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Intravesical protamine sulfate and potassium chloride as a model for bladder hyperactivity.

机译:膀胱内鱼精蛋白硫酸盐和氯化钾作为膀胱机能亢进的模型。

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OBJECTIVES: An acute animal model for hyperactive bladder in rats was developed using intravesical infusion of protamine sulfate (PS), an agent thought to break down urothelial barrier function, and physiologic concentrations of potassium chloride (KCl). METHODS: Continuous cystometrograms (CMGs) were performed in urethane-anesthetized female rats by filling the bladder (0.04 mL/min) with normal saline followed by intravesical infusion of a test solution consisting of either KCl (100 or 500 mM) or PS (10 or 30 mg/mL) for 60 minutes. Subsequently, the 10 mg/mL PS-treated animals were infused intravesically with 100, 300, or 500 mM KCl. Some animals were pretreated with capsaicin (125 mg/kg subcutaneously) 4 days before the experiments. RESULTS: Unlike KCl (100 or 500 mM) or a low concentration of PS (10 mg/mL) alone, the intravesical administration of a high concentration of PS (30 mg/mL) produced irritative effects with a decreased intercontraction interval (by 80.6%). After infusion of a low concentration of PS, infusion of 300 or 500 mM KCl produced irritative effects (intercontraction interval decreased by 76.9% or 82.9%, respectively). The onset of irritation occurred more rapidly after 500 mM KCl (10 to 15 minutes) than after 300 mM KCl (20 to 30 minutes). Capsaicin pretreatment delayed the onset (approximately 60 minutes) and reduced the magnitude (intercontraction interval decreased by 35.5%) of irritative effects. CONCLUSIONS: Intravesical administration of KCl after PS treatment activates capsaicin-sensitive afferents and detrusor muscle and presumably capsaicin-resistant afferents. Modest, noncytotoxic affronts to urothelial barrier function can result in dramatic irritative responses. This model may be useful in the study of bladder irritation and hyperactivity.
机译:目的:使用膀胱内注射硫酸鱼精蛋白(PS),一种认为可破坏尿道上皮屏障功能的药物和生理浓度的氯化钾(KCl),开发了一种大鼠膀胱过度活动症的急性动物模型。方法:在尿烷麻醉的雌性大鼠中,通过向膀胱(0.04 mL / min)注入生理盐水,然后膀胱内输注由KCl(100或500 mM)或PS(10)组成的测试溶液,进行连续膀胱测压(CMG)。或30 mg / mL)60分钟。随后,将10 mg / mL PS处理的动物膀胱内输注100、300或500 mM KCl。实验前4天,用辣椒素(皮下注射125 mg / kg)对一些动物进行了预处理。结果:与单独的KCl(100或500 mM)或低浓度的PS(10 mg / mL)不同,膀胱内施用高浓度的PS(30 mg / mL)产生刺激性作用,同时缩短了收缩间隔(降低了80.6) %)。输注低浓度的PS后,输注300或500 mM KCl会产生刺激作用(收缩间隔分别减少76.9%或82.9%)。在500 mM KCl(10至15分钟)后,刺激的发作比在300 mM KCl(20至30分钟)后更快。辣椒素预处理可延缓发作(约60分钟),并减少刺激作用的幅度(收缩间隔减少35.5%)。结论:PS治疗后膀胱内注射KCl可激活辣椒素敏感的传入和逼尿肌以及可能对辣椒素有抵抗力的传入。对尿路上皮屏障功能的轻度,无细胞毒性的冒犯会导致剧烈的刺激性反应。该模型可能对研究膀胱刺激和多动症有用。

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