Influence of Bradykinin on Catecholamine Release from the Rat Adrenal Medulla
Influence of Bradykinin on Catecholamine Release from the Rat Adrenal Medulla
- Dong-Yoon Lim Il-Hwan Kim Gwang-Moon Na Moo-Jin Kang Ok-Min Kim Deok-Ho Choi Young-Woo Ki
- 대한생리학회-대한약리학회
- The Korean Journal of Physiology & Pharmacology
- 제7권 제4호
- 등재여부 : KCI등재
- 2003.01
- 231 - 238 (8 pages)
The present study was undertaken to investigate the effect of bradykinin on secretion of catecholamines (CA) evoked by stimulation of cholinergic receptors and membrane depolarization from the isolated perfused model of the rat adrenal glands, and to elucidate its mechanism of action. Bradykinin (3⁓10<SUP>⁣8</SUP> M) alone produced a weak secretory response of the CA. however, the perfusion with bradykinin (3⁓10<SUP>⁣8</SUP> M) into an adrenal vein of the rat adrenal gland for 90 min enhanced markedly the secretory responses of CA evoked by ACh (5.32⁓10<SUP>⁣3</SUP> M), excess K<SUP>⁢</SUP> (5.6⁓10<SUP>⁣2</SUP> M, a membrane depolarizer), DMPP (10<SUP>⁣4 </SUP>M, a selective neuronal nicotinic agonist) and McN-A-343 (10<SUP>⁣4 </SUP>M, a selective M<SUB>1</SUB>-muscarinic agonist). Moreover, bradykinin (3⁓10<SUP>⁣8</SUP> M) in to an adrenal vein for 90 min also augmented the CA release evoked by BAY-K-8644, an activator of the dihydropyridine L-type Ca<SUP>2⁢</SUP> channels. However, in the presence of (N-Methyl-D-Phe<SUP>7</SUP>)-bradykinin trifluoroacetate salt (3⁓10<SUP>⁣8</SUP> M), an antagonist of BK<SUB>2</SUB>-bradykinin receptor, bradykinin no longer enhanced the CA secretion evoked by Ach and high potassium whereas the pretreatment with Lys-(des-Arg<SUP>9</SUP>, Leu<SUP>8</SUP>)-bradykinin trifluoroacetate salt (3⁓10<SUP>⁣8</SUP> M), an antagonist of BK<SUB>1</SUB>-bradykinin receptor did fail to affect them. Furthermore, the perfusion with bradykinin (3⁓10<SUP>⁣6</SUP> M) into an adrenal vein of the rabbit adrenal gland for 90 min enhanced markedly the secretory responses of CA evoked by excess K<SUP>⁢</SUP> (5.6⁓10<SUP>⁣2</SUP> M). Collectively, these experimental results suggest that bradykinin enhances the CA secretion from the rat adrenal medulla evoked by cholinergic stimulation (both nicotininc and muscarinic receptors) and membrane depolarization through the activation of B<SUB>2</SUB>-bradykinin receptors, not through B<SUB>1</SUB>-bradykinin receptors. This facilitatory effect of bradykinin seems to be associated to the increased Ca<SUP>2⁢</SUP> influx through the activation of the dihydropyridine L-type Ca<SUP>2⁢</SUP> channels.