Oncogene StarD4 had the function of promoting proliferation and metastasis of triple-negative breast cancer (TNBC), but its clinical value and molecular mechanism are unknown. This paper found that StarD4 was highly expressed in cancer tissues of TNBC patients, and higher expression level of StarD4 in TNBC patient resulted in poorer prognosis. Based on transcriptomics of MDA-MB-231 cell model, the results of bioinformatics analysis showed that down-regulated expression level of StarD4 led to overall downregulation of cholesterol-relative genes and significant enrichment of cancer mechanism and pathway. Further analysis and investigation verified that StarD4 might cross-promote the protein stability of receptor ITGA5 through the cholesterol pathway to enhance TNBC progression, which provides guidance for clinical application of TNBC diagnosis and treatment.
StarD4具有促三阴乳腺癌(TNBC)增殖转移功能,但临床价值和分子机制未明。本文发现StarD4在TNBC癌组织高表达,且高表达患者生存预后不良。通过TNBC细胞模型的转录组检测和分析发现:StarD4敲减表达引发胆固醇通路基因的整体下调和TNBC肿瘤通路的显著富集。进一步分析验证了StarD4可能通过胆固醇通路交叉调控细胞膜受体ITGA5的蛋白稳定性,发挥促癌的分子机制,为临床TNBC的诊疗应用提供了指导。.
Keywords: ITGA5; StarD4; cholesterol metabolism; triple negative breast cancer.