PKCθ is required for alloreactivity and GVHD but not for immune responses toward leukemia and infection in mice
Javier O. Valenzuela, Cristina Iclozan, Mohammad S. Hossain, Martin Prlic, Emily Hopewell, Crystina C. Bronk, Junmei Wang, Esteban Celis, Robert W. Engelman, Bruce R. Blazar, Michael J. Bevan, Edmund K. Waller, Xue-Zhong Yu, Amer A. Beg
Javier O. Valenzuela, Cristina Iclozan, Mohammad S. Hossain, Martin Prlic, Emily Hopewell, Crystina C. Bronk, Junmei Wang, Esteban Celis, Robert W. Engelman, Bruce R. Blazar, Michael J. Bevan, Edmund K. Waller, Xue-Zhong Yu, Amer A. Beg
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Research Article Immunology

PKCθ is required for alloreactivity and GVHD but not for immune responses toward leukemia and infection in mice

Abstract

When used as therapy for hematopoietic malignancies, allogeneic BM transplantation (BMT) relies on the graft-versus-leukemia (GVL) effect to eradicate residual tumor cells through immunologic mechanisms. However, graft-versus-host disease (GVHD), which is initiated by alloreactive donor T cells that recognize mismatched major and/or minor histocompatibility antigens and cause severe damage to hematopoietic and epithelial tissues, is a potentially lethal complication of allogeneic BMT. To enhance the therapeutic potential of BMT, we sought to find therapeutic targets that could inhibit GVHD while preserving GVL and immune responses to infectious agents. We show here that T cell responses triggered in mice by either Listeria monocytogenes or administration of antigen and adjuvant were relatively well preserved in the absence of PKC isoform θ (PKCθ), a key regulator of TCR signaling. In contrast, PKCθ was required for alloreactivity and GVHD induction. Furthermore, absence of PKCθ raised the threshold for T cell activation, which selectively affected alloresponses. Most importantly, PKCθ-deficient T cells retained the ability to respond to virus infection and to induce GVL effect after BMT. These findings suggest PKCθ is a potentially unique therapeutic target required for GVHD induction but not for GVL or protective responses to infectious agents.

Authors

Javier O. Valenzuela, Cristina Iclozan, Mohammad S. Hossain, Martin Prlic, Emily Hopewell, Crystina C. Bronk, Junmei Wang, Esteban Celis, Robert W. Engelman, Bruce R. Blazar, Michael J. Bevan, Edmund K. Waller, Xue-Zhong Yu, Amer A. Beg

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Figure 7

PKCθ–/– T cells can mount an effective anti-MCMV response after BMT.

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PKCθ–/– T cells can mount an effective anti-MCMV response after BMT. ...
Lethally irradiated CB6 recipients were transplanted with WT or PKCθ–/– (KO) TCD BM alone or with 5 × 106 splenocytes from WT or KO donors, respectively. 60 days after BMT, recipients were infected with MCMV, and MCMV tetramer–positive CD8 T cell numbers were determined after 10 days (A). Virus titers (B) were measured in recipient livers 10 days after infection. A few mice receiving BM alone were sacrificed on day 3 after infection to determine both tetramer-positive cells and virus titer in livers as indicated (BM on day 3). Horizontal bars indicate the averages of 3–5 mice in each group.