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The Cellular and Chemical Biology of Endocytic Trafficking and Intracellular Delivery—The GL–Lect Hypothesis

机译:内吞贩的细胞和化学生物学和细胞内递送 - GL-Lect假设

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摘要

Lipid membranes are common to all forms of life. While being stable barriers that delimitate the cell as the fundamental organismal unit, biological membranes are highly dynamic by allowing for lateral diffusion, transbilayer passage via selective channels, and in eukaryotic cells for endocytic uptake through the formation of membrane bound vesicular or tubular carriers. Two of the most abundant fundamental fabrics of membranes—lipids and complex sugars—are produced through elaborate chains of biosynthetic enzymes, which makes it difficult to study them by conventional reverse genetics. This review illustrates how organic synthesis provides access to uncharted areas of membrane glycobiology research and its application to biomedicine. For this Special Issue on Chemical Biology Research in France, focus will be placed on synthetic approaches (i) to study endocytic functions of glycosylated proteins and lipids according to the GlycoLipid–Lectin (GL–Lect) hypothesis, notably that of Shiga toxin; (ii) to mechanistically dissect its endocytosis and intracellular trafficking with small molecule; and (iii) to devise intracellular delivery strategies for immunotherapy and tumor targeting. It will be pointed out how the chemical biologist’s view on lipids, sugars, and proteins synergizes with biophysics and modeling to “look” into the membrane for atomistic scale insights on molecular rearrangements that drive the biogenesis of endocytic carriers in processes of clathrin-independent endocytosis.
机译:脂膜是所有生命形式。而在于圈定单元作为基本单元有机体稳定障碍,生物膜是通过允许经由选择性信道的横向扩散,跨双通道高度动态的,并且在真核细胞中通过膜的形成吞摄取结合囊泡或管状载体。的膜脂质和复合物中的最丰富的基本织物的两种糖-通过生物合成酶的复杂的链,其使得难以通过常规的反向遗传学研究它们产生的。本次审查是表示合成有机如何提供访问膜糖生物学研究及其应用生物医学的未知领域。有关化学生物学研究在法国这个特刊,重点将放在合成方法(一)研究根据糖脂凝集素(GL-LECT)假说糖基化蛋白和脂质的内吞作用,尤其是志贺毒素; (ii)向机械地解剖其内吞作用和与小分子的细胞内运输;和(iii),设计一种用于免疫疗法和肿瘤靶向细胞内递送策略。应当指出的是怎么化学生物学家对脂类,糖类,以及与生物物理学和建模,以“看”的蛋白质具有协同作用视图进入膜对推动内吞载体的生物合成中网格蛋白独立的内吞作用的过程分子重排原子论规模见解。

著录项

  • 期刊名称 Molecules
  • 作者

    Ludger Johannes;

  • 作者单位
  • 年(卷),期 2021(26),11
  • 年度 2021
  • 页码 3299
  • 总页数 15
  • 原文格式 PDF
  • 正文语种
  • 中图分类 分子生物学;
  • 关键词

    机译:糖磷脂;半胶质蛋白;糖基化;内吞作用;逆行贩运;筏;卡斯米尔力;免疫疗法;肿瘤靶向;小分子;

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