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不同大小的聚(L-赖氨酸)诱导心磷脂脂质体双层稳定化的分子机制

Molecular aspects of the bilayer stabilization induced by poly(L-lysines) of varying size in cardiolipin liposomes.

作者信息

de Kruijff B, Rietveld A, Telders N, Vaandrager B

出版信息

Biochim Biophys Acta. 1985 Nov 7;820(2):295-304. doi: 10.1016/0005-2736(85)90124-5.

Abstract

The interaction between poly(L-lysines) of varying size with cardiolipin was investigated via binding assays, X-ray diffraction, freeze-fracture electron microscopy, and 31P- and 13C-NMR. Binding of polylysines to the lipid only occurred when three or more lysine residues were present per molecule. The strength of the binding was highly dependent on the polymerization degree, suggesting a cooperative interaction of the lysines within the polymer. Upon binding, a structural reorganization of the lipids takes place, resulting in a closely packed multilamellar system in which the polylysines are sandwiched in between subsequent bilayers. Acyl chain motion is reduced in these liquid-crystalline peptide-lipid complexes. From competition experiments with Ca2+ it could be concluded that when the affinity of the polylysine for cardiolipin was much larger than that of Ca2+, a lamellar polylysine-lipid complex was formed, irrespective of whether an excess of Ca2+ was added prior to or after the polypeptide. When the affinity of the polylysine for cardiolipin was less or of the same order as that of Ca2+, the lipid was organized in the hexagonal HII phase in the presence of Ca2+. These results are discussed in the light of the peptide specificity of bilayer (de)stabilization in cardiolipin model membranes.

摘要

通过结合测定、X射线衍射、冷冻断裂电子显微镜以及31P和13C核磁共振,研究了不同大小的聚(L-赖氨酸)与心磷脂之间的相互作用。只有当每个分子中存在三个或更多赖氨酸残基时,聚赖氨酸才会与脂质发生结合。结合强度高度依赖于聚合度,这表明聚合物中的赖氨酸存在协同相互作用。结合后,脂质会发生结构重组,形成紧密堆积的多层系统,其中聚赖氨酸夹在随后的双层之间。在这些液晶肽-脂质复合物中,酰基链的运动减少。通过与Ca2+的竞争实验可以得出结论,当聚赖氨酸对心磷脂的亲和力远大于Ca2+对心磷脂的亲和力时,无论在多肽之前还是之后添加过量的Ca2+,都会形成层状聚赖氨酸-脂质复合物。当聚赖氨酸对心磷脂的亲和力小于或与Ca2+对心磷脂的亲和力相当时,在Ca2+存在的情况下,脂质会形成六方HII相。根据心磷脂模型膜中双层(去)稳定化的肽特异性对这些结果进行了讨论。

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