通过低通滤波器全基因组测序进行脑脊液液体活检,用于小儿胚胎性肿瘤的临床疾病监测。

IF 3.7 Q1 CLINICAL NEUROLOGY
Neuro-oncology advances Pub Date : 2024-07-25 eCollection Date: 2024-01-01 DOI:10.1093/noajnl/vdae126
Erin E Crotty, Vera A Paulson, Rebecca Ronsley, Nicholas A Vitanza, Amy Lee, Jason Hauptman, Hannah E Goldstein, Christina M Lockwood, Sarah E S Leary, Bonnie L Cole
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引用次数: 0

摘要

背景:检测脑脊液(CSF)中无细胞DNA(cfDNA)的液体活检测定是一种很有前途的工具,可用于原发性中枢神经系统(CNS)肿瘤儿科患者的疾病监测。作为对组织来源分子分析的补充,脑脊液液体活检有可能改变风险分层、预后和精准医疗方法:在这项试验性研究中,我们评估了一种临床流水线,以确定对中枢神经系统胚胎性肿瘤患者CSF衍生cfDNA进行低通滤波器全基因组测序(LP-WGS)的可行性和灵敏度。研究人员分析了从17名患者中采集的32份纵向CSF样本,这些患者分别患有分子特征髓母细胞瘤(12例)、多层片状胚胎瘤(2例)、中枢神经系统胚胎瘤,未在别处分类(NEC)(2例)和非典型畸胎瘤/横纹肌瘤(1例):结果:94%的样本(30/32)获得了足够的CSF衍生cfDNA用于LP-WGS分析。90%的样本(27/30)检测到了与肿瘤相匹配的拷贝数变异,其中包括关键性改变,如等中心ch17、单体6和MYCN扩增等。与组织标本相比,LP-WGS在CSF中检测到了更多以前未在相应原发肿瘤标本中发现的畸变,这表明肿瘤异质性或cfDNA图谱随时间演变的情况更为全面。在初始分期时获得的12份CSF样本中,只有2份(17%)细胞学阳性,而LP-WGS检测的11份样本(92%)拷贝数阳性:结论:利用临床平台对 CSF 衍生的 cfDNA 进行 LP-WGS 分析是可行的,与初始分期时的传统 CSF 细胞学分析相比,LP-WGS 对肿瘤检测的灵敏度更高。需要开展大型前瞻性研究,进一步评估 LP-WGS 作为预测性生物标志物的作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Cerebrospinal fluid liquid biopsy by low-pass whole genome sequencing for clinical disease monitoring in pediatric embryonal tumors.

Background: Liquid biopsy assays that detect cell-free DNA (cfDNA) in cerebrospinal fluid (CSF) are a promising tool for disease monitoring in pediatric patients with primary central nervous system (CNS) tumors. As a compliment to tissue-derived molecular analyses, CSF liquid biopsy has the potential to transform risk stratification, prognostication, and precision medicine approaches.

Methods: In this pilot study, we evaluated a clinical pipeline to determine feasibility and sensitivity of low-pass whole genome sequencing (LP-WGS) of CSF-derived cfDNA from patients with CNS embryonal tumors. Thirty-two longitudinal CSF samples collected from 17 patients with molecularly characterized medulloblastoma (12), embryonal tumor with multilayered rosettes (2), CNS embryonal tumor, not elsewhere classified (NEC) (2), and atypical teratoid/rhabdoid tumor (1) were analyzed.

Results: Adequate CSF-derived cfDNA for LP-WGS analysis was obtained in 94% of samples (30/32). Copy number variants compatible with neoplasia were detected in 90% (27/30) and included key alterations, such as isodicentric ch17, monosomy 6, and MYCN amplification, among others. Compared to tissue specimens, LP-WGS detected additional aberrations in CSF not previously identified in corresponding primary tumor specimens, suggesting a more comprehensive profile of tumor heterogeneity or evolution of cfDNA profiles over time. Among the 12 CSF samples obtained at initial staging, only 2 (17%) were cytologically positive, compared to 11 (92%) that were copy number positive by LP-WGS.

Conclusions: LP-WGS of CSF-derived cfDNA is feasible using a clinical platform, with greater sensitivity for tumor detection compared to conventional CSF cytologic analysis at initial staging. Large prospective studies are needed to further evaluate LP-WGS as a predictive biomarker.

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CiteScore
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