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首页> 外文期刊>Histochemistry and cell biology >Regulation of the NADPH-oxidase complex of phagocytic leukocytes. Recent insights from structural biology, molecular genetics, and microscopy.
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Regulation of the NADPH-oxidase complex of phagocytic leukocytes. Recent insights from structural biology, molecular genetics, and microscopy.

机译:吞噬白细胞NADPH-氧化酶复合物的调节。来自结构生物学,分子遗传学和显微镜的最新见解。

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摘要

The NADPH-oxidase complex is a multisubunit enzyme complex that catalyzes the formation of superoxide (O2-) by phagocytic leukocytes. This paper reviews some of the major advances in understanding the assembly and regulation of this enzyme system that have occurred during the past decade. For example, novel domains/motifs have been identified in p47-phox (PX and super SH3 domains) and p67-phox (tetratricopeptide repeat motifs). X-ray crystallography and NMR spectroscopy have provided detailed structural data on these domains and how p47-phox and p67-phox interact with p22-phox and activated Rac, respectively. Site-directed mutagenesis and knockout experiments have identified the critical phosphorylation sites in p47-phox, revealed an "activation domain" in p67-phox, and demonstrated that a specific pathway exists for activating Rac to participate in oxidase assembly/activation. Cytochemistry and immunofluorescence microscopy have provided new insights into the assembly of the oxidase and reveal a level of complexity not previously appreciated.
机译:NADPH-氧化酶复合物是一种多亚基酶复合物,可催化吞噬白细胞形成超氧化物(O2-)。本文回顾了过去十年中在了解该酶系统的组装和调控方面的一些重大进展。例如,已在p47-phox(PX和超级SH3域)和p67-phox(四肽重复基序)中鉴定出新的结构域/基序。 X射线晶体学和NMR光谱学提供了有关这些域的详细结构数据,以及p47-phox和p67-phox如何分别与p22-phox和活化的Rac相互作用。定点诱变和敲除实验已经鉴定出p47-phox中的关键磷酸化位点,揭示了p67-phox中的“激活域”,并证明存在激活Rac参与氧化酶组装/激活的特定途径。细胞化学和免疫荧光显微镜检查为氧化酶的组装提供了新的见识,并揭示了以前没有意识到的复杂程度。

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