Serine Protease Inhibitor-6 Differentially Affects the Survival of Effector and Memory Alloreactive CD8-T Cells

被引:10
|
作者
Azzi, J. [1 ]
Ohori, S.
Ting, C.
Uehara, M.
Abdoli, R.
Smith, B. D.
Safa, K.
Solhjou, Z.
Lukyanchykov, P.
Patel, J.
McGrath, M.
Abdi, R.
机构
[1] Harvard Univ, Brigham & Womens Hosp, Sch Med, Transplantat Res Ctr,Renal Div, Boston, MA 02115 USA
基金
美国国家卫生研究院;
关键词
Basic (laboratory) research; science; immunobiology; organ transplantation in general; rejection: T cell-mediated (TCMR); T cell biology; GRANZYME-B INHIBITOR; PERFORIN-DEFICIENT MICE; REGULATORY T-CELLS; CYTOTOXICITY; REJECTION; HOMEOSTASIS; EXPRESSION; ALLOGRAFTS; TOLERANCE; GRANULES;
D O I
10.1111/ajt.13051
中图分类号
R61 [外科手术学];
学科分类号
摘要
The clonal expansion of effector T cells and subsequent generation of memory T cells are critical in determining the outcome of transplantation. While cytotoxic T lymphocytes induce direct cytolysis of target cells through secretion of Granzyme-B (GrB), they also express cytoplasmic serine protease inhibitor-6 (Spi6) to protect themselves from GrB that has leaked from granules. Here, we studied the role of GrB/Spi6 axis in determining clonal expansion of alloreactive CD8-T cells and subsequent generation of memory CD8-T cells in transplantation. CD8-T cells from Spi6(-/-) mice underwent more GrB mediated apoptosis upon alloantigen stimulation in vitro and in vivo following adoptive transfer into an allogeneic host. Interestingly, while OT1.Spi6(-/-) CD8 T cells showed significantly lower clonal expansion following skin transplants from OVA mice, there was no difference in the size of the effector memory CD8-T cells long after transplantation. Furthermore, lack of Spi6 resulted in a decrease of short-lived-effector-CD8-cells but did not impact the pool of memory-precursor-effector-CD8-cells. Similar results were found in heart transplant models. Our findings suggest that the final alloreactive CD8-memory-pool-size is independent from the initial clonal-proliferation as memory precursors express low levels of GrB and therefore are independent of Spi6 for survival. These data advance our understanding of memory T cells generation in transplantation and provide basis for Spi6 based strategies to target effector T cells. Using in vitro and in vivo murine heart and skin transplant models, this study describes the key role of the serine protease inhibitor-6 in protecting CD8 alloreactive cytotoxic T cells from granzyme B-mediated self-inflicted damage. See editorial by Ashton-Rickardt on page .
引用
收藏
页码:234 / 241
页数:8
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