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Mandatory role of proteinase-activated receptor 1 in experimental bladder inflammation

机译:蛋白酶激活受体1在实验性膀胱炎症中的强制性作用

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摘要

BackgroundIn general, inflammation plays a role in most bladder pathologies and represents a defense reaction to injury that often times is two edged. In particular, bladder neurogenic inflammation involves the participation of mast cells and sensory nerves. Increased mast cell numbers and tryptase release represent one of the prevalent etiologic theories for interstitial cystitis and other urinary bladder inflammatory conditions. The activity of mast cell-derived tryptase as well as thrombin is significantly increased during inflammation. Those enzymes activate specific G-protein coupled proteinase-activated receptors (PAR)s.Four PARs have been cloned so far, and not only are all four receptors highly expressed in different cell types of the mouse urinary bladder, but their expression is altered during experimental bladder inflammation. We hypothesize that PARs may link mast cell-derived proteases to bladder inflammation and, therefore, play a fundamental role in the pathogenesis of cystitis.
机译:背景技术通常,炎症在大多数膀胱病理中均起作用,并代表对损伤的防御反应,通常是两边。特别地,膀胱神经源性炎症涉及肥大细胞和感觉神经的参与。肥大细胞数量增加和类胰蛋白酶释放代表间质性膀胱炎和其他膀胱炎性疾病的流行病因学理论之一。在炎症过程中,肥大细胞类胰蛋白酶和凝血酶的活性显着增加。这些酶激活特定的G蛋白偶联蛋白酶激活受体(PAR)。到目前为止已克隆了四个PAR,不仅所有四个受体在小鼠膀胱的不同细胞类型中都高表达,而且它们的表达在实验性膀胱炎症。我们假设PARs可能将肥大细胞衍生的蛋白酶与膀胱炎症联系在一起,因此在膀胱炎的发病机理中起着重要作用。

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