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配体诱导表面免疫球蛋白与B淋巴细胞的去污剂不溶性细胞骨架基质结合。

Ligand-induced association of surface immunoglobulin with the detergent-insoluble cytoskeletal matrix of the B lymphocyte.

作者信息

Braun J, Hochman P S, Unanue E R

出版信息

J Immunol. 1982 Mar;128(3):1198-204.

PMID:6976988
Abstract

Ligand binding is believed to induce surface immunoglobulin (Ig) to form a physical association with the underlying cell cytoskeleton. We investigated this interaction by use of nonionic detergents, which are known to dissolve membrane proteins but preserve a detergent-insoluble cytoskeletal residue. In the absence of ligand treatment, surface Ig in the B cell plasma membrane was fully dissolved by nonionic detergent; however, interaction with a ligand converted the receptor to a novel, detergent-insoluble state. The conversion of surface Ig to a detergent-insoluble form required receptor cross-linking but occurred independently of capping. Several types of experiments demonstrated that this form of Ig was not due to the size insolubility of immune complexes and involved a stable, noncovalent association of the receptor with the detergent-insoluble, cytoskeletal residue. Incubation of ligand-bound cells at 37 degrees C promoted the degradation of surface Ig and the appearance of new, lower m.w. species, including a major soluble protein (50,000 daltons) that was antigenically related to surface Ig. These events corresponded to receptor endocytosis by several criteria (time course, temperature sensitivity, and energy dependence). Taken together, these results were consistent with the ligand-induced transmembrane attachment of receptors to the underlying cytoskeletal matrix followed by receptor internalization and catabolism.

摘要

配体结合被认为可诱导表面免疫球蛋白(Ig)与潜在的细胞骨架形成物理关联。我们通过使用非离子去污剂来研究这种相互作用,已知非离子去污剂可溶解膜蛋白,但会保留不溶于去污剂的细胞骨架残余物。在未进行配体处理时,B细胞质膜中的表面Ig可被非离子去污剂完全溶解;然而,与配体的相互作用会使受体转变为一种新的、不溶于去污剂的状态。表面Ig转变为不溶于去污剂的形式需要受体交联,但与帽化无关。多种类型的实验表明,这种形式的Ig并非由于免疫复合物的大小不溶性所致,而是涉及受体与不溶于去污剂的细胞骨架残余物的稳定非共价结合。在37℃孵育配体结合的细胞会促进表面Ig的降解以及新的、分子量较低的物种的出现,包括一种与表面Ig具有抗原相关性的主要可溶性蛋白(50,000道尔顿)。通过几个标准(时间进程、温度敏感性和能量依赖性),这些事件与受体内吞作用相符。综上所述,这些结果与配体诱导受体跨膜附着于潜在的细胞骨架基质,随后发生受体内化和分解代谢一致。

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