Author:
Kuncová J,Faitová Š,Capouch J,Štengl M,Slavíková J
Abstract
Vasoactive intestinal polypeptide (VIP) is implicated in the
modulation of vagal effects on the heart rate. In this study, the
impact of acute and chronic atropine administration on VIP levels
in rat heart atria was investigated in relation to heart rate in the
course of vagus nerves stimulation. Anaesthetised control and
atropinised (10 mg/kg/day for 10 days) rats pretreated with
metipranolol and phentolamine that were either given or not a
single dose of atropine were subjected to bilateral vagus nerve
stimulation (30 min: 0.7 mA, 20 Hz, 0.2 ms). VIP concentrations
in the atria were determined after each stimulation protocol. In
control rats with or without single atropine administration, the
heart rate upon vagal stimulation was higher than in atropinised
animals with or without single atropine dose, respectively. VIP
concentrations in the control atria were significantly decreased
after the stimulation; the decrease was comparable both in the
absence and presence of a single dose of atropine. Compared to
controls, VIP levels were significantly decreased after chronic
atropine treatment and they were not further reduced by vagal
stimulation and single atropine administration. Administration of
VIP antagonist completely abolished the differences in the heart
rate upon vagal stimulation between control and atropinised
groups. In conclusion, the data indicate that chronic atropine
administration affects VIP synthesis in rat heart atria and
consequently it modifies the heart rate regulation.
Publisher
Institute of Physiology of the Czech Academy of Sciences
Subject
General Medicine,Physiology
Cited by
3 articles.
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