Characteristics of MYC Amplification and Their Association with Clinicopathological and Molecular Factors in Patients with Breast Cancer.

IF 2.6 4区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Li Cao, C. Ren, Guochun Zhang, Xuerui Li, Bo Chen, Kai Li, Cheukfai Li, H. Mok, Yulei N. Wang, L. Wen, M. Jia, Guangnan Wei, Jiali Lin, N. Liao
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引用次数: 1

Abstract

MYC amplification is detected in ∼15% of breast tumors and is associated with poor prognosis by mediating acquired resistance to anticancer therapies. This study aimed to determine the prevalence of MYC amplifications in Chinese women with breast cancer (BRCA) and investigate the correlation between MYC amplification and clinicopathological and molecular characteristics and its clinical implications. We analyzed MYC alterations in tissue specimens from 410 women diagnosed with BRCA in our hospital from June 1, 2017 to September 27, 2018. We compared our results with publicly available data from The Cancer Genome Atlas (TCGA) BRCA cohort (n = 1079). MYC amplification was identified in 12.4% (51/410) of our cohort, with mean copy number (CN) of 4.42 (range: 2.84-11.27). In TCGA cohort, MYC amplification was identified in 21.2% (229/1079) and was associated with age, estrogen receptor status, progesterone receptor status, human epidermal growth factor receptor 2 (HER2) status, and molecular subtype, whereas in our cohort, MYC amplification was associated with smaller tumor size (T1-2, p = 0.023) and higher Ki-67 levels (≥20%; p = 0.031). Analysis of molecular profiles revealed that MYC-amplified breast tumors had significantly more concurrent CN variations compared with MYC nonamplified BRCA in both Guangdong Provincial People's Hospital (GDPH) and TCGA cohorts (p < 0.001). Pathway mapping analysis demonstrated that MYC-amplified tumors had more mutations involved in 15 different but interrelated pathways critical in DNA repair, cell cycle, and cell proliferation. Patients in TCGA cohort with MYC-amplified hormone receptor (HR)-positive/HER2-positive BRCA (p = 0.038) and MYC nonamplified triple-negative BRCA (p = 0.027) had significantly shorter overall survival. In conclusion, this study contributes to a better understanding that MYC-amplified breast tumors had distinct clinicopathological and molecular features compared with MYC nonamplified breast tumors. Further research with a larger sample size is necessary to further elucidate the clinical and survival implications of MYC amplifications.
癌症患者MYC扩增特征及其与临床病理和分子因素的关系。
在约15%的乳腺肿瘤中检测到MYC扩增,并通过介导对抗癌疗法的获得性耐药性与不良预后有关。本研究旨在确定中国癌症(BRCA)妇女MYC扩增的患病率,并探讨MYC扩增与临床病理和分子特征之间的相关性及其临床意义。我们分析了2017年6月1日至2018年9月27日在我院诊断为BRCA的410名女性组织标本中MYC的变化。我们将我们的结果与癌症基因组图谱(TCGA)BRCA队列(n = 1079)。在我们的队列中,12.4%(51/410)的人发现了MYC扩增,平均拷贝数(CN)为4.42(范围:2.84-11.27)。在TCGA队列中,21.2%(229/1079)发现了MYC扩增,并且与年龄、雌激素受体状态、孕激素受体状态、人表皮生长因子受体2(HER2)状态和分子亚型有关,MYC扩增与较小的肿瘤大小相关(T1-2,p = 0.023)和更高的Ki-67水平(≥20%;p = 0.031)。分子谱分析显示,在广东省人民医院(GDPH)和TCGA队列中,MYC扩增的乳腺肿瘤与MYC未扩增的BRCA相比,同时发生的CN变异显著更多(p < 0.001)。通路映射分析表明,MYC扩增的肿瘤在DNA修复、细胞周期和细胞增殖中至关重要的15个不同但相互关联的通路中有更多的突变。MYC扩增激素受体(HR)阳性/HER2阳性BRCA的TCGA队列患者(p = 0.038)和MYC非扩增的三阴性BRCA(p = 0.027)的总生存期显著缩短。总之,本研究有助于更好地理解MYC扩增的乳腺肿瘤与MYC非扩增的乳腺瘤相比具有不同的临床病理和分子特征。有必要对更大样本量进行进一步研究,以进一步阐明MYC扩增的临床和生存意义。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
DNA and cell biology
DNA and cell biology 生物-生化与分子生物学
CiteScore
6.60
自引率
0.00%
发文量
93
审稿时长
1.5 months
期刊介绍: DNA and Cell Biology delivers authoritative, peer-reviewed research on all aspects of molecular and cellular biology, with a unique focus on combining mechanistic and clinical studies to drive the field forward. DNA and Cell Biology coverage includes: Gene Structure, Function, and Regulation Gene regulation Molecular mechanisms of cell activation Mechanisms of transcriptional, translational, or epigenetic control of gene expression Molecular Medicine Molecular pathogenesis Genetic approaches to cancer and autoimmune diseases Translational studies in cell and molecular biology Cellular Organelles Autophagy Apoptosis P bodies Peroxisosomes Protein Biosynthesis and Degradation Regulation of protein synthesis Post-translational modifications Control of degradation Cell-Autonomous Inflammation and Host Cell Response to Infection Responses to cytokines and other physiological mediators Evasive pathways of pathogens.
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