首页> 美国卫生研究院文献>The Journal of Biophysical and Biochemical Cytology >Fate of plasma membrane during endocytosis. II. Evidence for recycling (shuttle) of plasma membrane constituents
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Fate of plasma membrane during endocytosis. II. Evidence for recycling (shuttle) of plasma membrane constituents

机译:内吞过程中质膜的命运。二。质膜成分回收(穿梭)的证据

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摘要

Cultured rat embryo fibroblasts were first allowed to store for 24 h fluorescein-labeled goat immunoglobulins directed against rabbit immunoglobulins (F anti-R IgG), and were subsequently exposed for 24 h to [(3)H]acetylated rabbit immunoglobulins known to bind to the cell membrane either specifically (anti-plasma membrane IgG: A anti-PM IgG) or unspecifically (contol IgG: AC IgG). As a result of immunological interaction between the two antibodies (no effect was found if the cells had been preloaded with control goat FC IgG), a substantial portion of the stored F anti-R IgG was unloaded from its intracellular storage site, appearing in the medium in the form of soluble immune complexes with rabbit A IgG. Part of the unloaded F anti-R IgG also was recovered in association with the plasma membrane, but only when A anti-PM IgG was used. In addition, significant reverse translocation of AC IgG from plasma membrane to lysosomes or some related intracellular storage compartment was also observed. With A anti-PM IgG, this translocation was less marked and affecte at the same time the plasma membrane marker 5’- nucleotidase. Cells that had stored horseradish peroxidase (HRP) simultaneously with F anti-R IgG did not unload HRP when exposed to A anti-PM IgG. These results support strongly, though not unequivocally, the concept that plasma membrane patches interiorized by endocytosis are recycled, or shuttled, back to the cell surface. In the framework of this concept, recycling antibody-coated membrane is taken to serve as vehicle for the selective intracellular capture and extracellular discharge of immunologically bound F anti-R IgG. The alternative explanation of regurgitation triggered off by immune complexes is considered less likely in view of the lack of HRP unloading.
机译:首先,将培养的大鼠胚胎成纤维细胞储存针对兔免疫球蛋白(F抗-R IgG)的荧光素标记的山羊免疫球蛋白,然后暴露于已知与之结合的[(3)H]乙酰化兔免疫球蛋白24 h。细胞膜是特异性的(抗质膜IgG:抗PM IgG)还是非特异性的(对照IgG:AC IgG)。由于这两种抗体之间的免疫相互作用(如果细胞已预装了对照山羊FC IgG,则没有发现作用),所储存的大部分F抗R IgG从其细胞内存储位点被卸载,出现在可溶性免疫复合物与兔A IgG混合的培养基。还与质膜一起回收了部分未装载的F抗R IgG,但仅当使用A抗PM IgG时才被回收。另外,还观察到AC IgG从质膜到溶酶体或一些相关的细胞内储藏室的显着逆转。使用抗PM IgG时,这种移位的标记较少,并同时影响质膜标记5'-核苷酸酶。与F抗R IgG同时储存了辣根过氧化物酶(HRP)的细胞在暴露于A抗PM IgG时不会卸载HRP。这些结果有力地支持(尽管不是明确地)将通过内吞作用内化的质膜补丁回收或穿梭回到细胞表面的概念。在该概念的框架中,采用回收抗体包被的膜作为媒介,以选择性地捕获和结合免疫学上结合的F抗R IgG的细胞外。鉴于缺乏HRP卸载,由免疫复合物引发的反流的另一种解释被认为不太可能。

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