Abstract

The goal of this proposed research project is to develop a non-invasive method to detect early signs of acute graft rejection in solid-organ transplantation, specifically by nuclear magnetic resonance (NMR) techniques, such as magnetic resonance imaging (MRI) and magnetic resonance spectroscopy (MRS). In order to achieve our goal, we have assembled an interdisciplinary team consisting of three interactive laboratories: (I) Chien Ho, Ph.D. of Carnegie Mellon University, a biochemist-biophysicist, and an expert in applying MRI and MRS techniques to biomedical problems; (ii) Suzanne T. lldstad, M.D. of the University of Pittsburgh, a surgeon, an immunologist, and an expert in transplantation tolerance, stem cell biology, and xenotransplantation; and (iii) Pedro J. del Nido, M.D. of Harvard Medical School and Children's Hospital of Boston, a cardiac surgeon and an expert in pediatric heart surgery, heart transplantation, and organ rejection. These three researchers have complementary expertise, have carried out collaborative research during the past three years, and have published joint scientific papers. Despite significant advances in immunosuppressive therapy for the control of graft rejection, the diagnosis of rejection remains the most difficult aspect in the management of transplant patients. Tissue biopsy is generally accepted as the """"""""gold standard"""""""" in the diagnosis of graft rejection. The use of tissue biopsies to monitor graft rejection is not only invasive, but also has other limitations and complications. Early in acute rejection, the cellular invasion process is commonly focal, affecting a discrete area of the organ. The focal nature of the early rejection process increases the likelihood of sampling error when performing a tissue biopsy. Multiple biopsies are often required, thus increasing the risk of complications, especially in pediatric patients. Our working hypothesis is that if we can develop a non-invasive method to track the movement of T-cells to the site of graft rejection, we will have a non- invasive technique to detect the early signs of organ rejection. We have chosen the rat model as our experimental system.
The specific aims of our proposed research will include the following projects: (I) to optimize the labeling of isolated T-cells with suitable MRI contrast agents, (ii) to improve the MRI detection of iron-oxide labeled T-cells; (iii) to develop MRI techniques needed for tracking T-cells labeled with various MRI contrast agents in cardiac and renal transplantations; (iv) to determine the early signs of acute rejection by comparing the MRI results (obtained from tracking T-cell movement and organ perfusion studies) with those from 31P-MRS and the conventional histological findings; and (v) to investigate immunosuppressant effects on the rat transplant model and to correlate these findings with MRI, MRS, and histological results. If our proposed approach is successful, we have high hopes of developing our methodology as a non-invasive diagnostic tool for detecting early signs of acute rejection in organ transplantation in humans. Thus, a reliable, non- invasive diagnostic technique to detect early signs of graft rejection will allow physicians more time to administer appropriate immunosuppressants therapy to prevent and to control graft rejection.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Center for Research Resources (NCRR)
Type
Research Project (R01)
Project #
1R01RR010962-01
Application #
2286549
Study Section
Biomedical Research Technology Review Committee (BRC)
Project Start
1995-09-01
Project End
1998-08-31
Budget Start
1995-09-01
Budget End
1996-08-31
Support Year
1
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Carnegie-Mellon University
Department
Type
Organized Research Units
DUNS #
052184116
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

Kochanek, Patrick M; Hendrich, Kristy S; Jackson, Edwin K et al. (2005) Characterization of the effects of adenosine receptor agonists on cerebral blood flow in uninjured and traumatically injured rat brain using continuous arterial spin-labeled magnetic resonance imaging. J Cereb Blood Flow Metab 25:1596-612
Dodd, Stephen J; Ho, Chien (2002) Short planar gradient coils for MR microscopy using concentric return paths. J Magn Reson 156:1-9
Kochanek, P M; Hendrich, K S; Robertson, C L et al. (2001) Assessment of the effect of 2-chloroadenosine in normal rat brain using spin-labeled MRI measurement of perfusion. Magn Reson Med 45:924-9
Kanno, S; Lee, P C; Dodd, S J et al. (2000) A novel approach with magnetic resonance imaging used for the detection of lung allograft rejection. J Thorac Cardiovasc Surg 120:923-34
Zhang, Y; Dodd, S J; Hendrich, K S et al. (2000) Magnetic resonance imaging detection of rat renal transplant rejection by monitoring macrophage infiltration. Kidney Int 58:1300-10
Yoshida, S; Dodd, S J; del Nido, P J et al. (1999) Cardiac function of transplanted rat hearts using a working heart model assessed by magnetic resonance imaging. J Heart Lung Transplant 18:1054-64
Dodd, S J; Williams, M; Suhan, J P et al. (1999) Detection of single mammalian cells by high-resolution magnetic resonance imaging. Biophys J 76:103-9
Hendrich, K S; Kochanek, P M; Williams, D S et al. (1999) Early perfusion after controlled cortical impact in rats: quantification by arterial spin-labeled MRI and the influence of spin-lattice relaxation time heterogeneity. Magn Reson Med 42:673-81
Yoshida, S; Takeuchi, K; del Nido, P J et al. (1998) Diastolic dysfunction coincides with early mild transplant rejection: in situ measurements in a heterotopic rat heart transplant model. J Heart Lung Transplant 17:1049-56
Wang, J J; Hendrich, K S; Jackson, E K et al. (1998) Perfusion quantitation in transplanted rat kidney by MRI with arterial spin labeling. Kidney Int 53:1783-91

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