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通过脑脊液游离DNA进行胶质瘤纵向监测。

Longitudinal Glioma Monitoring via Cerebrospinal Fluid Cell-Free DNA.

作者信息

Riviere-Cazaux Cecile, Dong Xiaoxi, Mo Wei, Kumar Rahul, Dai Chao, Carlstrom Lucas P, Munoz-Casabella Amanda, Ghadimi Keyvan, Nesvick Cody L, Andersen Katherine M, Hoplin Matthew D, Canaday Nicholas, Jusue-Torres Ignacio, Malik Noor, Campian Jian L, Ruff Michael W, Uhm Joon H, Eckel Passow Jeanette E, Kaufmann Timothy J, Routman David M, Kizilbash Sani H, Sener Ugur, Warrington Arthur E, Jenkins Robert B, Du Pan, Jia Shidong, Burns Terry C

机构信息

Department of Neurological Surgery, Mayo Clinic, Rochester, Minnesota.

Predicine, Inc., Hayward, California.

出版信息

Clin Cancer Res. 2025 Mar 3;31(5):881-889. doi: 10.1158/1078-0432.CCR-24-1814.

Abstract

PURPOSE

Current methods for glioma response assessment are limited. This study aimed to assess the technical and clinical feasibility of molecular profiling using longitudinal intracranial cerebrospinal fluid (CSF) from patients with gliomas.

EXPERIMENTAL DESIGN

Adults with gliomas underwent longitudinal intracranial CSF collection via Ommaya reservoirs or ventriculoperitoneal shunts. Cell-free DNA (cfDNA) was extracted and analyzed using PredicineCARE for cancer variant profiling and/or PredicineSCORE for low-pass whole-genome sequencing.

RESULTS

Five patients (two females and three males; median age, 40 years; range, 32-64 years) underwent longitudinal intracranial CSF collection via Ommaya reservoirs (n = 4) or ventriculoperitoneal shunts (n = 1). In total, 47 CSF samples were obtained (median volume, 4.00 mL; 0.5-5 mL). Forty-one samples (87.2%) yielded sufficient cfDNA for testing. Patient-specific tumor-associated variant allelic frequencies (VAF), and thus tumor fraction, decreased in pre- versus postchemoradiation samples, including through pseudoprogression. These also increased with radiographic progression in three patients, although identifying the time of definitive disease progression from MRIs was a significant limitation. In two patients with isocitrate dehydrogenase (IDH)-mutant gliomas, decreasing IDH1 VAF after resection and chemoradiation correlated with decreased CSF D-2-hydroxyglutarate levels (0.64× and 0.62×, respectively, for the first patient and 0.01× and 0.07× for the other patient), although D-2-hydroxyglutarate and IDH1 VAF were not concordant in one patient thereafter. Moreover, the copy-number burden decreased below the limit of quantification during treatment and increased above the limit at progression.

CONCLUSIONS

Longitudinal intracranial CSF cfDNA can be obtained in patients with gliomas during their disease course. However, before deploying this technique, numerous questions and challenges should be answered.

摘要

目的

目前评估胶质瘤反应的方法存在局限性。本研究旨在评估利用胶质瘤患者的纵向颅内脑脊液(CSF)进行分子谱分析的技术和临床可行性。

实验设计

患有胶质瘤的成年人通过Ommaya储液器或脑室腹腔分流术进行纵向颅内脑脊液采集。提取无细胞DNA(cfDNA),并使用PredicineCARE进行癌症变异分析和/或使用PredicineSCORE进行低通量全基因组测序。

结果

5例患者(2例女性和3例男性;中位年龄40岁;范围32 - 64岁)通过Ommaya储液器(n = 4)或脑室腹腔分流术(n = 1)进行纵向颅内脑脊液采集。总共获得47份脑脊液样本(中位体积4.00 mL;0.5 - 5 mL)。41份样本(87.2%)产生了足够的cfDNA用于检测。患者特异性肿瘤相关变异等位基因频率(VAF),以及肿瘤比例,在放化疗前与放化疗后的样本中有所下降,包括通过假性进展。在3例患者中,这些指标也随着影像学进展而增加,尽管从磁共振成像中确定明确的疾病进展时间是一个重大限制。在2例异柠檬酸脱氢酶(IDH)突变型胶质瘤患者中,切除和放化疗后IDH1 VAF的降低与脑脊液D - 2 - 羟基戊二酸水平的降低相关(第一位患者分别为0.64倍和0.62倍,另一位患者为0.01倍和0.07倍),尽管此后有1例患者的D - 2 - 羟基戊二酸和IDH1 VAF不一致。此外,拷贝数负担在治疗期间降至定量限以下,在进展时升至定量限以上。

结论

胶质瘤患者在病程中可获得纵向颅内脑脊液cfDNA。然而,在应用这项技术之前,需要回答众多问题并应对挑战。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c90d/11873801/07732ee8f262/ccr-24-1814_f1.jpg

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