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一氧化氮合酶抑制剂改变乳头肌力量-频率关系。

Nitric oxide synthase inhibitor alters papillary muscle force-frequency relationship.

作者信息

Finkel M S, Oddis C V, Mayer O H, Hattler B G, Simmons R L

机构信息

Department of Medicine, University of Pittsburgh School of Medicine, Pennsylvania.

出版信息

J Pharmacol Exp Ther. 1995 Feb;272(2):945-52.

PMID:7531767
Abstract

We provide evidence for an immediate effect of NG-monomethyl-L-arginine (L-NMMA) on the force-frequency relationship in isolated hamster papillary muscles. L-NMMA (competitive inhibitor of nitric oxide synthase) reversed the force-frequency relationship (staircase effect) in isolated hamster papillary muscles from negative to positive (P < .01; ANOVA; n = 6). The addition of L-arginine (substrate for nitric oxide synthase) blocked the L-NMMA effect (P < .01; ANOVA; n = 6). The addition of the nitric oxide (NO) donor, sodium nitroprusside (NTP), significantly increased the level of cGMP in the tissue bath (P < .01; test; n = 6) and reversed the positive inotropic effect of L-NMMA on staircase (P < .01; ANOVA; n = 6). The addition of 8-Br-cGMP to the bath resulted in a concentration-dependent decrease in tension generated by the papillary muscles (n = 6). Methylene blue (known inhibitor of cGMP) mimicked the effect of L-NMMA on staircase (P < .01; ANOVA; n = 6). L-NMMA also significantly blunted the negative inotropic effect of ryanodine (SR calcium release channel regulator) (P < .01; ANOVA; n = 6). The positive inotropic effect of Bay K 8644 (sarcolemmal, L-type calcium channel regulator) was not affected by L-NMMA (P = NS; ANOVA; n = 6). L-NMMA had no effect on either [3H]ryanodine or [3H]PN200-110 (sarcolemmal, L-type calcium channel regulator) binding to cardiac membranes. These findings support a cGMP-dependent role for endogenous NO in myocardial E-C coupling.

摘要

我们提供了证据,证明NG-单甲基-L-精氨酸(L-NMMA)对离体仓鼠乳头肌的力-频率关系有即时影响。L-NMMA(一氧化氮合酶的竞争性抑制剂)使离体仓鼠乳头肌的力-频率关系(阶梯效应)从负向转为正向(P <.01;方差分析;n = 6)。添加L-精氨酸(一氧化氮合酶的底物)可阻断L-NMMA的作用(P <.01;方差分析;n = 6)。添加一氧化氮(NO)供体硝普钠(NTP)可显著提高组织浴中的cGMP水平(P <.01;检验;n = 6),并逆转L-NMMA对阶梯的正性肌力作用(P <.01;方差分析;n = 6)。向浴中添加8-溴-cGMP会导致乳头肌产生的张力呈浓度依赖性降低(n = 6)。亚甲蓝(已知的cGMP抑制剂)模拟了L-NMMA对阶梯的作用(P <.01;方差分析;n = 6)。L-NMMA还显著减弱了ryanodine(肌浆网钙释放通道调节剂)的负性肌力作用(P <.01;方差分析;n = 6)。Bay K 8644(肌膜L型钙通道调节剂)的正性肌力作用不受L-NMMA影响(P = 无显著性差异;方差分析;n = 6)。L-NMMA对[3H]ryanodine或[3H]PN200-110(肌膜L型钙通道调节剂)与心肌膜的结合均无影响。这些发现支持内源性NO在心肌兴奋-收缩偶联中依赖cGMP的作用。

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