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Bioinformatics analysis of gene expression alterations conferring drug resistance in tumor samples from melanoma patients with EGFR-activating BRAF mutations

机译：EGFR激活BRAF突变的黑色素瘤患者肿瘤样本中赋予耐药性的基因表达改变的生物信息学分析

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摘要

Melanoma is a highly malignant tumor of the skin melanocytes. Patients with this cancer have a high frequency (~50%) of oncogenic BRAF mutations, particularly BRAF V600E. Treatments for melanoma often target BRAF mutations or involve mitogen-activated protein kinase kinase/extracellular signal-regulated kinase inhibitors. A major challenge in melanoma treatment is resistance to BRAF inhibitor treatment, which may be enhanced by the BRAF mutation itself and/or epidermal growth factor receptor (EGFR) activation, leading to poor prognosis. However, no effective clinical treatment exists for patients with EGFR-activating feedback. The aim of the present study was to analyze gene expression changes in tumors from patients with EGFR-activating BRAF mutations during development of drug resistance. RNA-seq data was downloaded from the Gene Expression Omnibus (GEO) database for pre- and post-treatment tumor samples from three melanoma patients with EGFR-activating BRAF V600E mutations, and from The Cancer Genome Atlas (TCGA) melanoma database for tumor and non-tumor samples from patients with the BRAF V600E mutation and unknown EGFR activation status. Using functional enrichment and KEGG pathway analyses, the present study analyzed differentially expressed genes (DEGs) between pre- vs. post-treatment data from the GEO database and tumor or non-tumor sample data from the TCGA database. The results of the present study indicated that functional and structural changes to the plasma membrane may be associated with drug resistance. The present study identified 9 DEGs that were significantly different between tumor and non-tumor samples and also between prior to and following treatment. Thus, it was confirmed that patients with EGFR-activating BRAF V600E mutations undergo gene expression changes during disease development, and during therapy. These findings may provide potential directions for melanoma-specific therapy.

机译：黑色素瘤是皮肤黑素细胞的高度恶性肿瘤。患有这种癌症的患者具有较高的致癌BRAF突变频率（约50％），尤其是BRAF V600E。黑色素瘤的治疗通常针对BRAF突变或涉及促分裂原活化的蛋白激酶激酶/细胞外信号调节激酶抑制剂。黑色素瘤治疗的主要挑战是对BRAF抑制剂治疗的耐药性，这可能会因BRAF突变本身和/或表皮生长因子受体（EGFR）活化而增强，从而导致不良预后。但是，对于具有EGFR激活反馈的患者，尚无有效的临床治疗方法。本研究的目的是分析耐药性发展过程中EGFR激活BRAF突变患者肿瘤基因表达的变化。 RNA-seq数据从Gene Expression Omnibus（GEO）数据库下载，用于治疗三名具有EGFR激活的BRAF V600E突变的黑色素瘤患者的治疗前和治疗后的肿瘤样品，以及癌症和癌症基因组图谱（TCGA）黑色素瘤数据库的肿瘤和来自BRAF V600E突变且EGFR激活状态未知的患者的非肿瘤样本。使用功能富集和KEGG通路分析，本研究分析了GEO数据库中治疗前后数据与TCGA数据库中肿瘤或非肿瘤样品数据之间的差异表达基因（DEG）。本研究的结果表明质膜的功能和结构变化可能与耐药性有关。本研究确定了9个DEG，它们在肿瘤样品和非肿瘤样品之间以及治疗前后均显着不同。因此，证实了具有EGFR激活的BRAF V600E突变的患者在疾病发展期间以及在治疗期间经历基因表达改变。这些发现可能为黑色素瘤特异性疗法提供潜在的指导。

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期刊名称 Oncology Letters
作者
Yang Yu; Xueer Wang; Qinglin Li; Min Zhang; Pengcheng Xu; Yinghua Chen; Yuan Yan; Lin Zhang;
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作者单位

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年(卷),期 -1(15),1
年度 -1
页码 635–641
总页数 7
原文格式 PDF
正文语种
中图分类肿瘤学;
关键词
BRAF V600 melanoma molecular profiling treatment resistance;

机译：BRAF V600;黑色素瘤;分子谱分析;治疗耐药性;

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专利

1. Bioinformatics analysis of gene expression alterations conferring drug resistance in tumor samples from melanoma patients with EGFR-activating BRAF mutations [J] . Yu Yang, Wang Xueer, Li Qinglin, Oncology letters . 2018,第1aPta1期

机译：青素瘤患者EGFR激活BRAF突变肿瘤样品中肿瘤样品耐药改变的生物信息分析
2. SF3B1, NRAS, KIT, and BRAF Mutation; CD117 and cMYC Expression; and Tumoral Pigmentation in Sinonasal Melanomas An Analysis With Newly Found Molecular Alterations and Some Population-Based Molecular Differences [J] . Wroblewska Joanna P., Mull Jason, Wu Cheng-Lin, American Journal of Surgical Pathology . 2019,第2期

机译：SF3B1，NRA，套件和BRAF突变; CD117和CMYC表达; 和新发现的分子改变和一些基于群体的分子差异的分析和肿瘤色素沉着分析
3. Detailed imaging and genetic analysis reveal a secondary BRAF(L505H) resistance mutation and extensive intrapatient heterogeneity in metastatic BRAF mutant melanoma patients treated with vemurafenib [J] . Hoogstraat Marlous, Gadellaa-van Hooijdonk Christa G., Ubink Inge, Pigment cell & melanoma research . 2015,第3期

机译：详细的影像学和遗传学分析显示，接受维罗非尼治疗的转移性BRAF突变型黑色素瘤患者存在继发性BRAF（L505H）抗药性突变，且患者广泛异质
4. Gene Expression Models of BRAF Inhibitor Resistance in Melanoma Predict Drug Repurposing Candidates for Novel Combination Therapies [C] . Kelly Regan, Andrew R. Stiff, William E. Carson, International Molecular Medicine Tri-Conference. . 2016

机译：黑色素瘤中BRAF抑制剂抗性的基因表达模型预测了新型组合疗法的药物重新培养候选者
5. NRAS and BRAF mutations in primary cutaneous melanoma: A comparison of mutation rates between radial and vertical growth phases in individual tumors. [D] . Greene, Victoria R. 2007

机译：原发性皮肤黑素瘤中的NRAS和BRAF突变：单个肿瘤在径向和垂直生长期之间的突变率比较。
6. Dissecting Mechanisms of Melanoma Resistance to BRAF and MEK Inhibitors Revealed Genetic and Non-Genetic Patient- and Drug-Specific Alterations and Remarkable Phenotypic Plasticity [O] . Mariusz L. Hartman, Malgorzata Sztiller-Sikorska, Anna Gajos-Michniewicz, 2020

机译：黑色素瘤对BRAF和MEK抑制剂抗性的解剖机制揭示了遗传和非遗传的患者和药物特异性变化和显着的表型可塑性
7. Bioinformatics analysis of gene expression alterations conferring drug resistance in tumor samples from melanoma patients with EGFR-activating BRAF mutations [O] . Yang Yu, Xueer Wang, Qinglin Li, 2017

机译：EGFR激活BRAF突变对黑色素瘤患者肿瘤样品中肿瘤样品中耐药性改变的生物信息分析

Bioinformatics analysis of gene expression alterations conferring drug resistance in tumor samples from melanoma patients with EGFR-activating BRAF mutations

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