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首页> 外文期刊>European Journal of Pharmacology: An International Journal >Characterization of capsaicin induced responses in mice vas deferens: evidence of CGRP uptake.
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Characterization of capsaicin induced responses in mice vas deferens: evidence of CGRP uptake.

机译:辣椒素诱导小鼠输精管反应的特征:CGRP摄取的证据。

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摘要

Calcitonin gene-related peptide (CGRP) is extensively distributed in primary afferent sensory nerves, including those innervating the genitourinary tract. Capsaicin can stimulate the release of CGRP from intracellular stores of these nerves, but this phenomenon has not been investigated in-depth in isolated preparations. The present study sets out to study and characterize the capsaicin as well as CGRP-induced responses in isolated mouse vas deferens. The effects of capsaicin and CGRP family of peptides were studied on electrically-induced twitch responses in the absence or presence of transient receptor potential cation channel vanilloid subfamily member 1 (TRPV1) antagonist and CGRP receptor antagonists. Twitch responses were attenuated by capsaicin (1nM-30nM) and CGRP family of peptides. The potency order was CGRP>intermedin-long (IMDL)~[Cys(Et)(2,7)]alphaCGRP~adrenomedullin (AM)>[Cys(ACM)(2,7)]alphaCGRP>amylin (AMY). These responses were disinhibited by the CGRP receptor antagonists and TRPV1 antagonists. The addition of CGRP receptor antagonists caused a transient potentiation of the twitch response and this potentiation was blocked by pretreatment with capsaicin and enhanced by incubation with exogenous CGRP. During the second consecutive cumulative concentration-response curve with capsaicin, the first phase of concentration-response curve disappeared and this was partially restored when the mouse vas deferens was preincubated with CGRP, suggesting the uptake of exogenous CGRP by nerves. Besides showing capsaicin-induced CGRP releases this study shows that exogenous CGRP can be taken up in vas deferens and can be re-released. CGRP uptake will add another dimension in understanding the homeostasis of this neuropeptide.
机译:降钙素基因相关肽(CGRP)广泛分布于初级传入感觉神经,包括支配泌尿生殖道的那些。辣椒素可以刺激CGRP从这些神经的细胞内存储释放,但是这种现象尚未在单独的制剂中进行深入研究。本研究着手研究和表征辣椒素以及CGRP诱导的离体小鼠输精管反应。研究了辣椒素和CGRP肽家族在不存在或存在瞬时受体电位阳离子通道香草样亚家族成员1(TRPV1)拮抗剂和CGRP受体拮抗剂的情况下对电诱导抽搐反应的影响。辣椒素(1nM-30nM)和CGRP肽家族减弱了抽搐反应。效价顺序为:CGRP>长间质素(IMDL)〜[Cys(Et)(2,7)]αCGRP〜肾上腺髓质素(AM)> [Cys(ACM)(2,7)]αCGRP>淀粉状蛋白(AMY)。这些反应被CGRP受体拮抗剂和TRPV1拮抗剂抑制。 CGRP受体拮抗剂的添加引起抽搐反应的瞬时增强,并且该增强通过用辣椒素预处理被阻断并且通过与外源CGRP一起孵育而增强。在辣椒素连续第二次累积的浓度-反应曲线中,第一阶段的浓度-反应曲线消失了,当小鼠输精管与CGRP一起预孵育后,这部分恢复了,提示神经吸收了外源性CGRP。除了显示辣椒素诱导的CGRP释放外,这项研究还表明外源性CGRP可以在输精管中吸收并可以重新释放。 CGRP摄取将在理解该神经肽的体内平衡方面增加另一个维度。

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