Long Noncoding RNA NEXN-AS1 Mitigates Atherosclerosis by Regulating the Actin-binding Protein NEXN

Overview

Journal J Clin Invest

Specialty General Medicine

Date 2018 Dec 28

PMID 30589415

Citations 74

Authors

Yan-Wei Hu

Feng-Xia Guo

Yuan-Jun Xu

Pan Li

Zhi-Feng Lu

David G McVey

Lei Zheng

Qian Wang

John H Ye

Chun-Min Kang

Shao-Guo Wu

Jing-Jing Zhao

Xin Ma

Zhen Yang

Fu-Chun Fang

Yu-Rong Qiu

Bang-Ming Xu

Lei Xiao

Qian Wu

Li-Mei Wu

Li Ding

Tom R Webb

Nilesh J Samani

Shu Ye

Affiliations

Soon will be listed here.

Abstract

Noncoding RNAs are emerging as important players in gene regulation and disease pathogeneses. Here, we show that a previously uncharacterized long noncoding RNA, nexilin F-actin binding protein antisense RNA 1 (NEXN-AS1), modulates the expression of the actin-binding protein NEXN and that NEXN exerts a protective role against atherosclerosis. An expression microarray analysis showed that the expression of both NEXN-AS1 and NEXN was reduced in human atherosclerotic plaques. In vitro experiments revealed that NEXN-AS1 interacted with the chromatin remodeler BAZ1A and the 5' flanking region of the NEXN gene and that it also upregulated NEXN expression. Augmentation of NEXN-AS1 expression inhibited TLR4 oligomerization and NF-κB activity, downregulated the expression of adhesion molecules and inflammatory cytokines by endothelial cells, and suppressed monocyte adhesion to endothelial cells. These inhibitory effects of NEXN-AS1 were abolished by knockdown of NEXN. In vivo experiments using ApoE-knockout mice fed a Western high-fat diet demonstrated that NEXN deficiency promoted atherosclerosis and increased macrophage abundance in atherosclerotic lesions, with heightened expression of adhesion molecules and inflammatory cytokines, whereas augmented NEXN expression deterred atherosclerosis. Patients with coronary artery disease were found to have lower blood NEXN levels than healthy individuals. These results indicate that NEXN-AS1 and NEXN represent potential therapeutic targets in atherosclerosis-related diseases.

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