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钙调蛋白拮抗剂对去极化血管和肠道平滑肌张力及细胞钙含量的影响。

Effects of calmodulin antagonists on tension and cellular calcium content in depolarized vascular and intestinal smooth muscles.

作者信息

Karaki H, Murakami K, Nakagawa H, Ozaki H, Urakawa N

出版信息

Br J Pharmacol. 1982 Dec;77(4):661-6. doi: 10.1111/j.1476-5381.1982.tb09344.x.

Abstract

1 Several putative calmodulin antagonists have been examined for their inhibitory action on muscle tension and cellular Ca content in the K-depolarized vascular and intestinal smooth muscles. 2 The 65.4 mM K-induced sustained contraction in the media-intimal layer of rabbit aorta and the 45.4 mM K-induced sustained contraction in guinea-pig taenia coli were inhibited by the calmodulin antagonists, prenylamine, chlorpromazine, N2-dansyl-L-arginine-4-t-butylpiperadine amide (No. 233), and N-(6-aminohexyl)-5-chloro-1-naphthalenesulphonamide (W-7), and also by the organic Ca antagonists, verapamil and diltiazem. 3 The cellular Ca content in rabbit aorta and guinea-pig taenia coli as measured by a modified lanthanum technique increased in the high-K solutions. The increments were inhibited by these antagonists at concentrations similar to those required to inhibit the K-induced contractions. However, W-7 did not change (in aorta) or only slightly decreased (in taenia coli) the K-induced increase in the cellular Ca content. 4 A high concentration (2 X 10(-4)M) of W-7 increased the resting cellular Ca content without increasing the muscle tension in aorta. The increment was inhibited by verapamil, sodium nitroprusside or hypoxia (N2 aeration). 5 It is suggested that the inhibitory effects of prenylamine, chlorpromazine and No. 233 may be attributed mainly to the Ca antagonistic effect whereas W-7 may inhibit the process beyond the transmembrane Ca influx.

摘要
  1. 已对几种假定的钙调蛋白拮抗剂在钾去极化的血管和平滑肌中对肌肉张力和细胞钙含量的抑制作用进行了研究。2. 钙调蛋白拮抗剂普尼拉明、氯丙嗪、N2-丹磺酰-L-精氨酸-4-叔丁基哌啶酰胺(233号)和N-(6-氨基己基)-5-氯-1-萘磺酰胺(W-7),以及有机钙拮抗剂维拉帕米和地尔硫卓,均抑制了兔主动脉中膜-内膜层65.4 mM钾诱导的持续收缩以及豚鼠结肠带中45.4 mM钾诱导的持续收缩。3. 通过改良的镧技术测量,兔主动脉和豚鼠结肠带中的细胞钙含量在高钾溶液中增加。这些拮抗剂在与抑制钾诱导的收缩所需浓度相似的浓度下抑制了这种增加。然而,W-7并未改变(在主动脉中)或仅略微降低(在结肠带中)钾诱导的细胞钙含量增加。4. 高浓度(2×10⁻⁴M)的W-7增加了主动脉中静息细胞钙含量,而未增加肌肉张力。维拉帕米、硝普钠或缺氧(氮气通气)抑制了这种增加。5. 提示普尼拉明、氯丙嗪和233号的抑制作用可能主要归因于钙拮抗作用,而W-7可能抑制跨膜钙内流之后的过程。

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