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B淋巴细胞中膜IgG及单价抗原/膜IgG复合物的内吞作用、细胞内运输和加工

Endocytosis, intracellular trafficking, and processing of membrane IgG and monovalent antigen/membrane IgG complexes in B lymphocytes.

作者信息

Davidson H W, West M A, Watts C

机构信息

Department of Biochemistry, The University, Dundee, UK.

出版信息

J Immunol. 1990 Jun 1;144(11):4101-9.

PMID:2187925
Abstract

Human B lymphoblastoid cell lines specific for tetanus toxin/toxoid were used in our earlier studies to demonstrate the rapid endocytosis of monovalent Ag and its processing, as a complex with mIgG. Here we show that the mIgGR for Ag is endocytosed in the presence or absence of Ag and that at any given time about 60% of this recycling pool of membrane (m) Ig is inside the cell. During the earliest detectable stages of Ag processing a high proportion of Ag fragments resolved on SDS gels were bound to intact mIg. However, at later times, as fragmented Ag accumulated, the fragments were precipitable only with antibodies against the Fab region of mIgG indicating proteolytic fragmentation of this receptor. Fractionation of cell homogenates on self-forming Percoll gradients revealed that at least two compartments are involved in Ag processing: a low density endosome compartment and a dense "late endosome"/lysosomal compartment. The spectrum of Ag fragments observed in each fraction differed: fragments produced at later times during processing were detected only in the late endosome/lysomal fraction whereas the earliest observed fragments were found both in this fraction and in the low density fractions. Monovalent Ag/mIgG complexes appear to have an increased probability, compared to unoccupied mIgG, of targeting to proteolytically active compartments leading to processing of the Ag/mIg complex and to accelerated degradation of the mIgG.

摘要

在我们早期的研究中,使用了对破伤风毒素/类毒素具有特异性的人B淋巴母细胞系来证明单价抗原的快速内吞作用及其作为与mIgG的复合物的加工过程。在这里,我们表明,无论有无抗原,抗原的mIgGR都会被内吞,并且在任何给定时间,这个循环的膜(m)Ig池的约60%都在细胞内。在抗原加工的最早可检测阶段,SDS凝胶上分离出的高比例抗原片段与完整的mIg结合。然而,在后期,随着碎片化抗原的积累,这些片段仅能用抗mIgG Fab区域的抗体沉淀,这表明该受体发生了蛋白水解片段化。在自形成的Percoll梯度上对细胞匀浆进行分级分离显示,至少有两个区室参与抗原加工:一个低密度内体区室和一个致密的“晚期内体”/溶酶体区室。在每个级分中观察到的抗原片段谱不同:加工后期产生的片段仅在晚期内体/溶酶体级分中检测到,而最早观察到的片段在该级分和低密度级分中均有发现。与未占据的mIgG相比,单价抗原/mIgG复合物似乎更有可能靶向蛋白水解活性区室,从而导致抗原/mIg复合物的加工以及mIgG的加速降解。

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