Abstract

The hypothesis to be tested within this clinical Core and in Projects 1, 2 & 3 is that TA is triggered by HCMV. The projects will examine the direct and indirect effects of HCMV specifically focusing on how adaptive immune response to virus modulates the eNOS pathway. Because the various immunological and functional assays proposed in the individual projects will be correlated with TA in patients, and individual blood samples and heart biopsy specimens will be divided among the individual Principal Investigators for each project, we are proposing a Clinical Research Support Core. The Clinical Research Support Core will consist of Patient Management Core; Coronary Artery Disease Quantitation Laboratory; Specimen Processing, Virology/Immunopathology Laboratory; and Database Management Core. The function of the Clinical Research Support Core is to recruit subjects and assure that subjects? rights are respected; administer the protocol to ensure standardization of patient care, protocol adherence and long term follow-up; obtain quantitative data regarding progression to TA; provide centralized processing of blood and heart biopsy specimens (EMB); perform virological studies (culture and PCR); maintain a centralized database Clinical and laboratory results; and perform statistical analysis and modeling on the data. To aid in the recruitment of heart transplant patients we have established collaborations with one other heart transplant center (Cleveland Clinic) with whom we have a track record of collaborative research. The Coronary Artery Disease Quantitation Laboratory of the Clinical Research Support Core will implement protocols for intracoronary ultrasound recordings and analysis used in tracking progression to TA. The Virology/Immunopathology Laboratory will be composed of: 1) The specimen processing unit which will utilize a computer supported tracking system for logging and distribution of specimens to individual Project Principal Investigators. 2) A cell culture facility to maintain endothelial, smooth muscle, fibroblasts, and monocytes necessary to support all projects. 3) A virology unit to culture and isolate CMV from patient samples, and to perform assays to quantitate viral load. 4) An immunopathology unit to characterize the inflammatory cells and microvascular changes on EMB, extraction of nucleic acids, and determination of cytokine gene expression by in situ hybridization. A centralized database will be developed to capture clinical and assay information for analysis. The Clinical Research Support Core will allow for clinical study of the-subjects, the most efficient utilization of limited patient samples; and analysis of the combined data I obtained from clinical study as well as the results obtained from the individual projects.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI050153-02
Application #
6654553
Study Section
Special Emphasis Panel (ZAI1)
Project Start
2002-09-01
Project End
2003-06-30
Budget Start
Budget End
Support Year
2
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
Stanford University
Department
Type
DUNS #
800771545
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

Yang, Hyoung-Mo; Khush, Kiran; Luikart, Helen et al. (2016) Invasive Assessment of Coronary Physiology Predicts Late Mortality After Heart Transplantation. Circulation 133:1945-50
Okada, Kozo; Fearon, William F; Luikart, Helen et al. (2016) Attenuated-Signal Plaque Progression Predicts Long-Term Mortality After Heart Transplantation: IVUS Assessment of Cardiac Allograft Vasculopathy. J Am Coll Cardiol 68:382-92
Okada, Kozo; Kitahara, Hideki; Yang, Hyoung-Mo et al. (2015) Paradoxical Vessel Remodeling of the Proximal Segment of the Left Anterior Descending Artery Predicts Long-Term Mortality After Heart Transplantation. JACC Heart Fail 3:942-52
Haddad, François; Khazanie, Prateeti; Deuse, Tobias et al. (2012) Clinical and functional correlates of early microvascular dysfunction after heart transplantation. Circ Heart Fail 5:759-68
Yamasaki, Masao; Sakurai, Ryota; Hirohata, Atsushi et al. (2011) Impact of donor-transmitted atherosclerosis on early cardiac allograft vasculopathy: new findings by three-dimensional intravascular ultrasound analysis. Transplantation 91:1406-11
Holweg, Cécile T J; Potena, Luciano; Luikart, Helen et al. (2011) Identification and classification of acute cardiac rejection by intragraft transcriptional profiling. Circulation 123:2236-43
Tu, Wenwei; Lau, Yu-Lung; Zheng, Jian et al. (2008) Efficient generation of human alloantigen-specific CD4+ regulatory T cells from naive precursors by CD40-activated B cells. Blood 112:2554-62
Sinha, Seema S; Pham, Michael X; Vagelos, Randall H et al. (2008) Effect of rapamycin therapy on coronary artery physiology early after cardiac transplantation. Am Heart J 155:889.e1-6
Potena, Luciano; Fearon, William F; Sydow, Karsten et al. (2008) Asymmetric dimethylarginine and cardiac allograft vasculopathy progression: modulation by sirolimus. Transplantation 85:827-33
Sydow, Karsten; Mondon, Carl E; Schrader, Joerg et al. (2008) Dimethylarginine dimethylaminohydrolase overexpression enhances insulin sensitivity. Arterioscler Thromb Vasc Biol 28:692-7

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