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差示扫描量热法表明,人防御素HNP-2与生物膜模拟系统发生特异性相互作用。

Differential scanning microcalorimetry indicates that human defensin, HNP-2, interacts specifically with biomembrane mimetic systems.

作者信息

Lohner K, Latal A, Lehrer R I, Ganz T

机构信息

Institut für Biophysik und Röntgenstrukturforschung, Osterreichische Akademie der Wissenschaften, Graz, Austria.

出版信息

Biochemistry. 1997 Feb 11;36(6):1525-31. doi: 10.1021/bi961300p.

Abstract

alpha-Defensins are antimicrobial peptides with 29-35 amino acid residues and cysteine-stabilized amphiphilic, triple-stranded beta-sheet structures. We used high-precision differential scanning microcalorimetry to investigate the effects of a human neutrophil alpha-defensin, HNP-2, on the phase behavior of model membranes mimicking bacterial and erythrocyte cell membranes. In the presence of this positively charged peptide, the phase behavior of liposomes containing negatively charged phosphatidylglycerol was markedly altered even at a high lipid-to-peptide molar ratio of 500:1. Addition of HNP-2 to liposomes mimicking bacterial membranes (mixtures of dipalmitoylphosphatidylglycerol and -ethanolamine) resulted in phase separation owing to some domains being peptide-poor and others peptide-rich. The latter are characterized by an increase of the main transition temperature, most likely arising from electric shielding of the phospholipid headgroups by the peptide. On the other hand, HNP-2 did not affect the phase behavior of membranes mimicking erythrocyte membranes (equimolar mixtures of dipalmitoylphosphatidylcholine and sphingomyelin) as well as the pure single components. This is in contrast to melittin, which significantly affected the phase behavior of choline phospholipids in accordance with its unspecific lytic activity. These results support the hypothesis of preferential interaction of defensins with negatively charged membrane cell surfaces, a common feature of bacterial cell membranes, and demonstrate that HNP-2 discriminates between model membrane systems mimicking prokaryotic and eukaryotic cell membranes.

摘要

α-防御素是一种抗菌肽,含有29 - 35个氨基酸残基,具有半胱氨酸稳定的两亲性三链β-折叠结构。我们使用高精度差示扫描量热法研究了一种人类中性粒细胞α-防御素HNP-2对模拟细菌和红细胞细胞膜的模型膜相行为的影响。在这种带正电荷的肽存在下,即使在脂质与肽的摩尔比高达500:1时,含有带负电荷磷脂酰甘油的脂质体的相行为也会发生显著改变。将HNP-2添加到模拟细菌膜的脂质体(二棕榈酰磷脂酰甘油和二棕榈酰磷脂酰乙醇胺的混合物)中会导致相分离,这是由于一些区域肽含量低而其他区域肽含量高。后者的特征是主要转变温度升高,这很可能是由于肽对磷脂头部基团的电屏蔽作用。另一方面,HNP-2不会影响模拟红细胞膜的膜(二棕榈酰磷脂酰胆碱和鞘磷脂的等摩尔混合物)以及纯单一成分的相行为。这与蜂毒肽形成对比,蜂毒肽根据其非特异性裂解活性显著影响胆碱磷脂的相行为。这些结果支持了防御素与带负电荷的细胞膜表面优先相互作用的假说,这是细菌细胞膜的一个共同特征,并表明HNP-2能够区分模拟原核和真核细胞膜的模型膜系统。

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