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首次或主要免疫。二、诱导产生的免疫球蛋白携带转化生长因子β并抑制细胞溶解性T细胞对无关同种异体抗原的反应。

A first or dominant immunization. II. Induced immunoglobulin carries transforming growth factor beta and suppresses cytolytic T cell responses to unrelated alloantigens.

作者信息

Stach R M, Rowley D A

机构信息

Department of Pathology, University of Chicago, Illinois 60637.

出版信息

J Exp Med. 1993 Sep 1;178(3):841-52. doi: 10.1084/jem.178.3.841.

Abstract

Fresh sera from mice immunized by bearing an immunogenic tumor or by repeated injections of allogeneic spleen cells or xenogeneic erythrocytes powerfully suppress cytolytic T cell responses in one-way mixed lymphocyte cultures. Suppression is not antigen specific, though is mediated by immunoglobulin (Ig)G specific for the immunizing antigen. Suppression caused by IgG mimics that caused by active transforming growth factor beta (TGF-beta). IgG associates with or carries latent TGF-beta; however, suppression caused by the complex of IgG-TGF-beta requires macrophages (M phi), whereas active TGF-beta alone does not. Also, IgG dissociated from TGF-beta does not cause suppression, suggesting that M phi may take up Ig-TGF-beta, process the complex, and deliver active TGF-beta to lymphocytes. Indeed, suppression by immune serum was prevented by antibody to Fc receptors, by saturating Fc receptors with heterologous IgGs, and by antibodies against TGF-beta. The overall findings reveal a previously unrecognized regulatory circuit whereby IgG produced in response to one antigen nonspecifically downregulates cytolytic T lymphocyte responses to unrelated antigens. The findings introduce the intriguing possibility that TGF-beta delivered by IgG and processed by M phi may mediate important biological effects in processes such as wound healing, tumor growth, and some autoimmune diseases.

摘要

来自通过接种免疫原性肿瘤、反复注射同种异体脾细胞或异种红细胞免疫的小鼠的新鲜血清,能在单向混合淋巴细胞培养中强烈抑制细胞溶解性T细胞反应。抑制作用并非抗原特异性的,尽管它是由针对免疫抗原的免疫球蛋白(Ig)G介导的。IgG引起的抑制作用类似于活性转化生长因子β(TGF-β)引起的抑制作用。IgG与潜伏性TGF-β结合或携带它;然而,IgG-TGF-β复合物引起的抑制作用需要巨噬细胞(M phi),而单独的活性TGF-β则不需要。此外,从TGF-β解离的IgG不会引起抑制作用,这表明M phi可能摄取Ig-TGF-β,处理该复合物,并将活性TGF-β递送至淋巴细胞。事实上,免疫血清的抑制作用可被抗Fc受体抗体、用异源IgG饱和Fc受体以及抗TGF-β抗体所阻止。总体研究结果揭示了一个以前未被认识的调节回路,即针对一种抗原产生的IgG非特异性地下调细胞溶解性T淋巴细胞对无关抗原的反应。这些发现提出了一个有趣的可能性,即由IgG递送并由M phi处理的TGF-β可能在伤口愈合、肿瘤生长和一些自身免疫性疾病等过程中介导重要的生物学效应。

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