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肺表面活性物质蛋白B(SP-B):结构与功能的关系

Pulmonary surfactant protein B (SP-B): structure-function relationships.

作者信息

Cochrane C G, Revak S D

机构信息

Department of Immunology, Scripps Research Institute, La Jolla, CA 92037.

出版信息

Science. 1991 Oct 25;254(5031):566-8. doi: 10.1126/science.1948032.

Abstract

SP-B is a protein in pulmonary surfactant that is, in greatest part, responsible for resistance to surface tension and prevention of collapse of pulmonary alveoli. Peptides of 21 residues, synthesized following the sequence of SP-B or resembling the hydrophobic and hydrophilic domains of SP-B (such as RLLLLRLLLLRLLLLRLLLLR, R, Arg, and L, Leu), enhanced the abilities of phospholipids to reduce surface tension both in vitro and in vivo. Intermittent positively charged residues were essential for this activity. The SP-B-like peptides were found by tryptophan fluorescence to partition within the phospholipid layer in contact with both polar head groups and acyl side chains. These data, together with findings that the SP-B-related peptides increase inter- and intramolecular order of the phospholipid layer, suggest that SP-B resists surface tension by increasing lateral stability of the phospholipid layer.

摘要

表面活性蛋白B(SP - B)是肺表面活性剂中的一种蛋白质,在很大程度上负责抵抗表面张力并防止肺泡塌陷。按照SP - B的序列合成的或类似于SP - B的疏水和亲水结构域的21个残基的肽(如RLLLLRLLLLRLLLLRLLLLR,R代表精氨酸,L代表亮氨酸),在体外和体内均增强了磷脂降低表面张力的能力。间歇性带正电荷的残基对于此活性至关重要。通过色氨酸荧光发现,类SP - B肽在磷脂层内与极性头部基团和酰基侧链接触的位置进行分配。这些数据,连同与SP - B相关的肽增加磷脂层分子间和分子内有序性的研究结果,表明SP - B通过增加磷脂层的横向稳定性来抵抗表面张力。

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