Abstract

The morbidity and mortality of sickle cell patients surviving to adulthood is directly related to ischemia and end organ damage induced by vascular occlusion. While episodic painful events are proposed to also result from microvascular occlusion, there is no associated quantitative increase in proportions of sickle erythrocytes during these events. Thus, beta-globin mutations causing sickle cell disease are necessary but not sufficient for vascular occlusion and do not directly induce the episodic symptoms associated with sickle cell disease. It is hypothesized that the episodic pain, organ flow abnormalities and acute chest syndrome occurring from sickle cell disease are due to defective nitric oxide (.NO)-dependent vascular relaxation. Preliminary observations support his concept in as much as plasma L-arginine, the precursor for .NO biosynthesis, is decreased, as are serum and plasma .NO metabolites, nitrate (N02) and nitrate (N03) in patients suffering from sickle cell disease. Additionally, homocysteine levels are elevated, with this amino acid metabolite a recognized risk factor for loss of endothelial function and venous/arterial occlusion. In order to establish the role of .NO in mediating the vascular pathobiology of patients suffering from sickle cell disease three Specific Aims will be pursued: 1. The role of .NO in impaired endothelial-dependent relaxation in a development of vaso-occlusive crisis and ischemic tissue damage will be determined in patients with sickle cell disease. 2. The therapeutic role of interventions designed to augment .NO-dependent endothelial relaxation in patients having sickle cell disease will be examined. This includes a prospective, randomized trial of L-arginine infusion in the treatment of acute vascular occlusive crisis, a prospective randomized trial of inhaled .NO for the treatment of acute chest syndrome and a prospective evaluation of therapies designed to lower homocysteine levels in adults with sickle cell disease. 3. Finally, in order to develop additional strategies for relieving blood flow abnormalities in sickle cell patients, the actions of critical modulators of .NO-dependent endothelial relaxation will be assessed in cultured vascular endothelium and a transgenic mouse model of sickle cell disease. Successful accomplishment of the proposed aims will provide fundamental mechanistic information regarding the pathogenesis of vascular abnormalities associated with sickle cell disease and will provide novel clinical strategies for treatment of sickle cell disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Comprehensive Center (P60)
Project #
5P60HL058418-03
Application #
6325971
Study Section
Project Start
2000-04-01
Project End
2001-03-31
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
3
Fiscal Year
2000
Total Cost
$162,688
Indirect Cost

  Institution

Name
University of Alabama Birmingham
Department
Type
DUNS #
004514360
City
Birmingham
State
AL
Country
United States
Zip Code
35294

  Publications

Coats, Mamie T; Benjamin, W H; Hollingshead, S K et al. (2005) Antibodies to the pneumococcal surface protein A, PspA, can be produced in splenectomized and can protect splenectomized mice from infection with Streptococcus pneumoniae. Vaccine 23:4257-62
Telfair, Joseph; Alexander, Leah R; Loosier, Penny S et al. (2004) Providers' perspectives and beliefs regarding transition to adult care for adolescents with sickle cell disease. J Health Care Poor Underserved 15:443-61
Briles, David E; Hollingshead, Susan K; Paton, James C et al. (2003) Immunizations with pneumococcal surface protein A and pneumolysin are protective against pneumonia in a murine model of pulmonary infection with Streptococcus pneumoniae. J Infect Dis 188:339-48
Liu, Enli; Jelinek, Jaroslav; Pastore, Yves D et al. (2003) Discrimination of polycythemias and thrombocytoses by novel, simple, accurate clonality assays and comparison with PRV-1 expression and BFU-E response to erythropoietin. Blood 101:3294-301
Aslan, Mutay; Ryan, Thomas M; Townes, Tim M et al. (2003) Nitric oxide-dependent generation of reactive species in sickle cell disease. Actin tyrosine induces defective cytoskeletal polymerization. J Biol Chem 278:4194-204
Lim, Dong Gun; Sweeney, Scott; Bloodsworth, Allison et al. (2002) Nitrolinoleate, a nitric oxide-derived mediator of cell function: synthesis, characterization, and vasomotor activity. Proc Natl Acad Sci U S A 99:15941-6
Coles, Barbara; Bloodsworth, Allison; Eiserich, Jason P et al. (2002) Nitrolinoleate inhibits platelet activation by attenuating calcium mobilization and inducing phosphorylation of vasodilator-stimulated phosphoprotein through elevation of cAMP. J Biol Chem 277:5832-40
Coles, Barbara; Bloodsworth, Allison; Clark, Stephen R et al. (2002) Nitrolinoleate inhibits superoxide generation, degranulation, and integrin expression by human neutrophils: novel antiinflammatory properties of nitric oxide-derived reactive species in vascular cells. Circ Res 91:375-81
Robinson, D Ashley; Briles, David E; Crain, Marilyn J et al. (2002) Evolution and virulence of serogroup 6 pneumococci on a global scale. J Bacteriol 184:6367-75
O'Donnell, V B; Freeman, B A (2001) Interactions between nitric oxide and lipid oxidation pathways: implications for vascular disease. Circ Res 88:12-21

Showing the most recent 10 out of 22 publications