DPYD genotype-guided dose personalisation for fluoropyrimidine-based chemotherapy prescribing in solid organ cancer patients in Australia: GeneScreen 5-FU study protocol.

IF 3.4 2区 医学 Q2 ONCOLOGY BMC Cancer Pub Date : 2024-11-08 DOI:10.1186/s12885-024-13122-8
Cassandra White, Hannah Wardill, Christine Paul, Timothy Price, Christos Karapetis, Mark Nalder, Matthew E Burge, Ann Thomas, Chris Oldmeadow, Daniel Barker, Laura C Edney, Janet Coller, Joanne Bowen, Cheri Ostroff, Bruce Cheek, Mel Carlson, Trumaine Rankmore, Adnan Nagrial, Stephen Clarke, Lorraine Chantrill, Stephen Ackland, Rodney J Scott
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引用次数: 0

Abstract

Background: Fluoropyrimidine (FP) chemotherapies are commonly prescribed for upper and lower gastrointestinal, breast and head and neck malignancies. Over 16,000 people with cancer require FP chemotherapies per annum in Australia. Between 10 and 40% patients experience grade 3-4 (≥ G3) toxicities that require hospital-based management ± intensive care admission. Approximately 1% of patients die secondary to FP toxicities. Prospective screening for DPYD gene variants (encoding the key enzyme for FP catabolism) can identify patients at risk of ≥ G3 toxicity and allow for dose adjustment prior to first FP exposure. Evidence supports this as a cost-effective method of improving patient safety and reducing healthcare burden internationally; however, no Australian data confirms its feasibility on a large scale.

Method: This investigator-led, single-arm study will determine large scale feasibility of prospective DPYD genotyping, confirming patient safety and cost-effectiveness within the Australian health care system. 5000 patients aged 18 years and older with solid organ cancers requiring FP chemotherapy will be consented and genotyped prior to commencing treatment, and early toxicity (within 60 days) post-FP exposure will be determined. Toxicity data for DPYD variant carriers who have dose adjustments will be compared to the wild-type cohort and historical cohorts of carriers who did not undergo genotyping prior to FP exposure, and prospective variant carriers who do not undergo dose-adjustment. Prevalence of the four standard DPYD gene variants will be confirmed in an Australian population. Additionally, health economic analysis, implementation research via semi-structured interviews of patients and clinicians, and feasibility of UGT1A1 genotyping will be conducted.

Discussion: This study will determine the prevalence of DPYD gene variant status in Australia and its impact on FP-induced toxicity among Australians with cancer. Feasibility and cost-effectiveness for Australian health care system will be estimated to support national roll-out of prospective DPYD genotyping prior to FP administration. Additionally, feasibility will be confirmed with the intention of including UGT1A1 in future pharmacogenomic panels to aid chemotherapy prescribing.

Trial registration: This trial was registered with the Australian and New Zealand Cancer Trials Registry on 13th Dec 2023, ACTRN12623001301651.

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澳大利亚实体器官癌症患者基于氟嘧啶化疗处方的 DPYD 基因型指导剂量个性化:GeneScreen 5-FU研究方案。
背景:氟嘧啶(FP)化疗是治疗上下消化道、乳腺和头颈部恶性肿瘤的常用处方药。在澳大利亚,每年有 16,000 多名癌症患者需要接受 FP 化疗。10%到40%的患者会出现3-4级(≥ G3)毒性反应,需要住院治疗±重症监护。约1%的患者死于FP毒性反应。DPYD基因变异(编码FP分解代谢的关键酶)的前瞻性筛查可识别有≥G3毒性风险的患者,并在首次接触FP前调整剂量。有证据表明,这是一种具有成本效益的方法,可提高患者安全性并减轻国际医疗负担;然而,澳大利亚尚无数据证实其在大规模应用中的可行性:这项由研究者领导的单臂研究将确定前瞻性 DPYD 基因分型的大规模可行性,确认澳大利亚医疗保健系统内的患者安全性和成本效益。5000名年龄在18岁及以上、需要进行FP化疗的实体器官癌症患者将在开始治疗前获得同意并进行基因分型,并确定FP暴露后的早期毒性(60天内)。进行剂量调整的 DPYD 变异携带者的毒性数据将与野生型队列、FP 暴露前未进行基因分型的携带者历史队列以及未进行剂量调整的前瞻性变异携带者进行比较。将在澳大利亚人群中确认四种标准 DPYD 基因变异的流行率。此外,还将进行卫生经济分析、通过对患者和临床医生进行半结构化访谈开展实施研究,以及进行 UGT1A1 基因分型的可行性研究:本研究将确定 DPYD 基因变异状态在澳大利亚的流行程度及其对澳大利亚癌症患者中 FP 诱导毒性的影响。将对澳大利亚医疗保健系统的可行性和成本效益进行估算,以支持在使用 FP 之前在全国推广前瞻性 DPYD 基因分型。此外,还将对可行性进行确认,以便将UGT1A1纳入未来的药物基因组小组,帮助开具化疗处方:该试验已于2023年12月13日在澳大利亚和新西兰癌症试验注册中心注册,注册号为ACTRN12623001301651。
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来源期刊
BMC Cancer
BMC Cancer 医学-肿瘤学
CiteScore
6.00
自引率
2.60%
发文量
1204
审稿时长
6.8 months
期刊介绍: BMC Cancer is an open access, peer-reviewed journal that considers articles on all aspects of cancer research, including the pathophysiology, prevention, diagnosis and treatment of cancers. The journal welcomes submissions concerning molecular and cellular biology, genetics, epidemiology, and clinical trials.
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