Structure of the H107R variant of the extracellular domain of mouse NKR-P1A at 2.3 Å resolution

机译：小鼠NKR-P1A细胞外域H107R变体的结构分辨率为2.3Å

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摘要

The structure of the H107R variant of the extracellular domain of the mouse natural killer cell receptor NKR-P1A has been determined by X-ray diffraction at 2.3 Å resolution from a merohedrally twinned crystal. Unlike the structure of the wild-type receptor in space group I4122 with a single chain per asymmetric unit, the crystals of the variant belonged to space group I41 with a dimer in the asymmetric unit. Different degrees of merohedral twinning were detected in five data sets collected from different crystals. The mutation does not have a significant impact on the overall structure, but led to the binding of an additional phosphate ion at the interface of the molecules.

机译：小鼠自然杀伤细胞受体NKR-P1A胞外域的H107R变体的结构已通过X射线衍射从多面体孪晶上以2.3Å的分辨率确定。与每个不对称单元带有单链的空间群I4122中野生型受体的结构不同，该变体的晶体属于不对称单元中具有二聚体的空间群I41。在从不同晶体收集的五个数据集中检测到不同程度的多面体孪晶。突变不会对整体结构产生重大影响，但会导致分子界面处的另一个磷酸根离子结合。

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期刊名称 Acta Crystallographica Section F: Structural Biology and Crystallization Communications
作者
Petr Kolenko; Daniel Rozbeský; Ondřej Vaněk; Karel Bezouška; Jindřich Hašek; Jan Dohnálek;
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作者单位

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年(卷),期 2011(67),Pt 12
年度 2011
页码 1519–1523
总页数 5
原文格式 PDF
正文语种
中图分类分子生物学;生化遗传学;生化药理学;生物物理学;
关键词
NKR-P1A merohedral twinning mutation;

机译：NKR-P1A;多面体孪生;突变;

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专利

1. Model of the extracellular domain of the human alpha 7 nAChR based on the crystal structure of the mouse alpha 1 nAChR extracellular domain [J] . Konstantakaki M, Tzartos SJ, Pottlas K, Journal of molecular graphics & modelling . 2008,第8期

机译：基于小鼠alpha 1 nAChR细胞外结构域的晶体结构的人alpha 7 nAChR细胞外结构域模型
2. PHAGE P22 TAILSPIKE PROTEIN - CRYSTAL STRUCTURE OF THE HEAD-BINDING DOMAIN AT 2.3 ANGSTROM, FULLY REFINED STRUCTURE OF THE ENDORHAMNOSIDASE AT 1.56 ANGSTROM RESOLUTION, AND THE MOLECULAR BASIS OF O-ANTIGEN RECOGNITION AND CLEAVAGE [J] . Steinbacher S., Baxa U., Budisa N., Journal of Molecular Biology . 1997,第4期

机译：噬菌体蛋白P22阶段-头结合域在2.3埃时的晶体结构，内啡肽酶的精细结构在1.56埃时的解析度以及O-抗原识别和裂解的分子基础
3. The Crystal Structure Of Mouse Vdac1 At 2.3 A Resolution Reveals Mechanistic Insights Into Metabolite Gating [J] . Rachna Ujwal, Duilio Cascio, Jacques-Philippe Colletier, Proceedings of the National Academy of Sciences of the United States of America . 2008,第46期

机译：鼠标Vdac1在2.3分辨率下的晶体结构揭示了对代谢物门控的机理见解
4. A Study of Adhesion and Improvement of Adhesion Energy Using Hybrid Low-k (porous-PAr/ porous-SiOC(k=2.3/2.3)) Structures with Multi-layered Cu Interconnects for 45-nm Node Devices [C] . Usami, T., Maruyama, . 2007

机译：45纳米节点器件使用多层铜互连的低k（多孔PAr /多孔SiOC（k = 2.3 / 2.3））混合结构的粘合和粘合能提高的研究
5. Characterization of Native Chromatin Structures Respectively Containing the Methyl-CpG Binding Domain Protein MeCP2 and the Histone Variant H2A.Z. [D] . Thambirajah, Anita Annajothi. 2010

机译：分别包含甲基CpG结合域蛋白MeCP2和组蛋白变异H2A.Z的天然染色质结构的表征。
6. Phage P22 tailspike protein: crystal structure of the head-binding domain at 2.3 Å fully refined structure of the endorhamnosidase at 1.56 Å resolution and the molecular basis of O-antigen recognition and cleavage [O] . Stefan Steinbacher, Stefan Miller, Ulrich Baxa, -1

机译：噬菌体P22尾钉蛋白：头部结合结构域的晶体结构为2.3Å内啡肽酶的完全精制结构的分辨率为1.56Å以及O抗原识别和切割的分子基础
7. Crystal Structure of the Extracellular Domain of Mouse RANK Ligand at 2.2-Å Resolution [O] . Shuichiro Ito, Kenji Wakabayashi, Osamu Ubukata, 2002

机译：小鼠等级配体的细胞外结构域的晶体结构在2.2-å分辨率下

Structure of the H107R variant of the extracellular domain of mouse NKR-P1A at 2.3 Å resolution

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