Abstract

The ATP Degradation System in Acute Tissue Injury Candidate: The candidate is an assistant professor who has demonstrated clinical and teaching excellence. He has started his full time research training, and requests this grant to complete his development to an independent investigator. Environment: The three co-sponsors as well as the extensive interest at the University of Michigan in acute tissue injury and purine biochemistry provide an exceptional site for research development. Research: Aberrations in various cellular structures and metabolic pathways have been implicated in the pathogenesis of acute tissue injury. One system likely to play a role in acute tissue injury is the adenosine triphosphate (ATP) degradation cascade and its associated enzyme xanthine oxidase. Although the initial insults are different, ATP degradation may be important in the final mechanism of injury in two seemingly separate syndromes: adult respiratory distress syndromes (ARDS) and acute myocardial ischemia. ATP degradation leads to the accumulation of purine intermediates the amount of cellular damage, they may augment or suppress other injury generating systems, and their depletion may limit resynthesis of ATP, thus impairing cellular metabolism. Furthermore, accumulating hypoxanthine and xanthine provide increased substrate for the enzyme xanthine oxidase, which can cause direct tissue damage via reactive oxygen metabolites. I therefore hypothesize that ATP degradation is important in acute tissue injury. I plan to test this hypothesis in two isolated perfused organ systems.
My specific aims are: 1) To examine the role of the ATP degradation system in an acute isolated model of lung injury. I will determine the degree of ATP degradation, the activation of xanthine oxidase, the release of oxygen metabolites and the effect of xanthine oxidase blockade. 2) To study the role of ATP degradation and xanthine oxidase activation in an isolated perfused heart model of acute ischemia injury. I will determine the degree of ATP degradation, the amount of H202 production and the effect of allopurinol administration of these mechanisms. We hope that the resultant improvements in our understanding of ATP degradation, will lead to novel therapeutic interventions in humans with acute myocardial ischemia or ARDS.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Clinical Investigator Award (CIA) (K08)
Project #
5K08HL001930-05
Application #
3082352
Study Section
Research Manpower Review Committee (MR)
Project Start
1987-05-15
Project End
1992-05-14
Budget Start
1991-05-15
Budget End
1992-05-14
Support Year
5
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Type
Schools of Medicine
DUNS #
791277940
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Grum, C M (1993) Tissue oxygenation in low flow states and during hypoxemia. Crit Care Med 21:S44-9
Ljungman, A G; Grum, C M; Deeb, G M et al. (1991) Inhibition of cyclooxygenase metabolite production attenuates ischemia-reperfusion lung injury. Am Rev Respir Dis 143:610-7
Shlafer, M; Brosamer, K; Forder, J R et al. (1990) Cerium chloride as a histochemical marker of hydrogen peroxide in reperfused ischemic hearts. J Mol Cell Cardiol 22:83-97
Grum, C M; Gross, T J; Mody, C H et al. (1990) Expression of xanthine oxidase activity by murine leukocytes. J Lab Clin Med 116:211-8
Ketai, L H; Grum, C M; Supinski, G S (1990) Tissue release of adenosine triphosphate degradation products during shock in dogs. Chest 97:220-6
Deeb, G M; Grum, C M; Lynch, M J et al. (1990) Neutrophils are not necessary for induction of ischemia-reperfusion lung injury. J Appl Physiol 68:374-81
Grum, C M; Gallagher, K P; Kirsh, M M et al. (1989) Absence of detectable xanthine oxidase in human myocardium. J Mol Cell Cardiol 21:263-7
Badellino, M M; Morganroth, M L; Grum, C M et al. (1989) Hypothermia or continuous ventilation decreases ischemia-reperfusion injury in an ex vivo rat lung model. Surgery 105:752-60
Lynch, M J; Grum, C M; Gallagher, K P et al. (1988) Xanthine oxidase inhibition attenuates ischemic-reperfusion lung injury. J Surg Res 44:538-44