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溶细胞剂、细胞通透性和单层可透性。

Lytic agents, cell permeability, and monolayer penetrability.

机构信息

Department of Microbiology, New York University School of Medicine, New York 10016.

出版信息

J Gen Physiol. 1968 Jul 1;52(1):227-52.

Abstract

Cell lysis induced by lytic agents is the terminal phase of a series of events leading to membrane disorganization and breadkdown with the release of cellular macromolecules. Permeability changes following exposure to lytic systems may range from selective effects on ion fluxes to gross membrane damage and cell leakage. Lysis can be conceived as an interfacial phenomenon, and the action of surface-active agents on erythrocytes has provided a model in which to investigate relationships between hemolysis and chemical structure, ionic charge, surface tension lowering, and ability to penetrate monolayers of membrane lipid components. Evidence suggests that lysis follows the attainment of surface pressures exceeding a "critical collapse" level and could involve membrane cholesterol or phospholipid. Similarities of chemical composition of membranes from various cell types could account for lytic responses observed on interaction with surface-active agents. Cell membranes usually contain about 20-30 % lipid and 50-75 % protein. One or two major phospholipids are present in all cell membranes, but sterols are not detectable in bacterial membranes other than those of the Mycoplasma group. The rigid cell wall in bacteria has an important bearing on their response to treatment with lytic agents. Removal of the wall renders the protoplast membrane sensitive to rapid lysis with surfactants. Isolated membranes of erythrocytes and bacteria are rapidly dissociated by surface-active agents. Products of dissociation of bacterial membranes have uniform behavior in the ultracentrifuge (sedimentation coefficients 2-3S). Dissociation of membrane proteins from lipids and the isolation and characterization of these proteins will provide a basis for investigating the specificity of interaction of lytic agents with biomembranes.

摘要

溶细胞试剂诱导的细胞裂解是一系列导致膜结构紊乱和破裂并释放细胞大分子的事件的终末阶段。暴露于溶细胞系统后,通透性的改变范围可以从对离子流的选择性影响到严重的膜损伤和细胞渗漏。裂解可以被设想为一种界面现象,表面活性剂对红细胞的作用提供了一个模型,用于研究溶血与化学结构、离子电荷、表面张力降低以及穿透膜脂质成分单层的能力之间的关系。有证据表明,在达到超过“临界崩溃”水平的表面压力后,就会发生裂解,并且可能涉及膜胆固醇或磷脂。由于与表面活性剂相互作用而观察到的裂解反应,不同细胞类型的膜在化学成分上具有相似性,这可以得到解释。细胞膜通常含有约 20-30%的脂质和 50-75%的蛋白质。所有细胞膜中都存在一种或两种主要的磷脂,但甾醇在除支原体组以外的细菌膜中是不可检测到的。细菌的刚性细胞壁对其与溶细胞试剂的反应有重要影响。去除细胞壁会使原生质膜对表面活性剂的快速裂解变得敏感。红细胞和细菌的分离膜会被表面活性剂迅速解离。细菌膜的解离产物在超速离心机中具有一致的行为(沉降系数 2-3S)。膜蛋白从脂质中解离出来,以及这些蛋白质的分离和特性鉴定,将为研究溶细胞试剂与生物膜相互作用的特异性提供基础。

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