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中等转录和复制相关的染色体不稳定性与不良临床结局相关。

Medium levels of transcription and replication related chromosomal instability are associated with poor clinical outcome.

机构信息

OncoSarc, INSERM U1037, Cancer Research Center in Toulouse (CRCT), 31000, Toulouse, France.

Department of Medical Genetics, CHU de Bordeaux, 33000, Bordeaux, France.

出版信息

Sci Rep. 2021 Dec 6;11(1):23429. doi: 10.1038/s41598-021-02787-x.

Abstract

Genomic instability (GI) influences treatment efficacy and resistance, and an accurate measure of it is lacking. Current measures of GI are based on counts of specific structural variation (SV) and mutational signatures. Here, we present a holistic approach to measuring GI based on the quantification of the steady-state equilibrium between DNA damage and repair as assessed by the residual breakpoints (BP) remaining after repair, irrespective of SV type. We use the notion of Hscore, a BP "hotspotness" magnitude scale, to measure the propensity of genomic structural or functional DNA elements to break more than expected by chance. We then derived new measures of transcription- and replication-associated GI that we call iTRAC (transcription-associated chromosomal instability index) and iRACIN (replication-associated chromosomal instability index). We show that iTRAC and iRACIN are predictive of metastatic relapse in Leiomyosarcoma (LMS) and that they may be combined to form a new classifier called MAGIC (mixed transcription- and replication-associated genomic instability classifier). MAGIC outperforms the gold standards FNCLCC and CINSARC in stratifying metastatic risk in LMS. Furthermore, iTRAC stratifies chemotherapeutic response in LMS. We finally show that this approach is applicable to other cancers.

摘要

基因组不稳定性(GI)影响治疗效果和耐药性,但其准确测量方法仍存在不足。目前 GI 的测量方法基于特定结构变异(SV)和突变特征的计数。在这里,我们提出了一种基于 DNA 损伤和修复之间稳态平衡的整体测量 GI 的方法,这种平衡通过修复后残留的断点(BP)来评估,而与 SV 类型无关。我们使用 H 分数的概念,即 BP“热点”程度的衡量标准,来衡量基因组结构或功能 DNA 元件断裂的倾向性,即超过随机预期的断裂程度。然后,我们得出了与转录和复制相关的 GI 的新度量,我们称之为 iTRAC(转录相关染色体不稳定性指数)和 iRACIN(复制相关染色体不稳定性指数)。我们表明,iTRAC 和 iRACIN 可预测平滑肌肉瘤(LMS)的转移复发,并且它们可以结合形成一个新的分类器,称为 MAGIC(混合转录和复制相关基因组不稳定性分类器)。MAGIC 在 LMS 中分层转移风险的表现优于金标准 FNCLCC 和 CINSARC。此外,iTRAC 还可以对 LMS 的化疗反应进行分层。我们最后表明,这种方法适用于其他癌症。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d65b/8648741/7195a52f85eb/41598_2021_2787_Fig1_HTML.jpg

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