MTHFR基因变异与中国骨肉瘤患者中高剂量甲氨蝶呤诱导的毒性相关。
MTHFR variant is associated with high-dose methotrexate-induced toxicity in the Chinese osteosarcoma patients.
作者信息
Xu Leilei, Wang Lujun, Xue Bingchuan, Wang Shoufeng
机构信息
Department of Orthopedic Surgery, The Affiliated Drum Tower Hospital of Nanjing University Medical School, Zhongshan Road 321, Nanjing 210008, China.
Department of Pharmacy, The Affiliated Drum Tower Hospital of Nanjing University Medical School, China.
出版信息
J Bone Oncol. 2018 Nov 1;13:143-147. doi: 10.1016/j.jbo.2018.10.002. eCollection 2018 Nov.
BACKGROUND
The role of Methylene tetrahydrofolate reductase (MTHFR) C677T and A1298C polymorphisms in the efficacy and toxicity of MTX-based therapy remains uncertain. Our purpose was to clarify whether these two polymorphisms are associated with the outcome of chemotherapy in a cohort of Chinese osteosarcoma (OS) patients treated by high-dose MTX.
METHODS
109 OS patients who had sequentially received high-dose MTX therapy were included in this study. Plasma MTX level was measured routinely at 0, 24, 48 and 72 h after the administration of MTX. Two variants of MTHFR were genotyped using TaqMan SNP Genotyping Assay, including rs1801133 (C667T) and rs1801131 (A1298C). The extent of toxicity induced by MTX, including hematological toxicity, hepatic toxicity, renal toxicity and mucositis, was scored from grade 1 to 4. Severe toxicity was defined as a grade score of ≥3. Patients were dichotomized as follows: grade <3 or ≥3 for toxicity, and ≤0.2 µmol/L or >0.2 µmol/L for plasma MTX level at 72 h. The frequencies of genotypes and allele were compared between the dichotomized groups with the Chi-square test.
RESULTS
24.8% (27/109) of the patients were found to have significantly high plasma MTX level at the 72 h. Patients with high MTX level at 72 h were found to have significantly higher frequency of genotype TT of rs1801133 (p = 0.002). As for rs1801131, no significant association was found with plasma MTX level. Patients with severe hepatic toxicity or mucositis were found to have remarkably higher incidence of genotype TT of rs1801133 than those with mild toxicity (33.3% vs. 14.8%, p = 0.04 for hepatic toxicity; 34.8% vs. 19.8%, p = 0.05 for mucositis).
CONCLUSIONS
Variant rs1801133 was confirmed to have remarkable influence on the MTX-induced toxicity. We recommend identification of the genotype of MTHFR variant prior to the application of high-dose MTX to OS patients, which could be an important predictor to screen severe toxicities and thus improve treatment outcomes.
背景
亚甲基四氢叶酸还原酶(MTHFR)C677T和A1298C基因多态性在基于甲氨蝶呤(MTX)治疗的疗效和毒性方面的作用仍不明确。我们的目的是阐明这两种基因多态性是否与接受大剂量MTX治疗的中国骨肉瘤(OS)患者队列的化疗结果相关。
方法
本研究纳入了109例序贯接受大剂量MTX治疗的OS患者。在MTX给药后0、24、48和72小时常规测量血浆MTX水平。使用TaqMan SNP基因分型检测对MTHFR的两个变体进行基因分型,包括rs1801133(C667T)和rs1801131(A1298C)。MTX诱导的毒性程度,包括血液学毒性、肝毒性、肾毒性和口腔炎,从1级到4级进行评分。严重毒性定义为分级评分≥3级。患者按以下方式进行二分法分类:毒性分级<3级或≥3级,以及72小时时血浆MTX水平≤0.2 μmol/L或>0.2 μmol/L。采用卡方检验比较二分法分组之间的基因型和等位基因频率。
结果
24.8%(27/109)的患者在72小时时血浆MTX水平显著升高。发现72小时时MTX水平高的患者rs1801133的TT基因型频率显著更高(p = 0.002)。至于rs1801131,未发现与血浆MTX水平有显著关联。发现严重肝毒性或口腔炎患者rs1801133的TT基因型发生率明显高于轻度毒性患者(肝毒性:33.3%对14.8%,p = 0.04;口腔炎:34.8%对19.8%,p = 0.05)。
结论
证实rs1801133变体对MTX诱导的毒性有显著影响。我们建议在对OS患者应用大剂量MTX之前鉴定MTHFR变体的基因型,这可能是筛查严重毒性从而改善治疗结果的重要预测指标。
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