumers may use LCS beverages as a successful strategy to control food intake when in a state of craving. Recent data show frequent consumer show an “attentional bias” towards their favourite LCS beverage (as opposed to a generalised bias to sweet-tasting drinks). This would suggest they don’t promote sweet preference per se. However, long term risks and benefits of LCS consumption will be determined in the ongoing SWITCH trial and SWEET project.

Notes

Frequent consumers more concerned with their weight
Conflicting goals, enjoyment vs weight control.
- LCS can help achieve both
People who consume LC beverages report enjoying them, and believe they can help with weight management.
cravings paper
- LCB-consumers actively choose LCB, not other sweet alternatives, when facing situations of craving.

Validating novel biomarkers of dietary exposure to Riboflavin and Polyphenols and associated health impacts: Transnational DERiVE and VALID projects - The School of Advanced Studies in Food and Nutrition, University of Parma / NICHE Ulster

The metabolic interaction of the B-vitamins riboflavin and vitamin B6 within one-carbon metabolism in European adult cohorts – the DERiVE project

Mary Ward

Abstract

Riboflavin (vitamin B2), as FMN and FAD cofactors, is essential for energy metabolism although biomarker status is rarely measured. The UK and Ireland are the only countries worldwide to have included a riboflavin biomarker in national dietary surveys. Some concern exists in both countries regarding the large proportion of adults showing low riboflavin status, measured using erythrocyte glutathione reductase activation coefficient (EGRac) (the gold-standard marker), but the functional significance of such findings is unclear since in general, with the exception of younger women, dietary intakes of British and Irish adults are within dietary reference ranges. Among its metabolic roles, riboflavin is required (as FMN) to generate the active form of vitamin B6 in tissues. It has been shown previously that cells have a tendency to spare FAD at the expense of FMN therefore, in the condition of riboflavin deficiency, the FMN-dependent pathways would be expected to be primarily affected. Limited evidence indicates that riboflavin may act as the limiting nutrient for optimising vitamin B6 status among older adults deficient in vitamin B6, however, whether this effect is observed across adulthood is unknown.

As part of the transnational DERiVE project we examined the metabolic interaction between riboflavin and vitamin B6 in a large cohort (>5000) of Irish adults aged 18-102 years. Observational data were incorporated from two large cohorts (the Trinity Ulster Department of Agriculture, TUDA study and the Irish National Adult and Nutrition, NANS Survey) and a randomised controlled trial conducted at Ulster University. All biochemical analysis including the assessment of riboflavin (erythrocyte glutathione reductase activation coefficient) and vitamin B6 status (plasma pyridoxal phosphate (PLP) by HPLC) was carried out at Ulster. Results supporting a strong metabolic interdependency between riboflavin and vitamin B6 across adulthood will be presented and the implications of these findings will be discussed. Future studies will investigate the functional effects of changes in riboflavin status by measuring the response of vitamin B6 biomarker to interventions with different doses of riboflavin.

Validation of biomarkers to assess riboflavin status in Irish and Canadian population cohorts: the DERiVE project

Yvonne Lamers

Abstract

Optimizing micronutrient status globally is a major health priority. Nutritional biomarkers, i.e., biochemical indicators measured in accessible tissue such as blood, are critical for the diagnosis and monitoring of micronutrient status in individual healthcare and population-based surveys, and for the implementation of disease prevention strategies. To facilitate reliable and early diagnosis of inadequate nutritional status, prior to the development of physiologic symptoms or impaired health, it is critical to have reliable and sensitive biomarkers, as well as convenient, accessible, and internationally harmonized laboratory methods.

The B-vitamins riboflavin (B-2), folate, B-12, and B-6 are crucial nutrients for lifelong health given their role in cell formation and a healthy nervous system. Riboflavin also functions in iron and energy metabolism and in the formation of immunomodulatory metabolites. Low riboflavin intake has been associated with cardiovascular disease and cancer. Biochemical riboflavin status is rarely measured given the lack of convenient and accessible biomarkers. The current gold-standard biomarker is erythrocyte glutathione reductase activation coefficient (EGRac) that involves laborious sample processing. Most countries worldwide, except for the UK and Ireland, have monitored riboflavin status through dietary intake due to the lack of accessible biomarkers. Plasma riboflavin concentration may serve as an alternative indicator; its association with related metabolites however has not yet been investigated.

This talk will present novel findings of an international research collaboration awarded under the JPI-HDHL ‘Biomarkers for Nutrition and Health’ call. Our team developed a new and sensitive method to quantify riboflavin and related coenzyme forms, together with vitamin B6 and kynurenine metabolites in very small plasma volume. We will present findings about the validation of plasma riboflavin and related biomarkers for riboflavin status assessment in Canadian adults.

Notes

FMN increases and FAD decreases during storage. Total riboflavin is stable.
Plasma riboflavin is inversely related to EGRac, as expected.
- AUC 0.68 when predicting EGRac < 1.3, ok for a nutritional biomarker
- FMN and FAD are not useful
- Breakpoint analyses suggest a cutoff for plasma riboflavin of 11 nmol/L

COMMERCIAL SESSION Credibility vs. Clickbait: Communicating Nutrition Research to the Public - Eat Well Global

Session abstract

In the age of social media, misinformation about food, nutrition and health spreads like wildfire, making it increasingly important for credible, evidence-based information to find its way into the public domain. Nutrition scientists are relied upon for their contributions to the scientific literature and importantly, for their influence on nutrition guidelines and policies. But with the popularity of celebrities, self-proclaimed experts and other uncredentialled influencers delivering nutrition advice, and the ease with which unsubstantiated and sometimes dangerous claims are spread, there is an urgent need for credentialed experts to provide a credible counterpoint that’s more accessible to the public.

Join us for an interactive session, facilitated by Eat Well Global, where we will explore techniques and opportunities for researchers to extend their reach to the media and other communication channels. The objectives of this session are three-fold: - Identify how to promote accurate science reporting and open up new communication channels with the media - Understand how to amplify your messages and scientific findings - Explore opportunities to collaborate with public-facing professionals, such as dietitians, to translate research into consumer-friendly language

Developing, disseminating and translating high-quality research: closing the gap between nutrition and its application to public health policy and messaging

Taylor C Wallace

Abstract

Lifestyle choices heavily influence human health and disease prevention, giving the nutrition community the authority to act as “Chief Health Strategists” in guiding the development of new health systems and effective communication channels. International health systems and policies are currently undergoing critical transformation, with nutrition at the forefront of public health strategies to prevent or mitigate both age- and obesity-related chronic disease. During this health system and policy evolution, and in the current fiscal climate, public officials are looking for reproductive evidence of what works to guide their funding and policy decisions. Governments, nongovernmental associations (NGOs) and health professionals need evidence-based science for developing effective public health interventions and messaging. Timely distribution of quality evidence is often hindered by obstacles such as heterogeneous scientific literature, prolonged processes for developing policies and messaging, short-term emphasis on narrow sub-sets of the peer-reviewed literature, as well as the influence of the consumer, media, and ability to rapidly exchange information through digital communications. Today there is a large gap between development and dissemination of high-quality research in the field of nutrition and its application to developing strong policy and public health messaging. Statistical compilation of often heterogeneous data aims to give simple answers to complex (and often personalized) questions; this detrimental to our profession and public health. Adding to this conundrum, nutrition scientists have traditionally been trained to design research analogous to medicine, using a reductionist vs. global approach. This lecture will discuss four continuous steps to consider when developing, translating, and disseminating high-quality evidence.

Notes

Slides: www.drtaylorwallace.com
Podcast: Risky Behaviour (from november 2019)
Monumental findings are rapidly disseminated, but for most findings communication strategies are needed
4 pillars of successful communication
1. Identify and engage Stakeholders
  - Who is interested in our work?
  - Preaching to the choir is not a great strategy for making changes
  - Who has the power to implement your message
  - Build personal relationships with stakeholders
2. Build The Evidence base
  - How well do your stakeholders really know the evidence base?
3. Create a translation plan
  - How should you frame your findings?
  - Keep it simple stupid
  - What are the key take-home messages
4. Develop a dissemination strategy
  - Can you use non-traditional sources?
  - Use digital, social and mainstream media for dissemination.
Stop using hierachies of evidence.

Thursday

Plenary session 3

Current metabolic perspectives on malnutrition in obesity

Ellen Blaak

Notes

Malnutrition not restricted to deficiency, but any abnormal physiological condition caused by inadequate, unbalanced or excessive intakes
Insulin resistance is tissue-specific, and insulin resistance in different tissues may elicit different metabolic consequences
Hepatic insulin resistance
- Reduced ketone bodies, elevated ketogenic amino acids
- Increased TAG and DAG in women, but not in men
Muscle insulin resistance
- Increased isoleucine, valine and lactate
- Increased lysophosphatidylcholine
  - Lipid profile paper, Inflammation paper

Session 4C: Ultra-processed food - potential health impacts - FENS 2019 Scientific Committee

1030-1200 Liffey A (Level 1)

Session Abstract

Over the past decade, there has been a rapidly expanding scientific literature on the role of industrial food processing in human diet and health, with a particular focus on ultra-processed foods defined as formulations of refined substances and additives used to create a broad spectrum of new convenient and highly-palatable products. Epidemiological evidence has demonstrated that ultra-processed food consumption is associated with poorer diet quality and increased chronic diseases incidence. Recently, the journal PHN has published a special issue on this topic. (See https://www.cambridge.org/core/journals/public-health-nutrition/issue/31F497583856B2D965FF65B7C3CAB864?utm

This FENS symposium will highlight the current state of knowledge, particularly focusing on classification systems for such foods, the nutritional and toxicological aspects of these foods, the consumption patterns of these foods and their potential impact (including mechanisms) on specific disease endpoints and public health overall.

What are ultra-processed foods and how they have changed the quality of diets in Europe and worldwide

Jean-Claude Moubarac

Abstract

Over the past decade, there has been a rapidly expanding scientific literature on the role of industrial food processing in human diet and health, with a particular focus on ultra-processed foods. Epidemiological evidence has demonstrated that ultra-processed food consumption is associated with poorer diet quality and increased risk of chronic diseases and obesity. In this session, I will first discuss from a theoretical perspective why food processing matters to understand diet and health in the 21st century. I will then describe the NOVA food classification, a tool used to study food processing and its impact on diet and health worldwide. Last, I will present a summary of the evidence linking consumption of ultra-processed food to poor diet quality, as an important dimension of unhealthy diets, and discuss implications for research and policies

Notes

NOVA categories
1. WHole foods
2. Culinary ingredients (sugar, oils)
3. Processed foods (cured, preserved)
4. Ultraprocessed (artificially created foods)
NOVA multi-country study
- Higher intake of NOVA cat 4 foods associated with
  - Higher energy density
  - More added sugar
  - More salt
  - More saturated fat (a little)
  - Less fiber
  - Less protein and micronutrients

Ultra-processed foods and health: epidemiological approach

Mathilde Touvier

Abstract

The last decades are marked by an increase in the degree of food processing and formulation. Today, “ultra-processed” foods account for 25-to-60% of energy intakes in Europe, the USA, Canada, New Zealand, and Brazil. The notion of transformation is complex, since the possible processes (industrial or not) and the authorized additives (≈350 in Europe) are multiple. The “Nova” classification, developed by researchers at the University of São Paulo (Monteiro PHN 2017), opened the way for etiological research on the relationship between the degree of food processing and health. Foods are categorized into 4 groups: low/unprocessed foods, cooking ingredients, processed foods, ultra-processed foods. Ultra-processed foods have, on average, a lower nutritional quality (higher in salt, sugar, saturated fatty acids, lower in fiber and vitamins), they often contain food additives (emulsifiers, texturizers, sweeteners, etc.), are likely to carry substances coming from food-contact packaging, as well as certain compounds that are neoformed during the processes (high-temperature heating, hydrogenation, frying pre-treatment, etc.).

Several prospective studies have found a link between the consumption of ultra-processed foods and an increased risk of overweight / obesity (Mendonça 2016) and high blood pressure (Mendonca 2017) in a cohort of Spanish students, as well as and an increased risk of dyslipidemia in a cohort of Brazilian children (Rauber 2015). In the context of the NutriNet-Santé cohort (n=164,000 French adults) followed since 2009, after taking into account a wide range of potential confounders related to lifestyle, we observed a significant association between ultra-processed foods in the diet and an increased risk of overall and breast cancers (Fiolet BMJ 2018), cardiovascular diseases (Srour BMJ 2019), mortality (Schnabel JAMA Int Med 2019), depressive symptoms (Adjibade BMC Med 2019) and functional digestive disorders (Schnabel Am J Gastroenterol 2018). The analyzes carried out suggest that the nutritional quality of these products does not entirely explain those links.

In this field, the causal nature of the associations cannot be established by long-term interventions testing the impact of ultra-processed foods on health, for ethical reasons notably, as long as a deleterious effect is suspected. It will therefore be necessary to confirm these results in diverse populations, and also to go further in understanding the transformation processes, compounds and mechanisms potentially involved, through new epidemiological approaches, coupled with in vitro and in vitro experimental approaches. In the meantime, several countries have recently introduced into their official recommendations limiting ultra-processed foods as a precautionary principle.

Notes

NUTRI-SCORE vs NOVA
- NUTRI-SCORE assesses nutritional quality, NOVA degree of processing
- A scale from A-E
- In the E category, 85% of the foods are ultraprocessed
- In the A category, 24% of foods are ultra-processed, and B-D categories ~ 60-70%.
NutriNet-Santë cohort
- 3x24hrecall every 6 month, long followup
- Ultra-processed foods make up 18% of the food intake, but contributes with 35% of the energy intake
- CVD risk
- cancer risk
- mortality risk

Opportunity makes the Pathogen – potential Mechanisms connecting Ultra-processed Foods with Gut Inflammation

Marit Kolby Zinöcker

Abstract

Diet greatly influences the incidence of non-communicable diseases (NCDs), most of which are now recognized as conditions that involve elements of inflammation. A growing body of evidence is linking ultra-processed foods with several of these health outcomes, but biological mechanisms supporting a causal relationship have not been elucidated.

From the traditional nutrition researcher’s point of view, a grain that has been milled and extruded has the same nutritional value as a whole grain. To the microbes in the human gut, the processing applied to the food prior to digestion makes a world of difference.

Several physical and chemical processes commonly applied in manufacturing of foods, including refining, extrusion and addition of molecules (naturally occurring or synthetic), can change the growth potential and dynamics of gut microbes. Animal studies that have investigated various attributes of ultra-processed foods report increased pro-inflammatory potential of the gut flora along with adverse effects on host physiology. Thus, ultra-processed food products have the potential to induce structural and behavioural changes in the human gut microbiome that influences metabolic and inflammatory pathways and contribute to the growing burden of NCDs.

The characterization of our food supply is still incomplete in terms of predicting health effects, and the role of the microbiome is largely absent from the evidence underlying nutrition policies and dietary advice in most countries. Our foods should not just be judged by the sum of their nutrients, but by their potential to prevent inflammation and to sustain health in the human superorganism of man and microbe. Emphasis on food quality, not quantity, will be crucial in future strategies to limit NCDs

Notes

Unhealthy diets are drivers of metabolic diseases, but how?
- Degree of food processing
- Mediated through effects on gut microbiota?
Acellular nutrients
- Breaking the cell walls makes nutrients more available
- More accessible nutrients in the small intestine, increasing growth potential for bacteria
- Protective components removed during processing

Plenary session 4

Food environments and the obesity epidemic: lessons learned and future research challenges

Lauren Lissner

Abstract

The food environment consists of political, socioeconomic, and physical factors that affect accessibility and healthfulness of diets. Given the complexity of our food system and the diverse individuals that populate it, no single change in the food environment is likely to reverse the obesity epidemic. This presentation will select a few aspects of the food environment that are relevant to upcoming research on obesity prevention.

The political food environment holds promise for protecting citizens from poor nutrition via restrictions in marketing and taxation of unhealthy foods, as well as through informative labelling of pre-packaged foods. For researchers, a useful starting point is to conduct dietary simulation studies, which can inform future policies by estimating their potential health impacts. However, we still lack knowledge about the impact that enacted policies are having on the population’s actual diets, weights and health. Different components of the food system can increase or decrease socioeconomic inequalities. Modern food environments provide a surplus of inexpensive, nutrient-poor foods, thereby contributing to excess risk of obesity in those with least access to healthier diets. Thus, it may be concluded that high-risk socioeconomic groups should be targeted for primary prevention efforts through better nutrition, ideally early in life. However, there is only limited evidence that dietary interventions in family or school food environments are effective in children. In parallel with economic barriers, current social norms can obstruct healthy eating. Novel participatory research approaches will be useful in developing culturally appropriate interventions for obesity prevention in vulnerable communities.

At the individual level, the physical food environment can be portrayed in terms of the nutritional quality of available dietary exposures. This view may carry an implicit assumption that people can follow universal dietary recommendations to prevent or reverse overweight. Yet, given the heterogeneity between individuals in their weight responses to specific dietary approaches, together with ample evidence that these efforts frequently backfire, there is great interest in how personalized diets can become an accessible tool for individuals’ weight management efforts.

In closing, it should be noted that the effect of modern diets on the environment per se is not traditionally part of our food environment discussion. Fast-moving climate change suggests the value of adopting ecologically responsible diets, which could have dual actions: lowering greenhouse gas emissions while preventing malnutrition in all forms. In an era of obesity and environmental change, this represents a formidable research challenge for future nutritional scientists.

Notes

Dunford 2019, on average only 31% of the packaged
Hall 2019, processed foods facilitate faster eating, which may increase total energy intake
Food desert, not just a problem of too few healthy options, but also too many unhealthy options.
Lafner 2012, comparing children preferring low-fat/low-sugar to those preferring either high-sugar, high-fat or both, demonstrated a clearly higher prevalence of obesity in the latter.
Socio-cultural effects is important, families who often watch TV while eating have more overweight children
Front-of-package labels
- provide an incentive for industry to reformulate their products
- easily accessible to the consumer
Environmental aspects, plant-based diets
- Satija 2019, increasing plant-based food associated with less weight gain.

Session 3B: An Update on the Beneficial Health Impact of Specific Dietary Fatty Acids

Session Abstract

The aim of this session is to highlight ILSI Europe’s activities on the impact of dietary fatty acids on human health. Here we will provide an overview of the health impact of diets rich in Omega-3 and Omega -6 (talk 1), specific saturated fatty acids (talk 2) or gut derived short chain fatty acids (talk 3).

A systematic review of the effects of increasing arachidonic acid intake on pufa status, metabolism and health-related outcomes in humans

Philip Calder

Abstract

We conducted a systematic review of randomised controlled trials (RCTs) of increased intake of arachidonic acid (ARA) on fatty acid status and health outcomes in humans. We identified 22 articles from 14 RCTs. Most studies were conducted in adults. These used between 80 and 2000 mg ARA/day and were of 1 to 8 weeks duration. Supplementation with ARA doses as low as 80 mg/d increased the content of ARA in different blood fractions. Overall there seem to be few marked benefits for adults of increasing ARA intake from the typical usual intake of 100-200 mg/day to as much as 1000 mg/d or even more. However, there may be an impact on cognitive and muscle function which could be particularly relevant in the ageing population. The studies reviewed suggest no adverse effects in adults of increased ARA intake up to at least 1000 to 1500 mg/d on blood lipids, platelet aggregation and blood clotting, immune function, inflammation, or renal function. However, in many areas there are insufficient studies to make firm conclusions, and higher intakes of ARA are deserving of further study. Based on the RCTs reviewed, there are not enough data to make any recommendations for specific health effects of ARA intake.

Notes

Mean intake of AA 100-350 mg
Small proportion of total fatty acid, but often the most common PUFA in the body
- Precursor for prostaglandins, leukotriens, tromboxans etc
- Drugs targeting these pathways, such as aspirin
Increasing AA intake
- Fatty acid composition
  - More AA in blood lipids, red blood cells, platelets and dwhite blood cells
  - Often associated with less EPA, linoleic acid and DHA
- Blood lipids
  - No reported effect on blood lipid parameters
- Blood pressure
  - No effect -Platelet aggregation
  - No reported effect on hematologic parameters
  - Increased platelet aggregation with very high doses, clinical significance uncertain
- Immunity and inflammation
  - No effect on number of immune cells or markers of immunity
- Cognitive function
  - High dose AA intake protective against age-related decline in cognitice function (1 study), which should be followed up with new study
- Body composition, muscle function and physical performance
  - No effect on body composition, but a 8.5 % increase in anaerobic peak power
No reported harmful effects of increasing the intake to as much as 1000 mg
Effect of lowering AA intake is not known

ω -3 and ω -6 PUFA intakes, ratios and potential health effects

Ronald Mensink

Abstract

Fatty acids (FA) from dietary sources provide for adults living in Western countries about 35% of their dietary energy as a mix of FAs present in different lipids, mainly triacylglycerols (TAG). They have multiple vital functions in the human body: energy sources, major constituents of all cell membranes, components of signalling molecules, and precursors of bioactive lipid mediators. Through these roles, FAs affect cell and tissue function and physiological responses, and therefore have an impact on health, well-being, and disease risk and outcome. In this context, there is considerable interest in the biological roles of the long chain omega-6 polyunsaturated FA (PUFA), arachidonic acid (ARA), the omega-3 PUFAs eicosapentaenoic acid (EPA), and docosahexaenoic acid (DHA).

The PUFA composition differs between different complex lipids present in the blood, and between different cells and tissues. The precise PUFA composition of each individual FA pool is determined partly by PUFA intake from diet and partly by metabolic processes. For example, altering the amounts of EPA and DHA in the diet by eating more oily fish or by taking omega-3 FA supplements, increases the EPA and DHA content of complex lipids in the blood and of many cells and tissues. However, the resultant degree of enrichment in EPA and DHA in different body pools varies considerably. Thus, there is a relationship between PUFA intake from the diet, the PUFA content in a compartment, and possibly the effect of the PUFA on cell and tissue function. However, this series of relationships is complex because each step is influenced by metabolic processes and by many other factors, including the availability and content of other FAs that may have different biological activities. The aim of the present systematic review is to clarify the relationship of omega-6 and omega-3 PUFAs with dietary intake, blood/cell/tissue PUFA composition, and to assess the validity of commonly used PUFA biomarkers of dietary intake and n-3 and n-6 PUFA status.

Notes

3% of LA (intake ~15g) converted to AA
10% of ALA (intake ~2g) converted to EPA, < 1% converted to DHA
Intake is reflected in plasma lipid pool
- Considerable variation in incorporation
  - The ratio between LA/AA is vastly different in different blood lipid pools.
  - EPA/DHA is in general much higher than ALA in the lipid pools
- Lipid pools respond differently to changes in intake
  - Different half-life of the different fatty acids in different pools. Longer in red blood cells as compared to cholesteryl esters
- Metabolic interdependence
  - If you eat ALA, you see an increase in ALA/EPA, but a decrease in AA
  - If you eat EPA/DHA, you see a huge decrease in LA/AA.
  - The ratio between LA and ALA DOES NOT predict conversion to the longer chained PUFAs, this is determined by the absolute availability of substrate and product
- Metabolism depend on subject characteristics
  - Age, sec, genes etc
The ratio of omega-3/6 can reflect changes in omega-3, -6 or both. The ratio is not informative.
- The ratio may appear optimal, but the absolute intakes does not need to be
Omega-3 index
- Mainly determined by DHA, and not affected by ALA
- Insensitive to fasting status
- Insensitive to recent intake, good index of habitual status

Update on Health Effects of Different Dietary Saturated Fatty Acids

Peter Joris

Abstract

There are various types of Saturated Fatty Acids (SFAs) in the human diet that may differently affect cardiometabolic risk markers and the risk to develop cardiometabolic diseases. A new activity performed by this ILSI Expert Group is therefore to critically analyze the relation between these different types and sources of SFAs and their health effects. Currently, we are performing a systematic review of the scientific literature focusing on (i) the impact of individual dietary SFAs on traditional and novel cardiometabolic risk markers, and (ii) associations between dietary intakes of these SFAs and the risk to develop cardiometabolic diseases. The ultimate goal of this review is to provide evidence whether dietary guidelines should differentiate individual SFAs. This presentation will provide an update focusing on the progress of our systematic review and also some (preliminary) results will be presented.

Notes

When replacing carbohydrate with SFA
- Increased total, LDL and HDL cholesterol, lowered TG
The most beneficial profile obtained when replacing SFA with PUFA
SFA -> carbohydrate or protein, no effect on CVD risk
SFA -> PUFA, reduced risk.
Individual SFA
- C16 and C18 most abundant
- C12, C14 and C16 most potent in raising LDL and HDL cholesterol
- Different risk associations seen for different fatty acids
Important to focus on substitution effects between different fatty acids, not just absolute amounts
Longer chained fatty acids have less postprandial impact on blood lipids due to slower uptakes
Food matrix influence the effect of SFAs.

Session 2D Nutrition Sciences beyond reductionism

Session Abstract

Some of the Grand Societal challenges are strongly linked to nutrition, like obesity, healthy ageing. These challenges require scientific concepts, research questions, methods and research infrastructures that need to be developed and go beyond reductionistic thinking. Results from studies conducted with the reductionist approach, where cause-and-effect relationships are reduced to a binary “true” and “not true”, are more and more not supported by observations that consumption of foods, according to the reductionist approach composed of disease risk increasing nutrients, are probably disease risk reducing. The benefits of nutrition interventions aiming at prevention of chronic diseases can most often not be related to one single cause. Despite the multifactorial causation of most chronic diseases the pharmacological model of double blind placebo controlled intervention studies, usually called clinical studies, is considered as the method to prove causation. In most cases results from a reductionist approach cannot directly be translated into an individualistic benefit. Still the organisation of nutrition sciences is strongly influenced by a reductionistic focus. Political and governmental choices force scientists to search for private funding. This funding steers to nutrient and/or products related effects, creating possibilities for product related communication on single products, sometimes controversial to general recommendations. The evidence we seek, the questions we ask, and the way how nutrition sciences is organised and funded threaten our credibility. A discussion is needed to agree on different ways of working and knowing.

The concepts in Nutrition in Transition

Edith Feskens

Notes

Capable and credible

Result of discussion from the Satellite “Nutrition in Transition”

Pieter van het Veer

Notes

Nutrition, foods and diet can be studied as determinants of health outcomes, but also as outcomes of the food evironments and food choices

Ensuring Trust in Nutrition Science

Philip Calder

Notes

New FENS initiative on increasing the trust in nutrition science, interim results will be presented in Tokyo 2021

Friday

Session 3D: Chrono-Nutrition: the evidence for why ‘You are when you eat’

1045-1215 Auditorium (level 3)

Session Abstract

Most physiological processes exhibit daily (or ‘circadian’) rhythms. Indeed, the importance of circadian rhythms was formally recognised by the award of the 2017 Nobel Prize in Physiology or Medicine for characterisation of the molecular circadian clock.

One of the key roles of the circadian system is the regulation of metabolic physiology. It is therefore not surprising that there is a close relationship between our internal rhythms, metabolic health and nutrition. Emerging research indicates that meal timing regulates both acute post-prandial responses, as well as long-term energy storage and body composition. Furthermore, timed meals can feed back to regulate circadian rhythms and have long-term influences on metabolic function.

This symposium will bring together three leading researchers in the new field of chrono-nutrition, the interaction between circadian time and food intake. First, Dr Gerda Pot will present the epidemiological evidence linking meal timing to human health. Next, Dr Jonathan Johnston will describe controlled physiological studies that link circadian biology to human metabolism and mealtime. Finally, Dr David Bechtold will describe animal and cellular models that provide novel mechanistic insight into the link between meal timing, the molecular clockwork and energy metabolism.

Chrono-nutrition: epidemiological evidence of meal timing on health

Gerda Pot

Abstract

Studies on chrono-nutrition, studying the impact of when we eat on metabolic health, have seen a great increase in the past few years. Studying not only what we eat, but also when we eat, is very relevant at times characterized by changes in our temporal dietary patterns. Changes in temporal eating patterns could be due to a rise in people working in shifts, people consuming more meals outside the home and overall eating patterns having become more irregular, including more breakfast skipping and night-time eating. Temporal eating patterns are a possible modifiable risk factor for cardio-metabolic diseases. Many of the metabolic processes in our body follow a circadian pattern. Disruption of these circadian patterns or misalignment between the timing of eating and endogenous circadian systems can have adverse health effects, including impaired cardio-metabolic health. This presentation will report on recent findings and insights on epidemiological evidence of meal timing on cardio-metabolic health, including type 2 diabetes.

Notes

Components: clock time, regularity and frequency
Mice fed during their resting phase gain more weight compared to mice fed in their active phase
Clock time
- We eat later in the day compared to 40 years ago, which is associated with increased intake from snack foods
- Later eating associated with increased body weight
Irregularity
- Associated with increased BMI and metabolic syndrome
Frequency
- Mixed findings
Evening types are on average more unhealthy due to desynchrony between chronitype and social demands

Circadian metabolism in humans and its regulation by meal timing

Jonathan Johnston

Abstract

Endogenous circadian (~ 24-hour) rhythms exist in many key aspects of physiology, including metabolic function. As a result of these metabolic rhythms, physiological responses to food intake vary across the day. Moreover, the timing of energy intake is a key factor that can synchronise the timing of circadian rhythms in many peripheral tissues. The interaction between energy intake and time of day is therefore a complex, bi-directional phenomenon that has profound consequences for long-term metabolic health.

Much of our understanding of the mechanisms underlying circadian metabolism come from animal studies. However, advances in biopsy collection and molecular analyses are now enabling human studies to contribute further to this topical aspect of metabolic and nutritional physiology.

This presentation will briefly explain the basic science underlying links between circadian rhythms and metabolism, focussing mainly on human biology. It will then describe recent high-profile studies that have highlighted the intimate relationship between meal timing and human physiology.

Notes

Circadian rhythms are purely driven by biology
Zeitgebers act to synchronize biological clocks with the outside world
Disruption of peripheral clocks elicit whole body metabolic dysregulation
~2 % of adipose tissue genes have circadian rhythms
Dietary influence on circadian rhythm
- Temporal restriction of food desynchronizes rodent circadian clocks
Time-restricted feeding pilot study, suggests that restricting the eating window may contribute to reducing the total energy intake

Recipricol connections between the timing of food intake and the circadian clock

David Bechtold

Abstract

In mammals, endogenous circadian clocks sense and respond to daily feeding and lighting cues, adjusting internal ∼24 h rhythms to resonate with, and anticipate, external cycles of day and night. The mechanism underlying circadian entrainment to feeding time is critical for understanding why mistimed feeding, as occurs during shift work, disrupts circadian physiology, a state that is associated with increased incidence of chronic diseases such as type 2 (T2) diabetes. In this presentation, I will discuss our recent work detailing the molecular mechanisms which link the circadian clock to feeding time and energy metabolism on a cellular and systemic level.

Notes

5-15% of genes in any tissue is directly regualted by circadian rhythms
Crosby 2019 Insulin treatment influences biological clocks via PER2
REVERBα is a link between the clock and meatbolism, and knockout models suggests that alterations may disrupt the metabolic adaptation to low/high energy intakes.

Plenary session 5

Epigenetic reprogramming regulating adipose tissue plasticity and function

Christian Wolfrum

Abstract

The increase in the prevalence of overweight and obesity worldwide has reached a qualified epidemic stage1 and in line with this it is widely acknowledged that obesity-associated co-morbidities are the main cause of death. In simple terms, the basis of obesity is an excess accumulation of adipose tissue, however, with regards to the development of co-morbidities, studies in recent years have suggested adipose tissue quality to be an important denominator2. Adipose tissue can be divided into white (WAT) and brown adipose tissues (BAT)3. While WAT is the main storage site for lipids, BAT functions to dissipate energy in the form of heat in a process called non-shivering thermogenesis4, to contribute to the maintenance of body temperature homeostasis during both acute and chronic cold exposure5,6. The relevance of BAT in human physiology is demonstrated by its association with higher energy expenditure, lower adiposity and a reduced risk of type 2 diabetes7. In recent years, a number of studies have demonstrated a link between paternal preconception nutrient exposure and the phenotype of the offspring. Differences in gene expression patterns arise during development and can be retained through mitosis by epigenetic mechanisms8. In the context of thermoregulation, it was shown that environmentally induced changes in gene expression can affect cellular function and thereby also predisposition to certain diseases9. Additionally, different changes in the environment (i.e. weather, stress, nutrition, socioeconomic conditions) on the parent can be transmitted to subsequent generations leading to health advertises. The lecture will focus on the role of the epigenome in regulating adipose tissue composition thereby affecting systemic energy metabolism.

Notes

Hedonic system
- Experimental studies in animals where the offspring is given a choice of what to eat and drink, offspring off mothers fed a high fat diet tend to eat more sugar and fat, becoming overweight
  - Enhanced dopamine sensitivity
Birth month and brown fat
- Paternal cold exposure may be important