Underestimated risk of secondary complications in pathogenic and glucose-elevating GCK variant carriers with type 2 diabetes

Kelly M Schiabor Barrett; Natalie Telis; Lisa M McEwen; Evanette K Burrows; Basil Khuder; Daniel P Judge; Pamala A Pawloski; Joseph J Grzymski; Nicole L Washington; Alexandre Bolze; Elizabeth T Cirulli

doi:10.1038/s43856-024-00663-z

Underestimated risk of secondary complications in pathogenic and glucose-elevating GCK variant carriers with type 2 diabetes

Commun Med (Lond). 2024 Nov 20;4(1):239. doi: 10.1038/s43856-024-00663-z.

Affiliations

¹ Helix, 101 S Ellsworth Ave Suite 350, San Mateo, CA, USA. kelly.barrett@helix.com.
² Helix, 101 S Ellsworth Ave Suite 350, San Mateo, CA, USA.
³ Division of Cardiology, Medical University of South Carolina, Charleston, SC, USA.
⁴ HealthPartners, Minneapolis, MN, USA.
⁵ Renown Institute for Health Innovation, Reno, NV, USA.
⁶ Department of Internal Medicine, University of Nevada, Reno School of Medicine, Reno, NV, USA.

Abstract

Background: Natural HbA1c levels in GCK Maturity-onset diabetes of the young (GCK-MODY) patients often sit above the diagnostic threshold for type 2 diabetes (T2D). Treatments to lower HbA1c levels show reduced effectiveness in these individuals, yet in case studies to date, GCK-MODY patients often evade secondary T2D complications. Given these deviations, genetic screening of GCK may be clinically useful, but population studies are needed to more broadly understand T2D-related complications in GCK variant carriers.

Methods: To identify GCK variant carriers at the population level, we used both ACMG/AMP variant interpretation for GCK-MODY pathogenicity and a state-of-the-art variant interpretation strategy based on functional and statistical evidence to predict glucose elevations. Presence of pathogenic and glucose-elevating GCK variants was assessed in two cohorts (n~535,000). We identified 442 individuals with GCK variants predicted to increase glucose (~1/1200), with 150 (34%) of these individuals harboring variants reaching a pathogenic interpretation.

Results: In a retrospective analysis, we show that in addition to elevated HbA1c, pathogenic variant carriers are 10x as likely, and all other glucose-elevating GCK variant carriers are 3x as likely, to receive a T2D diagnosis compared to non-GCK carriers. Surprisingly, carriers of pathogenic and glucose-elevating GCK variants with T2D develop T2D-related complications at rates more than double that of individuals without T2D, comparable to non-GCK individuals with T2D.

Conclusions: This population-level assessment shows secondary complications in individuals with pathogenic and glucose-elevating GCK variants and T2D and suggests that genotyping for these variants should be considered in a precision medicine approach for T2D treatment and prevention.

Plain language summary

This study investigates the role of the GCK gene in Type 2 Diabetes (T2D). Variations in the GCK gene are known to cause a form of diabetes that is characterized by early onset and stable blood sugar levels, with a low risk of the type of complications often experienced by people with other causes of T2D. However, our study of a large number of people living in both the United Kingdom and the United States shows that some specific variations in the GCK gene give people a higher risk of developing T2D with the typical secondary complications. This suggests that knowledge of GCK variation in a person should be considered when optimizing T2D prevention and treatment strategies.