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氯胺酮诱导的尿路上皮毒性:接受氯胺酮治疗的心境障碍成人的潜在机制及转化。

Ketamine-induced urological toxicity: potential mechanisms and translation for adults with mood disorders receiving ketamine treatment.

机构信息

Mood Disorder Psychopharmacology Unit, University Health Network, 399 Bathurst Street, MP 9-325, Toronto, ON, M5T 2S8, Canada.

Canadian Rapid Treatment Center of Excellence, Mississauga, ON, Canada.

出版信息

Psychopharmacology (Berl). 2021 Apr;238(4):917-926. doi: 10.1007/s00213-021-05767-1. Epub 2021 Jan 23.

Abstract

Intravenous (IV) ketamine has been shown to have rapid and robust antidepressant effects in adults with treatment-resistant depression (TRD). Urological toxicity has been observed in chronic ketamine abusers as evidenced by dysuria, urgency, and hematuria. The foregoing observation provides the basis for evaluating whether ketamine-induced urological toxicity (KIUT) is associated with sub-anesthetic doses of ketamine (0.5-1.0 mg/kg) in adults with mood disorders. The overarching objective of this article is to identify potential mechanisms of KIUT which appears to be dose and frequency dependent. Available research indicates that high-frequency ketamine is associated with disruption of the urothelial barrier as well as direct ketamine toxicity (i.e., decreased expression of junction proteins) in KIUT of the bladder. Chronic and high-frequency ketamine use is also associated with bladder inflammation mediated via neurogenic and IgE inflammation. Other non-mutually exclusive causes are nerve hyperplasia, hypersensitivity, cell apoptosis, microvascular damage, and overexpression of carcinogenic genes. Notwithstanding the evidence of KIUT in ketamine abusers, there is no evidence that ketamine and/or esketamine treatment in adults with mood disorders is associated with KIUT. However, all patients receiving ketamine/esketamine for mood disorder treatment should be queried about genitourinary symptoms during acute and, where applicable, maintenance dosing.

摘要

静脉注射(IV)氯胺酮已被证明对治疗抵抗性抑郁症(TRD)的成年人具有快速而强大的抗抑郁作用。慢性氯胺酮滥用者出现了尿路上皮毒性,表现为尿痛、尿急和血尿。上述观察为评估氯胺酮诱导的尿路上皮毒性(KIUT)是否与心境障碍成年人的亚麻醉剂量氯胺酮(0.5-1.0mg/kg)有关提供了依据。本文的总体目标是确定 KIUT 的潜在机制,这似乎与剂量和频率有关。现有研究表明,高频氯胺酮与膀胱的尿路上皮屏障破坏以及直接的氯胺酮毒性(即连接蛋白表达减少)有关。慢性和高频氯胺酮的使用也与通过神经源性和 IgE 炎症介导的膀胱炎症有关。其他非互斥的原因包括神经增生、过敏、细胞凋亡、微血管损伤和致癌基因的过度表达。尽管有证据表明氯胺酮滥用者存在 KIUT,但没有证据表明心境障碍成年人的氯胺酮和/或依他硝唑治疗与 KIUT 有关。然而,所有接受氯胺酮/依他硝唑治疗心境障碍的患者都应在急性和适用的维持剂量期间询问其泌尿生殖系统症状。

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