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首页> 美国卫生研究院文献>The Journal of Physiology >Role of L- and N-type Ca2+ channels in muscarinic receptor-mediated facilitation of ACh and noradrenaline release in the rat urinary bladder.
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Role of L- and N-type Ca2+ channels in muscarinic receptor-mediated facilitation of ACh and noradrenaline release in the rat urinary bladder.

机译:L和N型Ca2 +通道在毒蕈碱受体介导的ACh促成和肾上腺素释放在大鼠膀胱中的作用。

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1. 3H-Noradrenaline (NA) and 14C-acetylcholine (ACh) released by electrical field stimulation were measured simultaneously in strips from the body of rat urinary bladder. 2. omega-Conotoxin GVIA (omega-CgTX; 20-100 nM) suppressed the non-facilitated transmitter release evoked by intermittent stimulation (IS), whereas nifedipine (1 microM) did not affect release. 3. Continuous electrical stimulation (CS) facilitated NA and ACh release via an atropine-sensitive mechanism. omega-CgTX reduced the facilitated release of NA (44% depression) but did not affect ACh release. Nifedipine depressed ACh release (43%) but not NA release. Combined administration of nifedipine and omega-CgTX (20 nM) produced a greater suppression of NA and ACh release (86 and 91%, respectively). 4. Maximal muscarinic facilitation of NA (5-fold) and ACh (17-fold) release occurred following administration of eserine, an anticholinesterase agent. Release of both NA and ACh was depressed by nifedipine (70 and 83%, respectively) but not by omega-CgTX. Combined application of omega-CgTX and nifedipine elicited a further depression of NA (95%) but not ACh release. 5. When NA and ACh release was facilitated with phorbol dibutyrate (0.5 microM), nifedipine inhibited ACh (67%) but not NA release, whereas omega-CgTX inhibited NA (73%) but not ACh release. Combined administration of both Ca2+ channel blockers did not elicit greater inhibition. 6. Bay K 8644, the L-type Ca2+ channel activator, increased ACh release in a dose-dependent manner (up to 5-fold) but did not significantly change NA release. 7. Both omega-CgTX (20-100 nM) and nifedipine (100 nM-1 microM) significantly decreased (50-80%) the neurally evoked contractions of the bladder strips. 8. It is concluded that L-type Ca2+ channels play a major role in muscarinic facilitation of NA and ACh release in the urinary bladder but are not essential for non-facilitated release. Other types of Ca2+ channels, including N-type, are involved to varying degrees in non-facilitated and facilitated release under different experimental conditions.
机译:1.在大鼠膀胱体的试纸中同时测量电场刺激释放的3H-去甲肾上腺素(NA)和14C-乙酰胆碱(ACh)。 2. omega-Conotoxin GVIA(omega-CgTX; 20-100 nM)抑制了间歇刺激(IS)引起的非促进性递质释放,而硝苯地平(1 microM)则不影响释放。 3.连续电刺激(CS)通过对阿托品敏感的机制促进NA和ACh的释放。 omega-CgTX降低了NA的释放(降低了44%),但不影响ACh的释放。硝苯地平抑制ACh释放(43%),但不抑制NA释放。硝苯地平和omega-CgTX(20 nM)的联合给药对NA和ACh释放的抑制作用更大(分别为86%和91%)。 4.给予抗胆碱酯酶血色氨酸后,毒蕈碱最大程度地促进了NA(5倍)和ACh(17倍)释放。硝苯地平抑制了NA和ACh的释放(分别为70%和83%),但omega-CgTX却没有。联合使用ω-CgTX和硝苯地平会引起NA的进一步降低(95%),但不会释放ACh。 5.当佛波二丁酸酯(0.5 microM)促进NA和ACh释放时,硝苯地平抑制ACh(67%)但不释放NA,而omega-CgTX抑制NA(73%)但不抑制ACh释放。两种Ca2 +通道阻滞剂的联合给药未引起更大的抑制作用。 6. Bay K 8644(L型Ca2 +通道激活剂)以剂量依赖性方式(最多5倍)增加了ACh的释放,但并未显着改变NA的释放。 7. omega-CgTX(20-100 nM)和硝苯地平(100 nM-1 microM)均显着降低(50-80%)膀胱条的神经诱发收缩。 8.结论是L型Ca2 +通道在毒蕈碱促进NA和ACh在膀胱中释放中起主要作用,但对于非促进释放不是必需的。在不同的实验条件下,其他类型的Ca2 +通道(包括N型)在不同程度上参与了非促进和促进释放。

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