Literature DB >> 9637485

Antigen activation rescues recent thymic emigrants from programmed cell death in the BB rat.

S Ramanathan1, K Norwich, P Poussier.   

Abstract

One of the diabetes susceptibility genes of the BB rat is a mutation at the lyp locus that decreases the thymic output of T cells and the life span of most recent thymic emigrants (RTE). Consequently, there is a 10-fold reduction in the number of CD4+ and CD8+ T cells in secondary lymphoid organs. Results presented in this work demonstrate that the BB rat lyp mutation is associated with an accelerated apoptotic death in vitro of mature CD4+ 8- and CD4- 8+ thymocytes and peripheral T cells. The stability of the pool of recirculating T cells (PRL) of BB rats over time results from a > 10-fold increase in the mitotic activity of T cells as assessed in vivo by bromodeoxyuridine incorporation. This increased mitotic activity is not observed when BB T cells develop in the context of a normal sized PRL. MHC haploidentical WF and BB rats differ at minor histocompatibility loci. Intravenous injection of (WF x BB)F1 T cells into euthymic BB rats led to the rejection of donor T cells within 3 wk by unprimed recipients and within 1 wk by primed recipients. This secondary immune response was unaffected by postpriming thymectomy. F1 T cells were not rejected, but rather expanded after their injection into thymectomized BB rats that had been primed as early as 48 h after thymectomy. These results strongly suggest that the BB rat PRL is devoid of long-lived naive T cells and that rescue of recent thymic emigrants from programmed cell death is initiated by Ags, exclusively.

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Year:  1998        PMID: 9637485

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  16 in total

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Review 4.  Negative regulators in homeostasis of naïve peripheral T cells.

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5.  Kinetics of T cell turnover following thymectomy.

Authors:  K H Norwich; S Ramanathan; P Poussier
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6.  Genetic dissection of Iddm26 in the spontaneously diabetic BBDP rat.

Authors:  J Sarmiento; R H Wallis; T Ning; L Marandi; G Y C Chao; A D Paterson; P Poussier
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Review 8.  The three as: Alternative splicing, alternative polyadenylation and their impact on apoptosis in immune function.

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10.  GIMAP1 Is Essential for the Survival of Naive and Activated B Cells In Vivo.

Authors:  Louise M C Webb; Preeta Datta; Sarah E Bell; Daisuke Kitamura; Martin Turner; Geoffrey W Butcher
Journal:  J Immunol       Date:  2015-11-30       Impact factor: 5.422

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