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首页> 外文期刊>The Journal of Physiology >Properties of spontaneous Ca2+ transients recorded from interstitial cells of Cajal-like cells of the rabbit urethra in situ.
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Properties of spontaneous Ca2+ transients recorded from interstitial cells of Cajal-like cells of the rabbit urethra in situ.

机译:从兔尿道的Cajal样细胞的间质细胞中记录的自发Ca2 +瞬变的特性。

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摘要

Interstitial cells of Cajal-like cells (ICC-LCs) in the urethra may act as electrical pacemakers of spontaneous contractions. However, their properties in situ and their interaction with neighbouring urethral smooth muscle cells (USMCs) remain to be elucidated. To further explore the physiological role of ICC-LCs, spontaneous changes in [Ca(2+)](i) (Ca(2+) transients) were visualized in fluo-4 loaded preparations of rabbit urethral smooth muscle. ICC-LCs were sparsely distributed, rather than forming an extensive network. Ca(2+) transients in ICC-LCs had a lower frequency and a longer half-width than those of USMCs. ICC-LCs often exhibited Ca(2+) transients synchronously with each other, but did not often show a close temporal relationship with Ca(2+) transients in USMCs. Nicardipine (1 mum) suppressed Ca(2+) transients in USMCs but not in ICC-LCs. Ca(2+) transients in ICC-LCs were abolished by cyclopiazonic acid (10 mum), ryanodine (50 mum) and caffeine (10 mm) or by removing extracellular Ca(2+), andinhibited by 2-aminoethoxydiphenyl borate (50 mum) and 3-morpholino-sydnonimine (SIN-1; 10 mum), but facilitated by increasing extracellular Ca(2+) or phenylephrine (1-10 mum). These results indicated that Ca(2+) transients in urethral ICC-LCs in situ rely on both Ca(2+) release from intracellular Ca(2+) stores and Ca(2+) influx through non-L-type Ca(2+) channel pathways. ICC-LCs may not act as a coordinated pacemaker electrical network as do ICC in the gastrointestinal (GI) tract. Rather they may randomly increase excitability of USMCs to maintain the tone of urethral smooth muscles.
机译:尿道中的Cajal样细胞(ICC-LC)的间质细胞可能充当自发性收缩的电起搏器。但是,它们的原位特性以及与邻近尿道平滑肌细胞(USMC)的相互作用仍有待阐明。为了进一步探讨ICC-LCs的生理作用,在兔尿道平滑肌的fluo-4加载制剂中可见[Ca(2 +)](i)(Ca(2+)瞬态)的自发变化。 ICC-LC稀疏分布,而不是形成广泛的网络。与USMC相比,ICC-LC中的Ca(2+)瞬变具有更低的频率和更长的半宽。 ICC-LC经常彼此同步显示Ca(2+)瞬变,但在USMC中通常不显示与Ca(2+)瞬变的紧密时间关系。尼卡地平(1妈妈)在USMC中抑制了Ca(2+)瞬变,但在ICC-LC中却没有。在ICC-LCs中的Ca(2+)瞬变被环吡嗪酸(10 mum),ryanodine(50 mum)和咖啡因(10 mm)或通过去除细胞外Ca(2+)消除,并被2-氨基乙氧基二苯基硼酸盐(50 mum)抑制)和3-吗啉代亚胺(SIN-1; 10毫米),但通过增加细胞外Ca(2+)或去氧肾上腺素(1-10毫米)来促进。这些结果表明Ca(2+)瞬态在尿道ICC-LCs既依赖于Ca(2+)从细胞内Ca(2+)存储释放,又通过非L型Ca(2)流入Ca(2+) +)渠道途径。 ICC-LC可能不像胃肠道(GI)中的ICC那样充当协调的起搏器电网。相反,它们可能会随机增加USMC的兴奋性,以维持尿道平滑肌的音调。

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