E-RAS is a member of the RAS family specifically expressed in embryonic stem cells, gastric tumors, and hepatic stellate cells. Unlike classical RAS isoforms (H-, N-, and K-RAS4B), E-RAS has, in addition to striking and remarkable sequence deviations, an extended 38-amino acid-long unique N-terminal region with still unknown functions. We investigated the molecular mechanism of E-RAS regulation and function with respect to its sequence and structural features. We found that N-terminal extension of E-RAS is important for E-RAS signaling activity. E-RAS protein most remarkably revealed a different mode of effector interaction as compared with H-RAS, which correlates with deviations in the effector-binding site of E-RAS. Of all these residues, tryptophan 79 (arginine 41 in H-RAS), in the interswitch region, modulates the effector selectivity of RAS proteins from H-RAS to E-RAS features.
The Function of Embryonic Stem Cell-expressed RAS (E-RAS), a Unique RAS Family Member, Correlates with Its Additional Motifs and Its Structural Properties.
胚胎干细胞表达的 RAS (E-RAS) 是 RAS 家族中独特的成员,其功能与其附加基序和结构特性相关
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作者:Nakhaei-Rad Saeideh, Nakhaeizadeh Hossein, Kordes Claus, Cirstea Ion C, Schmick Malte, Dvorsky Radovan, Bastiaens Philippe I H, Häussinger Dieter, Ahmadian Mohammad Reza
| 期刊: | Journal of Biological Chemistry | 影响因子: | 3.900 |
| 时间: | 2015 | 起止号: | 2015 Jun 19; 290(25):15892-15903 |
| doi: | 10.1074/jbc.M115.640607 | 研究方向: | 发育与干细胞、细胞生物学 |
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