Anatomical differences in responsiveness to vasoconstrictors in the mesenteric veins from normal and portal hypertensive rats

6533b861fe1ef96bd12c4433

RESEARCH PRODUCT

Anatomical differences in responsiveness to vasoconstrictors in the mesenteric veins from normal and portal hypertensive rats

J.m. Piqué M. Angeles Martinez-cuesta Juan V. Esplugues Jaume Bosch L. Moreno

subject

Male medicine.medical_specialty Vasopressin Contraction (grammar)Vasopressins Propranolol Iliac Vein In Vitro Techniques Muscle Smooth Vascular Mesenteric Vein Methoxamine Potassium Chloride Nitric oxide Rats Sprague-Dawley chemistry.chemical_compound Mesenteric Veins Internal medicine Hypertension Portal medicine Animals Vasoconstrictor Agents Pharmacology Endothelin-1 business.industry General Medicine medicine.disease Rats Atropine Endocrinology chemistry cardiovascular system Portal hypertension business medicine.drug

description

The present study evaluates the effects of pre-hepatic portal hypertension, induced in rats by partial portal vein ligation, on the responsiveness of rostral (proximal) and caudal (distal) rings from the mesenteric vein. The anatomical origin of the sample influenced the response to vasoconstrictors in sham-operated animals, and this pattern of reactivity was specifically modified in portal-ligated rats. In veins from sham-operated rats, contraction induced by a submaximal concentration of KCl (60 mM) was greater in proximal than in distal rings. Vasopressin and 5-hydroxytryptamine contracted mainly distal rings, methoxamine showed a greater effect on proximal rings, and endothelin-1 and angiotensin-II contracted vein rings independently of their anatomical origin. In veins from portal hypertensive rats, responses to KCl (60 mM) were increased in distal rings, and all rings exhibited enhanced reactivity to vasopressin and 5-hydroxyptyptamine as well as attenuation of the response to methoxamine. Responses to endothelin-1 were decreased in proximal vein rings from portal hypertensive rats whereas responses to angiotensin-II were not influenced by the anatomical origin. Incubation with atropine, propranolol or indomethacin, did not modify the responses to vasopressin and 5-hydroxytryptamine in tissues from either sham-operated or portal hypertensive animals. Likewise, the hyporeactivity to methoxamine and endothelin-1 in rings from portal hypertensive rats persisted in the presence of the nitric oxide inhibitor N G-nitro-l-arginine methyl ester. These results suggest the physiological existence of anatomical differences in the responsiveness to vasoconstrictors throughout the mesenteric vein and that changes in the responsiveness of the mesenteric vein induced by portal hypertension are specific for each agonist and possibly result from individual variations at a receptor or post-receptor level.

year	journal	country	edition	language
1996-10-01	Naunyn-Schmiedeberg's Archives of Pharmacology

https://doi.org/10.1007/bf00168439