Awardee OrganizationUNIVERSITY OF ALABAMA AT BIRMINGHAM
Description
Abstract Text
The long-term goals of this proposal are to study angiotensin II (AII)
receptor regulation in primary neuronal enriched (PNC) and vascular smooth
muscle cell (VSMC) cultures from SHR, WKY and Sprague-Dawley (SD) rats, to
examine the effects of captopril and other converting enzyme inhibitors
(CEI) on AII receptor regulation in these rats and to determine whether the
anti-hypertensive effect of CEI in SHR is related to a down-regulation of
brain AII receptors. We will utilize PNC and VSMC cultures from neonates
to compare AII receptor regulation in SHR vs normotensive rats and to
determine the effects of CEI on central and peripheral AII receptors. This
project is divided into two specific aims. Specific Aim 1: To test the
hypothesis that brain AII receptors are biochemically and functionally
different in SHR vs normotensive rat strains and that brain AII receptors
in SHR are regulated differently from those of WKY and SD rats. We will
utilize radioligand binding techniques to characterize AII receptor number
and affinity in PNC (hypothalamus/brain stem co-cultures) from SHR, WKY and
SD pups and compare these to AII receptors in VSMC cultured from the same
pups. Binding studies will be performed in intact cells and in membranes
prepared from these cells. We will incubate cells with agents known to
stimulate or decrease AII binding and determine whether there are
differences in the responses of AII receptors in SHR vs WKY and in PNC vs
VSMC cultures. We will functionally assess AII receptors in PNC and VSMC
from SHR as compared to WKY and SD by monitoring 45 Ca2+ efflux, cytosolic
[Ca2+], phosphoinositide turnover and AII stimulated release of vasopressin
(VP). We propose that a major signal pathway mediating AII action in
neuronal tissue is the inositol phosphate/Ca2+ pathway. Specific Aim 2:
To test the hypothesis that administration of CEI to SHR is associated with
down regulation of brain AII receptors. We will a) compare AII receptor
number and affinity in PNC and VSMC from SHR, WKY and SD pups subjected to
in utero treatment with CEI, b) we will determine the effects of short-term
incubation of PNC and VSMC cultures with CEI of different chemical
structures on AII binding kinetics. We will study the effects of these
agents on the Kd and Bmax and the association and dissociation constants.
We will also study the effect of these agents on AII receptor
internalization and the coupling of the AII receptor to its second
messenger. In order to determine the specificity of the effect of CEI on
the AII receptor we will simultaneously monitor the effect of CEI on
norepinephrine (NE) and VP binding. Results from the proposed study should
increase our understanding of brain AII receptors and the regulation and
how these receptors are altered in a genetic model of hypertension.
No Sub Projects information available for 5R01HL046554-03
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