Hannah Valantine-von Kaeppler
Academic Appointments
Appointment
Organization
Professor - Med Center Line
Member
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Administrative Appointments
Title
Organization
Start Year
End Year
President, Western State Affiliation
American Heart Association
2004
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Senior Associate Dean for Diversity and Faculty Development
School of Medicine
2005
-
Professional Education
Degree
Awarding Institution
Field of Study
Year of Graduation
MBBS
St Georges Hosp/London Univ, UK
Medicine (MD equivalent)
1978
MRCP
London University, London, UK
Internal Medicine
1982
Registrar
Hammersmith Hospital, London, UK
Cardiology Fellow
1984
Fellow
Stanford University
Cardiology
1986
MD
London University, London, UK
Cardiology (PhD equivalent)
1988
Research Interests
My lab is focused on understanding the mechanism mediating acute and chronic allograft failure, in particular on the role of microvascular injury in acute allograft failure and the mechanisms of mediating transplant coronary artery disease.
1. Role of microvascular injury in acute allograft failure. We observed decreased cardiac allograft function in patients to be significantly associated with loss of microvascular cell surface markers, consistent with altered biology of the vascular endothelium or injury, and with up-regulation of cytokines such as IL-6, IL-10, TGF-b, and TNF-a. Decreased cardiac allograft function, in particular diastolic dysfunction, was highly predictive of allograft vascular disease and poor outcome in long-term patients. To further characterize cellular and molecular mechanisms we developed quantitative methods to monitor allograft function and correlate it with cytokine expression in a rat heterotopic transplant model. We developed echocardiographic markers of systolic and diastolic function and found decreasing systolic and diastolic function highly correlated with up-regulation of IL-6 expression. Correlation with other key cytokines is now being examined. Future studies will determine if up-regulation of cytokine expression occurs in vascular endothelial cells or endogenous cells of the graft vs. infiltrating mononuclear cells. We will then inhibit transcription genes and block translation with cytokine monoclonal antibodies.
2. Mechanisms mediating allograft dysfunction. We observed the major risk factors for transplant atherosclerosis in patients to be metabolic (hyperglycemia, hypertriglyceridemia, and low HDL). To further study cellular and molecular mechanisms mediating this process, we recapitulated metabolic abnormalities in the rat heart transplant model and confirmed rapid development of transplant atherosclerosis. Later we will characterize the cytokines involved in metabolically deranged animals which develop rapid atherosclerosis, and examine the relative contributions of hyperlipidemia, hyperglycemia, and alloimmunity in this new model of transplant atherosclerosis.
1. Role of microvascular injury in acute allograft failure. We observed decreased cardiac allograft function in patients to be significantly associated with loss of microvascular cell surface markers, consistent with altered biology of the vascular endothelium or injury, and with up-regulation of cytokines such as IL-6, IL-10, TGF-b, and TNF-a. Decreased cardiac allograft function, in particular diastolic dysfunction, was highly predictive of allograft vascular disease and poor outcome in long-term patients. To further characterize cellular and molecular mechanisms we developed quantitative methods to monitor allograft function and correlate it with cytokine expression in a rat heterotopic transplant model. We developed echocardiographic markers of systolic and diastolic function and found decreasing systolic and diastolic function highly correlated with up-regulation of IL-6 expression. Correlation with other key cytokines is now being examined. Future studies will determine if up-regulation of cytokine expression occurs in vascular endothelial cells or endogenous cells of the graft vs. infiltrating mononuclear cells. We will then inhibit transcription genes and block translation with cytokine monoclonal antibodies.
2. Mechanisms mediating allograft dysfunction. We observed the major risk factors for transplant atherosclerosis in patients to be metabolic (hyperglycemia, hypertriglyceridemia, and low HDL). To further study cellular and molecular mechanisms mediating this process, we recapitulated metabolic abnormalities in the rat heart transplant model and confirmed rapid development of transplant atherosclerosis. Later we will characterize the cytokines involved in metabolically deranged animals which develop rapid atherosclerosis, and examine the relative contributions of hyperlipidemia, hyperglycemia, and alloimmunity in this new model of transplant atherosclerosis.
Publications
- Kuppahally SS, Hunt SA, Valantine HA, Berry GJ "Recurrence of iron deposition in the cardiac allograft in a patient with non-HFE hemochromatosis." J Heart Lung Transplant 2006; 25: 1: 144-7 More »
- Kuppahally S, Al-Khaldi A, Weisshaar D, Valantine HA, Oyer P, Robbins RC, Hunt SA "Wound healing complications with de novo sirolimus versus mycophenolate mofetil-based regimen in cardiac transplant recipients." Am J Transplant 2006; 6: 5: 986-92 More »
- Ma IW, Valantine HA, Shibata A, Waskerwitz J, Dafoe DC, Alfrey EJ, Tan JC, Millan M, Busque S, Scandling JD "Validation of a screening protocol for identifying low-risk candidates with type 1 diabetes mellitus for kidney with or without pancreas transplantation." Clin Transplant 2006; 20: 2: 139-46 More »
- Potena L, Holweg CT, Chin C, Luikart H, Weisshaar D, Narasimhan B, Fearon WF, Lewis DB, Cooke JP, Mocarski ES, Valantine HA "Acute Rejection and Cardiac Allograft Vascular Disease Is Reduced by Suppression of Subclinical Cytomegalovirus Infection." Transplantation 2006; 82: 3: 398-405 More »
- Fearon WF, Hirohata A, Nakamura M, Luikart H, Lee DP, Vagelos RH, Hunt SA, Valantine HA, Fitzgerald PJ, Yock PG, Yeung AC "Discordant Changes in Epicardial and Microvascular Coronary Physiology After Cardiac Transplantation: Physiologic Investigation for Transplant Arteriopathy II (PITA II) Study." J Heart Lung Transplant 2006; 25: 7: 765-771 More »
86 publications: view full list