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肺表面活性物质蛋白SP - B和SP - C在空气/水界面磷脂单分子层中的外反射吸收红外光谱研究

External reflection absorption infrared spectroscopy study of lung surfactant proteins SP-B and SP-C in phospholipid monolayers at the air/water interface.

作者信息

Pastrana-Rios B, Taneva S, Keough K M, Mautone A J, Mendelsohn R

机构信息

Department of Chemistry, Rutgers University, Newark College of Arts and Science, New Jersey 07102, USA.

出版信息

Biophys J. 1995 Dec;69(6):2531-40. doi: 10.1016/S0006-3495(95)80124-4.

Abstract

The interactions of the hydrophobic pulmonary surfactant proteins SP-B and SP-C with 1,2-dipalmitoylphosphatidylcholine in mixed, spread monolayer films have been studied in situ at the air/water interface with the technique of external reflection absorption infrared spectroscopy (IRRAS). SP-C has a mostly alpha-helical secondary structure both in the pure state and in the presence of lipids, whereas SP-B secondary structure is a mixture of alpha-helical and disordered forms. When films of SP-B/1,2-dipalmitoylphosphatidylcholine are compressed to surface pressures (pi) greater than approximately 40-43 mN/m, the protein is partially (15-35%) excluded from the surface, as measured by intensity ratios of the peptide bond amide l/lipid C==O stretching vibrations. The extent of exclusion increases as the protein/lipid ratio in the film increases. In contrast, SP-C either remains at the surface at high pressures or leaves accompanied by lipids. The amide l peak of SP-C becomes asymmetric as a result of the formation of intermolecular sheet structures (1615-1630 cm-1) suggestive of peptide aggregation. The power of the IRRAS experiment for determination of film composition and molecular structure, i.e., as a direct test of the squeeze-out hypothesis of pulmonary surfactant function, is evident from this work.

摘要

利用外反射吸收红外光谱(IRRAS)技术,在空气/水界面原位研究了疏水性肺表面活性物质蛋白SP-B和SP-C与1,2-二棕榈酰磷脂酰胆碱在混合铺展单分子层膜中的相互作用。SP-C在纯态和存在脂质的情况下,二级结构大多为α-螺旋,而SP-B的二级结构是α-螺旋和无序形式的混合物。当SP-B/1,2-二棕榈酰磷脂酰胆碱膜被压缩到表面压力(π)大于约40-43 mN/m时,通过肽键酰胺I/脂质C=O伸缩振动的强度比测量,蛋白质有部分(15-35%)被排除在表面之外。随着膜中蛋白质/脂质比例的增加,排除程度也增加。相比之下,SP-C在高压下要么留在表面,要么伴随着脂质离开。由于分子间片状结构(1615-1630 cm-1)的形成,提示肽聚集,SP-C的酰胺I峰变得不对称。IRRAS实验在确定膜组成和分子结构方面的能力,即作为肺表面活性物质功能挤出假说的直接测试,从这项工作中可见一斑。

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