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抗体诱导培养的人成纤维细胞上HLA抗原的聚集和内吞作用。

The antibody-induced clustering and endocytosis of HLA antigens on cultured human fibroblasts.

作者信息

Huet C, Ash J F, Singer S J

出版信息

Cell. 1980 Sep;21(2):429-38. doi: 10.1016/0092-8674(80)90479-1.

Abstract

It has previously been shown by immunofluorescence experiments that the cross-linking of HLA antigens into patches (by antibody reagents directed to human beta 2--microglobulin) on the surfaces of cultured human fibroblasts leads to the lining up of the patches over the actomyosin-containing stress fibers lying immediately under the surface membrane. These experiments have now been extended to the resolution of the electron microscope by the use of ferritin-conjugated antibody. The results show that a substantial part of the HLA surface clusters that form by 5 min after the addition of the antibody reagents is found in small uncoated surface invaginations which are subsequently endocytosed and ultimately fuse with lysosomal bodies. At no stage in this process is there any indication that coated pits or coated vesicles participate. These and other results suggest, therefore, that there are at least two distinct mechanisms for the ligand-induced endocytosis and lysosomal processing of membrane components, one involving coated pits and the other the noncoated invaginations described in this paper. Transmembrane associations of clusters with intracellular actomyosin-containing structures may have a role in the endocytosis of these noncoated invaginations.

摘要

此前通过免疫荧光实验表明,在培养的人成纤维细胞表面,(通过针对人β2 - 微球蛋白的抗体试剂)将HLA抗原交联成斑块会导致这些斑块排列在紧邻表面膜下方含肌动球蛋白的应力纤维上。现在通过使用铁蛋白偶联抗体,这些实验已扩展到电子显微镜分辨率水平。结果显示,在添加抗体试剂后5分钟内形成的HLA表面簇的很大一部分存在于小的无包被表面内陷中,这些内陷随后被内吞并最终与溶酶体融合。在这个过程的任何阶段都没有迹象表明有被膜小窝或有被小泡参与。因此,这些及其他结果表明,膜成分的配体诱导内吞和溶酶体加工至少有两种不同机制,一种涉及被膜小窝,另一种涉及本文所述的无包被内陷。簇与细胞内含肌动球蛋白结构的跨膜关联可能在这些无包被内陷的内吞作用中起作用。

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