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一种不可交换的荧光磷脂类似物作为内吞途径的膜运输标志物。

A non-exchangeable fluorescent phospholipid analog as a membrane traffic marker of the endocytic pathway.

作者信息

Willem J, ter Beest M, Scherphof G, Hoekstra D

机构信息

Laboratory of Physiological Chemistry, University of Groningen, The Netherlands.

出版信息

Eur J Cell Biol. 1990 Oct;53(1):173-84.

PMID:2076704
Abstract

The fluorescent phospholipid analog N-(lissamine rhodamine B sulfonyl)phosphatidylethanolamine (N-Rh-PE) was inserted into the plasma membrane of Baby hamster kidney cells at low temperature (2 degrees C). The mobility characteristics of the analog--as revealed by fluorescence photobleaching recovery--were very similar to those of membrane-inserted 1-acyl-2[6-[N-(7-nitro-2,1,3-benzoxadiazol-4-yl) amino]caproyl] phosphatidylcholine (C6-NBD-PC). Upon warming to 37 degrees C, followed by a 1-h incubation, all N-Rh-PE was located intracellularly. By contrast, after the same time interval, approximately 10% of the cell-associated PC-derivative was found intracellularly. Furthermore, the analogs moved to different intracellular sites, as N-Rh-PE associates with perinuclear and peri-Golgi structures, whereas C6-NBD-PC appears mainly in the Golgi complex. Colocalization with organelle-specific probes and Percoll gradient analysis identified the N-Rh-PE-labeled structures as lysosomes. Temperature and energy-dependent experiments supported the endocytic pathway as the mechanism of N-Rh-PE internalization. The mechanism of N-Rh-PE internalization appears to differ from that of C6-NBD-PC. In conjunction with a difference in the efficiency of removal of the lipid derivatives from the plasma membrane, the results suggest that N-Rh-PE is selectively internalized, implying that sorting of the lipid analogs already occurs at the level of the plasma membrane. The distinct difference in physical appearance of the probes after membrane insertion, i.e., N-Rh-PE being present as small clusters and C6-NBD-PC as monomers, could explain the selective sorting and internalization of N-Rh-PE. The results demonstrate that N-Rh-PE may serve as a useful marker for studying membrane traffic during endocytosis.

摘要

荧光磷脂类似物N-(丽丝胺罗丹明B磺酰基)磷脂酰乙醇胺(N-Rh-PE)在低温(2℃)下插入幼仓鼠肾细胞的质膜中。通过荧光漂白恢复揭示的该类似物的流动性特征与膜插入的1-酰基-2-[6-[N-(7-硝基-2,1,3-苯并恶二唑-4-基)氨基]己酰基]磷脂酰胆碱(C6-NBD-PC)非常相似。升温至37℃,随后孵育1小时后,所有N-Rh-PE都位于细胞内。相比之下,在相同的时间间隔后,发现约10%的细胞相关PC衍生物位于细胞内。此外,这些类似物移动到不同的细胞内位点,因为N-Rh-PE与核周和高尔基体周围结构相关联,而C6-NBD-PC主要出现在高尔基体复合物中。与细胞器特异性探针的共定位和Percoll梯度分析将N-Rh-PE标记的结构鉴定为溶酶体。温度和能量依赖性实验支持内吞途径作为N-Rh-PE内化的机制。N-Rh-PE内化的机制似乎与C6-NBD-PC不同。结合从质膜去除脂质衍生物效率的差异,结果表明N-Rh-PE被选择性内化,这意味着脂质类似物的分选已经在质膜水平发生。膜插入后探针物理外观的明显差异,即N-Rh-PE以小簇形式存在而C6-NBD-PC以单体形式存在,可以解释N-Rh-PE的选择性分选和内化。结果表明,N-Rh-PE可作为研究内吞作用期间膜运输的有用标记物。

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