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首页> 外文期刊>Molecular and Cellular Biology >DOCK180, a major CRK-binding protein, alters cell morphology upon translocation to the cell membrane.
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DOCK180, a major CRK-binding protein, alters cell morphology upon translocation to the cell membrane.

机译:DOCK180是一种主要的CRK结合蛋白,在易位至细胞膜后会改变细胞形态。

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摘要

CRK belongs to a family of adaptor proteins that consist mostly of SH2 and SH3 domains. Far Western blotting with CRK SH3 has demonstrated that it binds to 135- to 145-, 160-, and 180-kDa proteins. The 135- to 145-kDa protein is C3G, a CRK SH3-binding guanine nucleotide exchange protein. Here, we report on the molecular cloning of the 180-kDa protein, which is designated DOCK180 (180-kDa protein downstream of CRK). The isolated cDNA contains a 5,598-bp open reading frame encoding an 1,866-amino-acid protein. The deduced amino acid sequence did not reveal any significant homology to known proteins, except that an SH3 domain was identified at its amino terminus. To examine the function of DOCK180, a Ki-Ras farnesylation signal was fused to the carboxyl terminus of DOCK180, a strategy that has been employed successfully for activation of adaptor-binding proteins in vivo. Whereas wild-type DOCK180 accumulated diffusely in the cytoplasm and did not have any effect on cell morphology, farnesylated DOCK180 was localized on the cytoplasmic membrane and changed spindle 3T3 cells to flat, polygonal cells. These results suggest that DOCK180 is a new effector molecule which transduces signals from tyrosine kinases through the CRK adaptor protein.
机译:CRK属于衔接子蛋白家族,主要由SH2和SH3结构域组成。用CRK SH3进行的Western印迹分析表明,它可以结合135-Da,145-,160-和180-kDa蛋白。 135-145kDa蛋白是C3G,一种CRK SH3结合鸟嘌呤核苷酸交换蛋白。在这里,我们报道了180 kDa蛋白的分子克隆,该蛋白被命名为DOCK180(CRK下游的180 kDa蛋白)。分离的cDNA含有5,598-bp的开放阅读框,其编码1,866个氨基酸的蛋白质。推导的氨基酸序列与已知蛋白没有任何显着同源性,只是在其氨基末端鉴定出了一个SH3结构域。为了检查DOCK180的功能,将Ki-Ras法尼基化信号融合到DOCK180的羧基末端,该策略已成功用于体内激活衔接子结合蛋白。野生型DOCK180分散在细胞质中,对细胞形态没有任何影响,而法尼基化的DOCK180位于细胞质膜上,将纺锤体3T3细胞变为扁平的多边形细胞。这些结果表明DOCK180是一种新的效应分子,其通过CRK衔接子蛋白转导酪氨酸激酶的信号。

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