Targeting histone modifiers in bladder cancer therapy — preclinical and clinical evidence

IF 12.1 1区 医学 Q1 UROLOGY & NEPHROLOGY Nature Reviews Urology Pub Date : 2024-02-19 DOI:10.1038/s41585-024-00857-z
Shiyu Zhang, Tianhai Lin, Xingyu Xiong, Chong Chen, Ping Tan, Qiang Wei
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Abstract

Bladder cancer in the most advanced, muscle-invasive stage is lethal, and very limited therapeutic advances have been reported for decades. To date, cisplatin-based chemotherapy remains the first-line therapy for advanced bladder cancer. Late-line options have historically been limited. In the past few years, next-generation sequencing technology has enabled chromatin remodelling gene mutations to be characterized, showing that these alterations are more frequent in urothelial bladder carcinoma than in other cancer types. Histone modifiers have functional roles in tumour progression by modulating the expression of tumour suppressors and oncogenes and, therefore, have been considered as novel drug targets for cancer therapy. The roles of epigenetic reprogramming through histone modifications have been increasingly studied in bladder cancer, and the therapeutic efficacy of targeting those histone modifiers genetically or chemically is being assessed in preclinical studies. Results from preclinical studies in bladder cancer encouraged the investigation of some of these drugs in clinical trials, which yield mixed results. Further understanding of how alterations of histone modification mechanistically contribute to bladder cancer progression, drug resistance and tumour microenvironment remodelling will be required to facilitate clinical application of epigenetic drugs in bladder cancer. In this Perspective, the authors discuss the idea of targeting histone modifications in bladder cancer, providing a comprehensive overview of findings from preclinical and translational studies. Clinical trials in which the efficacy of molecules targeting histone modifiers was assessed in bladder cancer are also discussed.

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在膀胱癌治疗中靶向组蛋白修饰剂--临床前和临床证据。
膀胱癌最晚期的肌肉浸润期是致命的,几十年来,治疗进展非常有限。迄今为止,顺铂化疗仍是晚期膀胱癌的一线疗法。晚期选择历来有限。在过去几年中,新一代测序技术已能确定染色质重塑基因突变的特征,显示这些改变在尿路上皮膀胱癌中比在其他癌症类型中更为常见。组蛋白修饰因子通过调节肿瘤抑制因子和癌基因的表达,在肿瘤进展过程中发挥着功能性作用,因此被认为是治疗癌症的新型药物靶点。通过组蛋白修饰进行表观遗传学重编程在膀胱癌中的作用已得到越来越多的研究,临床前研究正在评估通过基因或化学方法靶向这些组蛋白修饰物的疗效。膀胱癌临床前研究的结果鼓励人们在临床试验中对其中一些药物进行研究,但结果喜忧参半。要促进表观遗传药物在膀胱癌中的临床应用,还需要进一步了解组蛋白修饰的改变是如何从机理上导致膀胱癌进展、耐药性和肿瘤微环境重塑的。
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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来源期刊
Nature Reviews Urology
Nature Reviews Urology 医学-泌尿学与肾脏学
CiteScore
12.50
自引率
2.60%
发文量
123
审稿时长
6-12 weeks
期刊介绍: Nature Reviews Urology is part of the Nature Reviews portfolio of journals.Nature Reviews' basic, translational and clinical content is written by internationally renowned basic and clinical academics and researchers. This journal targeted readers in the biological and medical sciences, from the postgraduate level upwards, aiming to be accessible to professionals in any biological or medical discipline. The journal features authoritative In-depth Reviews providing up-to-date information on topics within a field's history and development. Perspectives, News & Views articles, and the Research Highlights section offer topical discussions and opinions, filtering primary research from various medical journals. Covering a wide range of subjects, including andrology, urologic oncology, and imaging, Nature Reviews provides valuable insights for practitioners, researchers, and academics within urology and related fields.
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