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Resistance to paclitaxel is associated with a variant of the gene BCL2 in multiple tumor types

机译:对紫杉醇的耐药性与多种肿瘤类型中的BCL2基因变异有关

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摘要

Paclitaxel, the most commonly used form of chemotherapy, is utilized in curative protocols in different types of cancer. The response to treatment differs among patients. Biological interpretation of a mechanism to explain this personalized response is still unavailable. Since paclitaxel is known to target BCL2 and TUBB1, we used pan-cancer genomic data from hundreds of patients to show that a single-nucleotide variant in the BCL2 sequence can predict a patient’s response to paclitaxel. Here, we show a connection between this BCL2 genomic variant, its transcript structure, and protein abundance. We demonstrate these findings in silico, in vitro, in formalin-fixed paraffin-embedded (FFPE) tissue, and in patient lymphocytes. We show that tumors with the specific variant are more resistant to paclitaxel. We also show that tumor and normal cells with the variant express higher levels of BCL2 protein, a phenomenon that we validated in an independent cohort of patients. Our results indicate BCL2 sequence variations as determinants of chemotherapy resistance. The knowledge of individual BCL2 genomic sequences prior to the choice of chemotherapy may improve patient survival. The current work also demonstrates the benefit of community-wide, integrative omics data sources combined with in-lab experimentation and validation sets.
机译:紫杉醇是最常用的化疗形式,可用于不同类型癌症的治疗方案。不同患者对治疗的反应不同。仍然无法获得生物学解释这种个性化反应的机制的解释。由于已知紫杉醇靶向BCL2和TUBB1,因此我们使用了来自数百名患者的全癌基因组数据,表明BCL2序列中的单核苷酸变异体可以预测患者对紫杉醇的反应。在这里,我们显示了此BCL2基因组变体,其转录本结构和蛋白质丰度之间的联系。我们在体外,福尔马林固定石蜡包埋(FFPE)组织和患者淋巴细胞中证明了这些发现。我们显示具有特定变异的肿瘤对紫杉醇的耐药性更高。我们还显示具有该变体的肿瘤和正常细胞表达更高水平的BCL2蛋白,这一现象我们在独立的患者队列中得到了验证。我们的结果表明BCL2序列变异是化疗耐药的决定因素。选择化疗之前,了解单个BCL2基因组序列可提高患者的生存率。当前的工作还证明了社区范围内的综合组学数据源与实验室内实验和验证集相结合的好处。

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