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聚六亚甲基胍盐酸盐对平滑肌细胞、神经组织和大鼠血小板的膜作用:生物杀灭剂驱动磷脂双层形成孔道。

Membrane action of polyhexamethylene guanidine hydrochloride revealed on smooth muscle cells, nerve tissue and rat blood platelets: A biocide driven pore-formation in phospholipid bilayers.

机构信息

Department of Neurochemistry, Palladin Institute of Biochemistry, NAS of Ukraine, Leontovich Str.,9, 01030 Kyiv, Ukraine.

Department of Muscle Biochemistry, Palladin Institute of Biochemistry, NAS of Ukraine, Leontovich Str., 9, 01030 Kyiv, Ukraine.

出版信息

Toxicol In Vitro. 2019 Oct;60:389-399. doi: 10.1016/j.tiv.2019.06.008. Epub 2019 Jun 11.

Abstract

A well-known cationic biocide of guanidine polymer family, polyhexamethylene guanidine hydrochloride (PHMG) has been tested against smooth muscle cells isolated from swine myometrium, synaptosomes of rat brain nerve terminals and rat blood platelets for the membrane action. It was established that PHMG blocked the activity of Na,K-ATPase of smooth muscle cells plasma membrane by 82.2 ± 0.9% at a concentration of 7 ppm, whilst a dose-dependent depolarization of synaptosomes and platelets became appreciable at 100-500 ppm. Comparative studies by the methods of mass spectrometry (MALDI-TOF and PDMS-TOF), viscosimetry, dynamic light scattering and model phospholipid membranes revealed PHMG oligomers with various number of repeat units (8-16) that formed K-selective potential-dependent pores in sterol-free phosphatidylethanolamine-containing phospholipid bilayers at a concentration of 1 ppm. Obtained results suggest that besides acidic lipids and membrane proteins phosphatidylethanolamine and cholesterol are the other major factors responsible for the differences between PHMG-induced plasma membrane depolarization of microbial and eukaryotic cells and thus, diverse modes of PHMG membrane action.

摘要

一种广为人知的胍聚合物家族阳离子杀菌剂,盐酸聚六亚甲基胍(PHMG),已在猪平滑肌细胞、大鼠脑神经末梢突触体和大鼠血小板中进行了细胞膜作用测试。结果表明,PHMG 在 7ppm 的浓度下可使平滑肌细胞膜上的 Na,K-ATP 酶活性抑制 82.2±0.9%,而在 100-500ppm 时突触体和血小板的剂量依赖性去极化变得明显。通过质谱(MALDI-TOF 和 PDMS-TOF)、黏度、动态光散射和模型磷脂膜等方法的比较研究表明,PHMG 低聚物具有不同数量的重复单元(8-16),在无甾醇的含磷脂酰乙醇胺的磷脂双层中形成 K 选择性、电位依赖性孔,在 1ppm 的浓度下形成 K 选择性、电位依赖性孔。研究结果表明,除了酸性脂质和膜蛋白外,磷脂酰乙醇胺和胆固醇也是导致 PHMG 诱导微生物和真核细胞膜去极化的差异的主要因素,因此,PHMG 的膜作用具有多种模式。

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