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miRNA-181d 的表达水平对卡莫司汀植入剂治疗反应有显著影响。

MiRNA-181d Expression Significantly Affects Treatment Responses to Carmustine Wafer Implantation.

机构信息

Department of Neurosurgery, Faculty of Medicine, University of Saarland, Kirrbergerstraße, Homburg/ Saar, Germany.

Institute of Pathology, Faculty of Medicine, University of Saarland, Kaiserslautern, Germany.

出版信息

Neurosurgery. 2019 Jul 1;85(1):147-155. doi: 10.1093/neuros/nyy214.

Abstract

BACKGROUND

Standard therapeutic protocols for glioblastoma, the most aggressive type of brain cancer, include surgery followed by chemoradiotherapy. Additionally, carmustine-eluting wafers can be implanted locally into the resection cavity.

OBJECTIVE

To evaluate microRNA (miRNA)-181d as a prognostic marker of responses to carmustine wafer implantation.

METHODS

A total of 80 glioblastoma patients (40/group) were included in a matched pair analysis. One group (carmustine wafer group) received concomitant chemoradiotherapy with carmustine wafer implantation (Stupp protocol). The second group (control group) received only concomitant chemoradiotherapy. All tumor specimens were subjected to evaluations of miRNA-181d expression, results were correlated with further individual clinical data. The Cancer Genome Atlas (TCGA) dataset of 149 patients was used as an independent cohort to validate the results.

RESULTS

Patients in the carmustine wafer group with low miRNA-181d expression had significantly longer overall (hazard ratio [HR], 35.03, [95% confidence interval (CI): 3.50-350.23], P = .002) and progression-free survival (HR, 20.23, [95% CI: 2.19-186.86], P = .008) than patients of the same group with a high miRNA-181d expression. These correlations were not observed in the control group. The nonsignificance in the control group was confirmed in the independent TCGA dataset. The carmustine wafer group patients with low miRNA-181d expression also had a significantly longer progression-free (P = .049) and overall survival (OS) (P = .034), compared with control group patients. Gross total resection correlated significantly with longer OS (P = .023).

CONCLUSION

MiRNA-181d expression significantly affects treatment responses to carmustine wafer implantation.

摘要

背景

胶质母细胞瘤是最具侵袭性的脑癌类型,其标准治疗方案包括手术联合放化疗。此外,卡莫司汀植入剂还可以局部植入切除腔。

目的

评估微小 RNA(miRNA)-181d 作为卡莫司汀植入剂反应的预后标志物。

方法

共纳入 80 例胶质母细胞瘤患者(每组 40 例)进行配对分析。一组(卡莫司汀植入剂组)接受卡莫司汀植入剂联合放化疗(Stupp 方案)。第二组(对照组)仅接受同期放化疗。所有肿瘤标本均进行 miRNA-181d 表达评估,结果与进一步的个体临床数据相关。采用 149 例患者的癌症基因组图谱(TCGA)数据集作为独立队列验证结果。

结果

卡莫司汀植入剂组 miRNA-181d 低表达的患者总生存期(HR,35.03;95%CI:3.50-350.23;P=0.002)和无进展生存期(HR,20.23;95%CI:2.19-186.86;P=0.008)明显长于同一组中 miRNA-181d 高表达的患者。在对照组中未观察到这些相关性。在独立的 TCGA 数据集中也证实了对照组的无显著性。miRNA-181d 低表达的卡莫司汀植入剂组患者的无进展生存期(P=0.049)和总生存期(OS)(P=0.034)明显长于对照组患者。大体全切除与 OS 显著延长相关(P=0.023)。

结论

miRNA-181d 表达显著影响卡莫司汀植入剂的治疗反应。

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