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抗原诱导的半抗原特异性B淋巴细胞上受体的聚集与调节。

Antigen-induced aggregation and modulation of receptors on hapten-specific B lymphocytes.

作者信息

Nossal G J, Layton J E

出版信息

J Exp Med. 1976 Mar 1;143(3):511-28. doi: 10.1084/jem.143.3.511.

Abstract

Mouse spleen cells were subjected to a fractionation procedure designed to enrich for 4-hydroxy-3-iodo-5-nitro-phenylacetyl (NIP)- or DNP-specific B lymphocytes, which depended on adherence of specific cells to a layer of hapten-gelatin at 4 degrees C, recovery of bound cells by melting, and digestion of adherent antigen by collagenase. A population of cells resulted which contained 90% typical B cells and 37% of cells capable of binding a fluorescent, haptenated polymeric protein. Fractionated cells were reacted in vitro with fluorescent conjugates of the specific haptens with polymerized flagellin [NIP-polymerized flagellin (POL)-tetramethylrhodamine isothiocyanate conjugate or DNP-POL-fluorescein isothiocyanate conjugate] under a variety of conditions, with the aim of investigating the behavior of Ig receptors on B lymphocytes after exposure to antigen; Experiments were performed with immunogenic and tolerogenic concentrations of antigen. Furthermore, four experimental designs were used, namely: (a) brief labeling with fluorescent antigen followed by culture without antigen (pulse design); (b) culture in the continuous presence of fluorescent antigen (continuous-labeling design); (c) culture in the continuous presence of nonlabeled antigen followed by labeling of unoccupied receptors by fluorescent antigen (receptor status design); and (d) culture with nonlabeled antigen for 2 h followed by incubation without further antigen for 20 h and labeling with fluorescent antigen (modulation design). Further insight into receptor occupancy and distribution was gained by the use of fluorescent antihapten and antiglobulin reagents. It was found that both immunogenic and tolerogenic antigen concentrations caused rapid patching and capping of the receptors to which they attached, followed by endocytosis and probably some shedding of Ig receptors. However, a proportion of cells continued to bear some cell surface antigen for 24 h. The immunogenic antigen concentration failed to completely remove the receptor coat from the cell surface. At all stages of immunogenesis, plentiful unoccupied receptors could be demonstrated. The tolerogenic concentration nearly saturated available receptors, and in its continuous presence, only few unoccupied or antigen-occupied surface receptors could be detected after 24 h of culture. Experiments of the modulation design showed that brief incubation with the tolerogenic concentration appeared to suppress receptor resynthesis, as few new receptors could be demonstrated after 20 h of further culture without antigen. Experiments were performed to determine whether fractionated cells prepared from spleens of 8-day-old mice showed an unusual tendency for modulation, even with immunogenic antigen concentrations. They were found to behave essentially like adult fractionated cells. The results are discussed in the framework of current theories of B-lymphocyte activation and tolerization.

摘要

小鼠脾细胞经过一种分级分离程序,该程序旨在富集4-羟基-3-碘-5-硝基苯乙酰(NIP)或二硝基苯酚(DNP)特异性B淋巴细胞,这取决于特定细胞在4℃下与半抗原明胶层的黏附、通过融化回收结合的细胞以及用胶原酶消化黏附的抗原。得到的细胞群体包含90%的典型B细胞和37%能够结合荧光半抗原化聚合蛋白的细胞。分级分离的细胞在多种条件下与特定半抗原与聚合鞭毛蛋白的荧光偶联物[NIP-聚合鞭毛蛋白(POL)-异硫氰酸四甲基罗丹明偶联物或DNP-POL-异硫氰酸荧光素偶联物]在体外反应,目的是研究B淋巴细胞在接触抗原后Ig受体的行为;实验使用了免疫原性和致耐受性浓度的抗原。此外,采用了四种实验设计,即:(a)用荧光抗原短暂标记,然后在无抗原的情况下培养(脉冲设计);(b)在荧光抗原持续存在的情况下培养(持续标记设计);(c)在未标记抗原持续存在的情况下培养然后用荧光抗原标记未占据的受体(受体状态设计);以及(d)用未标记抗原培养2小时,然后在无进一步抗原的情况下孵育20小时,并用荧光抗原标记(调节设计)。通过使用荧光抗半抗原和抗球蛋白试剂,对受体占据和分布有了进一步了解。发现免疫原性和致耐受性抗原浓度均导致它们所附着受体的快速补丁形成和帽化,随后是内吞作用,可能还有一些Ig受体的脱落。然而,一部分细胞在24小时内仍继续带有一些细胞表面抗原。免疫原性抗原浓度未能完全从细胞表面去除受体覆盖物。在免疫发生的所有阶段,都能证明有大量未占据的受体。致耐受性浓度几乎使可用受体饱和,并且在其持续存在的情况下,培养24小时后仅能检测到很少的未占据或抗原占据的表面受体。调节设计的实验表明,用致耐受性浓度短暂孵育似乎会抑制受体的再合成,因为在无抗原的情况下进一步培养20小时后几乎没有新的受体被证明。进行实验以确定从8日龄小鼠脾脏制备的分级分离细胞是否表现出异常的调节倾向,即使是在免疫原性抗原浓度下。发现它们的行为基本上与成年分级分离细胞相似。在B淋巴细胞激活和耐受的当前理论框架内讨论了这些结果。

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