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The Twist box domain is required for Twist1-induced prostate cancer metastasis

机译:Twistbox域是Twist1诱导的前列腺癌转移所必需的

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Twist1, a basic helix-loop-helix transcription factor, plays a key role during development and is a master regulator of the epithelial-mesenchymal transition (EMT) that promotes cancer metastasis. Structure-function relationships of Twist1 to cancer-related phenotypes are underappreciated, so we studied the requirement of the conserved Twist box domain for metastatic phenotypes in prostate cancer. Evidence suggests that Twist1 is overexpressed in clinical specimens and correlated with aggressive/metastatic disease. Therefore, we examined a transactivation mutant, Twist1-F191G, in prostate cancer cells using in vitro assays, which mimic various stages of metastasis. Twist1 overexpression led to elevated cytoskeletal stiffness and cell traction forces at the migratory edge of cells based on biophysical single-cell measurements. Twist1 conferred additional cellular properties associated with cancer cell metastasis including increased migration, invasion, anoikis resistance, and anchorage-independent growth. The Twist box mutant was defective for these Twist1 phenotypes in vitro. Importantly, we observed a high frequency of Twist1-induced metastatic lung tumors and extrathoracic metastases in vivo using the experimental lung metastasis assay. The Twist box was required for prostate cancer cells to colonize metastatic lung lesions and extrathoracic metastases. Comparative genomic profiling revealed transcriptional programs directed by the Twist box that were associated with cancer progression, such as Hoxa9. Mechanistically, Twist1 bound to the Hoxa9 promoter and positively regulated Hoxa9 expression in prostate cancer cells. Finally, Hoxa9 was important for Twist1-induced cellular phenotypes associated with metastasis. These data suggest that the Twist box domain is required for Twist1 transcriptional programs and prostate cancer metastasis. Implications: Targeting the Twist box domain of Twist1 may effectively limit prostate cancer metastatic potential.
机译:Twist1是一种基本的螺旋-环-螺旋转录因子,在发育过程中起关键作用,并且是促进癌症转移的上皮-间质转化(EMT)的主要调节剂。 Twist1与癌症相关表型的结构-功能关系未得到充分认识,因此我们研究了保守Twist box结构域对前列腺癌转移表型的要求。有证据表明,Twist1在临床标本中过表达,并与侵袭性/转移性疾病相关。因此,我们使用体外测定法检测了前列腺癌细胞中的一个反式激活突变体Twist1-F191G,该方法模拟了转移的各个阶段。根据生物物理单细胞测量结果,Twist1的过表达导致细胞迁移边缘的细胞骨架硬度和细胞牵引力升高。 Twist1赋予了与癌细胞转移相关的其他细胞特性,包括增加的迁移,侵袭,厌食症抵抗力以及与锚定无关的生长。 Twist box突变体在体外对于这些Twist1表型是有缺陷的。重要的是,我们使用实验性肺转移试验在体内观察到了Twist1诱导的转移性肺肿瘤和胸外转移的高频率。前列腺癌细胞需要使用Twist盒来定居转移性肺部病变和胸外转移。比较基因组分析揭示了由Twist盒指导的与癌症进展相关的转录程序,例如Hoxa9。从机理上讲,Twist1与Hoxa9启动子结合并正向调节前列腺癌细胞中的Hoxa9表达。最后,Hoxa9对于Twist1诱导的与转移相关的细胞表型很重要。这些数据表明,Twist1盒结构域是Twist1转录程序和前列腺癌转移所必需的。启示:靶向Twist1的Twist盒结构域可能有效地限制前列腺癌的转移潜力。

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