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通过 X 射线溶液散射实时追踪 Ca ATPase 中间体。

Tracking Ca ATPase intermediates in real time by x-ray solution scattering.

机构信息

Department of Chemistry, Umeå University. Linnaeus Väg 10, 901 87 Umeå, Sweden.

European Synchrotron Radiation Facility, Grenoble, Cedex 38043, BP 220, France.

出版信息

Sci Adv. 2020 Mar 20;6(12):eaaz0981. doi: 10.1126/sciadv.aaz0981. eCollection 2020 Mar.

Abstract

Sarco/endoplasmic reticulum Ca ATPase (SERCA) transporters regulate calcium signaling by active calcium ion reuptake to internal stores. Structural transitions associated with transport have been characterized by x-ray crystallography, but critical intermediates involved in the accessibility switch across the membrane are missing. We combined time-resolved x-ray solution scattering (TR-XSS) experiments and molecular dynamics (MD) simulations for real-time tracking of concerted SERCA reaction cycle dynamics in the native membrane. The equilibrium [Ca]E1 state before laser activation differed in the domain arrangement compared with crystal structures, and following laser-induced release of caged ATP, a 1.5-ms intermediate was formed that showed closure of the cytoplasmic domains typical of E1 states with bound Ca and ATP. A subsequent 13-ms transient state showed a previously unresolved actuator (A) domain arrangement that exposed the ADP-binding site after phosphorylation. Hence, the obtained TR-XSS models determine the relative timing of so-far elusive domain rearrangements in a native environment.

摘要

肌浆/内质网 Ca2+-ATP 酶(SERCA)转运蛋白通过主动将钙离子重摄取到内部储存库来调节钙离子信号转导。通过 X 射线晶体学已经对与运输相关的结构转变进行了描述,但膜通透性开关中涉及的关键中间态仍然缺失。我们结合了时间分辨 X 射线溶液散射(TR-XSS)实验和分子动力学(MD)模拟,实时跟踪天然膜中协同 SERCA 反应循环动力学。与晶体结构相比,在激光激活之前,平衡时的 [Ca]E1 状态在结构域排列上存在差异,并且在激光诱导笼状 ATP 释放后,形成了一个 1.5ms 的中间产物,其表现出与结合 Ca2+和 ATP 的 E1 状态典型的细胞质结构域的闭合。随后的 13ms 瞬态显示了以前未解决的执行器(A)结构域排列,该排列在磷酸化后暴露出 ADP 结合位点。因此,所获得的 TR-XSS 模型确定了在天然环境中迄今为止难以捉摸的结构域重排的相对时间。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d2c3/7083613/c00d17db19dd/aaz0981-F1.jpg

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