A genome-first approach to variants in MLXIPL and their association with hepatic steatosis and plasma lipids

Leonida Hehl; Kate T. Creasy; Cecilia Vitali; Eleonora Scorletti; Katharina S. Seeling; Mara S. Vell; Miriam D. Rendel; Donna Conlon; Regeneron Genetics Center; Marijana Vujkovic; Inuk Zandvakili; Christian Trautwein; Kai M. Schneider; Daniel J. Rader; Carolin V. Schneider

doi:10.1097/HC9.0000000000000427

Hepatology Communications (May 2024)

A genome-first approach to variants in MLXIPL and their association with hepatic steatosis and plasma lipids

Leonida Hehl,
Kate T. Creasy,
Cecilia Vitali,
Eleonora Scorletti,
Katharina S. Seeling,
Mara S. Vell,
Miriam D. Rendel,
Donna Conlon,
Regeneron Genetics Center,
Marijana Vujkovic,
Inuk Zandvakili,
Christian Trautwein,
Kai M. Schneider,
Daniel J. Rader,
Carolin V. Schneider

Affiliations

Leonida Hehl: 1 Department of Medicine III, Gastroenterology, Metabolic diseases and Intensive Care, University Hospital RWTH Aachen, Aachen, Germany
Kate T. Creasy: 2 Department of Genetics, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania, USA
Cecilia Vitali: 3 Department of Medicine, Division of Translational Medicine and Human Genetics, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania, USA
Eleonora Scorletti: 2 Department of Genetics, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania, USA
Katharina S. Seeling: 1 Department of Medicine III, Gastroenterology, Metabolic diseases and Intensive Care, University Hospital RWTH Aachen, Aachen, Germany
Mara S. Vell: 1 Department of Medicine III, Gastroenterology, Metabolic diseases and Intensive Care, University Hospital RWTH Aachen, Aachen, Germany
Miriam D. Rendel: 1 Department of Medicine III, Gastroenterology, Metabolic diseases and Intensive Care, University Hospital RWTH Aachen, Aachen, Germany
Donna Conlon: 3 Department of Medicine, Division of Translational Medicine and Human Genetics, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania, USA
Regeneron Genetics Center: 5 Regeneron Genetics Center, Tarrytown, New York, USA
Marijana Vujkovic: 2 Department of Genetics, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania, USA
Inuk Zandvakili: 6 Department of Medicine, Division of Gastroenterology and Hepatology, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania, USA
Christian Trautwein: 1 Department of Medicine III, Gastroenterology, Metabolic diseases and Intensive Care, University Hospital RWTH Aachen, Aachen, Germany
Kai M. Schneider: 1 Department of Medicine III, Gastroenterology, Metabolic diseases and Intensive Care, University Hospital RWTH Aachen, Aachen, Germany
Daniel J. Rader: 3 Department of Medicine, Division of Translational Medicine and Human Genetics, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania, USA
Carolin V. Schneider: 1 Department of Medicine III, Gastroenterology, Metabolic diseases and Intensive Care, University Hospital RWTH Aachen, Aachen, Germany

DOI: https://doi.org/10.1097/HC9.0000000000000427
Journal volume & issue: Vol. 8, no. 5

Abstract

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Background:. Common variants of the max-like protein X (MLX)-interacting protein-like (MLXIPL) gene, encoding the transcription factor carbohydrate-responsive element-binding protein, have been shown to be associated with plasma triglyceride levels. However, the role of these variants in steatotic liver disease (SLD) is unclear. Methods:. We used a genome-first approach to analyze a variety of metabolic phenotypes and clinical outcomes associated with a common missense variant in MLXIPL, Gln241His, in 2 large biobanks: the UK Biobank and the Penn Medicine Biobank. Results:. Carriers of MLXIPL Gln241His were associated with significantly lower serum levels of triglycerides, apolipoprotein-B, gamma-glutamyl transferase, and alkaline phosphatase. Additionally, MLXIPL Gln241His carriers were associated with significantly higher serum levels of HDL cholesterol and alanine aminotransferase. Carriers homozygous for MLXIPL Gln241His showed a higher risk of SLD in 2 unrelated cohorts. Carriers of MLXIPL Gln241His were especially more likely to be diagnosed with SLD if they were female, obese, and/or also carried the PNPLA3 I148M variant. Furthermore, the heterozygous carriage of MLXIPL Gln241His was associated with significantly higher all-cause, liver-related, and cardiovascular mortality rates. Nuclear magnetic resonance metabolomics data indicated that carriage of MLXIPL Gln241His was significantly associated with lower serum levels of VLDL and increased serum levels of HDL cholesterol. Conclusions:. Analyses of the MLXIPL Gln241His polymorphism showed a significant association with a higher risk of SLD diagnosis and elevated serum alanine aminotransferase as well as significantly lower serum triglycerides and apolipoprotein-B levels. MLXIPL might, therefore, be a potential pharmacological target for the treatment of SLD and hyperlipidemia, notably for patients at risk. More mechanistic studies are needed to better understand the role of MLXIPL Gln241His on lipid metabolism and steatosis development.

Published in Hepatology Communications

ISSN: 2471-254X (Online)
Publisher: Wolters Kluwer Health/LWW
Country of publisher: United States
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Diseases of the digestive system. Gastroenterology
Website: https://journals.lww.com/hepcomm/pages/default.aspx

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