Segmental chromosome aberrations as a prognostic factor of neuroblastoma: a meta-analysis and systematic review.

IF 1.5 4区医学 Q2 PEDIATRICS Translational pediatrics Pub Date : 2024-10-01 Epub Date: 2024-10-28 DOI:10.21037/tp-24-200

Jianlei Geng, Xiaoyu Wang, Libo Zhao, Jianxiao Zhang, Huizhong Niu

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Abstract

Background: Segmental chromosome aberrations, defined as presence of aberrations, deletion, or imbalance in the chromosomal arms, have long been considered as a predictor of poor prognosis of patients with neuroblastoma. The objective of this meta-analysis is to quantitively analyze the hazard ratios (HRs) of different whole or segmental chromosome aberrations for overall survival (OS) rate or event-free survival (EFS) rate of patients with neuroblastoma.

Methods: Relevant studies about chromosome, neuroblastoma, predictor, prognosis, and survival published from the inception to April 2023 in the databases of PubMed, Embase, and Web of Science were searched, screened, and reviewed. The risk of bias of included articles was assessed using the Quality In Prognosis Studies tool. Basic characteristics, HRs of long term (>3 years) EFS and OS with 95% confidence intervals (CIs) of included articles were extracted. A random effects model of DerSimonian-Laird was used to analyze the extracted HRs. For studies that did not report HRs, narrative synthesis was used for summarization.

Results: There were 34 (including 14,356 patients) in 844 searched studies finally included for narrative and quantitative analysis. There were 24 articles rated as low risk of bias and 10 articles rated as moderate. Although the results were inconsistent, the pooled effect of HR for 1p loss was 4.46 (1.88-10.59) for EFS and 2.29 (1.26-4.15) for OS; the pooled effect of HR for 17q gain was 4.81 (3.29-7.04) for EFS and 3.98 (2.11-7.54) for OS; the pooled effect of HR for 11q loss was 2.54 (2.32-3.73) for OS. Results of 1p36 loss, 1p22 loss, 11q23 loss, 11q13-q14 gain, 1q gain, 1q22 gain, 2p gain, 3p loss, 4p loss, 14q loss, 14q32 loss, and other segmental chromosome aberrations were also summarized.

Conclusions: 1p loss, 11q loss, and 17q gain were identified as significant independent predictors for long-term OS and EFS of patients with neuroblastoma.

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作为神经母细胞瘤预后因素的节段性染色体畸变：一项荟萃分析和系统综述。

背景：片段染色体畸变是指染色体臂出现畸变、缺失或不平衡，长期以来一直被认为是神经母细胞瘤患者预后不良的预测因素。本荟萃分析的目的是定量分析不同染色体整体或片段畸变对神经母细胞瘤患者总生存率（OS）或无事件生存率（EFS）的危险比（HRs）：在PubMed、Embase和Web of Science等数据库中检索、筛选并审查了从开始到2023年4月发表的有关染色体、神经母细胞瘤、预测因子、预后和生存的相关研究。采用预后研究质量工具评估了纳入文章的偏倚风险。提取了纳入文章的基本特征、长期（>3年）EFS和OS的HRs及95%置信区间（CI）。采用DerSimonian-Laird随机效应模型对提取的HRs进行分析。对于未报告HRs的研究，采用叙事综合法进行总结：最终纳入了 844 项检索研究中的 34 篇文章（包括 14 356 名患者）进行叙事和定量分析。其中 24 篇文章被评为低度偏倚风险，10 篇文章被评为中度偏倚风险。虽然结果不一致，但1p缺失的HR汇总效应对EFS的影响为4.46（1.88-10.59），对OS的影响为2.29（1.26-4.15）；17q增益的HR汇总效应对EFS的影响为4.81（3.29-7.04），对OS的影响为3.98（2.11-7.54）；11q缺失的HR汇总效应对OS的影响为2.54（2.32-3.73）。此外，还总结了1p36缺失、1p22缺失、11q23缺失、11q13-q14增益、1q增益、1q22增益、2p增益、3p缺失、4p缺失、14q缺失、14q32缺失以及其他节段性染色体畸变的结果：结论：1p缺失、11q缺失和17q增益是神经母细胞瘤患者长期OS和EFS的重要独立预测因素。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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