| Literature DB >> 24096089 |
Hyun-Seok Jin1, Jeonghyun Kim1, Soo-Jin Lee2, Kyunga Kim3, Min Jin Go4, Jong-Young Lee4, Hye-Ja Lee5, Jihyun Song5, Byeong Tak Jeon6, Gu Seob Roh6, Sung-Jun Kim7, Bo-Young Kim1, Kyung-Won Hong8, Young-Hyun Yoo9, Beomseok Oh10, Yup Kang11, Seon-Yong Jeong12.
Abstract
Several association studies have implicated the PARK2 gene that encodes parkin--the key molecule orchestrating the mitochondrial quality control system--as a candidate susceptibility gene for diabetes. A total of 7551 unrelated Korean KARE cohort subjects were analyzed to investigate the association between the PARK2 single nucleotide polymorphism (SNP) and quantitative glycemic traits. Two SNPs, rs10455889 and rs9365294, were significantly associated with fasting plasma glucose level (p=∼1.2×10(-4)) and insulin secretion indices (p=∼7.4×10(-5)) in male KARE subjects. Parkin was expressed predominantly in the rat pancreatic islets. Downregulation of the Park2 gene in rat INS-1 β-cells resulted in a significant decrease in the glucose-stimulated insulin secretion, intracellular insulin gene expression, and intracellular ATP level. The Park2-depleted β-cells also exhibited increased mitochondrial fragmentation and ROS production and decreased mitochondrial membrane potential. Both population-based statistical evaluation and experimental evidence demonstrated a fundamental role of the PARK2 gene in the maintenance of β-cell function.Entities:
Keywords: Genetic association; Insulin secretion; Mitochondria; PARK2; Pancreatic β-cell; Type 2 diabetes
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Year: 2013 PMID: 24096089 DOI: 10.1016/j.mce.2013.09.031
Source DB: PubMed Journal: Mol Cell Endocrinol ISSN: 0303-7207 Impact factor: 4.102