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Scientific and Regulatory Policy Committee Points-to-consider Paper*: Drug-induced Vascular Injury Associated with Nonsmall Molecule Therapeutics in Preclinical Development: Part 2. Antisense Oligonucleotides

机译:科学与监管政策委员会的建议论文*:临床前开发中与非小分子药物治疗相关的药物诱发的血管损伤:第2部分。

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摘要

Drug-induced vascular injury (DIVI) is a recurrent challenge in the development of novel pharmaceutical agents. In recent years, DIVI has been occasionally observed in nonhuman primates given RNA-targeting therapeutics such as antisense oligonucleotide therapies (ASOs) during chronic toxicity studies. While DIVI in laboratory animal species has been well characterized for vasoactive small molecules, and immune-mediated responses against large molecule biotherapeutics have been well described, there is little published information regarding DIVI induced by ASOs to date. Preclinical DIVI findings in monkeys have caused considerable delays in development of promising new ASO therapies, because of the uncertainty about whether DIVI in preclinical studies is predictive of effects in humans, and the lack of robust biomarkers of DIVI. This review of DIVI discusses clinical and microscopic features of vasculitis in monkeys, their pathogenic mechanisms, and points to consider for the toxicologist and pathologist when confronted with ASO-related DIVI. Relevant examples of regulatory feedback are included to provide insight into risk assessment of ASO therapies.
机译:药物诱发的血管损伤(DIVI)是新型药物开发中的一个经常性挑战。近年来,在慢性毒性研究中,偶尔在非人灵长类动物中观察到DIVI给予RNA靶向治疗,例如反义寡核苷酸治疗(ASO)。虽然实验室动物物种中的DIVI具有良好的血管活性小分子特征,并且针对大分子生物治疗剂的免疫介导反应已有很好的描述,但迄今为止,关于ASO诱导的DIVI的信息很少。由于对临床前研究中的DIVI是否可预测对人类的影响尚存不确定性,并且缺乏可靠的DIVI生物标志物,猴子在临床前DIVI的发现已导致有希望的新ASO治疗方法的开发出现了相当大的延迟。这篇关于DIVI的综述讨论了猴子血管炎的临床和微观特征,它们的致病机制,以及当面对ASO相关DIVI时需要毒物学家和病理学家考虑的要点。包括监管反馈的相关示例,可深入了解ASO治疗的风险评估。

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