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Signalling pathways in bradykinin- and nitric oxide-induced hypotension in the normotensive rat; role of K+-channels

机译：血压正常大鼠缓激肽和一氧化氮诱导的低血压的信号通路； K +通道的作用

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class="enumerated" style="list-style-type:decimal">Bradykinin and nitric oxide (NO) are potent hypotensive agents. In the present study, the role of K⁺-channels in the signalling pathways responsible for their hypotensive action was investigated in normotensive, anaesthetized rats. The rats were treated with ion-channel inhibitors before administration of bradykinin (2.8, 5.6, 28 and 56 nmol kg⁻¹, i.v.) followed in some of the protocols by nitroprusside (1.1, 3.5, 7, 14, and 28 nmol kg⁻¹, i.v.).No attenuation of the hypotensive response to bradykinin was detected for inhibitors of the Na-K-Cl-cotransporter (30 μmol kg⁻¹ furosemide), the ATP-sensitive K⁺-channel (40 μmol kg⁻¹ glibenclamide), high conductance Ca²⁺-activated K⁺-channel (180 μmol kg⁻¹ tetraethylammonium, 54 μmol kg⁻¹ tetrabutylammonium, 35 nmol kg⁻¹ iberiotoxin, 35 nmol kg⁻¹ charybdotoxin) or the low conductance Ca²⁺-activated K⁺-channel (74 nmol kg⁻¹ apamin).However, the voltage-sensitive K⁺-channel (IA) inhibitor 4-aminopyridine (4.05–40.5 μmol kg⁻¹) induced a concentration-dependent (P<0.0001) attenuation of the hypotensive response (P<0.0001). Bradykinin had no effect on heart rate in anaesthetized rats and this observation was not altered by pretreatment with 4-aminopyridine.4-Aminopyridine (53 μmol kg⁻¹) also significantly attenuated the hypotensive response to nitroprusside (P<0.0003) without altering the heart rate concentration-response curve. Of the two Ca²⁺-activated K⁺-channel inhibitors tested on nitroprusside-induced hypotension, tetrabutylammonium induced a slight attenuation (P<0.0101), whereas iberiotoxin had no effect.We therefore concluded that, although the acute hypotensive response to bradykinin in the normotensive rat is not mediated through nitric oxide synthesis, the hypotensive response to both agents was mediated through opening of voltage-sensitive K⁺-channels (IA), resulting in a decrease in peripheral vascular resistance.

机译：class =“ enumerated” style =“ list-style-type：decimal”> <！-list-behavior =枚举前缀-word = mark-type = decimal max-label-size = 0-> 缓激肽和一氧化氮（NO）是有效的降压药。在本研究中，在正常血压，麻醉大鼠中研究了K ^{+ 通道在负责其降压作用的信号通路中的作用。在给予缓激肽（2.8、5.6、28和56μmol·kg ^{-1 ，iv）之前，先用离子通道抑制剂治疗大鼠，然后在某些方案中先用硝普钠（1.1、3.5、7， 14和28 nmol kg ^{-1 ，iv）。对于Na-K-Cl-co-transporter抑制剂（30molμmol），未检测到对缓激肽的降压反应减弱kg ^{−1 速尿），ATP敏感的K ^{+ 通道（40μmolkg ^{-1 格列本脲），高电导Ca ^{2 + 活化的K ^{+ 通道（180μmolkg ^{-1 四乙铵，54μmolkg ^{-1 四丁基铵，35 nmol kg ^{−1 埃博毒素，35nmol kg ^{-1 炭疽毒素）或低电导率的Ca ^{2 + 活化的K ^{+ -通道（74 nmol kg ^{−1 阿帕明）。但是，电压敏感型K ^{+ -通道（IA）抑制剂4-氨基吡啶（4.05–40.5μmolkg ^{−1 ）引起浓度依赖性（P <0.0001）衰减o f降压反应（P <0.0001）。缓激肽对麻醉大鼠的心律没有影响，并且用4-氨基吡啶预处理并没有改变这一现象。 4-氨基吡啶（53μmolkg ^{−1 ）也明显减弱对硝普钠的降压反应（P <0.0003）而没有改变心率浓度-反应曲线。在硝普钠诱导的低血压中测试的两种由Ca ^{2 + 激活的K ^{+ 通道抑制剂中，四丁基铵诱导了轻微的衰减（P <0.0101），而纤毛毒素没有作用因此，我们得出结论，尽管正常血压大鼠对缓激肽的急性降压反应不是通过一氧化氮合成介导的，但对两种药物的降压反应都是通过打开电压敏感的K ^{来介导的。 + -通道（IA），导致外周血管阻力降低。}}}}}}}}}}}}}}}}}}}}}

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期刊名称 British Journal of Pharmacology and Chemotherapy
作者
Torill Berg; Øyvind Koteng;
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作者单位

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年(卷),期 1997(121),6
年度 1997
页码 1113–1120
总页数 8
原文格式 PDF
正文语种
中图分类药学 ;
关键词
Bradykinin nitric oxide blood pressure hypotension Ksup+/sup-channels voltage-sensitive Ksup+/sup-channels (IA) 4-aminopyridine;

机译：缓激肽;一氧化氮;血压;低血压;K sup + / sup通道;电压敏感的K sup + / sup通道（IA）;4-氨基吡啶;

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专利

1. Signalling pathways in bradykinin-and nitric oxide-induced hypotension in the normotensive art: role of K~+ -channels [J] . Torill Berg, Oyvind Koteng British Journal of Pharmacology . 1997 ,第6期

机译：降血压药中缓激肽和一氧化氮引起的低血压的信号通路：K〜+通道的作用
2. Nitric oxide at a low concentration protects murine macrophage RAW264 cells against nitric oxide-induced death via cGMP signaling pathway [J] . Y. Yoshioka, A. Yamamuro, S. Maeda British Journal of Pharmacology . 2003 ,第1期

机译：低浓度一氧化氮通过cGMP信号通路保护鼠巨噬细胞RAW264细胞免受一氧化氮诱导的死亡
3. Exploring the role and inter-relationship among nitric oxide, opioids, and KATP channels in the signaling pathway underlying remote ischemic preconditioning induced cardioprotection in rats [J] . Sapna Aggarwal, Jasleen Kaur Virdi, Nirmal Singh, Iranian Journal of Basic Medical Sciences . 2019 ,第7期

机译：在大鼠中远程缺血预处理诱导的大鼠心脏保护型心脏保护中的一氧化氮，阿片类药物和KATP通道中的作用和相互关系
4. Modulation of the L-arginine/nitric oxide signalling pathway in vascular endothelial cells [C] . Amanda W.Wyatt, Joern R.Steinert, Giovanni E.Mann Biochemical Society Symposium . 2004

机译：血管内皮细胞中L-精氨酸/一氧化氮信号通路的调节
5. Nitric oxide biological chemistry in a systems biology context: Influence of biosystems diversity on nitric oxide signal transduction pathways. [D] . Hyduke, Daniel Robert. 2006

机译：系统生物学环境中的一氧化氮生物化学：生物系统多样性对一氧化氮信号传导途径的影响。
6. Nitric oxide at a low concentration protects murine macrophage RAW264 cells against nitric oxide-induced death via cGMP signaling pathway [O] . Y Yoshioka, A Yamamuro, S Maeda 2003

机译：低浓度一氧化氮通过cGMP信号通路保护鼠巨噬细胞RAW264细胞免受一氧化氮诱导的死亡
7. Nitric oxide at a low concentration protects murine macrophage RAW264 cells against nitric oxide-induced death via cGMP signaling pathway [O] . Yoshioka, Y, Yamamuro, A, Maeda, S 2003

机译：低浓度一氧化氮通过cGMP信号通路保护鼠巨噬细胞RAW264细胞免受一氧化氮诱导的死亡

Signalling pathways in bradykinin- and nitric oxide-induced hypotension in the normotensive rat; role of K+-channels

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