Abstract

Ischemia is a widespread and important clinical problem manifested in diverse conditions such as hemorrhagic shock, myocardial infarction, stroke, or local tissue trauma. After reperfusion, a period of microcirculatory no-reflow often ensues, leading to deterioration of microvascular and organ function. Leukocyte adhesion and cytotoxic release are important determinants of the reperfusion injury, but the role of leukocyte deformability and attendant capillary plugging in the injury remains controversial. This study is designed to test the central hypothesis that leukocyte deformability is a significant determinant of the microvascular resistance and tissue injury under pathological conditions and that alterations in cell deformability are primarily mediated by reorganization of the cell cytoskeleton. The long-range goal is to advance understanding of the cellular mechanisms responsible for deterioration of microvascular function in low-flow organ pathology.
The specific aims of the research are to measure the leukocyte deformability in vivo, the frequency and duration of leukocyte-capillary plugging, the microvascular resistance, and the extent of tissue injury during leukocyte activation by the chemoattractant peptide FMLP, and in a model of local ischemia and reperfusion in skeletal muscle, both with and without leukocyte cytoskeletal reorganization. Intravital microscopy of the rat spinotrapezius muscle will be employed to measure l) microvascular pressure gradients across single leukocyte-capillary entrance plugs using a dual micropuncture technique, 2) leukocyte plug dimensions and durations and vessel dimensions using video methods, and 3) propidium iodide uptake by non-viable skeletal muscle cells using fluorescence imaging. The measurements allow determination of the leukocyte deformability, the extent of leukocyte-capillary plugging, the microvascular resistance in arteriovenous capillary units, and the distribution of tissue injury in the same units. Using cytochalasin-D, colchicine, and pentoxifylline in conjunction with the FMLP and ischemia-reperfusion protocols, a test will be made of the hypothesis that leukocyte deformability is a significant determinant of microvascular resistance under pathological conditions, and that reorganization of cytoskeletal F-actin mediates the deformability changes. Histological reconstruction of serial sections will be used to determine the cellular composition of permanent plugs. Finally, using a hemodynamic computer network model to link the measured cell deformabilities to microvascular resistance changes, a test will made of the hypothesis that the macroscopic no-reflow response is quantitatively related to underlying changes in leukocyte cytoskeletal properties. The capability to link cellular or microcirculatory events to macroscopic organ hemodynamics provides a basis for understanding the relative roles of cell cytoskeletal reorganization and adhesion/cytotoxic release in ischemic injury, leading ultimately to improved therapeutic measures.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL049146-02
Application #
2225256
Study Section
Experimental Cardiovascular Sciences Study Section (ECS)
Project Start
1994-04-01
Project End
1997-03-31
Budget Start
1995-04-01
Budget End
1996-03-31
Support Year
2
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
University of Virginia
Department
Biomedical Engineering
Type
Schools of Engineering
DUNS #
001910777
City
Charlottesville
State
VA
Country
United States
Zip Code
22904

  Publications

Kadambi, A; Skalak, T C (2000) Role of leukocytes and tissue-derived oxidants in short-term skeletal muscle ischemia-reperfusion injury. Am J Physiol Heart Circ Physiol 278:H435-43
Price, R J; Skalak, T C (1998) Arteriolar remodeling in skeletal muscle of rats exposed to chronic hypoxia. J Vasc Res 35:238-44
Zeller, P J; Skalak, T C (1998) Contribution of individual structural components in determining the zero-stress state in small arteries. J Vasc Res 35:8-17
Linka, A Z; Skyba, D M; Price, R J et al. (1998) Spontaneous redistribution after reperfusion: a unique property of AIP 201, an ultrasound contrast agent. J Am Coll Cardiol 32:1765-72
Price, R J; Skalak, T C (1998) Distribution of cellular proliferation in skeletal muscle transverse arterioles during maturation. Microcirculation 5:39-47
Skyba, D M; Camarano, G; Goodman, N C et al. (1996) Hemodynamic characteristics, myocardial kinetics and microvascular rheology of FS-069, a second-generation echocardiographic contrast agent capable of producing myocardial opacification from a venous injection. J Am Coll Cardiol 28:1292-300
Harris, A G; Skalak, T C (1996) Effects of leukocyte capillary plugging in skeletal muscle ischemia-reperfusion injury. Am J Physiol 271:H2653-60
Skalak, T C; Price, R J (1996) The role of mechanical stresses in microvascular remodeling. Microcirculation 3:143-65
Price, R J; Skalak, T C (1996) Chronic alpha 1-adrenergic blockade stimulates terminal and arcade arteriolar development. Am J Physiol 271:H752-9
Price, R J; Skalak, T C (1995) A circumferential stress-growth rule predicts arcade arteriole formation in a network model. Microcirculation 2:41-51