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与不同长度的TCRζ片段结合的SIVmac239 Nef核心结构域的正交晶体中的假准面孪晶和非晶体学对称性。

Pseudo-merohedral twinning and noncrystallographic symmetry in orthorhombic crystals of SIVmac239 Nef core domain bound to different-length TCRzeta fragments.

作者信息

Kim Walter M, Sigalov Alexander B, Stern Lawrence J

机构信息

University of Massachusetts Medical School, USA.

出版信息

Acta Crystallogr D Biol Crystallogr. 2010 Feb;66(Pt 2):163-75. doi: 10.1107/S090744490904880X. Epub 2010 Jan 22.

Abstract

HIV/SIV Nef mediates many cellular processes through interactions with various cytoplasmic and membrane-associated host proteins, including the signalling zeta subunit of the T-cell receptor (TCRzeta). Here, the crystallization strategy, methods and refinement procedures used to solve the structures of the core domain of the SIVmac239 isolate of Nef (Nef(core)) in complex with two different TCRzeta fragments are described. The structure of SIVmac239 Nef(core) bound to the longer TCRzeta polypeptide (Leu51-Asp93) was determined to 3.7 A resolution (R(work) = 28.7%) in the tetragonal space group P4(3)2(1)2. The structure of SIVmac239 Nef(core) in complex with the shorter TCRzeta polypeptide (Ala63-Arg80) was determined to 2.05 A resolution (R(work) = 17.0%), but only after the detection of nearly perfect pseudo-merohedral crystal twinning and proper assignment of the orthorhombic space group P2(1)2(1)2(1). The reduction in crystal space-group symmetry induced by the truncated TCRzeta polypeptide appears to be caused by the rearrangement of crystal-contact hydrogen-bonding networks and the substitution of crystallographic symmetry operations by similar noncrystallographic symmetry (NCS) operations. The combination of NCS rotations that were nearly parallel to the twin operation (k, h, -l) and a and b unit-cell parameters that were nearly identical predisposed the P2(1)2(1)2(1) crystal form to pseudo-merohedral twinning.

摘要

HIV/SIV Nef通过与多种细胞质和膜相关的宿主蛋白相互作用来介导许多细胞过程,这些宿主蛋白包括T细胞受体(TCRzeta)的信号ζ亚基。本文描述了用于解析与两个不同TCRzeta片段复合的SIVmac239分离株Nef的核心结构域(Nef(core))结构的结晶策略、方法和优化程序。与较长的TCRzeta多肽(Leu51 - Asp93)结合的SIVmac239 Nef(core)结构在四方空间群P4(3)2(1)2中分辨率达到3.7 Å(R(work) = 28.7%)。与较短的TCRzeta多肽(Ala63 - Arg80)复合的SIVmac239 Nef(core)结构分辨率达到2.05 Å(R(work) = 17.0%),但这是在检测到近乎完美的假单形晶体孪晶并正确确定正交空间群P2(1)2(1)2(1)之后。由截短的TCRzeta多肽引起的晶体空间群对称性降低似乎是由晶体接触氢键网络的重排以及用相似的非晶体学对称性(NCS)操作替代晶体学对称操作所导致的。几乎与孪晶操作(k,h,-l)平行的NCS旋转以及几乎相同的a和b晶胞参数的组合使P2(1)2(1)2(1)晶体形式易于出现假单形孪晶。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b2c3/2815668/a96bda19e6db/d-66-00163-fig1.jpg

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