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Plasma membrane microorganization of LR73 multidrug-resistant cells revealed by FCS

机译:FCS揭示LR73多药耐药细胞的质膜微组织

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摘要

Tumoral cells could present a multidrug resistance (MDR) to chemotherapeutic treatments. This drug resistance would be associated to biomechanisms occurring at the plasma membrane level, involving modification of membrane fluidity, drug permeability, presence of microdomains (rafts, caveolae...), and membrane proteins overexpression such as P-glycoprotein. Fluorescence correlation spectroscopy (FCS) is the relevant method to investigate locally the fluidity of biological membranes through the lateral diffusion of a fluorescent membrane probe. Thus, we use FCS to monitor the plasma membrane local organization of LR73 carcinoma cells and three derived multidrug-resistant cancer cells lines. Measurements were conducted at the single cell level, which enabled us to get a detailed overview of the plasma membrane microviscosity distribution of each cell line studied. Moreover, we propose 2D diffusion simulation based on a Monte Carlo model to investigate the membrane organisation in terms of microdomains. This simulation allows us to relate the differences in the fluidity distributions with microorganization changes in plasma membrane of MDR cells.
机译:肿瘤细胞可能对化学疗法表现出多重耐药性。这种抗药性与在质膜水平发生的生物机制有关,包括膜流动性的改变,药物的渗透性,微区(筏,小窝等)的存在以及膜蛋白的过度表达,例如P-糖蛋白。荧光相关光谱法(FCS)是通过荧光膜探针的侧向扩散局部研究生物膜流动性的相关方法。因此,我们使用FCS来监测LR73癌细胞和三个衍生的多药耐药癌细胞系的质膜局部组织。在单个细胞水平上进行测量,这使我们能够详细了解所研究的每个细胞系的质膜微粘度分布。此外,我们提出了基于蒙特卡洛模型的二维扩散模拟,以研究微结构方面的膜组织。该模拟使我们能够将流动性分布的差异与MDR细胞质膜中微生物的变化联系起来。

著录项

  • 来源
    《Single molecule spectroscopy and imaging IV》|2011年|p.79050I.1-79050I.8|共8页
  • 会议地点 San Francisco CA(US)
  • 作者单位

    Laboratoire de Nanotechnologie et d'lnstrumentation Optique, LRC CEA, CNRS UMR 6279-STMR, Institut Charles Delaunay, Universite de Technologie de Troyes,12 rue Marie Curie, BP 2060,10 010 Troyes cedex, France;

    Laboratoire de Nanotechnologie et d'lnstrumentation Optique, LRC CEA, CNRS UMR 6279-STMR, Institut Charles Delaunay, Universite de Technologie de Troyes,12 rue Marie Curie, BP 2060,10 010 Troyes cedex, France;

    Laboratoire de Nanotechnologie et d'lnstrumentation Optique, LRC CEA, CNRS UMR 6279-STMR, Institut Charles Delaunay, Universite de Technologie de Troyes,12 rue Marie Curie, BP 2060,10 010 Troyes cedex, France,Laboratoire MEDyC , CNRS UMR 6237, URCAIFR53, Faculte de Pharmacie,51 rue Cognacq Jay, 51096 Reims, France;

    Laboratoire MEDyC , CNRS UMR 6237, URCAIFR53, Faculte de Pharmacie,51 rue Cognacq Jay, 51096 Reims, France;

    Laboratoire MEDyC , CNRS UMR 6237, URCAIFR53, Faculte de Pharmacie,51 rue Cognacq Jay, 51096 Reims, France;

    Laboratoire de Nanotechnologie et d'lnstrumentation Optique, LRC CEA, CNRS UMR 6279-STMR, Institut Charles Delaunay, Universite de Technologie de Troyes,12 rue Marie Curie, BP 2060,10 010 Troyes cedex, France;

  • 会议组织
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 医用物理学;
  • 关键词

    plasma membrane; fluorescence correlation spectroscopy; fluidity; p-glycoprotein; multidrug resistance; monte carlo simulation;

    机译:质膜荧光相关光谱流动性对糖蛋白多药耐药性;蒙特卡洛模拟;

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