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The long noncoding RNA CHROME regulates cholesterol homeostasis in primate.

Nat Metab. 2019; 
Hennessy EJ#, van Solingen C#, Scacalossi KR, Ouimet M, Afonso MS, Prins J, Koelwyn GJ, Sharma M, Ramkhelawon B, Carpenter S, Busch A,, Chernogubova E, Matic LP, Hedin U, Maegdefessel L,, Caffrey BE, Hussein MA, Ricci EP, Temel RE, Garabedian MJ, Berger JS, Vickers KC, Kanke M, Sethupathy P, Teupser D, Holdt LM, Moore KJ.
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Custom Vector Construction To create CHROME-overexpressing cell lines, CHROME cDNAs were obtained from Genscript, cloned into the pMSCV-PIG vector (Addgene, 21654) and transfected into HEK293T cells with packaging vectors pCMV-VSV-G (Addgene, 8454) and pCMV-Gag-Pol (Cell Biolabs, RV-111). Get A Quote

摘要

The human genome encodes thousands of long non-coding RNAs (lncRNAs), the majority of which are poorly conserved and uncharacterized. Here we identify a primate-specific lncRNA (CHROME), elevated in the plasma and atherosclerotic plaques of individuals with coronary artery disease, that regulates cellular and systemic cholesterol homeostasis. LncRNA CHROME expression is influenced by dietary and cellular cholesterol via the sterol-activated liver X receptor transcription factors, which control genes mediating responses to cholesterol overload. Using gain- and loss-of-function approaches, we show that CHROME promotes cholesterol efflux and HDL biogenesis by curbing the actions of a set of functionally related mi... More

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