炭疽致死因子对底物和抑制剂选择性的结构基础。

The structural basis for substrate and inhibitor selectivity of the anthrax lethal factor.

作者信息

Turk Benjamin E, Wong Thiang Yian, Schwarzenbacher Robert, Jarrell Emily T, Leppla Stephen H, Collier R John, Liddington Robert C, Cantley Lewis C

机构信息

Division of Signal Transduction, Department of Medicine, Beth Israel Deaconess Medical Center, and Harvard Medical School, 330 Brookline Avenue, Boston, Massachusetts 02215, USA.

出版信息

Nat Struct Mol Biol. 2004 Jan;11(1):60-6. doi: 10.1038/nsmb708. Epub 2003 Dec 29.

DOI:10.1038/nsmb708

PMID:14718924

Abstract

Recent events have created an urgent need for new therapeutic strategies to treat anthrax. We have applied a mixture-based peptide library approach to rapidly determine the optimal peptide substrate for the anthrax lethal factor (LF), a metalloproteinase with an important role in the pathogenesis of the disease. Using this approach we have identified peptide analogs that inhibit the enzyme in vitro and that protect cultured macrophages from LF-mediated cytolysis. The crystal structures of LF bound to an optimized peptide substrate and to peptide-based inhibitors provide a rationale for the observed selectivity and may be exploited in the design of future generations of LF inhibitors.

摘要

近期发生的事件迫切需要新的治疗策略来治疗炭疽病。我们采用了基于混合物的肽库方法，以快速确定炭疽致死因子（LF）的最佳肽底物，LF是一种金属蛋白酶，在该疾病的发病机制中起重要作用。使用这种方法，我们已经鉴定出在体外抑制该酶并保护培养的巨噬细胞免受LF介导的细胞溶解的肽类似物。与优化的肽底物和基于肽的抑制剂结合的LF晶体结构为观察到的选择性提供了理论依据，并可用于设计下一代LF抑制剂。

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炭疽致死因子对底物和抑制剂选择性的结构基础。

The structural basis for substrate and inhibitor selectivity of the anthrax lethal factor.

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