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miRNA regulation is important for DNA damage repair and recognition in malignant pleural mesothelioma

机译:miRNA调节对于恶性胸膜间皮瘤的DNA损伤修复和识别是重要的

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摘要

Platin-containing regimes are currently considered as state-of-the-art therapies in malignant pleural mesotheliomas (MPM) but show dissatisfying response rates ranging from 6 to 16% only. Still, the reasons for the rather poor efficacy remain largely unknown. A clear stratification of patients based on new biomarkers seems to be a promising approach to enhance clinical management, which would be a long-needed improvement for MPM patients but does not seem likely soon unless new biomarkers can be validated. Twenty-four formalin-fixed, paraffin-embedded (FFPE) tumour specimens were subjected to a miRNA expression screening of 800 important miRNAs using digital quantification via the nCounter technique (NanoString). We defined a small subset of miRNAs regulating the key enzymes involved in the repair of platin-associated DNA damage. Particularly, the TP53 pathway network for DNA damage recognition as well as genes related to the term "BRCAness" are the main miRNA targets within this context. The TP53 pathway network for DNA damage recognition as well as genes related to the term "BRCAness" are the main players for risk stratification in patients suffering from this severe disease. Taking the specific molecular profile of the tumour into account can help to enhance the clinical management prospectively and to smooth the way to better response prediction.
机译:含铂的制度目前被认为是恶性胸膜间皮瘤(MPM)的最先进的疗法,但表现出不满意的反应率范围为6%至16%。尽管如此,疗效相当差的原因仍然很大程度上是未知的。基于新生物标志物的患者的清晰分层似乎是提高临床管理的有希望的方法,这将是MPM患者的长期改善,但除非可以验证新的生物标志物,否则否则似乎很快就会很快。使用NCounter技术(纳米型),对二十四个福尔马林固定的石蜡包埋(FFPE)肿瘤标本进行800个重要miRNA的miRNA表达筛选。我们定义了调节铂相关的DNA损伤修复中涉及的关键酶的小麦芽肿。特别地,用于DNA损伤识别的TP53途径网络以及与术语“BRCANESS”相关的基因是本文中的主要miRNA靶标。用于DNA损伤识别的TP53途径网络以及与“BRCANESS”一词相关的基因是患有这种严重疾病的患者风险分层的主要参与者。考虑到肿瘤的特定分子谱可以有助于预期提高临床管理,并顺利以更好的反应预测。

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