Efficacy and safety of oral pharmacological and supplementary therapies in bladder pain syndrome: a systematic review

被引:0
作者
I Putu Eka Widyadharma
Valentina Tjandra Dewi
Ida Ayu Sri Wijayanti
Kadek Budi Santosa
机构
[1] Udayana University/Sanglah General Hospital,Department of Neurology, Faculty of Medicine
[2] Udayana University/Universitas Udayana Hospital,Department of Neurology, Faculty of Medicine
[3] Udayana University/Sanglah General Hospital,Department of Urology, Faculty of Medicine
来源
The Egyptian Journal of Neurology, Psychiatry and Neurosurgery | / 58卷
关键词
Bladder pain syndrome; Interstitial cystitis; Oral therapy;
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学科分类号
摘要
Treatment goals in bladder pain syndrome (BPS) or interstitial cystitis (IC) focusing on relieving symptoms to improve quality of life and avoiding adverse events (AEs) since curative treatment for BPS/IC is not available. The readily available pharmacologic options for BPS/IC including oral, intravesical, and transdermal therapy. The purpose of this study is to review randomized trial studies over the last 15 years examining the efficacy and safety of oral pharmacological and supplementary therapies for BPS/IC. A systematic search was conducted in PubMed and Medline Library. Only randomized-controlled trials and randomized comparative trials published between 2005 and 2020 on the efficacy and safety of oral therapies for BPS/IC were included. The keywords used were “bladder pain syndrome”, or “interstitial cystitis”, and “random” or “trial”. From 629 articles, nine were included in this review. Oral therapies included consist of cyclosporine A (CyA), amitriptyline, amitriptyline plus alpha lipoic acid (ALA) and omega-3 fatty acids (n-3 PUFA), PD-0299685, sildenafil, pentosan polysulfate sodium (PPS), AQX-1125, and hydrogen-rich water. Among retrieved trials, amitriptyline in combination with ALA and n-3 PUFA, sildenafil, and cyclosporine A proved their efficacy for BPS/IC. Sildenafil was generally well tolerated, while amitriptyline and CyA must be used with caution, the supplementation of ALA/n-3 PUFAs possibly lower dosage of amitriptyline, subsequently reduce its AEs. CyA was superior to PPS but possessed greater AEs. Further studies focusing on etiopathology and phenotype differentiation of this syndrome will greatly contribute to the development of effective therapy.
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