FAAH Inhibitor Improves Function of Inflamed Bladders by Modulation of Anandamide and Palmitoylethanolamide

A. Charrua, R. Matos, T. Marczylo, I. Nagy, F. Cruz
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Abstract

Introduction: We aim to study the effect of fatty acid amide hydrolase (FAAH) blockade on bladder hyperactivity and on fatty acid amides levels during cystitis. Material and Methods: Cystitis was induced in female Wistar rats using 5 mg/mL lipopolysaccharide (LPS). Control group were intravesical instilled with saline. LPS and control groups received intravenously (caudal vein) during cystometry: URB 937 (URB; FAAH antagonist) in doses of 0.007, 0.07, 0.7 and 7 mg/kg (cumulative, with 10 minutes interval). Using the maximal effective dose of URB (0.7 mg/kg, see below) animals received 10 uM MJ15 (CB1 receptor antagonist) or 0.3 mg SR144528 /kg (SR; CB2 receptor antagonist). At dose of 7 mg/kg, animals receive 1.4 μg SB366791/kg (SB; TRPV1 antagonist). Control and inflamed (without and with 0.7 and 7 mg/kg URB) group were euthanized and the bladder was harvested for the determination of anandamide (AEA) and palmitoylethanolamide (PEA) by mass spectrometry. Results: Frequency of control was not changed by URB treatment at any dose. LPS increase bladder frequency. 0.007 mg and 0.07 mg URB decrease bladder frequency of LPS-inflamed rats. 0.7 URB reversed LPS-induced bladder hyperactivity. At 7 mg, URB was unable to reverse or reduce LPS-induced bladder hyperactivity. The administration of CB1, CB2 and TRPV1 antagonists did not change the frequency of voiding contractions of naive animals. CB1 antagonist reversed the effect of 0.7 URB while TRPV1 antagonist reduced the effect of 7 URB. AEA levels increase during inflammation. Treating LPS-inflamed animals with 0.7 mg URB brought AEA levels to control levels. Treating LPS-inflamed animals with 7 mg URB did not change AEA levels, compared to LPS-inflamed animals. PEA levels decrease during inflammation. Treating LPS-inflamed animals with 0.7 mg URB brought AEA levels to control levels. Treating LPS-inflamed animals with 7 mg URB, decreased PEA levels to values similar to the ones observed in LPS- -inflamed animals. Conclusion: During cystitis, the FAAH inhibitor raises the levels of PEA and reverses the urinary frequency by a CB1 receptor- mediated mechanism. When used in very high doses, the FAAH antagonist raises the levels of AEA and increases the urinary frequency by a TRPV1-dependent mechanism. Therefore, the choice of FAAH inhibitor dosage to be used in the clinics should consider the putative effects over the endocannabinoid levels in the system.
FAAH抑制剂通过调节Anandamide和棕榈酰乙醇酰胺改善发炎膀胱功能
简介:我们的目的是研究脂肪酸酰胺水解酶(FAAH)阻断对膀胱炎期间膀胱亢进和脂肪酸酰胺水平的影响。材料与方法:用5 mg/mL脂多糖(LPS)诱导雌性Wistar大鼠膀胱炎。对照组患者膀胱内灌注生理盐水。LPS组和对照组在造囊术中静脉注射(尾静脉):URB 937 (URB;FAAH拮抗剂),剂量分别为0.007、0.07、0.7和7mg /kg(累积,间隔10分钟)。使用URB的最大有效剂量(0.7 mg/kg,见下),动物接受10 uM MJ15 (CB1受体拮抗剂)或0.3 mg SR144528 /kg (SR;CB2受体拮抗剂)。在7 mg/kg剂量下,动物接受1.4 μg SB366791/kg (SB;TRPV1拮抗剂)。对照组和炎症组(无URB组、含0.7和7 mg/kg URB组)安乐死,取膀胱,质谱法测定anandamide (AEA)和palmitoylethanolamide (PEA)含量。结果:任何剂量的URB治疗均未改变对照频率。LPS增加膀胱频率。0.007 mg和0.07 mg URB可降低lps炎症大鼠膀胱频率。0.7 URB逆转lps诱导的膀胱亢进。在7 mg时,URB不能逆转或减少lps诱导的膀胱亢进。给药CB1、CB2和TRPV1拮抗剂没有改变幼年动物排尿收缩的频率。CB1拮抗剂可逆转0.7 URB的作用,而TRPV1拮抗剂可降低7 URB的作用。炎症期间AEA水平升高。用0.7 mg URB治疗lps炎症动物,使AEA水平达到控制水平。与lps炎症动物相比,用7毫克URB治疗lps炎症动物没有改变AEA水平。炎症期间PEA水平降低。用0.7 mg URB治疗lps炎症动物,使AEA水平达到控制水平。用7毫克URB治疗LPS炎症动物,将PEA水平降低到与LPS炎症动物相似的水平。结论:在膀胱炎期间,FAAH抑制剂通过CB1受体介导的机制提高PEA水平并逆转尿频。当使用非常高剂量时,FAAH拮抗剂通过trpv1依赖机制提高AEA水平并增加尿频。因此,临床应用FAAH抑制剂剂量的选择应考虑对系统内源性大麻素水平的影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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