Abstract
We evaluated the role of Fas ligand and perforin, the major T cell-mediated cytotoxic pathways that regulate T cell homeostasis, in a CD8+ T cell mediated model of graft-versus-host disease (GVHD) where donor and recipients differ at a single MHC class I antigen (B6 → bm1). Lethally irradiated (11Gy) bm1 mice were transplanted with T cell depleted BM and CD8+ T cells from either wild type (wt) or cytotoxic double deficient (cdd, deficient in both pathways) B6 donors. We hypothesized that cdd CD8+ T cells would be unable to mediate significant GVHD. Contrary to our hypothesis, recipients of cdd donor CD8+ T cells demonstrated significantly greater histopathologic damage from GVHD and increased serum levels of IFN-gamma and TNF-alpha compared to controls (Table 1). In order to understand this increase, we evaluated the in vivo expansion of donor T cells in these recipients as well as in BMT recipients of allogeneic CD8+ T cells from FasL deficient (gld) and perforin deficient (pfp−/−) donors. CD8+ wt T cells expanded until at day 10 after BMT, followed by a rapid decline. By contrast, cdd CD8+ T cells expanded continuously up to day 30 after BMT, peaking at almost one hundred times the number of wt T cells. gld T cells showed kinetics similar to wt T cells, whereas the pfp−/− T cells showed a significantly greater peak on day 10 but a similar contraction by day 30. Percentages of annexin+ cdd donor CD8+ T cells were significantly reduced compared to the other groups. Persistence of host antigen presenting cells did not account for the unrestrained expansion of cdd donor T cells because host dendritic cells were not detected in either the spleen, BM or gut of recipients of cdd CD8+ T cells on day 6 after BMT. In addition, alloantigen expression on epithelial target cells did not enhance GVHD because B6 donor cdd T cells induced equivalently lethal GVHD in [bm1 → B6] and [bm1 → bm1] chimeras (MST of 30 days and 27 days, respectively). We conclude that both perforin and Fas ligand pathways are required for alloreactive CD8+ T cell populations to contract after their initial expansion during a GVH reaction and that the absence of both these pathways results in donor CD8+ T cell unrestricted expansion and more severe GVHD.
Table 1
. | GVHD score (gut) . | IFN-g (pg/ml) . | TNF-a (pg/ml) . | CD8+T cell (x10e6) . | Annexin+CD8+(%) . |
---|---|---|---|---|---|
cdd vs. wt, *P<0.05 | |||||
Wt | 4.0±0.4 | 110±12 | 6.5±2.7 | 0.9±0.2 | 81±3.3 |
Cdd | 5.7±0.3* | 263±71* | 64.6±3.2* | 80.1±4.0* | 62±3.6* |
Pfp−/− | ND | ND | ND | 2.6±0.7 | 73±5.1 |
Gld | ND | ND | ND | 1.7±0.4 | 80±0.6 |
. | GVHD score (gut) . | IFN-g (pg/ml) . | TNF-a (pg/ml) . | CD8+T cell (x10e6) . | Annexin+CD8+(%) . |
---|---|---|---|---|---|
cdd vs. wt, *P<0.05 | |||||
Wt | 4.0±0.4 | 110±12 | 6.5±2.7 | 0.9±0.2 | 81±3.3 |
Cdd | 5.7±0.3* | 263±71* | 64.6±3.2* | 80.1±4.0* | 62±3.6* |
Pfp−/− | ND | ND | ND | 2.6±0.7 | 73±5.1 |
Gld | ND | ND | ND | 1.7±0.4 | 80±0.6 |
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