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胶质瘤脑脊液蛋白质组的现场资源:切除和位置对生物标志物发现的影响。

A field resource for the glioma cerebrospinal fluid proteome: Impacts of resection and location on biomarker discovery.

作者信息

Riviere-Cazaux Cecile, Graser Christopher J, Warrington Arthur E, Hoplin Matthew D, Andersen Katherine M, Malik Noor, Palmer Elizabeth A, Carlstrom Lucas P, Dasari Surendra, Munoz-Casabella Amanda, Ikram Samar, Ghadimi Keyvan, Himes Benjamin T, Jusue-Torres Ignacio, Sarkaria Jann N, Meyer Fredric B, Van Gompel Jamie J, Kizilbash Sani H, Sener Ugur, Michor Franziska, Campian Jian L, Parney Ian F, Burns Terry C

机构信息

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

Department of Stem Cell and Regenerative Biology, Harvard University, Cambridge, Massachusetts, USA.

出版信息

Neuro Oncol. 2025 May 15;27(4):948-962. doi: 10.1093/neuonc/noae277.

Abstract

BACKGROUND

While serial sampling of glioma tissue is rarely performed prior to recurrence, cerebrospinal fluid (CSF) is an underutilized longitudinal source of candidate glioma biomarkers for understanding therapeutic impacts. However, the impact of key variables to consider in longitudinal CSF samples for monitoring biomarker discovery, including anatomical location and post-surgical changes, remains unknown.

METHODS

Aptamer-based proteomics was performed on 147 CSF samples from 74 patients; 71 of whom had grade 2-4 astrocytomas or grade 2-3 oligodendrogliomas. This included pre- versus post-resection intracranial CSF samples obtained at early (1-16 days; n = 20 patients) or delayed (86-153 days; n = 11 patients) time points for patients with glioma. Paired lumbar versus intracranial glioma CSF samples were also obtained (n = 14 patients).

RESULTS

Significant differences were identified in the CSF proteome between lumbar, subarachnoid, and ventricular CSF in patients with gliomas. Importantly, we found that resection had a significant, evolving longitudinal impact on the CSF proteome, with distinct sets of proteins present at different time points since resection. Our analysis of serial intracranial CSF samples suggests the early potential for disease monitoring and evaluation of pharmacodynamic impact of targeted therapies, such as bevacizumab and immunotherapies.

CONCLUSIONS

The intracranial glioma CSF proteome serves as a rich and dynamic reservoir of potential biomarkers that can be used to evaluate the effects of resection and other therapies over time. All data within this study, including detailed individual clinical annotations, are shared as a resource for the neuro-oncology community to collectively address these unanswered questions and further understand glioma biology through CSF proteomics.

摘要

背景

虽然在复发前很少对胶质瘤组织进行连续采样,但脑脊液(CSF)作为了解治疗效果的候选胶质瘤生物标志物的纵向来源,其利用不足。然而,在纵向脑脊液样本中用于监测生物标志物发现的关键变量(包括解剖位置和手术后变化)的影响仍不清楚。

方法

对74例患者的147份脑脊液样本进行基于适配体的蛋白质组学分析;其中71例患有2-4级星形细胞瘤或2-3级少突胶质细胞瘤。这包括对胶质瘤患者在早期(1-16天;n = 20例患者)或延迟(86-153天;n = 11例患者)时间点采集的切除术前与术后颅内脑脊液样本。还获得了配对的腰椎与颅内胶质瘤脑脊液样本(n = 14例患者)。

结果

在胶质瘤患者中,腰椎、蛛网膜下腔和脑室脑脊液的蛋白质组存在显著差异。重要的是,我们发现切除对脑脊液蛋白质组有显著的、不断演变的纵向影响,自切除后不同时间点存在不同的蛋白质组。我们对连续颅内脑脊液样本的分析表明,早期有监测疾病和评估靶向治疗(如贝伐单抗和免疫疗法)药效学影响的潜力。

结论

颅内胶质瘤脑脊液蛋白质组是潜在生物标志物的丰富且动态的储存库,可用于评估切除和其他治疗随时间的效果。本研究中的所有数据,包括详细的个体临床注释,作为一种资源共享,供神经肿瘤学界共同解决这些未解答的问题,并通过脑脊液蛋白质组学进一步了解胶质瘤生物学。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ea12/12083222/0c9cc3ce41da/noae277_fig1.jpg

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