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EphA2 跨膜结构域左手二聚体:受体酪氨酸激酶的螺旋包装多样性。

Left-handed dimer of EphA2 transmembrane domain: Helix packing diversity among receptor tyrosine kinases.

机构信息

Shemyakin-Ovchinnikov Institute of Bioorganic Chemistry RAS, Moscow, Russia.

出版信息

Biophys J. 2010 Mar 3;98(5):881-9. doi: 10.1016/j.bpj.2009.11.008.

Abstract

The Eph receptor tyrosine kinases and their membrane-bound ephrin ligands control a diverse array of cell-cell interactions in the developing and adult organisms. During signal transduction across plasma membrane, Eph receptors, like other receptor tyrosine kinases, are involved in lateral dimerization and subsequent oligomerization presumably with proper assembly of their single-span transmembrane domains. Spatial structure of dimeric transmembrane domain of EphA2 receptor embedded into lipid bicelle was obtained by solution NMR, showing a left-handed parallel packing of the transmembrane helices (535-559)(2). The helices interact through the extended heptad repeat motif L(535)X(3)G(539)X(2)A(542)X(3)V(546)X(2)L(549) assisted by intermolecular stacking interactions of aromatic rings of (FF(557))(2), whereas the characteristic tandem GG4-like motif A(536)X(3)G(540)X(3)G(544) is not used, enabling another mode of helix-helix association. Importantly, a similar motif AX(3)GX(3)G as was found is responsible for right-handed dimerization of transmembrane domain of the EphA1 receptor. These findings serve as an instructive example of the diversity of transmembrane domain formation within the same family of protein kinases and seem to favor the assumption that the so-called rotation-coupled activation mechanism may take place during the Eph receptor signaling. A possible role of membrane lipid rafts in relation to Eph transmembrane domain oligomerization and Eph signal transduction was also discussed.

摘要

Eph 受体酪氨酸激酶及其膜结合的 Ephrin 配体在发育和成年生物体中控制着多种多样的细胞-细胞相互作用。在穿过质膜的信号转导过程中,Eph 受体,像其他受体酪氨酸激酶一样,参与了侧二聚化,随后可能是其单一跨膜结构域的寡聚化。通过溶液 NMR 获得了嵌入脂质双层体中的 EphA2 受体二聚体跨膜结构域的空间结构,显示出跨膜螺旋(535-559)(2)的左手平行堆积。螺旋通过扩展的七肽重复基序 L(535)X(3)G(539)X(2)A(542)X(3)V(546)X(2)L(549)相互作用,由(FF(557))(2)的芳环分子间堆积相互作用辅助,而特征性串联 GG4 样基序 A(536)X(3)G(540)X(3)G(544)未被使用,从而实现了另一种螺旋-螺旋缔合模式。重要的是,发现的类似基序 AX(3)GX(3)G 负责 EphA1 受体跨膜结构域的右手二聚化。这些发现为同一蛋白激酶家族内跨膜结构域形成的多样性提供了一个有益的范例,并似乎支持了所谓的旋转偶联激活机制可能发生在 Eph 受体信号转导过程中的假设。还讨论了膜脂筏与 Eph 跨膜结构域寡聚化和 Eph 信号转导的可能关系。

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