Long noncoding RNA forms a growth promoting complex with HNRNPL in human glioblastoma through stabilization of ACTN4 and activation of NF-κB signaling.

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2019
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Abstract
Long noncoding RNAs (lncRNAs) have essential roles in diverse cellular processes, both in normal and diseased cell types, and thus have emerged as potential therapeutic targets. A specific member of this family, the SWI/SNF complex antagonist associated with prostate cancer 1 (), has been shown to promote aggressive prostate cancer growth by antagonizing the SWI/SNF complex and therefore serves as a biomarker for poor prognosis. Here, we investigated whether plays a potential role in the development of human glioblastoma (GBM).RNA-ISH and immunohistochemistry were performed on a tissue microarray to assess expression of and associated proteins in human gliomas. Proteins complexed with were identified using RNA pull-down and mass spectrometry. Lentiviral constructs were used for functional analysis and Results: was increased in primary GBM samples and cell lines, and knockdown of the lncRNA suppressed growth. was found to bind heterogeneous nuclear ribonucleoprotein L (HNRNPL) which stabilized the lncRNA and led to an enhanced interaction with the protein actinin alpha 4 (ACTN4). was also highly expressed in primary GBM samples and was associated with poorer overall survival in glioma patients. The -HNRNPL complex led to stabilization of ACTN4 through suppression of proteasomal degradation, which resulted in increased nuclear localization of the p65 subunit of NF-κB and activation of NF-κB signaling, a pathway associated with cancer development.Our results implicated as a driver of GBM growth as well as a potential therapeutic target in treatment of the disease.
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Authors Ji, Jianxiong;Xu, Ran;Ding, Kaikai;Bao, Guoqing;Zhang, Xin;Huang, Bin;Wang, Xinyu;Martinez, Aurora;Wang, Xiuying;Li, Gang;Miletic, Hrvoje;Thorsen, Frits;Bjerkvig, Rolf;Xiang, Lei;Han, Bo;Chen, Anjing;Li, Xin-Gang;Wang, Jian;
Journal clinical cancer research : an official journal of the american association for cancer research
Year 2019
DOI
clincanres.0747.2019
URL
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