The Role of Sirt7 in Beta Cell Function and Insulin Secretion

Authors

Trevor C. Kendrick, Brigham Young University - ProvoFollow
Jeffrey S. Tessem, Brigham Young University - ProvoFollow
Connor Littlefield, Brigham Young University - Provo

Files

Keywords

Diabetes, Sirt7, NKX6.1

Abstract

Diabetes is a chronic metabolic disease characterized by an inability of beta cells to produce or secrete insulin due to decreasing beta cell mass, a condition induced by beta cell death or overuse. Current treatment consists of daily administration of insulin to diabetic individuals. We have shown that Sirtuin 7 (Sirt7), a deacetylase located in the nucleus, directly interacts with Nkx6.1, a transcription factor essential for beta cell function and proliferation. We have shown that one of the post translational modifications that impinges on Nkx6.1 activity is acetylation. Given Sirt7’s role as a deacetylase, and published reports demonstrating its impact on glucose stimulated insulin secretion (GSIS), we hypothesized that the interaction betweenNkx6.1 and Sirt7 maybe needed for the Nkx6.1 mediated enhancement of glucose stimulated insulin secretion. Here we present data regarding the interaction between Nkx6.1 and Sirt7 in terms of Nkx6.1 acetylation status, effect on GSIS, and the effect of cultured glucose concentration on this interaction. These findings may be leveraged to develop interventions to better treat patients with type 1 and type 2 diabetes.

BYU ScholarsArchive Citation

Kendrick, Trevor C.; Tessem, Jeffrey S.; and Littlefield, Connor, "The Role of Sirt7 in Beta Cell Function and Insulin Secretion" (2024). Library/Life Sciences Undergraduate Poster Competition 2024. 13.
https://scholarsarchive.byu.edu/library_studentposters_2024/13

Document Type

Poster

Publication Date

2024-03-21

Language

English

College

Life Sciences

Department

Nutrition, Dietetics, and Food Science

University Standing at Time of Publication

Junior

Copyright Use Information

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