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Targeting BCAA Catabolism to Treat Obesity-Associated Insulin Resistance.

Authors :
Meiyi Zhou
Jing Shao
Cheng-Yang Wu
Le Shu
Weibing Dong
Yunxia Liu
Mengping Chen
Wynn, R. Max
Jiqiu Wang
Ji Wang
Wen-Jun Gui
Xiangbing Qi
Lusis, Aldons J.
Zhaoping Li
Weiqing Wang
Guang Ning
Xia Yang
Chuang, David T.
Yibin Wang
Haipeng Sun
Source :
Diabetes; Sep2019, Vol. 68 Issue 9, p1730-1746, 17p
Publication Year :
2019

Abstract

Recent studies implicate a strong association between elevated plasma branched-chain amino acids (BCAAs) and insulin resistance (IR). However, a causal relationship and whether interrupted BCAA homeostasis can serve as a therapeutic target for diabetes remain to be established experimentally. In this study, unbiased integrative pathway analyses identified a unique genetic link between obesity-associated IR and BCAA catabolic gene expression at the pathway level in human and mouse populations. In genetically obese (ob/ob) mice, rate-limiting branched-chain α-keto acid (BCKA) dehydrogenase deficiency (i.e., BCAA and BCKA accumulation), a metabolic feature, accompanied the systemic suppression of BCAA catabolic genes. Restoring BCAA catabolic flux with a pharmacological inhibitor of BCKA dehydrogenase kinase (BCKDK) ( a suppressor of BCKA dehydrogenase) reduced the abundance of BCAA and BCKA and markedly attenuated IR in ob/ob mice. Similar outcomes were achieved by reducing protein (and thus BCAA) intake, whereas increasing BCAA intake did the opposite; this corroborates the pathogenic roles of BCAAs and BCKAs in IR in ob/ob mice. Like BCAAs, BCKAs also suppressed insulin signaling via activation of mammalian target of rapamycin complex 1. Finally, the small-molecule BCKDK inhibitor significantly attenuated IR in high-fat diet-induced obese mice. Collectively, these data demonstrate a pivotal causal role of a BCAA catabolic defect and elevated abundance of BCAAs and BCKAs in obesity-associated IR and provide proof-of-concept evidence for the therapeutic validity of manipulating BCAA metabolism for treating diabetes. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
00121797
Volume :
68
Issue :
9
Database :
Complementary Index
Journal :
Diabetes
Publication Type :
Academic Journal
Accession number :
138217309
Full Text :
https://doi.org/10.2337/db18-0927