| Literature DB >> 30673611 |
Yongxu Zhao1, Zhuanghui Feng2, Yongxian Zhang2, Yingmin Sun2, Yanhao Chen2, Xiaojian Liu2, Shuang Li2, Tingting Zhou2, Lanlan Chen2, Yuda Wei2, Danjun Ma3, Kathy O Lui4, Hao Ying2, Yan Chen2, Qiurong Ding5.
Abstract
DNA variants in the SLC16A11 coding region were identified to be strongly associated with type 2 diabetes (T2DM) in a Mexican population. Previous studies suggested that these variants disrupt SLC16A11 function and therefore proposed to revive SLC16A11 levels or activity to achieve therapeutic benefit. However, with knockout mouse models, here we show that Slc16a11 depletion has no significant metabolic defects. Further studies demonstrate that reconstitution of the mutant, but not the wild-type Slc16a11, in the liver of knockout mice causes more triglyceride accumulation and induction of insulin resistance via upregulation of lipin 1, suggesting gaining of aberrant functions of the mutant protein that affects lipid metabolism. Our findings offer a different explanation to the function of these diabetic variants, challenging the concept of enhancing SLC16A11 function to treat T2DM. The contradictory results by our and previous studies suggest that how the SLC16A11 locus contributes to human metabolism warrants further investigation.Entities:
Keywords: Lipin 1; SLC16A11; triglyceride metabolism; type 2 diabetes
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Year: 2019 PMID: 30673611 DOI: 10.1016/j.celrep.2018.12.100
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423