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从单细胞祖先到多细胞动物进化过程中Src酪氨酸激酶的功能发育。

Functional development of Src tyrosine kinases during evolution from a unicellular ancestor to multicellular animals.

作者信息

Segawa Yuko, Suga Hiroshi, Iwabe Naoyuki, Oneyama Chitose, Akagi Tsuyoshi, Miyata Takashi, Okada Masato

机构信息

Department of Oncogene Research, Research Institute for Microbial Diseases, Osaka University, Osaka 565-0871, Japan.

出版信息

Proc Natl Acad Sci U S A. 2006 Aug 8;103(32):12021-6. doi: 10.1073/pnas.0600021103. Epub 2006 Jul 27.

Abstract

The Src family of tyrosine kinases play pivotal roles in regulating cellular functions characteristic of multicellular animals, including cell-cell interactions, cell-substrate adhesion, and cell migration. To investigate the functional alteration of Src kinases during evolution from a unicellular ancestor to multicellular animals, we characterized Src orthologs from the unicellular choanoflagellate Monosiga ovata and the primitive multicellular sponge Ephydatia fluviatilis. Here, we show that the src gene family and its C-terminal Src kinase (Csk)-mediated regulatory system already were established in the unicellular M. ovata and that unicellular Src has unique features relative to multicellular Src: It can be phosphorylated by Csk at the negative regulatory site but still exhibits substantial activity even in the phosphorylated form. Analyses of chimera molecules between M. ovata and E. fluviatilis Src orthologs reveal that structural alterations in the kinase domain are responsible for the unstable negative regulation of M. ovata Src. When expressed in vertebrate fibroblasts, M. ovata Src can induce cell transformation irrespective of the presence of Csk. These findings suggest that a structure of Src required for the stable Csk-mediated negative regulation still is immature in the unicellular M. ovata and that the development of stable negative regulation of Src may correlate with the evolution of multicellularity in animals.

摘要

酪氨酸激酶的Src家族在调节多细胞动物特有的细胞功能中发挥着关键作用,这些功能包括细胞间相互作用、细胞与底物的黏附以及细胞迁移。为了研究从单细胞祖先到多细胞动物进化过程中Src激酶的功能变化,我们对单细胞领鞭毛虫卵形单鞭滴虫和原始多细胞海绵河流壶海绵中的Src直系同源物进行了表征。在此,我们表明src基因家族及其C端Src激酶(Csk)介导的调节系统在单细胞的卵形单鞭滴虫中就已经建立,并且单细胞Src相对于多细胞Src具有独特的特征:它可以在负调控位点被Csk磷酸化,但即使在磷酸化形式下仍表现出相当大的活性。对卵形单鞭滴虫和河流壶海绵Src直系同源物之间的嵌合分子分析表明,激酶结构域的结构改变是卵形单鞭滴虫Src负调控不稳定的原因。当在脊椎动物成纤维细胞中表达时无论是否存在Csk,卵形单鞭滴虫Src都能诱导细胞转化。这些发现表明,在单细胞的卵形单鞭滴虫中,Csk介导的稳定负调控所需的Src结构仍然不成熟,并且Src稳定负调控的发展可能与动物多细胞性的进化相关。

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