A. Hilditch scite author profile

1 The effect of GRI 17289, an angiotensin AT, receptor antagonist, on diastolic blood pressure (DBP) was determined in angiotensin-dependent and angiotensin-independent models of hypertension in rats. In addition, the antagonist profile of GRi 17289 at angiotensin AT1 receptors was determined in conscious renal hypertensive rats and conscious normotensive rats, dogs and marmosets. 2 Intra-arterial and oral administration of GRI17289 (0.3-3mgkg-', i.a.; 1-10mgkg-', p.o.) to 6-day left renal artery ligated hypertensive (RALH) rats (DBP> 140 mmHg) produced significant, dose-related reductions in DBP with little apparent effect on heart rate (< 15%). The antihypertensive effect of GRI 17289 developed progressively over several hours and with some doses persisted for 24-48 h after administration. 3 Administration of GRI17289 (1 mg kg-', i.a.) on 5 consecutive days to RALH rats reduced DBP on each day. The antihypertensive effect of GR1 17289 was not cumulative as DBP had almost returned to base-line values, 24 h after administration of each dose. 4 A dose of GRI 17289 (3 mg kg', i.a.), which produced a substantial reduction in DBP (about 70 mmHg) in RALH rats, was administered to rats in which blood pressure was elevated either by unilateral renal artery clipping, sustained infusion of angiotensin II (All), DOCA-salt administration or genetic inbreeding. GR1 17289 reduced DBP in rats in which the renin-angiotensin system was activated by renal artery clipping or All infusion but had little effect in normotensive rats, DOCA-salt rats and SHR. 5 Systemic administration of All to RALH rats and to normotensive rats, dogs and marmosets elicited reproducible pressor responses in all species. Systemic or oral administration of GR1 17289 (3 mg kg-') inhibited the pressor responses produced by All, resulting in parallel, rightward displacements of All dose-response curves. 6 Maximal displacements of All dose-response curves occurred 1 h and 1-7 h after systemic and oral administration, respectively. GR1 17289 produced a 32-246 fold displacement after systemic administration and a 4-12 fold displacement after oral administration. The effect in dogs was short lasting after systemic administration but the effect of GR I17289 lasted for up to 24 h in rats and marmosets and for up to 24 h after oral administration in all species. The antagonist activity appeared specific for angiotensin receptors as GRi17289 did not inhibit pressor responses to phenylephrine or vasopressin. 7 These experiments demonstrate that GRI 17289 reduces blood pressure in conscious hypertensive rats after both systemic and oral administration, and is an effective antagonist at angiotensin AT, receptors in conscious rats, dogs and marmosets.

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SCH 23390 is a very potent and selective antagonist at vascular dopamine receptors

Hilditch¹,

Drew²,

Naylor³

1984

European Journal of Pharmacology

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Peripheral dopamine receptor subtypes — a closer look

Hilditch¹,

Drew

1985

Trends in Pharmacological Sciences

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Dopamine receptors in human basilar arteries

Förster

Drew

Hilditch

et al. 1983

European Journal of Pharmacology

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Characteristics of the dopamine receptors in the rabbit isolated splenic artyery

Hilditch¹,

Drew²

1981

European Journal of Pharmacology

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A. Hilditch

Cardiovascular effects of GR117289, a novel angiotensin AT₁ receptor antagonist

SCH 23390 is a very potent and selective antagonist at vascular dopamine receptors

Peripheral dopamine receptor subtypes — a closer look

Dopamine receptors in human basilar arteries

Characteristics of the dopamine receptors in the rabbit isolated splenic artyery

Contact Info

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Resources

About

A. Hilditch

Cardiovascular effects of GR117289, a novel angiotensin AT1 receptor antagonist

SCH 23390 is a very potent and selective antagonist at vascular dopamine receptors

Peripheral dopamine receptor subtypes — a closer look

Dopamine receptors in human basilar arteries

Characteristics of the dopamine receptors in the rabbit isolated splenic artyery

Contact Info

Product

Resources

About

Cardiovascular effects of GR117289, a novel angiotensin AT₁ receptor antagonist