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肺表面活性物质蛋白SP-B N端区域内的关键结构-功能决定因素。

Critical structure-function determinants within the N-terminal region of pulmonary surfactant protein SP-B.

作者信息

Serrano Alicia G, Ryan Marnie, Weaver Timothy E, Pérez-Gil Jesús

机构信息

Departamento de Bioquímica y Biología Molecular I, Facultad de Biología, Universidad Complutense, Madrid, Spain.

出版信息

Biophys J. 2006 Jan 1;90(1):238-49. doi: 10.1529/biophysj.105.073403. Epub 2005 Oct 7.

Abstract

Surfactant protein SP-B is absolutely required for the surface activity of pulmonary surfactant and postnatal lung function. The results of a previous study indicated that the N-terminal segment of SP-B, comprising residues 1-9, is specifically required for surface activity, and suggested that prolines 2, 4, and 6 as well as tryptophan 9, may constitute essential structural motifs for protein function. In this work, we assessed the role of these two motifs in promoting the formation and maintenance of surface-active films. Three synthetic peptides were synthesized including a peptide corresponding to the N-terminal 37 amino acids of native SP-B and two variants in which prolines 2, 4, 6, or tryptophan 9 were substituted by alanines. All three synthetic peptides were surface-active, as expected from their amphipathic structure. The peptides were also able to insert into dipalmitoylphosphatidylcholine/palmitoyloleoylphosphatidylglycerol (7:3 w/w ratio) monolayers preformed at pressures >30 mN/m, indicating that they perturb and insert into membranes. Substitution of alanine for tryptophan at position 9 significantly decreased both the rate of adsorption/insertion of the peptide into the interface and reinsertion of surface-active material excluded from the film during successive compression-expansion cycles. Substitution of alanines for prolines at positions 2, 4, and 6 did not produce substantial changes in the rate of adsorption/insertion; however, reinsertion of surface-active material into the expanding interface film was not as effective as in the presence of the nativelike peptide. These results suggest that W9 is critical for optimal interface affinity, whereas prolines may promote a conformation that facilitates rapid insertion of the peptide into phospholipid monolayers compressed to the highest pressures during compression-expansion cycling.

摘要

表面活性蛋白SP - B对于肺表面活性剂的表面活性和出生后肺功能是绝对必需的。先前一项研究的结果表明,SP - B的N端片段(包含第1至9位残基)对于表面活性是特异性必需的,并表明脯氨酸2、4和6以及色氨酸9可能构成蛋白质功能的基本结构基序。在这项工作中,我们评估了这两个基序在促进表面活性膜的形成和维持中的作用。合成了三种合成肽,包括一种对应于天然SP - B N端37个氨基酸的肽以及两种变体,其中脯氨酸2、4、6或色氨酸9被丙氨酸取代。正如预期的那样,由于它们的两亲结构,所有三种合成肽都具有表面活性。这些肽还能够插入在压力>30 mN/m下预先形成的二棕榈酰磷脂酰胆碱/棕榈酰油酰磷脂酰甘油(7:3 w/w比例)单层中,表明它们会扰动并插入膜中。将第9位的色氨酸替换为丙氨酸显著降低了肽吸附/插入界面的速率以及在连续压缩 - 膨胀循环期间从膜中排出的表面活性物质的重新插入速率。将第2、4和6位的脯氨酸替换为丙氨酸在吸附/插入速率上没有产生实质性变化;然而,表面活性物质重新插入膨胀的界面膜中的效果不如存在类似天然肽时有效。这些结果表明,W9对于最佳界面亲和力至关重要,而脯氨酸可能促进一种构象,该构象有助于肽在压缩 - 膨胀循环期间快速插入压缩至最高压力的磷脂单层中。

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