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表面活性蛋白A三聚体碳水化合物识别结构域和颈部结构域的晶体结构

Crystal structure of trimeric carbohydrate recognition and neck domains of surfactant protein A.

作者信息

Head James F, Mealy Tanya R, McCormack Francis X, Seaton Barbara A

机构信息

Department of Physiology and Biophysics, Boston University School of Medicine, Boston, Massachusetts 02118, USA.

出版信息

J Biol Chem. 2003 Oct 31;278(44):43254-60. doi: 10.1074/jbc.M305628200. Epub 2003 Aug 11.

Abstract

Surfactant protein A (SP-A), one of four proteins associated with pulmonary surfactant, binds with high affinity to alveolar phospholipid membranes, positioning the protein at the first line of defense against inhaled pathogens. SP-A exhibits both calcium-dependent carbohydrate binding, a characteristic of the collectin family, and specific interactions with lipid membrane components. The crystal structure of the trimeric carbohydrate recognition domain and neck domain of SP-A was solved to 2.1-A resolution with multiwavelength anomalous dispersion phasing from samarium. Two metal binding sites were identified, one in the highly conserved lectin site and the other 8.5 A away. The interdomain carbohydrate recognition domain-neck angle is significantly less in SP-A than in the homologous collectins, surfactant protein D, and mannose-binding protein. This conformational difference may endow the SP-A trimer with a more extensive hydrophobic surface capable of binding lipophilic membrane components. The appearance of this surface suggests a putative binding region for membrane-derived SP-A ligands such as phosphatidylcholine and lipid A, the endotoxic lipid component of bacterial lipopolysaccharide that mediates the potentially lethal effects of Gram-negative bacterial infection.

摘要

表面活性蛋白A(SP-A)是与肺表面活性剂相关的四种蛋白质之一,它以高亲和力与肺泡磷脂膜结合,使该蛋白处于抵御吸入病原体的第一道防线。SP-A既表现出依赖钙的碳水化合物结合特性(这是凝集素家族的特征),又能与脂质膜成分发生特异性相互作用。通过钐的多波长反常散射相位法,将SP-A三聚体的碳水化合物识别结构域和颈部结构域的晶体结构解析到了2.1埃的分辨率。确定了两个金属结合位点,一个在高度保守的凝集素位点,另一个在其8.5埃远处。SP-A中结构域间的碳水化合物识别结构域-颈部夹角明显小于同源凝集素、表面活性蛋白D和甘露糖结合蛋白中的夹角。这种构象差异可能使SP-A三聚体具有更广泛的疏水表面,能够结合亲脂性膜成分。该表面的出现表明存在一个假定的膜衍生SP-A配体结合区域,如磷脂酰胆碱和脂多糖的内毒素脂质成分脂质A,脂质A介导革兰氏阴性菌感染的潜在致死效应。

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