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循环 microRNAs 作为有前途的睾丸可转化的安全生物标志物:现状与未来展望。

Circulating microRNAs as promising testicular translatable safety biomarkers: current state and future perspectives.

机构信息

Drug Safety Research & Development, Pfizer Worldwide Research, Development & Medical, 10777 Science Center Dr, San Diego, CA, USA.

Drug Safety Research & Development, Pfizer Worldwide Research, Development & Medical, 445 Eastern Point Rd., Groton, CT, USA.

出版信息

Arch Toxicol. 2023 Apr;97(4):947-961. doi: 10.1007/s00204-023-03460-0. Epub 2023 Feb 16.

Abstract

Drug-induced testicular injury (DITI) is one of the often-observed and challenging safety issues seen during drug development. Semen analysis and circulating hormones currently utilized have significant gaps in their ability to detect testicular damage accurately. In addition, no biomarkers enable a mechanistic understanding of the damage to the different regions of the testis, such as seminiferous tubules, Sertoli, and Leydig cells. MicroRNAs (miRNAs) are a class of non-coding RNAs that modulate gene expression post-transcriptionally and have been indicated to regulate a wide range of biological pathways. Circulating miRNAs can be measured in the body fluids due to tissue-specific cell injury/damage or toxicant exposure. Therefore, these circulating miRNAs have become attractive and promising non-invasive biomarkers for assessing drug-induced testicular injury, with several reports on their use as safety biomarkers for monitoring testicular damage in preclinical species. Leveraging emerging tools such as 'organs-on-chips' that can emulate the human organ's physiological environment and function is starting to enable biomarker discovery, validation, and clinical translation for regulatory qualification and implementation in drug development.

摘要

药物引起的睾丸损伤(DITI)是药物开发过程中经常观察到的具有挑战性的安全问题之一。目前用于检测睾丸损伤的精液分析和循环激素在准确检测睾丸损伤方面存在明显的不足。此外,没有生物标志物能够对睾丸的不同区域(如曲细精管、支持细胞和间质细胞)的损伤进行机制上的理解。微小 RNA(miRNA)是一类非编码 RNA,能够在后转录水平上调节基因表达,并且已经表明它们可以调节广泛的生物途径。由于组织特异性细胞损伤/损伤或毒物暴露,循环 miRNA 可以在体液中测量。因此,这些循环 miRNA 已成为评估药物引起的睾丸损伤的有吸引力和有前途的非侵入性生物标志物,已有一些关于它们在临床前物种中作为监测睾丸损伤的安全性生物标志物的使用的报道。利用“器官芯片”等新兴工具可以模拟人体器官的生理环境和功能,这开始能够发现、验证和转化生物标志物,用于监管资格的临床翻译,并在药物开发中实施。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ec3f/9933818/87eca35ef5d8/204_2023_3460_Fig1_HTML.jpg

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