LncRNA <i>PSMB8-AS1</i> Instigates Vascular Inflammation to Aggravate Atherosclerosis
Shu Li, Run-Chao He, S Wu, Yu Song, Kelan Zhang, Mao-Lin Tang, Yanrou Bei, Ting Zhang, Jin-Bo Lu, Xin Ma, Min Jiang, Liang-Jun Qin, Yudan Xu, Xian-Hui Dong, Jia Wu, Xiaoyan Dai, Yan‐Wei Hu
Abstract
BACKGROUND: Increasing evidence suggests that long noncoding RNAs play significant roles in vascular biology and disease development. One such long noncoding RNA, PSMB8-AS1 , has been implicated in the development of tumors. Nevertheless, the precise role of PSMB8-AS1 in cardiovascular diseases, particularly atherosclerosis, has not been thoroughly elucidated. Thus, the primary aim of this investigation is to assess the influence of PSMB8-AS1 on vascular inflammation and the initiation of atherosclerosis. METHODS: We generated PSMB8-AS1 knockin and Apoe (Apolipoprotein E) knockout mice ( Apoe −/− PSMB8-AS1 KI ) and global Apoe and proteasome subunit-β type-9 ( Psmb9 ) double knockout mice ( Apoe −/− Psmb9 −/− ). To explore the roles of PSMB8-AS1 and Psmb9 in atherosclerosis, we fed the mice with a Western diet for 12 weeks. RESULTS: Long noncoding RNA PSMB8-AS1 is significantly elevated in human atherosclerotic plaques. Strikingly, Apoe −/− PSMB8-AS1 KI mice exhibited increased atherosclerosis development, plaque vulnerability, and vascular inflammation compared with Apoe −/− mice. Moreover, the levels of VCAM1 (vascular adhesion molecule 1) and ICAM1 (intracellular adhesion molecule 1) were significantly upregulated in atherosclerotic lesions and serum of Apoe −/− PSMB8-AS1 KI mice. Consistently, in vitro gain- and loss-of-function studies demonstrated that PSMB8-AS1 induced monocyte/macrophage adhesion to endothelial cells and increased VCAM1 and ICAM1 levels in a PSMB9-dependent manner. Mechanistic studies revealed that PSMB8-AS1 induced PSMB9 transcription by recruiting the transcription factor NONO (non-POU domain-containing octamer-binding protein) and binding to the PSMB9 promoter. PSMB9 (proteasome subunit-β type-9) elevated VCAM1 and ICAM1 expression via the upregulation of ZEB1 (zinc finger E-box-binding homeobox 1). Psmb9 deficiency decreased atherosclerotic lesion size, plaque vulnerability, and vascular inflammation in Apoe −/− mice in vivo. Importantly, endothelial overexpression of PSMB8-AS1 -increased atherosclerosis and vascular inflammation were attenuated by Psmb9 knockout. CONCLUSIONS: PSMB8-AS1 promotes vascular inflammation and atherosclerosis via the NONO / PSMB9/ZEB1 axis. Our findings support the development of new long noncoding RNA–based strategies to counteract atherosclerotic cardiovascular disease.