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首页> 外文期刊>Molecular cancer therapeutics >The FA/BRCA Pathway Identified as the Major Predictor of Cisplatin Response in Head and Neck Cancer by Functional Genomics
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The FA/BRCA Pathway Identified as the Major Predictor of Cisplatin Response in Head and Neck Cancer by Functional Genomics

机译:通过功能基因组学通过功能基因组织鉴定为头部和颈部癌症中顺铂反应的主要预测因子

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摘要

Patients with advanced stage head and neck squamous cell carcinoma (HNSCC) are often treated with cisplatin-containing chemoradiation protocols. Although cisplatin is an effective radiation sensitizer, it causes severe toxicity and not all patients benefit from the combination treatment. HNSCCs expectedly not responding to cisplatin may better be treated with surgery and postoperative radiation or cetuximab and radiation, but biomarkers to personalize chemoradiotherapy are not available. We performed an unbiased genome-wide functional genetic screen in vitro to identify genes that influence the response to cisplatin in HNSCC cells. By siRNA-mediated knockdown, we identified the Fanconi anemia/BRCA pathway as the predominant pathway for cisplatin response in HNSCC cells. We also identified the involvement of the SHFM1 gene in the process of DNA cross-link repair. Furthermore, expression profiles based on these genes predict the prognosis of radiation-and chemoradiation-treated head and neck cancer patients. This genome-wide functional analysis designated the genes that are important in the response of HNSCC to cisplatin and may guide further biomarker validation. Cisplatin imaging as well as biomarkers that indicate the activity of the Fanconi anemia/BRCA pathway in the tumors are the prime candidates.
机译:患有先进的阶段头和颈部鳞状细胞癌(HNSCC)的患者通常用含顺铂的化学地理方案治疗。虽然顺铂是一种有效的辐射敏化剂,但它会导致严重的毒性,并非所有患者都受益于组合治疗。预期没有响应顺铂的HNSCC可能会更好地用手术和术后辐射或西妥昔单抗和辐射治疗,但无法使用疗养化学疗法的生物标志物。我们在体外进行了一个无偏的基因组型功能遗传筛网,以鉴定影响HNSCC细胞中对顺铂的反应的基因。通过siRNA介导的敲低,我们将FANCONI贫血/ BRCA途径鉴定为HNSCC细胞中顺铂响应的主要途径。我们还确定了SHFM1基因在DNA交联修复过程中的参与。此外,基于这些基因的表达分布预测了辐射和化学地理治疗的头部和颈部癌症患者的预后。该基因组宽的功能分析指定了HNSCC对顺铂的反应中重要的基因,并可引导进一步的生物标志物验证。顺铂成像以及表明肿瘤中FANCONI贫血/ BRCA途径的活性的生物标志物是主要候选者。

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  • 来源
    《Molecular cancer therapeutics》 |2017年第3期|共11页
  • 作者单位

    Vrije Univ Amsterdam Dept Otolaryngol Head &

    Neck Surg Med Ctr Amsterdam Netherlands;

    Vrije Univ Amsterdam Dept Otolaryngol Head &

    Neck Surg Med Ctr Amsterdam Netherlands;

    Vrije Univ Amsterdam Dept Med Oncol RNA Interference Funct Oncogen Lab Med Ctr Amsterdam;

    Vrije Univ Amsterdam Dept Clin Epidemiol &

    Biostat Med Ctr Amsterdam Netherlands;

    Vrije Univ Amsterdam Dept Clin Epidemiol &

    Biostat Med Ctr Amsterdam Netherlands;

    Vrije Univ Amsterdam Dept Otolaryngol Head &

    Neck Surg Med Ctr Amsterdam Netherlands;

    Vrije Univ Amsterdam Dept Med Oncol RNA Interference Funct Oncogen Lab Med Ctr Amsterdam;

    Vrije Univ Amsterdam Dept Otolaryngol Head &

    Neck Surg Med Ctr Amsterdam Netherlands;

    Vrije Univ Amsterdam Dept Otolaryngol Head &

    Neck Surg Med Ctr Amsterdam Netherlands;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 肿瘤学;
  • 关键词

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