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Hepatocyte-specific HIF-1α ablation improves obesity-induced glucose intolerance by reducing first-pass GLP-1 degradation.
Citation | “Hepatocyte-Specific Hif-1Α Ablation Improves Obesity-Induced Glucose Intolerance By Reducing First-Pass Glp-1 Degradation.”. Science Advances, p. eaaw4176. . |
Center | UCSD-UCLA |
Author | Yun Sok Lee, Matthew Riopel, Pedro Cabrales, Guatam K Bandyopadhyay |
Abstract |
The decrease in incretin effects is an important etiologic component of type 2 diabetes with unknown mechanisms. In an attempt to understand obesity-induced changes in liver oxygen homeostasis, we found that liver HIF-1α expression was increased mainly by soluble factors released from obese adipocytes, leading to decreased incretin effects. Deletion of hepatocyte HIF-1α protected obesity-induced glucose intolerance without changes in body weight, liver steatosis, or insulin resistance. In-depth mouse metabolic phenotyping revealed that obesity increased first-pass degradation of an incretin hormone GLP-1 with increased liver DPP4 expression and decreased sinusoidal blood flow rate, reducing active GLP-1 levels in peripheral circulation. Hepatocyte HIF-1α KO blocked these changes induced by obesity. Deletion of hepatocyte HIF-2α did not change liver DPP4 expression but improved hepatic steatosis. Our results identify a previously unknown pathway for obesity-induced impaired beta cell glucose response (incretin effects) and the development of glucose intolerance through inter-organ communications. |
Year of Publication |
2019
|
Journal |
Science advances
|
Volume |
5
|
Issue |
7
|
Number of Pages |
eaaw4176
|
Date Published |
12/2019
|
ISSN Number |
2375-2548
|
DOI |
10.1126/sciadv.aaw4176
|
Alternate Journal |
Sci Adv
|
PMID |
31281892
|
PMCID |
PMC6609217
|
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