| Literature DB >> 31332289 |
Qiao-Yang Sun1, Ling-Wen Ding2, Kara Johnson3, Siqin Zhou1, Jeffrey W Tyner3, Henry Yang1, Ngan B Doan4, Jonathan W Said4, Jin-Fen Xiao1, Xin-Yi Loh1, Xue-Bin Ran1, Nachiyappan Venkatachalam1, Zhentang Lao1, Ye Chen1, Liang Xu1, Li-Fei Fan1,5, Wenwen Chien6, De-Chen Lin6, H Phillip Koeffler1,6.
Abstract
Apoptosis of cancer cells occurs by a complex gene regulatory network. Here we showed that SOX7 was significantly downregulated in different cancer types, especially in lung and breast cancers. Low expression of SOX7 was associated with advantage stage of cancer with shorter overall survival. Cancer cells with loss of SOX7 promoted cell survival and colony formation, suppressed cellular apoptosis and produced a drug resistant phenotype against a variety of chemo/targeting therapeutic agents. Mechanistically, SOX7 induced cellular apoptosis through upregulation of genes associated with both P38 and apoptotic signaling pathway, as well as preventing the proteasome mediated degradation of pro-apoptotic protein BIM. Treatment of either a proteasome inhibitor MG132 or bortezomib, or with a p-ERK/MEK inhibitor U0126 attenuate the SOX7 promoted BIM degradation. We identified Panobinostat, an FDA approved pan-HDAC inhibitor, could elevate and restore SOX7 expression in SOX7 silenced lung cancer cells. Taken together, these data revealed an unappreciated role of SOX7 in regulation of cellular apoptosis through control of MAPK/ERK-BIM signaling.Entities:
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Year: 2019 PMID: 31332289 DOI: 10.1038/s41388-019-0865-8
Source DB: PubMed Journal: Oncogene ISSN: 0950-9232 Impact factor: 9.867