Chie Lyndon, Friedman Fred K, Duncan Thomas, Chen James M, Chung Denise, Pincus Matthew
Department of Pathology and Laboratory Medicine, New York Harbor VA Medical Center, Brooklyn, NY 11209, USA.
Protein J. 2004 Apr;23(3):229-34. doi: 10.1023/b:jopc.0000026418.82786.5e.
In the accompanying paper, we found, using molecular dynamics calculations, four domains of the ras-specific SOS guanine nucleotide exchange protein (residues 589-601, 654-675, 746-761, and 980-989) that differ markedly in conformation when SOS is complexed with either oncogenic (Val 12-) ras-p21 or wild-type ras-p21. Three of these domains contain three crystallographically undefined loops that we modeled in these calculations, and one is a newly identified non-loop domain containing SOS residues 980-989. We have now synthesized peptides corresponding to these four domains and find that all of them block Val 12-ras-p21-induced oocyte maturation. All of them also block insulin-induced oocyte maturation, but two of these peptides, corresponding to SOS residues 589-601 and 980-989, block oncogenic ras to a significantly greater extent. These results suggest that SOS contains domains, including the three loop domains, that are important for ras signaling and that several of these domains can activate different pathways specific to oncogenic or wild-type ras-p21.
在随附的论文中,我们通过分子动力学计算发现,ras特异性SOS鸟嘌呤核苷酸交换蛋白有四个结构域(第589 - 601位、654 - 675位、746 - 761位和980 - 989位残基),当SOS与致癌性(Val 12 -)ras - p21或野生型ras - p21形成复合物时,其构象有显著差异。其中三个结构域包含三个在晶体学上未定义的环,我们在这些计算中对其进行了建模,另一个是新鉴定的非环结构域,包含SOS的第980 - 989位残基。我们现已合成了与这四个结构域相对应的肽段,发现它们都能阻断Val 12 - ras - p21诱导的卵母细胞成熟。它们也都能阻断胰岛素诱导的卵母细胞成熟,但其中两个肽段,对应于SOS的第589 - 601位和980 - 989位残基,对致癌性ras的阻断作用明显更强。这些结果表明,SOS包含对ras信号传导很重要的结构域,包括三个环结构域,并且这些结构域中的几个可以激活致癌性或野生型ras - p21特有的不同信号通路。
