Activation of Protein Kinase C as a Modulator of Potentiated UK-14304-Induced Contractions in Dog Mesenteric Artery and Vein

abstract

We assessed the role of protein kinase C (PKC) in the mechanism responsible for the potentiation of UK-14304-induced contractions produced when isolated dog mesenteric vascular rings were pretreated with threshold concentrations of 12-O-tetradecanoyl-phorbol-13-acetate (TPA), KCl, or endothelin-1 (ET-1). In dog mesenteric artery. UK-14304 produced a biphasic concentration-response curve in the presence of TPA, KCl, or ET-1, with the curve portion at lower concentrations being alpha 2-adrenoceptor dependent and the portion at higher concentrations being alpha 1-adrenoceptor dependent. Calphostin C (10(-6)M), a PKC inhibitor, abolished amplified UK-14304-induced contraction in the TPA-pretreated tissues. In the KCl- and ET-1-pretreated tissues. 10(-6)M calphostin C antagonized amplified UK-14304-induced contractions by approximately 20% in both parts of the concentration-response curve. In contrast, in dog mesenteric vein, amplified UK-14304-induced contractions by TPA, KCl, and ET-1 were entirely dependent on alpha 2-adrenoceptors. Calphostin C (10(-6)M), which in control experiments had no effect on KCl-induced contraction and antagonized responses to TPA by 60.1%, inhibited UK-14304-induced contraction by 18.3%. Amplified UK-14304-induced contraction was antagonized by 10(-6)M calphostin C by 21.8% in KCl-precontracted tissues, 58.1% in ET-1-precontracted tissues, and 66.3% in TPA-precontracted tissues. In the ET-1- and TPA-pretreated dog mesenteric veins, 10(-6)M calphostin C decreased maximal tensions of enhanced UK-14304-induced contractions to the same level as the UK-14304-induced maximal tension inhibited by 10(-6)M calphostin C in untreated dog mesenteric vein. Therefore, TPA can be a precontracting agent that amplifies UK-14304-induced contractions through PKC activation in both dog mesenteric artery and vein. PKC predominantly mediates the contraction amplification mechanisms after exposure to ET-1 in dog mesenteric vein and does not play a major role in the amplification of UK-14304-induced contraction by KCl in both dog mesenteric artery and vein. These data show that a common mechanism need not underlie amplification of adrenergic responses in mesenteric artery and vein.

authors

Shimamoto, Hiroyuki
Shimamoto, Yoriko
Kwan, Chiu-yin
Daniel, Edwin E

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published

publication date

December 1995

has subject area

1102 Cardiorespiratory Medicine and Haematology (FoR)
1115 Pharmacology and Pharmaceutical Sciences (FoR)
Adrenergic alpha-Agonists (MeSH)
Animals (MeSH)
Brimonidine Tartrate (MeSH)
Cardiovascular System & Hematology (Science Metrix)
Dogs (MeSH)
Female (MeSH)
In Vitro Techniques (MeSH)
Male (MeSH)
Mesenteric Arteries (MeSH)
Mesenteric Veins (MeSH)
Naphthalenes (MeSH)
Potassium Chloride (MeSH)
Protein Kinase C (MeSH)
Quinoxalines (MeSH)
Receptors, Adrenergic, alpha-1 (MeSH)
Receptors, Adrenergic, alpha-2 (MeSH)
Vasoconstriction (MeSH)

published in

Journal of Cardiovascular Pharmacology Journal

Activation of Protein Kinase C as a Modulator of Potentiated UK-14304-Induced Contractions in Dog Mesenteric Artery and Vein Journal Articles

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