Abstract

Hope of slowing the progression of renal disease has stimulated investigation into the mechanisms responsible for glomerular injury. A useful model is the rat subjected to partial nephrectomy. In this model, removal of a large portion of the renal mass results in elevation of the glomerular filtration rate in the remaining nephrons, due to increases in the glomerular capillary plasma flow rate and transcapillary hydraulic pressure gradient (delta P). These hemodynamic changes appear to be maladaptive, in that they are associated with progressive hypertension (HTN), proteinuria, and glomerular sclerosis. Therapeutic interventions which attenuate these hemodynamic changes (in particular, reduction in delta P) slow the progression of experimental renal disease. One factor which contributes to delta P is hematocrit; increasing hematocrit augments, and lowering of hematocrit lessens, systemic and glomerular HTN in rats with partial renal ablation. Patients with renal disease typically have low values for hematocrit. While anemia may have adverse systemic effects, correction of anemia often results in HTN. Anemia may in fact be a favorable renal adaptation, in that prevention of anemia in partially nephrectomized rats leads to aggravation of systemic and glomerular HTN, and acceleration of proteinuria and glomerular injury. This proposal will study the role of hematocrit and systemic and glomerular HTN in a number of experimental models of progressive renal disease. Renal disease is also accompanied by proteinuria. It has been suggested that interventions which reduce proteinuria do so by lowering delta P, but inability to measure delta P in humans has made interpretation of these observations difficult. Fractional clearance measurements of exogenous macromolecules provide an effective means of examining changes in proteinuria which accompany hemodynamic or structural changes. Using measurements of hemodynamic factors, including delta P, and fractional macromolecular clearances in the rat, we propose to derive methods for inferring delta P from hemodynamic parameters which can ultimately be applied in humans. Together, these approaches promise to provide important new strategies for the treatment of patients with renal disease, as well as useful methods for assessing efficacy of therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Program Projects (P01)
Project #
5P01DK040839-04
Application #
3840151
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
4
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
Brigham and Women's Hospital
Department
Type
DUNS #
071723621
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Kelley, V R; Strom, T B (1995) A paradigm 1994: the allograft response. Blood Purif 13:199-205
Ballermann, B J; Ott, M J (1995) Adhesion and differentiation of endothelial cells by exposure to chronic shear stress: a vascular graft model. Blood Purif 13:125-34
Yokoyama, H; Kreft, B; Kelley, V R (1995) Biphasic increase in circulating and renal TNF-alpha in MRL-lpr mice with differing regulatory mechanisms. Kidney Int 47:122-30
Yokoyama, H; Zheng, X; Strom, T B et al. (1994) B7(+)-transfectant tubular epithelial cells induce T cell anergy, ignorance or proliferation. Kidney Int 45:1105-12
Diamond, J R (1994) The adverse effects of cholesterol in progressive glomerular injury. Md Med J 43:451-5
Kim, E G; Choi, M E; Ballermann, B J (1994) Spatially restricted expression of set mRNA in developing rat kidney. Am J Physiol 266:F155-61
Rennke, H G (1994) How does glomerular epithelial cell injury contribute to progressive glomerular damage? Kidney Int Suppl 45:S58-63
Oliver 3rd, J D; Simons, J L; Troy, J L et al. (1994) Proteinuria and impaired glomerular permselectivity in uninephrectomized fawn-hooded rats. Am J Physiol 267:F917-25
Simons, J L; Provoost, A P; Anderson, S et al. (1994) Modulation of glomerular hypertension defines susceptibility to progressive glomerular injury. Kidney Int 46:396-404
Rubin Kelley, V; Bloom, R D; Yui, M A et al. (1994) Pivotal role of colony stimulating factor-1 in lupus nephritis. Kidney Int Suppl 45:S83-5

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