携带致病变异型 DPYD 的患者接受氟嘧啶化疗的相关治疗死亡率:系统评价和荟萃分析。
Pathogenic DPYD Variants and Treatment-Related Mortality in Patients Receiving Fluoropyrimidine Chemotherapy: A Systematic Review and Meta-Analysis.
机构信息
Dartmouth-Hitchcock Medical Center, Lebanon, New Hampshire, USA.
Geisel School of Medicine at Dartmouth, Lebanon, New Hamphsire, USA.
出版信息
Oncologist. 2021 Dec;26(12):1008-1016. doi: 10.1002/onco.13967. Epub 2021 Sep 29.
BACKGROUND
Pathogenic variants of the DPYD gene are strongly associated with grade ≥3 toxicity during fluoropyrimidine chemotherapy. We conducted a systematic review and meta-analysis to estimate the risk of treatment-related death associated with DPYD gene variants.
MATERIALS AND METHODS
We searched for reports published prior to September 17, 2020, that described patients receiving standard-dose fluoropyrimidine chemotherapy (5-fluorouracil or capecitabine) who had baseline testing for at least one of four pathogenic DPYD variants (c.1129-5923C>G [HapB3], c.1679T>G [*13], c.1905+1G>A [*2A], and c.2846A>T) and were assessed for toxicity. Two reviewers assessed studies for inclusion and extracted study-level data. The primary outcome was the relative risk of treatment-related mortality for DPYD variant carriers versus noncarriers; we performed data synthesis using a Mantel-Haenszel fixed effects model.
RESULTS
Of the 2,923 references screened, 35 studies involving 13,929 patients were included. DPYD variants (heterozygous or homozygous) were identified in 566 patients (4.1%). There were 14 treatment-related deaths in 13,363 patients without identified DPYD variants (treatment-related mortality, 0.1%; 95% confidence interval [CI], 0.1-0.2) and 13 treatment-related deaths in 566 patients with any of the four DPYD variants (treatment-related mortality, 2.3%; 95% CI, 1.3%-3.9%). Carriers of pathogenic DPYD gene variants had a 25.6 times increased risk of treatment-related death (95% CI, 12.1-53.9; p < .001). After excluding carriers of the more common but less deleterious c.1129-5923C>G variant, carriers of c.1679T>G, c.1905+1G>A, and/or c.2846A>T had treatment-related mortality of 3.7%.
CONCLUSION
Patients with pathogenic DPYD gene variants who receive standard-dose fluoropyrimidine chemotherapy have greatly increased risk for treatment-related death.
IMPLICATIONS FOR PRACTICE
The syndrome of dihydropyrimidine dehydrogenase (DPD) deficiency is an uncommon but well-described cause of severe toxicity related to fluoropyrimidine chemotherapy agents (5-fluorouracil and capecitabine). Patients with latent DPD deficiency can be identified preemptively with genotyping of the DPYD gene, or with measurement of the plasma uracil concentration. In this systematic review and meta-analysis, the authors study the rare outcome of treatment-related death after fluoropyrimidine chemotherapy. DPYD gene variants associated with DPD deficiency were linked to a 25.6 times increased risk of fluoropyrimidine-related mortality. These findings support the clinical utility of DPYD genotyping as a screening test for DPD deficiency.
背景
DPYD 基因的致病性变异与氟嘧啶化疗期间≥3 级毒性密切相关。我们进行了系统评价和荟萃分析,以估计与 DPYD 基因变异相关的治疗相关死亡风险。
材料和方法
我们检索了截至 2020 年 9 月 17 日之前发表的描述接受标准剂量氟嘧啶化疗(5-氟尿嘧啶或卡培他滨)且基线检测至少有四种致病性 DPYD 变异(c.1129-5923C>G [HapB3]、c.1679T>G [*13]、c.1905+1G>A [*2A]和 c.2846A>T)之一并评估毒性的患者报告。两位评审员评估了研究的纳入情况并提取了研究水平的数据。主要结局是 DPYD 变异携带者与非携带者治疗相关死亡率的相对风险;我们使用 Mantel-Haenszel 固定效应模型进行了数据综合。
结果
在筛选出的 2923 篇参考文献中,有 35 项研究纳入了 13929 名患者。在 13363 名未发现 DPYD 变异的患者中,有 14 例治疗相关死亡(治疗相关死亡率为 0.1%;95%置信区间 [CI],0.1-0.2),在 566 名有任何一种四种 DPYD 变异的患者中,有 13 例治疗相关死亡(治疗相关死亡率为 2.3%;95% CI,1.3%-3.9%)。携带致病性 DPYD 基因突变的患者治疗相关死亡风险增加 25.6 倍(95% CI,12.1-53.9;p<0.001)。排除更常见但毒性较小的 c.1129-5923C>G 变异携带者后,c.1679T>G、c.1905+1G>A 和/或 c.2846A>T 变异携带者的治疗相关死亡率为 3.7%。
结论
接受标准剂量氟嘧啶化疗的携带致病性 DPYD 基因突变的患者治疗相关死亡风险大大增加。
临床意义
二氢嘧啶脱氢酶(DPD)缺乏症综合征是氟嘧啶化疗药物(5-氟尿嘧啶和卡培他滨)相关严重毒性的一种罕见但已充分描述的原因。可以通过 DPYD 基因的基因分型或血浆尿嘧啶浓度的测量来预先识别潜在的 DPD 缺乏症患者。在这项系统评价和荟萃分析中,作者研究了氟嘧啶化疗后治疗相关死亡的罕见结局。与 DPD 缺乏相关的 DPYD 基因突变与氟嘧啶相关死亡率增加 25.6 倍相关。这些发现支持 DPYD 基因分型作为 DPD 缺乏症筛查试验的临床效用。
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