Literature DB >> 1700506

Inhibition of alloresponsive naive and memory T cells by CD7 and CD25 antibodies and by cyclosporine.

A N Akbar1, P L Amlot, K Ivory, A Timms, G Janossy.   

Abstract

Human naive and memory T cells can be isolated from each other by their CD45RA and CD45RO expression, respectively. This enables the assessment of their differential sensitivities to immunosuppressive agents for the first time. We have investigated the ability of cyclosporine or CD7 and CD25 antibodies to selectively block alloantigen stimulated naive and memory T cells in vitro. CD7 antibodies blocked the proliferation of naive (P less than 0.025) but not memory T cells in a primary MLR. CD25 antibody inhibited both naive and memory subsets but a significantly greater effect was found on the memory T cells (P less than 0.005). The constitutive CD7 and CD25 antigen expression on resting naive or memory T cells was related to the inhibitory activities of these antibodies on both subsets. Accordingly, naive T cells expressed more CD7 antigen than memory cells while memory T cells displayed low levels of CD25 antigen that was absent from naive populations before activation. Cyclosporine, like CD25 antibody, inhibited both subsets in a primary MLR but had a greater effect on memory cells (P less than 0.02). Memory T cells, therefore, are more dependent than naive cells on IL-2 for proliferation. There was great individual variation in the ability of CsA to block the MLR. The simultaneous addition of CD25 or CD7 antibody together with CsA, however, enhanced the MLR inhibition as the effects of all three were additive. This suggested interference by these agents at different points during T cell activation. Thus, in CsA sensitive individuals, one-tenth of the optimal CsA concentration together with CD25 antibody maintained maximum immunosuppression in vitro. These results demonstrate the possibility of using CD7 and CD25 antibodies for selective inhibition of naive or memory T cells and also the possibility of augmenting the inhibition of and reducing the CsA concentration required for clinically effective immunosuppression.

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Year:  1990        PMID: 1700506     DOI: 10.1097/00007890-199011000-00016

Source DB:  PubMed          Journal:  Transplantation        ISSN: 0041-1337            Impact factor:   4.939


  8 in total

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2.  Increased adherence of CD2 peripheral blood lymphocytes to cytomegalovirus-infected fibroblasts is blocked by anti-LFA-3 antibody.

Authors:  J E Grundy; G S Pahal; A N Akbar
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3.  CD7-negative T cells represent a separate differentiation pathway in a subset of post-thymic helper T cells.

Authors:  U Reinhold; L Liu; J Sesterhenn; H Abken
Journal:  Immunology       Date:  1996-11       Impact factor: 7.397

4.  Molecular cloning and expression analysis of pig CD7.

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5.  Programmed cell death of T lymphocytes during acute viral infection: a mechanism for virus-induced immune deficiency.

Authors:  E S Razvi; R M Welsh
Journal:  J Virol       Date:  1993-10       Impact factor: 5.103

6.  Isolation and characterization of mouse CD7 cDNA.

Authors:  K Yoshikawa; M Seto; R Ueda; Y Obata; H Fukatsu; A Segawa; T Takahashi
Journal:  Immunogenetics       Date:  1993       Impact factor: 2.846

7.  Delayed activation-induced T lymphocytes death in aplastic anemia: related with abnormal Fas system.

Authors:  S C Kim; Y H Min; S Lee; S Y Chung; N C Yoo; J W Lee; J S Hahn; Y W Ko
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8.  The significance of low bcl-2 expression by CD45RO T cells in normal individuals and patients with acute viral infections. The role of apoptosis in T cell memory.

Authors:  A N Akbar; N Borthwick; M Salmon; W Gombert; M Bofill; N Shamsadeen; D Pilling; S Pett; J E Grundy; G Janossy
Journal:  J Exp Med       Date:  1993-08-01       Impact factor: 14.307

  8 in total

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