作者
Jiancheng Hu, Edward C Stites, Haiyang Yu, Elizabeth A Germino, Hiruy S Meharena, Philip JS Stork, Alexandr P Kornev, Susan S Taylor, Andrey S Shaw
发表日期
2013/8/29
期刊
Cell
卷号
154
期号
5
页码范围
1036-1046
出版商
Elsevier
简介
Although RAF kinases are critical for controlling cell growth, their mechanism of activation is incompletely understood. Recently, dimerization was shown to be important for activation. Here we show that the dimer is functionally asymmetric with one kinase functioning as an activator to stimulate activity of the partner, receiver kinase. The activator kinase did not require kinase activity but did require N-terminal phosphorylation that functioned allosterically to induce cis-autophosphorylation of the receiver kinase. Based on modeling of the hydrophobic spine assembly, we also engineered a constitutively active mutant that was independent of Ras, dimerization, and activation-loop phosphorylation. As N-terminal phosphorylation of BRAF is constitutive, BRAF initially functions to activate CRAF. N-terminal phosphorylation of CRAF was dependent on MEK, suggesting a feedback mechanism and explaining a key difference …
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