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体外免疫反应中的细胞相互作用。V. 通过抗原与胸腺来源细胞免疫球蛋白复合物的特异性协作。

Cell interactions in the immune response in vitro. V. Specific collaboration via complexes of antigen and thymus-derived cell immunoglobulin.

作者信息

Feldmann M

出版信息

J Exp Med. 1972 Oct 1;136(4):737-60. doi: 10.1084/jem.136.4.737.

Abstract

The mechanism of interaction of T and B lymphocytes was investigated in an in vitro hapten carrier system using culture chambers with two compartments separated by a cell impermeable nucleopore membrane. Because specific cell interaction occurred efficiently across this membrane, contact of T and B lymphocytes was not essential for cooperation which must have been mediated by a subcellular component or "factor." By using different lymphoid cell populations in the lower culture chamber and activated thymus cells in the upper chamber (with antigen present in both), it was found that the antigen-specific mediator acted indirectly on B cells, through the agency of macrophages. Macrophages which had been cultured in the presence of activated T cells and antigen acquired the capacity to specifically induce antibody responses in B cell-containing lymphoid populations. Trypsinization of these macrophages inhibited their capacity to induce immune responses, indicating that the mediator of cell cooperation is membrane bound. By using antisera to both the haptenic and carrier determinants of the antigen as blocking reagents, it was demonstrated that the whole antigen molecule was present on the surface of macrophages which had been exposed to activated T cells and antigen. Because specifically activated T cells were essential a component of the antigen-specific mediator must be derived from these cells. By using anti-immunoglobulin sera as inhibitors of the binding of the mediator to macrophages, the T cell component was indeed found to contain both kappa- and micro-chains and was thus presumably a T cell-derived immunoglobulin. It was proposed that cell cooperation is mediated by complexes of T cell IgM and antigen, bound to the surface of macrophage-like cells, forming a lattice of appropriately spaced antigenic determinants. B cells become immunized by interacting with this surface. With this mechanism of cell cooperation, the actual pattern of antigen-B cell receptor interactions in immunization would be the same with both thymus-dependent and independent antigens. An essential feature of the proposed mechanism of cell cooperation is that macrophage-B cell interaction must occur at an early stage of the antibody response, a concept which is supported by many lines of evidence. Furthermore this mechanism of cell interaction can be elaborated to explain certain phenomena such as the highly immunogenic macrophage-bound antigen, antigenic competition, the distinction between immunity and tolerance in B lymphocytes, and the possible mediation of tolerance by T lymphocytes.

摘要

在体外半抗原载体系统中,使用由细胞不可渗透的核孔膜分隔为两个隔室的培养室,研究了T淋巴细胞和B淋巴细胞的相互作用机制。由于特异性细胞相互作用能有效地穿过该膜,因此T淋巴细胞和B淋巴细胞的接触对于合作并非必不可少,这种合作必定是由亚细胞成分或“因子”介导的。通过在下层培养室中使用不同的淋巴细胞群体,并在上层培养室中使用活化的胸腺细胞(两者中均存在抗原),发现抗原特异性介质通过巨噬细胞间接作用于B细胞。在活化的T细胞和抗原存在的情况下培养的巨噬细胞获得了在含B细胞的淋巴细胞群体中特异性诱导抗体反应的能力。用胰蛋白酶处理这些巨噬细胞会抑制其诱导免疫反应的能力,这表明细胞合作的介质是膜结合的。通过使用针对抗原的半抗原和载体决定簇的抗血清作为阻断剂,证明了整个抗原分子存在于已暴露于活化T细胞和抗原的巨噬细胞表面。由于特异性活化的T细胞是必不可少的,抗原特异性介质的一个成分必定源自这些细胞。通过使用抗免疫球蛋白血清作为介质与巨噬细胞结合的抑制剂,确实发现T细胞成分同时含有κ链和μ链,因此推测是一种T细胞衍生的免疫球蛋白。有人提出,细胞合作是由T细胞IgM和抗原的复合物介导的,这些复合物结合在巨噬细胞样细胞的表面,形成具有适当间隔的抗原决定簇的晶格。B细胞通过与该表面相互作用而被免疫。通过这种细胞合作机制,在免疫中抗原 - B细胞受体相互作用的实际模式在胸腺依赖性抗原和非胸腺依赖性抗原中是相同的。所提出的细胞合作机制的一个基本特征是巨噬细胞 - B细胞相互作用必须在抗体反应的早期发生,这一概念得到了许多证据的支持。此外,这种细胞相互作用机制可以进一步阐述以解释某些现象,如高度免疫原性的巨噬细胞结合抗原、抗原竞争、B淋巴细胞中免疫与耐受的区别以及T淋巴细胞可能介导的耐受。

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