NITRIC OXIDE SUPPRESSION OF DIABETIC HEART CONTRACTION
Project Number1R15HL056356-01
Contact PI/Project LeaderSMITH, JACQUELYN M
Awardee OrganizationMIDWESTERN UNIVERSITY
Description
Abstract Text
The overall hypothesis of this proposal is that inducible nitric oxide
synthase (iNOS) is elevated in cardiac myocytes during the development
of insulin-deficient diabetes mellitus and the subsequent production of
nitric oxide (NO) and cGMP suppress the response of the cardiac myocyte
to beta-adrenergic stimulation. The specific aims to address this
hypothesis are as follows: (A) To determine if NO production in the
diabetic cardiac myocyte modulates the beta-adrenergic stimulation of
contraction. It is hypothesized that the production of NO by iNOS
decreases the beta-adrenergic stimulation of contraction in diabetic
cardiac myocytes. Moreover, it is hypothesized that inhibition of iNOS
will enhance beta-adrenergic stimulation of contraction in diabetic
cardiac myocytes. (B) To determine if NO production in the diabetic
cardiac myocyte modulates the beta-adrenergic stimulation of calcium
current. It is hypothesized that production of NO by iNOS decreases the
beta-adrenergic stimulation of calcium current (ICa) in the diabetic
cardiac myocyte and that inhibition of iNOS will enhance B-adrenergic
stimulation of ICa. (C) To determine if cGMP production mediates the
suppression of beta-adrenergic-stimulated calcium current and contraction
in the diabetic cardiac myocyte. It is hypothesized that increased
production of cGMP in the diabetic cardiac myocyte suppresses Beta-
adrenergic stimulation of ICa and contraction. It is further
hypothesized that an increased production of NO by iNOS results in an
increased production of cGMP in the cardiac myocyte. Therefore,
inhibition of cGMP production will enhance the beta-adrenergic
stimulation of both ICa and contraction in diabetic cardiac myocyte.
Diabetes will be induced by intravenous streptozotocin injection (60
mg/Kg). Isolated cardiac myocytes will be used to measure nitric oxide,
cGMP and cAMP production. These parameters will be correlated with
measurements of cardiac myocyte contraction and calcium currents using
whole cell voltage clamp techniques. Measurements will be determined
under basal conditions, in response to isoproterenol, and in the presence
of selective nitric oxide synthase inhibitors.
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