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合成表面活性蛋白类似物。

Synthetic surfactant protein analogues.

作者信息

Johansson J, Gustafsson M, Palmblad M, Zaltash S, Robertson B, Curstedt T

机构信息

Department of Medical Biochemistry and Biophysics, Karolinska Institutet, Stockholm, Sweden.

出版信息

Biol Neonate. 1998 Sep;74 Suppl 1:9-14. doi: 10.1159/000047029.

DOI:10.1159/000047029
PMID:9730586
Abstract

Surfactant preparations for the treatment of respiratory distress syndrome (RDS) that contain phospholipids and small amounts of the two hydrophobic proteins, SP-B and SP-C, are presently obtained from animal lungs. Since structural information about SP-B and SP-C is available, it appears possible to design analogues that can replace the native proteins in synthetic surfactants. SP-C contains a single helix, but analogues with the poly-Val sequence of the native molecule do not fold into a native-like alpha-helical conformation. However, replacement of all Val with Leu yields efficient folding into a helical structure and Leu-based SP-C analogues effectively accelerate spreading of surfactant lipids and exhibit some physiological activity in animal models of RDS. The inferior in vivo activity of synthetic surfactants containing SP-C only compared to that of surfactant preparations derived from natural sources may be caused by a lack of covalently linked palmitoyl groups in the analogues and/or absence of SP-B. SP-B is significantly larger than SP-C and has a tertiary fold of several amphipathic helices in a dimeric structure. A single simplified amphipathic helical peptide containing only Leu and Lys does not mimic the surface properties of SP-B in vitro. These circumstances make the design of SP-B analogues from solely structural considerations less likely to be successful than in the case of SP-C.

摘要

目前用于治疗呼吸窘迫综合征(RDS)的表面活性剂制剂含有磷脂以及少量两种疏水蛋白,即表面活性蛋白B(SP-B)和表面活性蛋白C(SP-C),这些制剂是从动物肺中获取的。由于已有关于SP-B和SP-C的结构信息,因此似乎有可能设计出能够替代合成表面活性剂中天然蛋白的类似物。SP-C包含一个单螺旋结构,但具有天然分子多聚缬氨酸序列的类似物不会折叠成类似天然的α-螺旋构象。然而,将所有缬氨酸替换为亮氨酸可使其有效折叠成螺旋结构,且基于亮氨酸的SP-C类似物能有效加速表面活性剂脂质的铺展,并在RDS动物模型中表现出一定的生理活性。与天然来源的表面活性剂制剂相比,仅含SP-C的合成表面活性剂在体内活性较差,这可能是由于类似物中缺乏共价连接的棕榈酰基团和/或缺少SP-B。SP-B比SP-C大得多,并且在二聚体结构中有几个两亲性螺旋的三级折叠。仅含有亮氨酸和赖氨酸的单一简化两亲性螺旋肽在体外不能模拟SP-B的表面性质。这些情况使得仅从结构考虑设计SP-B类似物比设计SP-C类似物更难成功。

相似文献

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Effect of hydrophobic surfactant proteins SP-B and SP-C on binary phospholipid monolayers: II. Infrared external reflectance-absorption spectroscopy.疏水性表面活性蛋白SP-B和SP-C对二元磷脂单分子层的影响:II. 红外外反射-吸收光谱法
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