Abstract

The goal of this project is to test novel therapeutic strategies to combat accelerated graft (Tx) rejection and to dissect cellular/humoral cascade contributing to this fulminant immune response in sensitized hosts. The study uses agents targeting selectively CD4 and/or CD25 (IL-2R) cell surface molecules + low doses of CsA in the treatment of presensitized rat recipients of heterotopic cardiac Tx.
The specific aims are: (1) To determine the effectiveness of CD4/CD25 targeted therapies in preventing/treating accelerated Tx loss: Dose response and time course studies for panels of CD4/CD25 mAbs distinct epitope/isotype specificities will be conducted to erase sensitization and abrogate otherwise 24-36h accelerated Tx rejection. CD4 (BWH-4) and CD25 (ART-18) mAbs proved highly effective in pilot experiments, stressing the importance of these new potential targets for immunosuppression in sensitized recipients. (2) To devise principles of optimal mAb selection for therapeutic use: First, radioactive tracer studies with CD4/CD25 mAbs will be performed in sensitized rats and biodistribution patterns correlated with their in vivo efficacy. Second, mAb mediated elimination vs. modulation/inhibition of target cell function will be addressed by comparing the in vivo effects of intact mAb and its F(ab')2 fragments, and analyzing cell phenotype in lymphoid tissues and at the Tx by FMF and immunohistology. (3) To evaluate the effects of applied therapies upon host cell mediated immunity: The in vitro (LMC, MLR, FMF, immunohistology) and in vivo (adoptive transfer) assays will be used to unravel putative feedbacks between mAb(s) and host cell repertoire. Sparing of cells of T suppressor circuit will be studied in parallel with screening for cell alloaggressive functions; the effects of individual cell subsets will be contrasted. (4) To explore the cytokine network in unmodified/mAb conditioned recipients: Two approaches will be undertaken to delineate the contribution of cytokines to accelerated rejection. First, intra-Tx production of cytokines will be assessed by immunohistology. Second, cytokine transcriptional events will be studied in RNA extracted from the Tx/spleen by Northern blot analysis, hybridization with cDNA probes and amplification by PCR. (5) To assess the effects of mAb treatment upon host humoral immunity: The kinetics of anti-donor Ig responses in untreated/mAb treated recipients will be proved by serial screening of sera by FMF, CDC, ADCC and in adoptive transfer studies. Intra-Tx elaboration of IgG, IgM, C3 will be followed by immunohistology. Anti-Ig, anti-idiotype (Id) and anti-Id-Id responses in mAb treated hosts will be evaluated by ELISA techniques.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
2R01AI023847-04
Application #
3136310
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Project Start
1988-04-01
Project End
1996-03-31
Budget Start
1991-09-30
Budget End
1992-03-31
Support Year
4
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
Harvard University
Department
Type
Schools of Medicine
DUNS #
082359691
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Ji, Haofeng; Shen, Xiu-Da; Gao, Feng et al. (2011) Alloreactive CD8 T-cell primed/memory responses and accelerated graft rejection in B-cell-deficient sensitized mice. Transplantation 91:1075-81
Shen, Xiu-Da; Ke, Bibo; Uchida, Yoichiro et al. (2011) Native macrophages genetically modified to express heme oxygenase 1 protect rat liver transplants from ischemia/reperfusion injury. Liver Transpl 17:201-10
Uchida, Yoichiro; Freitas, Maria Cecilia S; Zhao, Danyun et al. (2010) The protective function of neutrophil elastase inhibitor in liver ischemia/reperfusion injury. Transplantation 89:1050-6
Yamaura, K; Boenisch, O; Watanabe, T et al. (2010) Differential requirement of CD27 costimulatory signaling for naïve versus alloantigen-primed effector/memory CD8+ T cells. Am J Transplant 10:1210-20
Uchida, Yoichiro; Ke, Bibo; Freitas, Maria Cecilia S et al. (2010) T-cell immunoglobulin mucin-3 determines severity of liver ischemia/reperfusion injury in mice in a TLR4-dependent manner. Gastroenterology 139:2195-206
Ji, Haofeng; Shen, Xiuda; Gao, Feng et al. (2010) Programmed death-1/B7-H1 negative costimulation protects mouse liver against ischemia and reperfusion injury. Hepatology 52:1380-9
Ke, Bibo; Shen, Xiu-Da; Gao, Feng et al. (2010) Adoptive transfer of ex vivo HO-1 modified bone marrow-derived macrophages prevents liver ischemia and reperfusion injury. Mol Ther 18:1019-25
Uchida, Yoichiro; Ke, Bibo; Freitas, Maria Cecilia S et al. (2010) The emerging role of T cell immunoglobulin mucin-1 in the mechanism of liver ischemia and reperfusion injury in the mouse. Hepatology 51:1363-72
Ke, Bibo; Shen, Xiu-Da; Gao, Feng et al. (2009) Small interfering RNA targeting heme oxygenase-1 (HO-1) reinforces liver apoptosis induced by ischemia-reperfusion injury in mice: HO-1 is necessary for cytoprotection. Hum Gene Ther 20:1133-42
Shen, Xiuda; Wang, Yue; Gao, Feng et al. (2009) CD4 T cells promote tissue inflammation via CD40 signaling without de novo activation in a murine model of liver ischemia/reperfusion injury. Hepatology 50:1537-46

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