Review of the fluoropyrimidine antidote uridine triacetate.

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2024-10-28 DOI:10.1111/bcp.16319
Jack T Thompson, David M Wood, Paul I Dargan
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Abstract

In 2015, the United States Food and Drug Administration (FDA) approved uridine triacetate to treat overdose and severe toxicity of the fluoropyrimidine chemotherapy agents 5-fluorouracil (5-FU) and its oral prodrug capecitabine. Uridine triacetate is as an oral prodrug of uridine that competes with cytotoxic fluoropyrimidine metabolites for incorporation into nucleotides. Two million people worldwide start fluoropyrimidine chemotherapy each year, with 20-30% developing severe or life-threatening adverse effects, often attributable to a genetic predisposition such as dihydropyrimidine dehydrogenase deficiency. Whilst genetic prescreening is recommended prior to starting fluoropyrimidine agents, this only prevents 20-30% of early-onset life-threatening toxicity and so does not obviate the need for an antidote. Initial in-human studies established that uridine triacetate more than doubles the maximum tolerated weekly 5-FU bolus dose. A lack of clinical equipoise meant a placebo-controlled phase III trial was not ethical and so the phase III trials used historical controls. These found that uridine triacetate improved survival in those with fluoropyrimidine overdose and severe toxicity from 16% to 94%, with 34% able to resume chemotherapy within 30 days. Five case reports of delayed fluoropyrimidine toxicity demonstrate improvement following uridine triacetate treatment 120-504 h after last fluoropyrimidine administration, suggesting efficacy beyond the FDA licencing indications. Mechanistically uridine triacetate would be expected to be effective for overdose and severe toxicity of tegafur (a 5-FU prodrug), but there are no published case reports describing this. Uridine triacetate is available internationally through an expanded access scheme and has been available in the UK since 2019 on a named patient basis.

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审查氟嘧啶解毒剂三乙酸尿苷。
2015 年,美国食品和药物管理局(FDA)批准三醋酸尿苷治疗氟嘧啶类化疗药 5-氟尿嘧啶(5-FU)及其口服原药卡培他滨的过量和严重毒性。三乙酸尿苷作为尿苷的口服原药,可与具有细胞毒性的氟嘧啶代谢物竞争,以掺入核苷酸中。全世界每年有 200 万人开始接受氟嘧啶化疗,其中 20%-30% 会出现严重或危及生命的不良反应,这些不良反应通常可归因于遗传倾向,如二氢嘧啶脱氢酶缺乏症。虽然建议在开始使用氟嘧啶类药物前进行基因预检,但这只能预防 20-30% 的早期危及生命的毒性,因此并不能避免对解毒剂的需求。最初的人体研究证实,三乙酸尿苷可使 5-FU 每周最大耐受栓剂剂量增加一倍以上。由于缺乏临床等效性,安慰剂对照的 III 期试验不符合道德标准,因此 III 期试验采用了历史对照。这些试验发现,三醋酸尿苷可将氟嘧啶过量和严重毒性患者的生存率从 16% 提高到 94%,其中 34% 的患者可在 30 天内恢复化疗。五份氟嘧啶延迟毒性病例报告显示,在最后一次服用氟嘧啶后 120-504 小时服用三乙酸尿苷治疗后,毒性有所改善,这表明其疗效超出了美国食品及药物管理局的许可适应症范围。从机理上讲,三乙酸尿苷有望对替加氟(一种 5-FU 原药)的过量和严重毒性产生疗效,但目前还没有这方面的公开病例报告。三醋酸尿苷在国际上可通过扩大准入计划获得,自2019年起,英国也可根据指定患者的情况提供三醋酸尿苷。
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来源期刊
CiteScore
7.20
自引率
4.30%
发文量
567
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