Hoess A, Watson S, Siber G R, Liddington R
Laboratory of X-Ray Crystallography, Dana-Farber Cancer Institute, Boston, MA.
EMBO J. 1993 Sep;12(9):3351-6. doi: 10.1002/j.1460-2075.1993.tb06008.x.
Lipopolysaccharide (LPS), or endotoxin, is the major mediator of septic shock, a serious complication of Gram-negative bacterial infections in humans. Molecules that bind LPS and neutralize its biological effects or enhance its clearance could have important clinical applications. Limulus anti-LPS factor (LALF) binds LPS tightly, and, in animal models, reduces mortality when administered before or after LPS challenge or bacterial infection. Here we present the high resolution structure of a recombinant LALF. It has a single domain consisting of three alpha-helices packed against a four-stranded beta-sheet. The wedge-shaped molecule has a striking charge distribution and amphipathicity that suggest how it can insert into membranes. The binding site for LPS probably involves an extended amphipathic loop, and we propose that two mammalian LPS-binding proteins will have a similar loop. The amphipathic loop structure may be used in the design of molecules with therapeutic properties against septic shock.
脂多糖(LPS),即内毒素,是脓毒症休克的主要介质,脓毒症休克是人类革兰氏阴性菌感染的一种严重并发症。能够结合LPS并中和其生物学效应或增强其清除的分子可能具有重要的临床应用价值。鲎抗LPS因子(LALF)能紧密结合LPS,并且在动物模型中,在LPS攻击或细菌感染之前或之后给药可降低死亡率。在此我们展示了重组LALF的高分辨率结构。它有一个单一结构域,由三个α螺旋与一个四链β折叠堆积而成。这个楔形分子具有显著的电荷分布和两亲性,这表明了它如何插入细胞膜。LPS的结合位点可能涉及一个延伸的两亲性环,并且我们推测两种哺乳动物LPS结合蛋白会有类似的环。两亲性环结构可用于设计具有抗脓毒症休克治疗特性的分子。
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