Identification of Gm15441, a Txnip Antisense LncRNA, As a Critical Regulator in Liver Metabolic Homeostasis

Overview

Journal Cell Biosci

Publisher Biomed Central

Specialty Biology

Date 2021 Dec 15

PMID 34906243

Citations 1

Authors

Mingyang Xin

Qian Guo

Qingchun Lu

Juan Lu

Po-Shun Wang

Yun Dong

Tao Li

Ye Chen

Glenn S Gerhard

Xiao-Feng Yang

Michael Autieri

Ling Yang

Affiliations

Soon will be listed here.

Abstract

Background: The majority of mammalian genome is composed of non-coding regions, where numerous long non-coding RNAs (lncRNAs) are transcribed. Although lncRNAs have been identified to regulate fundamental biological processes, most of their functions remain unknown, especially in metabolic homeostasis. Analysis of our recent genome-wide screen reveals that Gm15441, a thioredoxin-interacting protein (Txnip) antisense lncRNA, is the most robustly induced lncRNA in the fasting mouse liver. Antisense lncRNAs are known to regulate their sense gene expression. Given that Txnip is a critical metabolic regulator of the liver, we aimed to investigate the role of Gm15441 in the regulation of Txnip and liver metabolism.

Methods: We examined the response of Gm15441 and Txnip under in vivo metabolic signals such as fasting and refeeding, and in vitro signals such as insulin and key metabolic transcription factors. We investigated the regulation of Txnip expression by Gm15441 and the underlying mechanism in mouse hepatocytes. Using adenovirus-mediated liver-specific overexpression, we determined whether Gm15441 regulates Txnip in the mouse liver and modulates key aspects of liver metabolism.

Results: We found that the expression levels of Gm15441 and Txnip showed a similar response pattern to metabolic signals in vivo and in vitro, but that their functions were predicted to be opposite. Furthermore, we found that Gm15441 robustly reduced Txnip protein expression in vitro through sequence-specific regulation and translational inhibition. Lastly, we confirmed the Txnip inhibition by Gm15441 in vivo (mice) and found that Gm15441 liver-specific overexpression lowered plasma triglyceride and blood glucose levels and elevated plasma ketone body levels.

Conclusions: Our data demonstrate that Gm15441 is a potent Txnip inhibitor and a critical metabolic regulator in the liver. This study reveals the therapeutic potential of Gm15441 in treating metabolic diseases.

Citing Articles

A novel NEDD4L-TXNIP-CHOP axis in the pathogenesis of nonalcoholic steatohepatitis.

Guo Q, Xin M, Lu Q, Feng D, Yang V, Peng L Theranostics. 2023; 13(7):2210-2225.

PMID: 37153733 PMC: 10157740. DOI: 10.7150/thno.81192.

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