Abstract

This grant proposal focuses on the cascade of ionic events involved in acute and chronic regulation of aldosterone secretion. The role of cytosolic Ca2+ in adrenal glomerulosa cells during stimulation by angiotensin II and external K+ has been well established. Less well studied are the effects of cytosolic Na+ and pH during agonist-stimulated aldosterone secretion. Our preliminary data show that adrenal glomerulosa cells have a low basal Na+ permeability which is markedly enhanced by both agonists. Angiotensin II and external K+ activate Na+ entry and H+ efflux via Na+ -H+ exchange, although through different mechanisms. This enhanced Na+ influx results in an elevation of cytosolic Na+ and activation of Na+ efflux coupled to K+ influx via the Na+ -K+ pump. Inhibition of either the Na+ H+ exchanger or the Na+ -K+ pump blocks secretagogue-stimulated aldosterone production, indicating that cytosolic Na+ regulation is critical to steroidogenesis and that changes in cytosolic Na+ may be significant events during agonist- stimulated aldosterone secretion. These findings led us to the central hypothesis of this proposal: angiotensin II and external K+ induce changes in cytosolic Na+ mediated by activation of Na+ -H+ exchange, which are critical for signal transduction. One mechanism by which these changes in cytosolic Na+ may participate in agonist-stimulated aldosterone secretion is the regulation of the enzymatic steps in aldosterone synthesis located in the mitochondria through control of mitochondrial Ca2+. An alternative but not necessarily exclusive corollary to this hypothesis proposes that activation of Na+ -H+ exchange is necessary for regulation of cytosolic pH in response to the cellular acidifying effects of increased Ca2+ extrusion and metabolic activity during stimulation. A major factor controlling the amount of aldosterone secretion by adrenal glomerulosa is the state of Na+ balance in vivo. Steroid production by adrenal glomerulosa cells is enhanced when dietary Na+ intake is restricted and appears to be mediated, in part, by an increase in the enzymatic activity of the late pathway for aldosterone synthesis. Our preliminary findings on the effects of dietary salt show salt restrict increased the basal activity of Na+-H+ exchange and its stimulation by angiotensin II, implying that signal transduction through changes in cytosolic Na+ is also modified by dietary salt restriction. These data suggest that increased adrenal responsiveness may also result from the impact of these ionic transduction changes on the late pathway of aldosterone synthesis. To address this issue, modifications of these ionic pathways will be examined and their effect on the steps leading to aldosterone synthesis. These studies will provide a better understanding of the ionic transduction pathways involved in stimulation of adrenal glomerulosa cells and help in clarifying the mechanisms controlling aldosterone secretion in vivo.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL042120-05
Application #
2220298
Study Section
Experimental Cardiovascular Sciences Study Section (ECS)
Project Start
1989-07-01
Project End
1997-03-31
Budget Start
1995-04-01
Budget End
1996-03-31
Support Year
5
Fiscal Year
1995
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

Smith, Caren E; Coltell, Oscar; SorlĂ­, Jose V et al. (2016) Associations of the MCM6-rs3754686 proxy for milk intake in Mediterranean and American populations with cardiovascular biomarkers, disease and mortality: Mendelian randomization. Sci Rep 6:33188
Cirillo, M; Canessa, M; Quinn, S et al. (1998) Protein kinase C activation stimulates calcium transport in adrenal zona glomerulosa cells. Biochem Biophys Res Commun 245:466-71
Ceolotto, G; Conlin, P; Clari, G et al. (1997) Protein kinase C and insulin regulation of red blood cell Na+/H+ exchange. Am J Physiol 272:C818-26
Romero, J R; Fabry, M E; Suzuka, S M et al. (1997) K:Cl cotransport in red cells of transgenic mice expressing high levels of human hemoglobin S. Am J Hematol 55:112-4
Romero, J R; Fabry, M E; Suzuka, S et al. (1997) Red blood cells of a transgenic mouse expressing high levels of human hemoglobin S exhibit deoxy-stimulated cation flux. J Membr Biol 159:187-96
Rivera, A; Conlin, P R; Williams, G H et al. (1996) Elevated lymphocyte cytosolic calcium in a subgroup of essential hypertensive subjects. Hypertension 28:213-8
Zerbini, G; Ceolotto, G; Gaboury, C et al. (1995) Sodium-lithium countertransport has low affinity for sodium in hyperinsulinemic hypertensive subjects. Hypertension 25:986-93
Canessa, M; Salazar, G; Werner, E et al. (1994) Cell growth and Na-K-Cl cotransport responses of vascular smooth muscle cells of Milan rats. Hypertension 23:1022-6
Canessa, M (1994) Erythrocyte sodium-lithium countertransport: another link between essential hypertension and diabetes. Curr Opin Nephrol Hypertens 3:511-7
Canessa, M; Romero, J R; Lawrence, C et al. (1994) Rate of activation and deactivation of K:Cl cotransport by changes in cell volume in hemoglobin SS, CC and AA red cells. J Membr Biol 142:349-62

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