VASARI胶质瘤特征十年:对其影响和性能的系统回顾和荟萃分析。

Aynur Azizova, Yeva Prysiazhniuk, Ivar J H G Wamelink, Jan Petr, Frederik Barkhof, Vera C Keil
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引用次数: 0

摘要

背景:目的:我们的目的是对用于胶质瘤评估的VASARI特征集的性能进行系统回顾和荟萃分析:数据来源:对MEDLINE、Web of Science、EMBASE和Cochrane图书馆进行了系统检索,直至2023年9月26日:数据分析:数据分析:采用修改后的诊断准确性研究质量评估-2(QUADAS-2)工具评估偏倚风险。如果提供的偏倚风险较低或中等的可比研究≥5项,则采用随机效应模型和森林图可视化进行荟萃分析:共纳入 35 项研究(3304 名患者)。偏倚风险评分为中等(n = 33)和低(n = 2)。重复出现的目标是总生存期(n = 18)和异柠檬酸脱氢酶突变(IDH;n = 12)预测。7项研究对无进展生存期进行了检测。在 4 项研究(胶质母细胞瘤 n = 2、2/3 级胶质瘤 n = 1、3 级胶质瘤 n = 1)中,发现无进展生存期与 VASARI 单个特征之间存在显著关联。预测总生存期的单一特征中,汇总危险比最高的是多灶性(危险比=1.80;95%-CI,1.21-2.67;I2=53%)、内膜外侵(危险比=1.73;95% CI,1.45-2.05;I2=0%)和肿瘤强化越过中线(危险比=2.08;95% CI,1.35-3.18;I2=52%)。结合 VASARI 特征的 IDH 突变预测模型的接收者操作特征曲线下的集合面积为 0.82(95% CI,0.76-0.88),异质性相当高(I2 = 100%)。在所有相关研究中,使用VASARI加上临床和/或放射组学特征的组合输入模型优于单一数据类型模型(n = 17):局限性:研究设计不统一,样本量通常较小。有几项研究使用了癌症成像档案数据库,其队列可能存在重叠。对IDH的荟萃分析因研究异质性较高而受到限制:结论:VASARI的某些特征在预测总生存率和IDH突变状态方面表现良好,但综合模型优于单一特征。需要更多异质性较低的研究来提高证据水平。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Ten Years of VASARI Glioma Features: Systematic Review and Meta-Analysis of Their Impact and Performance.

Background: Visually Accessible Rembrandt (Repository for Molecular Brain Neoplasia Data) Images (VASARI) features, a vocabulary to establish reproducible terminology for glioma reporting, have been applied for a decade, but a systematic performance evaluation is lacking.

Purpose: Our aim was to conduct a systematic review and meta-analysis of the performance of the VASARI features set for glioma assessment.

Data sources: MEDLINE, Web of Science, EMBASE, and the Cochrane Library were systematically searched until September 26, 2023.

Study selection: Original articles predicting diagnosis, progression, and survival in patients with glioma were included.

Data analysis: The modified Quality Assessment of Diagnostic Accuracy Studies-2 (QUADAS-2) tool was applied to evaluate the risk-of-bias. The meta-analysis used a random effects model and forest plot visualizations, if ≥5 comparable studies with a low or medium risk of bias were provided.

Data synthesis: Thirty-five studies (3304 patients) were included. Risk-of-bias scores were medium (n = 33) and low (n = 2). Recurring objectives were overall survival (n = 18) and isocitrate dehydrogenase mutation (IDH; n = 12) prediction. Progression-free survival was examined in 7 studies. In 4 studies (glioblastoma n = 2, grade 2/3 glioma n = 1, grade 3 glioma n = 1), a significant association was found between progression-free survival and single VASARI features. The single features predicting overall survival with the highest pooled hazard ratios were multifocality (hazard ratio = 1.80; 95%-CI, 1.21-2.67; I2 = 53%), ependymal invasion (hazard ratio = 1.73; 95% CI, 1.45-2.05; I2 = 0%), and enhancing tumor crossing the midline (hazard ratio = 2.08; 95% CI, 1.35-3.18; I2 = 52%). IDH mutation-predicting models combining VASARI features rendered a pooled area under the receiver operating characteristic curve of 0.82 (95% CI, 0.76-0.88) at considerable heterogeneity (I2 = 100%). Combined input models using VASARI plus clinical and/or radiomics features outperformed single data-type models in all relevant studies (n = 17).

Limitations: Studies were heterogeneously designed and often with a small sample size. Several studies used The Cancer Imaging Archive database, with likely overlapping cohorts. The meta-analysis for IDH was limited due to a high study heterogeneity.

Conclusions: Some VASARI features perform well in predicting overall survival and IDH mutation status, but combined models outperform single features. More studies with less heterogeneity are needed to increase the evidence level.

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