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Antigen presentation by hapten-specific B lymphocytes. I. Role of surface immunoglobulin receptors

机译:半抗原特异性B淋巴细胞的抗原呈递。一表面免疫球蛋白受体的作用

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摘要

The present study examines the ability of hapten-specific murine splenic B lymphocytes to present hapten-proteins to carrier-specific T cell hybridomas. BALB/cB cells specific for 2,4,6-trinitrophenyl (TNP) were isolated from spleens of immune mice by elution from TNP-gelatin- coated dishes. Such cells presented the TNP-modified terpolymer, GL phi, at concentrations as low as 0.1 microgram/ml, to a GL phi- specific, I-Ed-restricted, interleukin 2-producing T cell hybridoma. In contrast, the same B lymphocytes required 1,000-fold higher concentrations of unmodified GL phi to stimulate the same T cell hybridoma. The presentation of low concentrations of TNP-GL phi by TNP- specific B lymphocytes was significantly or completely blocked by anti- Ig antibody or TNP-proteins, indicating that surface Ig receptors were critically involved in this phenomenon. Finally, binding of TNP- proteins did not alter the ability of the B cells to present unrelated, unhaptenated proteins or to stimulate alloreactive T cells. These results suggest that surface Ig receptors serve to focus antigens onto specific B lymphocytes and that such cells are highly efficient at presenting linked antigenic determinants to T cells. The implications of these findings for the mechanisms of physiologic, histocompatibility- restricted T-B collaboration are discussed.
机译:本研究检查了半抗原特异性小鼠脾脏B淋巴细胞向载体特异性T细胞杂交瘤呈递半抗原蛋白的能力。通过从TNP-明胶包被的皿中洗脱,从免疫小鼠的脾脏中分离出对2,4,6-三硝基苯基(TNP)具有特异性的BALB / cB细胞。此类细胞以低至0.1微克/毫升的浓度呈递TNP修饰的三元共聚物GL phi,以产生GL phi特异性,I-Ed限制,产生白介素2的T细胞杂交瘤。相反,相同的B淋巴细胞需要1000倍高浓度的未修饰GL phi才能刺激相同的T细胞杂交瘤。 TNP特异性B淋巴细胞低浓度的TNP-GL phi呈递被抗Ig抗体或TNP蛋白显着或完全阻断,表明表面Ig受体严重参与了这一现象。最后,TNP-蛋白的结合不会改变B细胞呈递不相关的,未结合的蛋白或刺激同种反应性T细胞的能力。这些结果表明表面Ig受体用于将抗原聚焦在特定的B淋巴细胞上,并且这种细胞在将连接的抗原决定簇呈递给T细胞方面非常有效。讨论了这些发现对生理学,组织相容性受限的T-B合作机制的影响。

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