Abstract

Disrupting the CD40-CD40L pathway is an effective means to prolong allograft survival. However, the majority of studies have disrupted the pathway by targeting CD40L with anti-CD40L mAb or the use of CD40L-/- mice. Hence, the individual contributions of CD40 vs. CD40L to the rejection process have not been defined. The use of anti-CD40L mAb is frequently referred to as a blockade"""""""" of the CD40-CD40L 'pathway, implying a physical disruption of the interactions between these molecules. In fact, the precise mechanisms by which anti-CD40L mAb mediate their protective effects have not been established. Evidence suggests that anti-CD40L mAb may induce apoptosis of T cells or may result in complement-mediated cytolysis of T cells. Much less is known about the role of CD40 in the rejection response. The overall hypothesis of this proposal is that disrupting CD40-CD40L interactions by targeting CD40 vs. CD40L yields distinct immunological outcomes, which differentially impact long-term graft acceptance. Hence, the proposed studies will define individual roles for CD40 and CD40L in the mouse vascularized cardiac allograft model. Specifically, CD40-/- mice, agonistic anti-CD40 mAb, CD40L-/- mice, and anti-CD40L mAb will be employed in conjunction with donor-derived dendritic cells (DC) to elucidate the roles of CD40 and CD40L, and how DC bypass the need for this pathway in the rejection process.
Specific Aim 1 will directly assess the roles of donor and recipient CD40 to rejection by combining agonistic anti-CD40 mAb with CD40-1- donors or recipients, CD40L-/- recipients, or recipient treatment with anti-CD40L mAb. The contributions of donor DC and recipient CD4+ and CD8+ cells will be investigated.
Specific Aim 2 will address the mechanism of action of anti-CD40L mAb using Bcl-xL transgenic mice (T cells resistant to apoptosis), complement -/- mice (no complement mediated cytolysis), and CD40-/- mice (to investigate direct effects of anti-CD40L).
Specific Aim 3 will test the hypothesis that distinct forms of regulation develop when CD40 vs. CD40L is targeted to promote long-term graft acceptance. Identifying the mechanisms by which CD40 and CD40L contribute to rejection should facilitate development of therapies that target this critical pathway in transplant rejection.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI061469-03
Application #
7083746
Study Section
Special Emphasis Panel (ZRG1-SRB-G (02))
Program Officer
Kehn, Patricia J
Project Start
2004-07-01
Project End
2009-06-30
Budget Start
2006-07-01
Budget End
2007-06-30
Support Year
3
Fiscal Year
2006
Total Cost
$319,790
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Surgery
Type
Schools of Medicine
DUNS #
073133571
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Booth, Adam Jared; Grabauskiene, Svetlana; Wood, Sherri Chan et al. (2011) IL-6 promotes cardiac graft rejection mediated by CD4+ cells. J Immunol 187:5764-71
Burrell, Bryna E; Bishop, D Keith (2010) Th17 cells and transplant acceptance. Transplantation 90:945-8
Booth, A J; Csencsits-Smith, K; Wood, S C et al. (2010) Connective tissue growth factor promotes fibrosis downstream of TGFbeta and IL-6 in chronic cardiac allograft rejection. Am J Transplant 10:220-30
Booth, Adam J; Bishop, D Keith (2010) TGF-beta, IL-6, IL-17 and CTGF direct multiple pathologies of chronic cardiac allograft rejection. Immunotherapy 2:511-20
Diaz, J A; Booth, A J; Lu, G et al. (2009) Critical role for IL-6 in hypertrophy and fibrosis in chronic cardiac allograft rejection. Am J Transplant 9:1773-83
Burrell, Bryna E; Lu, Guanyi; Li, Xian C et al. (2009) OX40 costimulation prevents allograft acceptance induced by CD40-CD40L blockade. J Immunol 182:379-90
Faust, Susan M; Lu, Guanyi; Wood, Sherri C et al. (2009) TGFbeta neutralization within cardiac allografts by decorin gene transfer attenuates chronic rejection. J Immunol 183:7307-13
Faust, Susan M; Lu, Guanyi; Marini, Bernard L et al. (2009) Role of T cell TGFbeta signaling and IL-17 in allograft acceptance and fibrosis associated with chronic rejection. J Immunol 183:7297-306
Burrell, Bryna E; Csencsits, Keri; Lu, Guanyi et al. (2008) CD8+ Th17 mediate costimulation blockade-resistant allograft rejection in T-bet-deficient mice. J Immunol 181:3906-14
Welling, Theodore H; Lu, Guanyi; Csencsits, Keri et al. (2008) Regulation of alloimmune Th1 responses by the cyclin-dependent kinase inhibitor p21 following transplantation. Surgery 143:394-403

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