Abstract

The investigators have shown previously that after whole organ transplantation, resident bone marrow- derived """"""""passenger leukocytes"""""""" migrate out of the graft into the recipient and establish microchimerism. Furthermore, the ubiquitous presence of the donor chimeric cells in the tissues of long functioning allograft recipients, suggested that these cells may play a seminal role in graft acceptance and the induction of donor-specific tolerance. In a direct extension of this """"""""natural"""""""" phenomenon, they have augmented the leukocyte load conveyed by the transplanted organs by treating a pilot group of 89 human recipients of liver, kidney, heart, lung, and pancreas allografts with simultaneous infusion of unmodified bone marrow cells (3 - 5 x 108/kg body weight). Fifty-nine patients in whom consent to harvest donor vertebral bodies was not available, served as contemporaneous controls. The patients did not receive any cytoablative or cytoreductive conditioning prior to transplantation, and were maintained on routine immunosuppression with TacrolimusTM and steroids after transplantation. The adjuvant procedure of bone marrow augmentation was safe. The patient and graft survival, according to the investigators, was substantially improved in the augmented group as compared to the controls. The frequency and severity of rejection was also comparable in both study and control groups. Furthermore, a higher level of chimerism and increased frequency of donor-specific immune modulation was witnessed in the augmented patients. Based on these and other observations, they hypothesize that both short and long-term allograft survival and function will improve in bone marrow augmented patients. Additionally, augmentation of chimerism may also reduce the rate of chronic rejection and most importantly endow the investigators with the capacity to wean or eventually withdraw immuno-suppression. They propose a systematic evaluation of donor bone marrow augmentation in liver transplant recipients and to compare the outcome with that of non-augmented contemporaneous controls. In addition, the outcome in the bone marrow-liver cohort will be compared with that of bone marrow augmented recipients of other organs (i.e., kidney, heart, pancreas, lung, etc.); each of these will also acquire their own non-augmented organ-specific controls. The primary end-points that are to be examined are: (a) organ function and survival, (b) patient survival, and (c) the ability to reduce or withdraw immunosuppression. Secondarily, they also wish to monitor the frequency and severity of rejection, as well as that of GVHD. They will serially quantitate levels of donor cell chimerism and assess the immune status of these patients. These primary and secondary end-points will be correlated to obtain comprehensive information regarding the eventual outcome of bone-marrow augmented and control patients.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI040329-05
Application #
6170285
Study Section
Special Emphasis Panel (ZRG7-SB (01))
Program Officer
Rose, Stephen M
Project Start
1996-04-01
Project End
2001-03-31
Budget Start
2000-04-01
Budget End
2001-03-31
Support Year
5
Fiscal Year
2000
Total Cost
$314,178
Indirect Cost

  Institution

Name
University of Pittsburgh
Department
Surgery
Type
Schools of Medicine
DUNS #
004514360
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

Koike, Chihiro; Fung, John J; Geller, David A et al. (2002) Molecular basis of evolutionary loss of the alpha 1,3-galactosyltransferase gene in higher primates. J Biol Chem 277:10114-20
Koike, C; Friday, R; Fung, J J et al. (2001) Comparison of the regulatory regions of the alpha1,3galactosyltransferase gene between murine and porcine species. Transplant Proc 33:710-1
Bellamy, C O; DiMartini, A M; Ruppert, K et al. (2001) Liver transplantation for alcoholic cirrhosis: long term follow-up and impact of disease recurrence. Transplantation 72:619-26
Lunz 3rd, J G; Contrucci, S; Ruppert, K et al. (2001) Replicative senescence of biliary epithelial cells precedes bile duct loss in chronic liver allograft rejection: increased expression of p21(WAF1/Cip1) as a disease marker and the influence of immunosuppressive drugs. Am J Pathol 158:1379-90
Jain, A; Demetris, A J; Kashyap, R et al. (2001) Does tacrolimus offer virtual freedom from chronic rejection after primary liver transplantation? Risk and prognostic factors in 1,048 liver transplantations with a mean follow-up of 6 years. Liver Transpl 7:623-30
Koike, C; Friday, R P; Nakashima, I et al. (2000) Isolation of the regulatory regions and genomic organization of the porcine alpha1,3-galactosyltransferase gene. Transplantation 70:1275-83
Pham, S M; Rao, A S; Zeevi, A et al. (2000) A clinical trial combining donor bone marrow infusion and heart transplantation: intermediate-term results. J Thorac Cardiovasc Surg 119:673-81
Starzl, T E; Murase, N; Demetris, A et al. (2000) The mystique of hepatic tolerogenicity. Semin Liver Dis 20:497-510
Pham, S M; Rao, A S; Zeevi, A et al. (2000) Effects of donor bone marrow infusion in clinical lung transplantation. Ann Thorac Surg 69:345-50
Gandhi, C R; Kuddus, R; Subbotin, V M et al. (1999) A fresh look at augmenter of liver regeneration in rats. Hepatology 29:1435-45

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