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Hodson Group: Human in vivo and in vitro lipid metabolism

  • Oxford Centre for Diabetes, Endocrinology and Metabolism
Lipid droplets in hepatocytes

Our research investigates the metabolic consequences that specific diets have on the regulation of major metabolic organs in individuals with different phenotypes and genotypes, to understand how this influences their risk of cardiometabolic diseases, including fatty liver disease, diabetes and cardiovascular disease.

We work to understand how dietary components regulate specific metabolic pathways that may impact on liver, adipose tissue and skeletal muscle health and function. Our research has helped to define the role of specific metabolic pathways in the pathogenesis of metabolic disease and has contributed to a paradigm shift away the effect of total dietary calories to focussing on the macronutrient composition of the diet in a weight neutral setting. Although we focus primarily on lifestyle factors we also have an interest in understanding the effect that some therapeutic medications have on metabolic pathways and how they may alter disease risk.

We take the observations of our in vivo human work forward into in vitro cellular models to gain insight into the potential mechanisms underpinning these observations. We deliver a translational program of research; our aim is to understand the molecular mechanisms by which dietary nutrients modulate metabolic phenotype including lipid and carbohydrate metabolism as well as insulin signalling and action in liver, adipose tissue and muscle. The group uses in vitro cell culture models, and translates these findings through to state-of-the-art metabolic clinical studies in individuals across a range of phenotypes and genotypes. My group, is one of the few worldwide to use stable-isotope tracers to investigate human fatty acid and carbohydrate metabolism to probe metabolic pathways of interest in vivo in humans and in vitro in cells.

Collaborators

  • Fredrik Karpe, RDM
  • Jeremy Tomlinson, RDM
  • Hannele Yki-Jarvinen, University of Helsinki
  • Javier Gonzalez, University of Bath
  • Soren Nielsen, Aarhus University
  • Michael O'Reilly, Dublin

Funders

British Heart Foundation

NIHR Biomedical Research Centre: Oxford

Our team

Selected publications

Human MASLD is a diurnal disease driven by multisystem insulin resistance and reduced insulin availability at night.

Journal article

Marjot T. et al, (2026), Cell Metab, 38, 474 - 492.e6

Greater oxidation of dietary linoleate compared to palmitate in humans following an acute high-carbohydrate diet.

Journal article

Srnic N. et al, (2024), Clin Nutr, 43, 2305 - 2315

Dissociation between liver fat content and fasting metabolic markers of selective hepatic insulin resistance in humans.

Journal article

Westcott FA. et al, (2024), Eur J Endocrinol, 191, 463 - 472

MLX plays a key role in lipid and glucose metabolism in humans: Evidence from in vitro and in vivo studies.

Journal article

Nagarajan SR. et al, (2023), Metabolism, 144

Determining the temporal, dose, and composition effects of nutritional substrates in an in vitro model of intrahepatocellular triglyceride accumulation.

Journal article

Nagarajan SR. et al, (2022), Physiol Rep, 10

Distinct contributions of metabolic dysfunction and genetic risk factors in the pathogenesis of non-alcoholic fatty liver disease.

Journal article

Luukkonen PK. et al, (2022), J Hepatol, 76, 526 - 535

Modifying nutritional substrates induces macrovesicular lipid droplet accumulation and metabolic alterations in a cellular model of hepatic steatosis.

Journal article

Gunn PJ. et al, (2020), Physiol Rep, 8

Intrahepatic Fat and Postprandial Glycemia Increase After Consumption of a Diet Enriched in Saturated Fat Compared With Free Sugars.

Journal article

Parry SA. et al, (2020), Diabetes Care, 43, 1134 - 1141

Hepatic de novo lipogenesis is suppressed and fat oxidation is increased by omega-3 fatty acids at the expense of glucose metabolism

Journal article

Green C. et al, (2019), Endocrine Abstracts

Saturated Fat Is More Metabolically Harmful for the Human Liver Than Unsaturated Fat or Simple Sugars.

Journal article

Luukkonen PK. et al, (2018), Diabetes Care, 41, 1732 - 1739

Chylomicron-Derived Fatty Acid Spillover in Adipose Tissue: A Signature of Metabolic Health?

Journal article

Piché M-E. et al, (2018), J Clin Endocrinol Metab, 103, 25 - 34

Metabolic signatures of human adipose tissue hypoxia in obesity.

Journal article

Hodson L. et al, (2013), Diabetes, 62, 1417 - 1425

The contribution of splanchnic fat to VLDL triglyceride is greater in insulin-resistant than insulin-sensitive men and women: studies in the postprandial state.

Journal article

Hodson L. et al, (2007), Diabetes, 56, 2433 - 2441

Related research themes

Metabolism in Molecular Medicine
Metabolism in Molecular Medicine