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首页> 外文期刊>Journal of Molecular Biology >Structure-based Analysis of GPCR Function: Conformational Adaptation of both Agonist and Receptor upon Leukotriene B(4) Binding to Recombinant BLT1.
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Structure-based Analysis of GPCR Function: Conformational Adaptation of both Agonist and Receptor upon Leukotriene B(4) Binding to Recombinant BLT1.

机译:GPCR功能的基于结构的分析:激动剂和受体在白三烯B(4)结合重组BLT1上的构象适应。

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摘要

We produced the human leukotriene B(4) (LTB(4)) receptor BLT1, a G-protein-coupled receptor, in Escherichia coli with yields that are sufficient for the first structural characterization of this receptor in solution. Overexpression was achieved through codon optimization and the search for optimal refolding conditions of BLT1 recovered from inclusion bodies. The detergent-solubilized receptor displays a 3D-fold compatible with a seven transmembrane (TM) domain with ca 50% alpha-helix and an essential disulfide bridge (circular dichroism evidence); it binds LTB(4) with K(a)=7.8(+/-0.2)x10(8)M(-1) and a stoichiometric ratio of 0.98(+/-0.02). Antagonistic effects were investigated using a synthetic molecule that shares common structural features with LTB(4). We report evidence that both partners, LTB(4) and BLT1, undergo a rearrangement of their respective conformations upon complex formation: (i) a departure from planarity of the LTB(4) conjugated triene moiety; (ii) a change in the environment of Trp234(TM-VI helix) and in the exposure of the cytoplasmic region of this transmembrane helix.
机译:我们在大肠杆菌中生产了人类白三烯B(4)(LTB(4))受体BLT1(一种G蛋白偶联受体),其产量足以解决该受体在溶液中的第一个结构特征。通过密码子优化和寻找从包涵体中回收的BLT1的最佳重折叠条件来实现过表达。洗涤剂溶解的受体显示出与具有约50%α-螺旋和必不可少的二硫键的七个跨膜(TM)域兼容的3D折叠(圆形二色性证据);它结合LTB(4)与K(a)= 7.8(+/- 0.2)x10(8)M(-1)和化学计量比为0.98(+/- 0.02)。使用与LTB(4)共享共同结构特征的合成分子研究了拮抗作用。我们报告的证据表明,两个伙伴,LTB(4)和BLT1,在复杂形成时都经历了各自构象的重排:(i)偏离LTB(4)共轭三烯部分的平面性; (ii)Trp234(TM-VI螺旋)的环境和该跨膜螺旋的胞质区暴露的变化。

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