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SPA-1 controls the invasion and metastasis of human prostate cancer.

机译:SPA-1控制人前列腺癌的侵袭和转移。

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Recent studies suggest that SIPA1 encoding a Rap GTPase-activating protein SPA-1 is a candidate metastasis efficiency-modifying gene in human breast cancer. In this study, we investigated the expression and function of SPA-1 in human prostate cancer (CaP). Immunohistochemical studies of tumor specimens from CaP patients revealed a positive correlation of SPA-1 expression with disease progression and metastasis. The correlation was recapitulated in human CaP cell lines; LNCaP that rarely showed metastasis in SCID mice expressed an undetectable level of SPA-1, whereas highly metastatic PC3 showed abundant SPA-1 expression. Moreover, SIPA1 transduction in LNCaP caused prominent abdominal lymph node metastasis without affecting primary tumor size, whereas shRNA-mediated SIPA1 knockdown or expression of a dominant-active Rap1 mutant (Rap1V12) in PC3 suppressed metastasis. LNCaP transduced with SPA-1 (LNCaP/SPA-1) showed attenuated adhesion to the precoated extracellular matrices (ECM) including collagens and fibronectin, due to defective ECM-medicated Rap1 activation. In addition, LNCaP/SPA-1 showed a diminished level of nuclear Brd4, which is known to bind SPA-1, resulting in reduced expression of a series of ECM-related genes. These results suggest that SPA-1 plays an important role in controlling metastasis efficiency of human CaP by regulating the expression of and interaction with ECM in the primary sites.
机译:最近的研究表明,编码Rap GTPase激活蛋白SPA-1的SIPA1是人类乳腺癌中候选转移效率修饰基因。在这项研究中,我们调查了SPA-1在人前列腺癌(CaP)中的表达和功能。 CaP患者肿瘤标本的免疫组织化学研究表明SPA-1表达与疾病进展和转移呈正相关。在人CaP细胞系中概括了相关性;在SCID小鼠中很少显示转移的LNCaP表达的SPA-1水平未检出,而高度转移的PC3显示了大量的SPA-1表达。此外,LNCaP中的SIPA1转导引起显着的腹部淋巴结转移,而不会影响原发肿瘤的大小,而shRNA介导的SIPA1敲低或PC3中显性激活的Rap1突变体(Rap1V12)的表达抑制了转移。 SPA-1(LNCaP / SPA-1)转导的LNCaP由于与ECM结合的Rap1激活缺陷,显示与包括胶原蛋白和纤连蛋白在内的预涂细胞外基质(ECM)的粘附力减弱。另外,LNCaP / SPA-1的核Brd4水平降低,已知与SPA-1结合,导致一系列ECM相关基因的表达降低。这些结果表明SPA-1通过调节主要部位中ECM的表达并与之相互作用,在控制人CaP转移效率中起重要作用。

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