Genistein inhibits contractile force, intracellular Ca2+ increase and Ca2+ oscillations induced by serotonin in rat aortic smooth muscle

SPERONI F; REBOLLEDO A; SALEMME S; AÑON MC; TANZI F; MILESI V

JOURNAL OF PHYSIOLOGY AND BIOCHEMISTRY

Año: 2007 vol. 63 p. 143 - 152

1138-7548

The soy-derived isoflavones genistein and daidzein affect the contractile state of differentkinds of smooth muscle. We describe acute effects of genistein and daidzein on contractileforce and intracellular Ca2+ concentration ([Ca2+]i) in in situ smooth muscle of rat aorta.Serotonin (5-HT) (2 µM) or a depolarizing high K+ solution produced the contraction of aorticrings, which were immediately relaxed by 20 µM genistein and by 20 µM daidzein.Accordingly, both 5-HT and a high K+ solution increased the [Ca2+]i in in situ smooth musclecells. Genistein strongly inhibited the [Ca2+]i increase evoked by 5-HT (74.0 ± 7.3%, n=11,p<0.05), and had a smaller effect on high K+ induced [Ca2+]i increase (19.9 ± 4.0%, n=7,p<0.05). The K+ channels blocker tetraethylammonium (TEA) (0.5 mM) diminished genisteineffects on 5-HT-induced [Ca2+]i increase. Interestingly, during prolonged application of 5-HT,the [Ca2+]i oscillated and a short (90 s) preincubation with genistein (20 µM) significantlydiminished the frequency of the oscillations. This effect was totally abolished by TEA. Inconclusion, in rat aortic smooth muscle, genistein is capable of diminishing the increase in[Ca2+]i and in force evoked by 5-HT and high K+ solution, and of decreasing the frequency of[Ca2+]i oscillations induced by 5-HT. The short time required by genistein, and the relaxingeffect of daidzein suggest that tyrosine kinases inhibition is not involved. The small inhibitingeffect of genistein on the [Ca2+]i increase evoked by high K+ and the effect of TEA point tothe activation by genistein of calcium-activated K+ channels.