From the School of Biological Sciences, Nanyang Technological University, 60 Nanyang Drive, 637551 Singapore.
J Biol Chem. 2014 May 2;289(18):12535-49. doi: 10.1074/jbc.M114.560094. Epub 2014 Mar 25.
Coronavirus envelope (CoV E) proteins are ∼100-residue polypeptides with at least one channel-forming α-helical transmembrane (TM) domain. The extramembrane C-terminal tail contains a completely conserved proline, at the center of a predicted β-coil-β motif. This hydrophobic motif has been reported to constitute a Golgi-targeting signal or a second TM domain. However, no structural data for this or other extramembrane domains in CoV E proteins is available. Herein, we show that the E protein in the severe acute respiratory syndrome virus has only one TM domain in micelles, whereas the predicted β-coil-β motif forms a short membrane-bound α-helix connected by a disordered loop to the TM domain. However, complementary results suggest that this motif is potentially poised for conformational change or in dynamic exchange with other conformations.
冠状病毒包膜(CoV E)蛋白是约 100 个残基的多肽,至少具有一个形成通道的α-螺旋跨膜(TM)结构域。膜外 C 端尾部含有一个完全保守的脯氨酸,位于预测的β-发夹-β基序的中心。据报道,这个疏水性基序构成了高尔基体靶向信号或第二个 TM 结构域。然而,目前还没有关于 CoV E 蛋白中其他膜外结构域的结构数据。在此,我们表明严重急性呼吸系统综合症病毒(SARS-CoV)的 E 蛋白在胶束中只有一个 TM 结构域,而预测的β-发夹-β基序形成一个短的膜结合α-螺旋,通过无序环与 TM 结构域相连。然而,互补的结果表明,这个基序可能处于构象变化的准备状态,或者与其他构象处于动态交换中。
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