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A novel oncogene ost encodes a guanine nucleotide exchange factor that potentially links Rho and Rac signaling pathways.

机译:一种新型致癌基因ost编码一种鸟嘌呤核苷酸交换因子该因子潜在地连接Rho和Rac信号通路。

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摘要

Transfection of NIH3T3 cells with an osteosarcoma expression cDNA library led to the appearance of foci of morphologically transformed cells which were found to harbor a novel oncogene, ost. The ost product was activated by truncation of the N-terminal domain of the ost proto-oncogene and was highly tumorigenic in nude mouse assays. The proto-ost cDNA, isolated subsequently, encodes a predicted protein of 100 kDa containing DH (Db1 homology) and PH (pleckstrin homology) domains. Ost is mainly phosphorylated on serine and localized in the cytoplasm. Purified Ost protein catalyzed guanine nucleotide exchange on RhoA and Cdc42 among the Rho and Ras family members tested, indicating that Ost can activate these small GTP-binding proteins. Ost did not detectably associate with RhoA or Cdc42, but interacted specifically with the GTP-bound form of Rac1, suggesting that Ost can function as an effector of Rac1. These results suggest that Ost is a critical regulatory component which links pathways that signal through Rac1, RhoA and Cdc42. Of the tissues examined, expression of ost was the highest in brain and could be localized to neurons and alpha-tanycytes, suggesting that Ost may participate in axonal transport in these specialized cells.
机译:用骨肉瘤表达cDNA文库转染NIH3T3细胞导致出现形态学转化细胞的病灶,这些细胞被发现含有一种新的癌基因ost。 ost产物通过ost原始致癌基因的N末端结构域的截短而被激活,并且在裸鼠实验中具有高度致瘤性。随后分离出的原始cDNA编码一个100 kDa的预测蛋白,其中包含DH(Db1同源)和PH(pleckstrin同源)域。 Ost主要在丝氨酸上磷酸化并定位在细胞质中。纯化的Ost蛋白催化了Rho和Ras家族成员中RhoA和Cdc42上鸟嘌呤核苷酸的交换,表明Ost可以激活这些小的GTP结合蛋白。 Ost未检测到与RhoA或Cdc42缔合,但与Gac结合形式的Rac1特异性相互作用,表明Ost可以充当Rac1的效应子。这些结果表明,Ost是连接通过Rac1,RhoA和Cdc42发出信号的途径的关键调控成分。在所检查的组织中,ost表达在脑中最高,并且可以定位于神经元和α-单核细胞,这表明Ost可能参与了这些特殊细胞中的轴突运输。

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