Pathogenic monoallelic variants in GLIS3 increase type 2 diabetes risk and identify a subgroup of patients sensitive to sulfonylureas

Sarah Meulebrouck; Victoria Scherrer; Raphaël Boutry; Bénédicte Toussaint; Emmanuel Vaillant; Aurélie Dechaume; Hélène Loiselle; Beverley Balkau; Guillaume Charpentier; Sylvia Franc; Michel Marre; Morgane Baron; Martine Vaxillaire; Mehdi Derhourhi; Mathilde Boissel; Philippe Froguel; Amélie Bonnefond

doi:10.1007/s00125-023-06035-x

Pathogenic monoallelic variants in GLIS3 increase type 2 diabetes risk and identify a subgroup of patients sensitive to sulfonylureas

Diabetologia. 2024 Feb;67(2):327-332. doi: 10.1007/s00125-023-06035-x. Epub 2023 Dec 5.

Authors

Sarah Meulebrouck¹, Victoria Scherrer¹, Raphaël Boutry¹, Bénédicte Toussaint¹, Emmanuel Vaillant¹, Aurélie Dechaume¹, Hélène Loiselle¹, Beverley Balkau², Guillaume Charpentier³, Sylvia Franc^{3

4}, Michel Marre^{5

6}, Morgane Baron¹, Martine Vaxillaire¹, Mehdi Derhourhi¹, Mathilde Boissel¹, Philippe Froguel^{7

8}, Amélie Bonnefond^{9

10}

Affiliations

¹ Inserm UMR1283, CNRS UMR8199, European Genomic Institute for Diabetes (EGID), Université de Lille, Institut Pasteur de Lille, Lille University Hospital, Lille, France.
² Inserm U1018 Clinical Epidemiology, Center for Research in Epidemiology and Population Health, Paris-Saclay University, Paris-Sud University, UVSQ, Villejuif, France.
³ CERITD (Centre d'Étude et de Recherche pour l'Intensification du Traitement du Diabète), Evry, France.
⁴ Department of Diabetes, Sud-Francilien Hospital, Paris-Sud University, Corbeil-Essonnes, France.
⁵ Institut Necker-Enfants Malades, Inserm, Université de Paris, Paris, France.
⁶ Clinique Ambroise Paré, Neuilly-sur-Seine, France.
⁷ Inserm UMR1283, CNRS UMR8199, European Genomic Institute for Diabetes (EGID), Université de Lille, Institut Pasteur de Lille, Lille University Hospital, Lille, France. p.froguel@imperial.ac.uk.
⁸ Department of Metabolism, Digestion and Reproduction, Imperial College London, London, UK. p.froguel@imperial.ac.uk.
⁹ Inserm UMR1283, CNRS UMR8199, European Genomic Institute for Diabetes (EGID), Université de Lille, Institut Pasteur de Lille, Lille University Hospital, Lille, France. amelie.bonnefond@inserm.fr.
¹⁰ Department of Metabolism, Digestion and Reproduction, Imperial College London, London, UK. amelie.bonnefond@inserm.fr.

Abstract

Aims/hypothesis: GLIS3 encodes a transcription factor involved in pancreatic beta cell development and function. Rare pathogenic, bi-allelic mutations in GLIS3 cause syndromic neonatal diabetes whereas frequent SNPs at this locus associate with common type 2 diabetes risk. Because rare, functional variants located in other susceptibility genes for type 2 diabetes have already been shown to strongly increase individual risk for common type 2 diabetes, we aimed to investigate the contribution of rare pathogenic GLIS3 variants to type 2 diabetes.

Methods: GLIS3 was sequenced in 5471 individuals from the Rare Variants Involved in Diabetes and Obesity (RaDiO) study. Variant pathogenicity was assessed following the criteria established by the American College of Medical Genetics and Genomics (ACMG). To address the pathogenic strong criterion number 3 (PS3), we conducted functional investigations of these variants using luciferase assays, focusing on capacity of GLIS family zinc finger 3 (GLIS3) to bind to and activate the INS promoter. The association between rare pathogenic or likely pathogenic (P/LP) variants and type 2 diabetes risk (and other metabolic traits) was then evaluated. A meta-analysis combining association results from RaDiO, the 52K study (43,125 individuals) and the TOPMed study (44,083 individuals) was finally performed.

Results: Through targeted resequencing of GLIS3, we identified 105 rare variants that were carried by 395 participants from RaDiO. Among them, 49 variants decreased the activation of the INS promoter. Following ACMG criteria, 18 rare variants were classified as P/LP, showing an enrichment in the last two exons compared with the remaining exons (p<5×10^-6; OR>3.5). The burden of these P/LP variants was strongly higher in individuals with type 2 diabetes (p=3.0×10^-3; OR 3.9 [95% CI 1.4, 12]), whereas adiposity, age at type 2 diabetes diagnosis and cholesterol levels were similar between variant carriers and non-carriers with type 2 diabetes. Interestingly, all carriers with type 2 diabetes were sensitive to oral sulfonylureas. A total of 7 P/LP variants were identified in both 52K and TOPMed studies. The meta-analysis of association studies obtained from RaDiO, 52K and TOPMed showed an enrichment of P/LP GLIS3 variants in individuals with type 2 diabetes (p=5.6×10^-5; OR 2.1 [95% CI 1.4, 2.9]).

Conclusions/interpretation: Rare P/LP GLIS3 variants do contribute to type 2 diabetes risk. The variants located in the distal part of the protein could have a direct effect on its functional activity by impacting its transactivation domain, by homology with the mouse GLIS3 protein. Furthermore, rare P/LP GLIS3 variants seem to have a direct clinical effect on beta cell function, which could be improved by increasing insulin secretion via the use of sulfonylureas.

Keywords: ACMG; Functional genetics; GLIS3; Luciferase assays; Rare variants; Type 2 diabetes.

Publication types

Meta-Analysis

MeSH terms

Animals
DNA-Binding Proteins / metabolism
Diabetes Mellitus, Type 2* / drug therapy
Diabetes Mellitus, Type 2* / genetics
Gene Expression Regulation
Humans
Infant, Newborn
Insulin-Secreting Cells* / metabolism
Mice
Mutation
Repressor Proteins / metabolism
Trans-Activators / metabolism
Transcription Factors / genetics
Transcription Factors / metabolism

Substances

Transcription Factors
GLIS3 protein, human
DNA-Binding Proteins
Repressor Proteins
Trans-Activators

Grants and funding

101043671/ERC_/European Research Council/International