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首页> 外文期刊>Human Molecular Genetics >An eQTL-based method identifies CTTN and ZMAT3 as pemetrexed susceptibility markers
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An eQTL-based method identifies CTTN and ZMAT3 as pemetrexed susceptibility markers

机译:基于eQTL的方法将CTTN和ZMAT3识别为培美曲塞药敏标记

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摘要

Pemetrexed, approved for the treatment of non-small cell lung cancer and malignant mesothelioma, has adverse effects including neutropenia, leucopenia, thrombocytopenia, anemia, fatigue and nausea. The results we report here represent the first genome-wide study aimed at identifying genetic predictors of pemetrexed response. We utilized expression quantitative trait loci (eQTLs) mapping combined with drug-induced cytotoxicity data to gain mechanistic insights into the observed genetic associations with pemetrexed susceptibility. We found that CTTN and ZMAT3 expression signature explained >30% of the pemetrexed susceptibility phenotype variation for pemetrexed in the discovery population. Replication using PCR and a semi-high-throughput, scalable assay system confirmed the initial discovery results in an independent set of samples derived from the same ancestry. Furthermore, functional validation in both germline and tumor cells demonstrates a decrease in cell survival following knockdown of CTTN or ZMAT3. In addition to our particular findings on genetic and gene expression predictors of susceptibility phenotype for pemetrexed, the work presented here will be valuable to the robust discovery and validation of genetic determinants and gene expression signatures of various chemotherapeutic susceptibilities.
机译:培美曲塞被批准用于治疗非小细胞肺癌和恶性间皮瘤,其不良反应包括嗜中性白血球减少症,白细胞减少症,血小板减少症,贫血,疲劳和恶心。我们在这里报告的结果代表了第一个全基因组研究,旨在确定培美曲塞反应的遗传预测因子。我们利用表达定量性状基因座(eQTLs)作图结合药物诱导的细胞毒性数据来获得对培美曲塞敏感性的观察到的遗传关联的机械见解。我们发现CTTN和ZMAT3表达特征解释了发现人群中培美曲塞的培美曲塞敏感性表型变异的> 30%。使用PCR和半高通量,可扩展的测定系统进行的复制确认了来自同一祖先的独立样本集中的初始发现结果。此外,在种系和肿瘤细胞中的功能验证均表明,敲低CTTN或ZMAT3后,细胞存活率降低。除了我们对培美曲塞敏感性表型的遗传和基因表达预测因子的特定发现外,此处介绍的工作对于可靠地发现和验证各种化学敏感性的遗传决定子和基因表达特征具有重要意义。

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