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Two phenotypically distinct populations of T cells have suppressor capabilities simultaneously in the maintenance phase of immunologic enhancement.

作者信息

Padberg W M, Lord R H, Kupiec-Weglinski J W, Williams J M, Di Stefano R, Thornburg L E, Araneda D, Strom T B, Tilney N L

出版信息

J Immunol. 1987 Sep 15;139(6):1751-7.

PMID:2957435
Abstract

The events leading to immunologic enhancement in LEW rats immunized actively with Brown Norway (BN) rat spleen cells and passively with LEW anti-BN hyperimmune serum 11 and 10 days before receiving (LEW X BN)F1 cardiac allografts, respectively, have been studied. Cellular suppressor mechanisms developing during the induction phase of this phenomenon have recently been shown to be mediated by W3/25+ T cells in an antigen-specific manner. The present study suggests that the late maintenance phase of immunologic enhancement is mediated in vivo by simultaneously present separate donor-specific T cell subpopulations of W3/25+ and OX8+ phenotypes. Splenocyte subsets from grafted recipients greater than 100 days after transplantation were adoptively transferred into unmodified syngeneic LEW rats that received a specific test allograft 24 hr later, or into B recipients bearing indefinitely surviving heart grafts. Test graft survival was prolonged significantly in the first group and not altered in the second. Indeed, nonoverlapping W3/25+ and OX8+ cell fractions were separately responsible for suppression. However, when suppressor activity was tested in vitro in a three-component coculture mixed lymphocyte reaction, no suppression by T cells was obtained; this lack of correlation between in vivo and in vitro results has also been noted by other investigators in different systems. Thus, in the maintenance phase of actively and passively induced immunologic enhancement, interplay between two phenotypically distinct T cells with suppressor characteristics, but not putative cell-surface blocking factors, seems to prevent development of an alloreactive response and mediate host unresponsiveness.

摘要

相似文献

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J Immunol. 1987 Sep 15;139(6):1751-7.
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引用本文的文献

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The Potential of IgG to Induce Murine and Human Thymic Maturation of IL-10+ B Cells (B10) Revealed in a Pilot Study.IgG 诱导小鼠和人 IL-10+B 细胞(B10)胸腺成熟的潜力:一项初步研究。
Cells. 2020 Oct 5;9(10):2239. doi: 10.3390/cells9102239.
2
CD4(+)Foxp3(+) regulatory T cell therapy in transplantation.移植中 CD4(+)Foxp3(+) 调节性 T 细胞治疗。
J Mol Cell Biol. 2012 Feb;4(1):11-21. doi: 10.1093/jmcb/mjr047. Epub 2011 Dec 14.
3
Specific unresponsiveness in rats with prolonged cardiac allograft survival after treatment with cyclosporine. III. Further characterization of the CD4+ suppressor cell and its mechanisms of action.
环孢素治疗后心脏同种异体移植长期存活大鼠的特异性无反应性。III. CD4 + 抑制细胞的进一步特征及其作用机制
J Exp Med. 1990 Jan 1;171(1):141-57. doi: 10.1084/jem.171.1.141.
4
The biology of acute transplant rejection.急性移植排斥反应的生物学
Ann Surg. 1991 Aug;214(2):98-106. doi: 10.1097/00000658-199108000-00002.
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Immunological tolerance induced by liver grafting in the rat: splenic macrophages and T cells mediate distinct phases of immunosuppressive activity.大鼠肝移植诱导的免疫耐受:脾巨噬细胞和T细胞介导免疫抑制活性的不同阶段。
Clin Exp Immunol. 1991 Jul;85(1):121-7. doi: 10.1111/j.1365-2249.1991.tb05692.x.
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Mechanisms in passive enhancement of cardiac and renal allografts by serum from liver-grafted rats.肝移植大鼠血清被动增强心脏和肾脏同种异体移植物的机制。
Immunology. 1991 Jan;72(1):79-84.