头颈部癌新辅助化疗中双氢嘧啶脱氢酶突变:神话还是现实?
Dihydropyrimidine dehydrogenase mutation in neoadjuvant chemotherapy in head and neck cancers: Myth or reality?
作者信息
Patil Vijay M, Noronha Vanita, Joshi Amit, Zanwar Saurabh, Ramaswamy Anant, Arya Supreeta, Mahajan Abhishek, Bhattacharjee Atanu, Prabhash Kumar
机构信息
Department of Medical Oncology, Tata Memorial Hospital, Mumbai, Maharashtra, India.
Department of Radiodiagnosis, Tata Memorial Hospital, Mumbai, Maharashtra, India.
出版信息
South Asian J Cancer. 2016 Oct-Dec;5(4):182-185. doi: 10.4103/2278-330X.195338.
PURPOSE
The docetaxel, 5-fluorouracil (5-FU), and cisplatin (TPF) regimen in India is associated with high percentages of Grade 3-4 toxicity. This analysis was planned to evaluate the incidence of dihydropyrimidine dehydrogenase (DPD) mutation in patients with severe gastrointestinal toxicity, to assess whether the mutation could be predicted by a set of clinical criteria and whether it has any impact on postneoadjuvant chemotherapy response.
METHODS
All consecutive patients who received TPF regimen in head and neck cancers between January 2015 and April 2015 were selected. Patients who had predefined set of toxicities in Cycle 1 were selected for DPD mutation testing. Depending on the results, C2 doses were modified. Postcompletion of two cycles, patients underwent radiological response assessment. Descriptive statistics has been performed. The normally distributed continuous variables were compared by unpaired Student's -test, whereas variables which were not normally distributed by Wilcoxon sum rank test. For noncontinuous variables, comparison was performed by Fisher's exact test.
RESULTS
Out of 34 patients, who received TPF, 12 were selected for DPD testing, and 11 (32.4%, 95% confidence interval [95% CI]: 19.1-49.3%) had DPD mutation. The predictive accuracy of the criteria for the tested DPD mutations was 81.3% (95% CI: 62.1-100%). Of the 11 DPD mutation positive patients, except for one patient, all others received the second cycle of TPF. The dose adjustments done in 5-FU were 50% dose reduction in 9 patients and no dose reduction in one patient. The response rate in DPD mutated patients was 27.3% (3/11) and that in DPD nonmutated/nontested was 39.1% (9/23) ( = 0.70).
CONCLUSION
In this small study, it seems that the incidence of DPD mutation is more common in Indian then it's in the Caucasian population. Clinical toxicity criteria can accurately predict for DPD mutation. Postdose adjustments of 5-FU from C2 onward, TPF can safely be delivered in the majority of patients with DPD heterozygous mutations without decrement in efficacy.
目的
在印度,多西他赛、5-氟尿嘧啶(5-FU)和顺铂(TPF)方案与3-4级毒性的高发生率相关。本分析旨在评估严重胃肠道毒性患者中二氢嘧啶脱氢酶(DPD)突变的发生率,评估该突变是否可通过一组临床标准预测,以及它对新辅助化疗反应是否有任何影响。
方法
选取2015年1月至2015年4月间所有接受TPF方案治疗头颈癌的连续患者。选取在第1周期有预定义毒性的患者进行DPD突变检测。根据结果调整第2周期(C2)的剂量。两个周期完成后,对患者进行放射学反应评估。进行了描述性统计。正态分布的连续变量采用非配对学生t检验进行比较,非正态分布的变量采用Wilcoxon秩和检验。对于非连续变量,采用Fisher精确检验进行比较。
结果
在接受TPF治疗的34例患者中,12例被选进行DPD检测,11例(32.4%,95%置信区间[95%CI]:19.1-49.3%)有DPD突变。所检测的DPD突变标准的预测准确率为81.3%(95%CI:62.1-100%)。在11例DPD突变阳性患者中,除1例患者外,所有其他患者均接受了第2周期的TPF治疗。9例患者的5-FU剂量调整为降低50%,1例患者未降低剂量。DPD突变患者的缓解率为27.3%(3/11),DPD未突变/未检测患者的缓解率为39.1%(9/23)(P = 0.70)。
结论
在这项小型研究中,似乎DPD突变的发生率在印度比在白种人群中更常见。临床毒性标准可准确预测DPD突变。从第2周期(C2)起对5-FU进行剂量调整后,大多数DPD杂合突变患者可安全接受TPF治疗,且疗效不会降低。
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