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钙敏感受体在大鼠子宫平滑肌中的免疫组化和功能研究。

Immunohistochemical and functional studies on calcium-sensing receptors in rat uterine smooth muscle.

机构信息

Department of Obstetrics and Gynecology, McMaster University, Hamilton, Ontario, Canada.

出版信息

Clin Exp Pharmacol Physiol. 2012 Jan;39(1):37-42. doi: 10.1111/j.1440-1681.2011.05631.x.

Abstract
  1. Activation of calcium-sensing receptors (CaS) leads to relaxation of vascular smooth muscle. However, the role of CaS in uterine smooth muscle is unknown. Therefore the aim of the present study was to investigate the expression and function of CaS in the uterus. 2. The expression of CaS in the oestrogen-dominated rat uterus was investigated using immunohistochemistry. The effects of putative CaS ligands on oxytocin-induced contractions of longitudinally orientated uterine strips from oestrogen-dominated rats were determined at reduced extracellular Ca²⁺ concentrations using conventional organ bath techniques. 3. Immunohistochemical evidence showed the presence of CaS in the endometrium and smooth muscle layers of the rat uterus. Oxytocin-induced contractions were inhibited by cations (Gd³⁺ > Ca²⁺ = Mg²⁺), polyamines (spermine > spermidine) and the positive allosteric modulators cinacalcet and calindol. However (R)- and (S)-cinacalcet were equipotent, indicating a lack of stereoselectivity, and the negative allosteric modulator calhex-231 also caused dose-dependent relaxation. In addition, although intermediate-conductance calcium-activated potassium channels and cytochrome P450-dependent signal transduction have been implicated in CaS-induced relaxation of vascular smooth muscle, neither Tram-34 nor miconazole (1 μmol/L), which block these pathways, respectively, had any effect on the ability of cinacalcet to inhibit oxytocin-induced contractions. 4. Calcium-sensing receptors are expressed in smooth muscle layers of the rat uterus and their ligands produce potent relaxation of longitudinally orientated uterine strips. However, the pharmacological profile of inhibition of contractility by CaS ligands is not consistent with a role for CaS in the regulation of uterine contractility in the rat.
摘要
  1. 钙敏感受体(CaS)的激活会导致血管平滑肌松弛。然而,CaS 在子宫平滑肌中的作用尚不清楚。因此,本研究旨在探讨 CaS 在子宫中的表达和功能。

  2. 采用免疫组织化学方法研究了雌激素主导的大鼠子宫中 CaS 的表达。使用传统的器官浴技术,在降低细胞外 Ca²⁺浓度的情况下,确定了假定的 CaS 配体对来自雌激素主导的大鼠的纵向定向子宫带中催产素诱导的收缩的影响。

  3. 免疫组织化学证据表明 CaS 存在于大鼠子宫的子宫内膜和平滑肌层中。催产素诱导的收缩被阳离子(Gd³⁺ > Ca²⁺ = Mg²⁺)、多胺(精胺 > 亚精胺)和正变构调节剂西那卡塞和钙林醇抑制。然而,(R)-和(S)-西那卡塞具有同等效力,表明缺乏立体选择性,负变构调节剂 calhex-231 也引起剂量依赖性松弛。此外,尽管中间电导钙激活钾通道和细胞色素 P450 依赖性信号转导已被牵连到 CaS 诱导的血管平滑肌松弛中,但 Tram-34 或咪康唑(1 μmol/L),分别阻断这些途径,对西那卡塞抑制催产素诱导的收缩的能力没有任何影响。

  4. 钙敏感受体在大鼠子宫的平滑肌层中表达,其配体产生对纵向定向子宫带的强烈松弛作用。然而,CaS 配体对收缩性的抑制作用的药理学特征与 CaS 在调节大鼠子宫收缩性中的作用不一致。

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