Oligodendroglioma patient survival is associated with circulating B-cells and age.

IF 4.1 Q1 CLINICAL NEUROLOGY Neuro-oncology advances Pub Date : 2024-08-19 eCollection Date: 2024-01-01 DOI:10.1093/noajnl/vdae143
Jennie W Taylor, Gayathri Warrier, Helen M Hansen, Lucie McCoy, Terri Rice, Geno Guerra, Stephen S Francis, Jennifer L Clarke, Paige M Bracci, Sara Hadad, Karl T Kelsey, Margaret Wrensch, Annette M Molinaro, John K Wiencke
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Abstract

Background: Variations in survival among patients with oligodendroglioma are unexplained by known prognostic factors. To assess the impact of peripheral immune profiles on prognosis, we applied immunomethylomics analyses-DNA methylation of archived whole blood samples, to characterize immune cells.

Methods: We compared the proportions of immune cells from patients with oligodendroglioma to other glioma subtypes and controls. We used recursive partitioning analysis (RPA) within the oligodendrogliomas to correlate with survival.

Results: Patients with oligodendrogliomas (141) were median age at diagnosis of 44 years; 57% male; 75% White; 60% prior chemotherapy; and 25% on dexamethasone at sample collection. Patients with oligodendrogliomas had immune profiles more similar to controls than other glioma subtypes, though with notably lower B-cells. RPA of patients with oligodendrogliomas delineated 2 survival groups based on an interaction between age and B-naïve cells. Patients with longer survival (median 24.2 years) were ≤42 years of age with higher B-naïve cells versus worse survival (median 16.9 years) who were ≤42 years of age with lower B-naïve cells or >42 years of age (P = .00032). Patients with worse survival also had lower CD4- and CD8-naïve T-cells. Similar immune profiles were observed in an independent cohort of oligodendroglioma patients prior to surgery.

Conclusions: Peripheral blood immune profiles in oligodendroglioma suggested that younger patients with lower B-naïve cells experienced shorter survival. Though our findings lack of validation cohort and use a heterogenous patient population, they suggest peripheral blood immune profiles may be prognostic for patients with glioma and warrant further investigation.

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少突胶质细胞瘤患者的存活率与循环 B 细胞和年龄有关。
背景:已知的预后因素无法解释少突胶质细胞瘤患者生存率的变化。为了评估外周免疫特征对预后的影响,我们对存档全血样本进行了免疫组学分析--DNA甲基化,以确定免疫细胞的特征:我们比较了少突胶质细胞瘤患者与其他胶质瘤亚型和对照组的免疫细胞比例。我们在少突胶质细胞瘤中使用递归分区分析法(RPA)将其与存活率联系起来:少突胶质细胞瘤患者(141例)诊断时的中位年龄为44岁;57%为男性;75%为白人;60%曾接受化疗;25%在采集样本时服用地塞米松。与其他胶质瘤亚型相比,少突胶质细胞瘤患者的免疫特征与对照组更为相似,但B细胞明显较少。少突胶质细胞瘤患者的RPA根据年龄和B-幼稚细胞之间的相互作用划分出两个生存组。生存期较长(中位 24.2 年)的患者年龄小于 42 岁,B-幼稚细胞较高,而生存期较差(中位 16.9 年)的患者年龄小于 42 岁,B-幼稚细胞较低或大于 42 岁(P = 0.00032)。存活率较低的患者的 CD4- 和 CD8- 天性 T 细胞也较低。在一个独立的少突胶质细胞瘤患者队列中也观察到了类似的术前免疫特征:少突胶质细胞瘤患者的外周血免疫图谱显示,B-幼稚细胞较少的年轻患者生存期较短。虽然我们的研究结果缺乏验证队列,而且使用的是异质性患者人群,但它们表明外周血免疫图谱可能是胶质瘤患者的预后指标,值得进一步研究。
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6.20
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审稿时长
12 weeks
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