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新生小鼠B细胞的体外耐受性诱导

In vitro tolerance induction of neonatal murine B cells.

作者信息

Metcalf E S, Klinman N R

出版信息

J Exp Med. 1976 Jun 1;143(6):1327-40. doi: 10.1084/jem.143.6.1327.

Abstract

The susceptibility of neonatal and adult B lymphocytes to tolerance induction was analyzed by a modification of the in vitro splenic focus technique. This technique permits stimulation of individual hapten-specific clonal precursor cells from both neonatal and adult donors. Neonatal or adult BALB/c spleen cells were adoptively transferred into irradiated, syngeneic, adult recipients which had been carrier-primed to hemocyanin (Hy), thus maximizing stimulation to the hapten 2,4-dinitrophenyl coupled by Hy (DNP-Hy). Cultures were initially treated with DNP on several heterologous (non-Hy) carriers and subsequently stimulated with DNP-Hy. Whereas the responsiveness of adult B cells was not diminished by pretreatment with any DNP conjugate, the majority of the neonatal B-cell response was abolished by in vitro culture with all of the DNP-protein conjugates. During the 1st wk of life, the ability to tolerize neonatal splenic B cells progressively decreased. Thus, tolerance in this system is: (a) restricted to B cells early in development; (b) established by both tolerogens and immunogens; (c) achieved at low (10(-9) M determinant) antigen concentrations; and (d) highly specific, discriminating between DNP- and TNP-specific B cells. We conclude that: (a) B lymphocytes, during their development, mature through a stage in which they are extremely susceptible to tolerogenesis; (b) the specific interaction of B-cell antigen receptors with multivalent antigens, while irrelevant to mature B cells, is tolerogenic to neonatal (immature) B cells unless antigen is concomitantly recognized by primed T cells; and (c) differences in the susceptibility of immature and mature B lymphocytes to tolerance induction suggest intrinsic differences between neonatal and adult B cells and may provide a physiologically relevant model for the study of tolerance to self-antigens.

摘要

通过对体外脾集落技术进行改进,分析了新生和成年B淋巴细胞对耐受诱导的敏感性。该技术可刺激来自新生和成年供体的单个半抗原特异性克隆前体细胞。将新生或成年BALB/c脾细胞过继转移至经照射的、同基因的成年受体中,这些受体已用血蓝蛋白(Hy)进行载体致敏,从而使对半抗原2,4 -二硝基苯基与Hy偶联物(DNP - Hy)的刺激最大化。培养物最初用几种异源(非Hy)载体上的DNP处理,随后用DNP - Hy刺激。成年B细胞的反应性不会因任何DNP偶联物预处理而降低,而新生B细胞的大部分反应在与所有DNP - 蛋白质偶联物进行体外培养后被消除。在出生后的第1周内,使新生脾B细胞产生耐受的能力逐渐下降。因此,该系统中的耐受具有以下特点:(a)在发育早期仅限于B细胞;(b)由耐受原和免疫原共同建立;(c)在低(10⁻⁹M决定簇)抗原浓度下即可实现;(d)具有高度特异性,能区分DNP特异性和TNP特异性B细胞。我们得出以下结论:(a)B淋巴细胞在发育过程中会经历一个对耐受形成极为敏感的阶段;(b)B细胞抗原受体与多价抗原的特异性相互作用,虽然与成熟B细胞无关,但对新生(未成熟)B细胞具有致耐受性,除非抗原同时被致敏T细胞识别;(c)未成熟和成熟B淋巴细胞对耐受诱导敏感性的差异表明新生和成年B细胞之间存在内在差异,可能为研究自身抗原耐受提供一个生理相关模型。

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