Oxidative Stress and Its Relation to Lower Urinary Tract Symptoms.

IF 1.8 3区 医学 Q3 UROLOGY & NEPHROLOGY
International Neurourology Journal Pub Date : 2022-12-01 Epub Date: 2022-12-30 DOI:10.5213/inj.2244190.095
Karl-Erik Andersson
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Abstract

The aim of this review is to discuss how to link lower urinary tract symptoms (LUTS) and oxidative stress (OS) and to define relevant targets for therapeutic intervention. Narrative review based on published literature. Many of the multifactorial pathophysiological mechanisms behind LUTS can initiate reactive oxygen species (ROS) generation. Assuming that OS is a consequence rather than a primary cause of LUTS it seems reasonable to identify both the disease mechanism initiating LUTS, and the source of ROS involved. There are many possible sources of ROS overproduction, but the NADPH oxidase (NOX) family of enzymes is the primary source; NOX activation in turn, may result in the activation of secondary ROS sources, i.e., ROS-dependent ROS production. Selective NOX inhibition therefore seems an attractive therapeutic strategy in LUTS treatment. The finding of NOX2 localization to centers in the brain associated with micturition control, opens up for further studies of NOX involvement in the central control of micturition, normally and in disease. Further information on the localization of the different isoforms of NOX in the LUT e.g., the bladder wall and its components and the prostate, is desirable. To optimize treatment, the pathophysiological mechanism initiating LUTS, and the activated isoform of NOX, should be identified. Unfortunately, in most cases of LUTS this is currently not possible. Even if selective NOX inhibitors have entered the clinical trial stage for treatment of disorders other than LUT dysfunction, their efficacy for LUTS treatment has to be demonstrated. If this can be achieved, an attractive approach would be combination of selective NOX inhibition with established drug therapies.

Abstract Image

Abstract Image

氧化应激及其与下尿路症状的关系
本综述旨在讨论如何将下尿路症状(LUTS)与氧化应激(OS)联系起来,并确定相关的治疗干预目标。根据已发表的文献进行叙述性综述。下尿路症状背后的许多多因素病理生理机制都会引发活性氧(ROS)的产生。假定OS是LUTS的后果而非主要原因,那么确定引发LUTS的疾病机制和所涉及的ROS来源似乎是合理的。ROS 过量产生的可能来源有很多,但 NADPH 氧化酶(NOX)家族酶是主要来源;NOX 的激活反过来又可能导致次要 ROS 来源的激活,即 ROS 依赖性 ROS 的产生。因此,选择性抑制 NOX 似乎是治疗 LUTS 的一种有吸引力的治疗策略。NOX2 定位于大脑中与控制排尿有关的中枢,这一发现为进一步研究 NOX 在正常和疾病情况下参与排尿中枢控制开辟了道路。我们希望进一步了解 NOX 不同异构体在 LUT(如膀胱壁及其组成部分和前列腺)中的定位情况。为了优化治疗,应确定引发 LUTS 的病理生理机制和激活的 NOX 同工酶。遗憾的是,在大多数 LUTS 病例中,目前还无法做到这一点。即使选择性 NOX 抑制剂已进入临床试验阶段,用于治疗 LUT 功能障碍以外的其他疾病,但其治疗 LUTS 的疗效仍有待证实。如果能够做到这一点,一种有吸引力的方法就是将选择性 NOX 抑制剂与已有的药物疗法相结合。
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来源期刊
International Neurourology Journal
International Neurourology Journal UROLOGY & NEPHROLOGY-
CiteScore
4.40
自引率
21.70%
发文量
41
审稿时长
4 weeks
期刊介绍: The International Neurourology Journal (Int Neurourol J, INJ) is a quarterly international journal that publishes high-quality research papers that provide the most significant and promising achievements in the fields of clinical neurourology and fundamental science. Specifically, fundamental science includes the most influential research papers from all fields of science and technology, revolutionizing what physicians and researchers practicing the art of neurourology worldwide know. Thus, we welcome valuable basic research articles to introduce cutting-edge translational research of fundamental sciences to clinical neurourology. In the editorials, urologists will present their perspectives on these articles. The original mission statement of the INJ was published on October 12, 1997. INJ provides authors a fast review of their work and makes a decision in an average of three to four weeks of receiving submissions. If accepted, articles are posted online in fully citable form. Supplementary issues will be published interim to quarterlies, as necessary, to fully allow berth to accept and publish relevant articles.
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