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首页> 外文期刊>Journal of experimental & clinical cancer research : >LncRNA CARMN overexpression promotes prognosis and chemosensitivity of triple negative breast cancer via acting as miR143-3p host gene and inhibiting DNA replication
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LncRNA CARMN overexpression promotes prognosis and chemosensitivity of triple negative breast cancer via acting as miR143-3p host gene and inhibiting DNA replication

机译:LNCRNA CARMN过表达促进三重阴性乳腺癌的预后和化学敏感度,作为MIR143-3P宿主基因并抑制DNA复制

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Triple negative breast cancer (TNBC) is a subtype of breast cancer with poor prognosis and lack of effective treatment target. Here we screened differentially expressed lncRNAs through bioinformatics analysis and identified CARMN as a downregulated lncRNA which is lowest expressed in TNBC. We aimed to identify the potential role and molecular mechanisms of CARMN in TNBC. Predictive value of CARMN was explored in breast cancer cohorts. TNBC cell lines with CARMN overexpression or CARMN silence and were used for in vitro and in vivo experiments. RNA-seq of CARMN overexpressed cells was performed for exploring downstream of CARMN. CARMN is downregulated at different phase of malignant transformation of breast tissue. CARMN can predict both better prognosis and higher response rate of cisplatin-based neoadjuvant chemotherapy in breast cancer. A nomogram is built to predict cisplatin-based chemotherapy response in breast cancer. Through in vitro and in vivo studies, we confirmed CARMN can also inhibit tumorigenesis and enhance sensitivity to cisplatin in TNBC cells. RNA-seq and further experiments revealed CARMN can inhibit DNA replication. MCM5, an important DNA replication initiation factor, is the most downregulated gene in DNA replication pathway following CARMN overexpression. We confirmed CARMN can produce miR143-3p from its exon5 which is DROSHA and DICER dependent, resulting binding and decrease of MCM5. Moreover, suppressing miR143-3p can weaken function of CARMN in suppressing tumorigenesis and promoting chemosensitivity. Our results indicated lncRNA CARMN is a predictive biomarker of better prognosis and enhanced cisplatin sensitivity in TNBC. CARMN is the host gene of miR143-3p which downregulates MCM5, causing inhibited DNA replication.
机译:三重阴性乳腺癌(TNBC)是乳腺癌的亚型,预后差和缺乏有效的治疗目标。在这里,我们通过生物信息学分析筛选差异表达的LNCRNA,并将CARMN鉴定为下调的LNCRNA,其在TNBC中最低。我们旨在识别TNBC中CARMN的潜在作用和分子机制。乳腺癌队列探讨了CARMN的预测价值。 TNBC细胞系具有Carmn过表达或Carmn沉默,并用于体外和体内实验。对Carmn过表达细胞的RNA-SEQ进行了用于探索CARMN的下游。 Carmn在乳腺组织的恶性转化的不同阶段下调。 CARMN可以预测乳腺癌中顺铂的新辅助化疗的更好预后和更高的反应速率。建立一个载体以预测乳腺癌中基于顺铂的化学疗法反应。通过体外和体内研究,我们确认CARMN还可以抑制肿瘤瘤,增强TNBC细胞中顺铂的敏感性。 RNA-SEQ和进一步的实验显示CARMN可以抑制DNA复制。 MCM5是重要的DNA复制启动因子,是CARMN过表达后DNA复制途径中最下调的基因。我们确认CARMN可以从其外部5产生MIR143-3P,这是DROSHA和DICER所依赖的,导致MCM5的结合和减少。此外,抑制MiR143-3P可以削弱CARMN在抑制肿瘤发生和促进化学敏感度时的函数。我们的结果表明,LNCRNA CARMN是TNBC中更好预后和增强顺铂敏感性的预测生物标志物。 CARMN是MIR143-3P的宿主基因,其下调MCM5,导致抑制DNA复制。

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