Moncalián Gabriel, Cárdenes Nayra, Deribe Yonathan Lissanu, Spínola-Amilibia Mercedes, Dikic Ivan, Bravo Jerónimo
Signal Transduction Group, Structural Biology and Biocomputing Programme, Centro Nacional de Investigaciones Oncológicas, Melchor Fernández Almagro 3, E-28029 Madrid, Spain.
J Biol Chem. 2006 Dec 15;281(50):38845-53. doi: 10.1074/jbc.M606411200. Epub 2006 Oct 3.
The CIN85/CMS (human homologs of mouse SH3KBP1/CD2AP) family of endocytic adaptor proteins has the ability to engage multiple effectors and couple cargo trafficking with the cytoskeleton. CIN85 and CMS (Cas ligand with multiple Src homology 3 (SH3) domains) facilitate the formation of large multiprotein complexes required for an efficient internalization of cell surface receptors. It has recently been shown that c-Cbl/Cbl-b could mediate the formation of a ternary complex between one c-Cbl/Cbl-b molecule and two SH3 domains of CIN85, important for the ability of Cbl to promote epidermal growth factor receptor down-regulation. To further investigate whether multimerization is conserved within the family of adaptor proteins, we have solved the crystal structures of the CMS N-terminal SH3 domain-forming complexes with Cbl-b- and CD2-derived peptides. Together with biochemical evidence, the structures support the notion that, despite clear differences in the interaction surface, both Cbl-b and CD2 can mediate multimerization of N-terminal CMS SH3 domains. Detailed analyses on the interacting surfaces also provide the basis for a differential Cbl-b molecular recognition of CMS and CIN85.
内吞衔接蛋白的CIN85/CMS(小鼠SH3KBP1/CD2AP的人类同源物)家族具有结合多种效应器并将货物运输与细胞骨架偶联的能力。CIN85和CMS(具有多个Src同源3(SH3)结构域的Cas配体)促进细胞表面受体有效内化所需的大型多蛋白复合物的形成。最近有研究表明,c-Cbl/Cbl-b可介导一个c-Cbl/Cbl-b分子与CIN85的两个SH3结构域之间三元复合物的形成,这对Cbl促进表皮生长因子受体下调的能力很重要。为了进一步研究多聚化在衔接蛋白家族中是否保守,我们解析了CMS N端SH3结构域与Cbl-b和CD2衍生肽形成复合物的晶体结构。结合生化证据,这些结构支持以下观点:尽管相互作用表面存在明显差异,但Cbl-b和CD2都能介导N端CMS SH3结构域的多聚化。对相互作用表面的详细分析也为Cbl-b对CMS和CIN85的差异分子识别提供了基础。
