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New insulin-like proteins with atypical disulfide bond pattern characterized in Caenorhabditis elegans by comparative sequence analysis and homology modeling

机译:通过比较序列分析和同源建模,发现秀丽隐杆线虫具有新的具有非典型二硫键模式的胰岛素样蛋白

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摘要

We have identified three new families of insulin homologs in Caenorhabditis elegans. In two of these families, concerted mutations suggest that an additional disulfide bond links B and A domains, and that the A-domain internal disulfide bond is substituted by a hydrophobic interaction. Homology modeling remarkably confirms these predictions and shows that despite this atypical disulfide bond pattern and the absence of C-like peptide, all these proteins may adopt the same fold as the insulin. Interestingly, whereas we identified 10 insulin-like peptides, only one insulin-like-receptor (daf-2) has been found. We propose that these insulin-related peptides may correspond to different activators or inhibitors of the daf-2 insulin-regulating pathway.
机译:我们在秀丽隐杆线虫中鉴定了三个新的胰岛素同源物家族。在这些家族中的两个家族中,一致的突变表明一个额外的二硫键连接了B和A结构域,而A结构域内部的二硫键被疏水相互作用所取代。同源性模型显着证实了这些预测,并表明尽管具有这种非典型的二硫键模式并且不存在C样肽,但所有这些蛋白可能采用与胰岛素相同的折叠倍数。有趣的是,尽管我们鉴定了10种胰岛素样肽,但仅发现一种胰岛素样受体(daf-2)。我们建议这些胰岛素相关的肽可能对应于daf-2胰岛素调节途径的不同激活剂或抑制剂。

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