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一种在血浆游离DNA中全基因组靶向结构变异的实用方法。

A Practical Approach for Targeting Structural Variants Genome-wide in Plasma Cell-free DNA.

作者信息

Tanaka Hisashi, Murata Michael, Igari Fumie, Urbanowicz Ryan, Mouakkad Lila, Kim Sungjin, Chen Zijing, Di Vizio Dolores, Posadas Edwin, Giuliano Armando

机构信息

Cedars-Sinai Medical Center.

Juntendo University.

出版信息

Res Sq. 2024 Jan 5:rs.3.rs-3492157. doi: 10.21203/rs.3.rs-3492157/v1.

Abstract

Interrogating plasma cell-free DNA (cfDNA) to detect cancer offers promise; however, no current tests scan structural variants (SVs) throughout the genome. Here, we report a simple molecular workflow to enrich a tumorigenic SV (DNA palindromes/fold-back inversions) that often demarcates genomic amplification and its feasibility for cancer detection by combining low-throughput next-generation sequencing with automated machine learning (Genome-wide Analysis of Palindrome Formation, GAPF-seq). Tumor DNA signal manifested as skewed chromosomal distributions of high-coverage 1-kb bins (HCBs), differentiating 39 matched breast tumor DNA from normal DNA with an average AUC of 0.9819. In a proof-of-concept liquid biopsy study, cfDNA from 0.5 mL plasma from prostate cancer patients was sufficient for binary classification against matched buffy coat DNA with an average AUC of 0.965. HCBs on the X chromosome emerged as a determinant feature and were associated with AR amplification. GAPF-seq could generate unique cancer-specific SV profiles in an agnostic liquid biopsy setting.

摘要

通过检测血浆游离DNA(cfDNA)来检测癌症具有一定前景;然而,目前尚无检测能够扫描全基因组中的结构变异(SVs)。在此,我们报告了一种简单的分子流程,用于富集一种致癌性SV(DNA回文/折返倒位),这种SV通常界定基因组扩增,并且通过将低通量下一代测序与自动化机器学习相结合(全基因组回文形成分析,GAPF-seq),展示了其在癌症检测中的可行性。肿瘤DNA信号表现为高覆盖度1千碱基片段(HCBs)的染色体分布偏斜,可将39例匹配的乳腺肿瘤DNA与正常DNA区分开来,平均曲线下面积(AUC)为0.9819。在一项概念验证性液体活检研究中,来自前列腺癌患者0.5毫升血浆中的cfDNA足以与匹配的血沉棕黄层DNA进行二元分类,平均AUC为0.965。X染色体上的HCBs成为一个决定性特征,并与雄激素受体(AR)扩增相关。GAPF-seq能够在无偏见的液体活检环境中生成独特的癌症特异性SV图谱。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ea11/10802711/28613f810b6b/nihpp-rs3492157v1-f0001.jpg

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