基于北中央癌症治疗组的探索性研究:还原型叶酸载体基因(SLC19A1)多态性与培美曲塞为基础的治疗后非小细胞肺癌患者生存的相关性。
Correlation between polymorphisms of the reduced folate carrier gene (SLC19A1) and survival after pemetrexed-based therapy in non-small cell lung cancer: a North Central Cancer Treatment Group-based exploratory study.
机构信息
Departments of Pharmacology & Therapeutics, Roswell Park Cancer Institute, Buffalo, NY 14263, USA.
出版信息
J Thorac Oncol. 2010 Sep;5(9):1346-53. doi: 10.1097/JTO.0b013e3181ec18c4.
PURPOSE
To correlate polymorphisms in genes involved in the transport, activation, and inactivation of pemetrexed with the outcome of patients with advanced non-small cell lung cancer (NSCLC) treated with pemetrexed.
EXPERIMENTAL DESIGN
Data from a phase II NSCLC trial evaluating the optimal schedule of gemcitabine and pemetrexed were used. All patients with available DNA were genotyped for polymorphisms in FPGS, GGH, and SLC19A1 genes. Patients with various genotypes were compared for efficacy and adverse events resulting from pemetrexed.
RESULTS
Fifty-four patients had genotype results for all polymorphisms studied. Patients with the homozygous variant genotypes for SLC19A1 IVS4(2117) C>T, IVS5(9148) C>A, and wild-type genotype for exon6(2522) C>T had a significantly better overall survival compared with their counterparts (median overall survival in months: 8.9 [CC] versus 14.0 [CT] versus 16.7 [TT]; 9.4 [CC] versus 10.3 [CA] versus 22.7 [AA]; and 22.7 [CC] versus 10.3 [CT] versus 9.4 [TT] respectively; all log rank p = 0.03). Patients with the heterozygous TC genotype for GGH IVS5(1042) T>C had greater rates of confirmed response + stable disease compared with the TT genotype (85% versus 60%; odds ratio = 4.0; p = 0.06). A greater risk for grade 3/4 SGPT (ALT) elevation was observed in patients heterozygous (GA) for the FPGS IVS1 (28) G>A polymorphism compared with the GG genotype (43% versus 13%; odds ratio = 5.0, p = 0.07). All results were largely consistent within patients with nonsquamous (n = 40) histology.
CONCLUSION
Polymorphisms in SLC1A91 seem to predict for survival differences in pemetrexed-treated NSCLC. Additionally, polymorphisms in GGH and FPGS have marginal associations with response and adverse event. These results should be validated in larger prospective studies using pemetrexed.
目的
研究与培美曲塞转运、激活和失活相关的基因多态性与培美曲塞治疗晚期非小细胞肺癌(NSCLC)患者结局的相关性。
实验设计
使用了评估吉西他滨和培美曲塞最佳方案的 II 期 NSCLC 试验的数据。对所有可获得 DNA 的患者进行 FPGS、GGH 和 SLC19A1 基因多态性的基因分型。比较不同基因型患者的培美曲塞疗效和不良反应。
结果
54 例患者的所有研究多态性均有基因型结果。SLC19A1 IVS4(2117) C>T、IVS5(9148) C>A 纯合变异基因型和外显子 6(2522) C>T 野生型的患者总生存显著优于相应患者(中位总生存月数:8.9[CC] vs. 14.0[CT] vs. 16.7[TT];9.4[CC] vs. 10.3[CA] vs. 22.7[AA];22.7[CC] vs. 10.3[CT] vs. 9.4[TT];所有 log rank p=0.03)。GGH IVS5(1042) T>C 杂合 TC 基因型的患者比 TT 基因型的患者更有确认缓解+稳定疾病的反应率(85% vs. 60%;优势比=4.0;p=0.06)。FPGS IVS1(28) G>A 多态性杂合(GA)的患者比 GG 基因型的患者更易发生 3/4 级 SGPT(ALT)升高(43% vs. 13%;优势比=5.0,p=0.07)。所有结果在非鳞状(n=40)组织学患者中基本一致。
结论
SLC1A91 中的多态性似乎可预测培美曲塞治疗 NSCLC 患者的生存差异。此外,GGH 和 FPGS 中的多态性与反应和不良事件有轻微关联。这些结果应在使用培美曲塞的更大前瞻性研究中进行验证。
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