Retrospective Comparison of Targeted Anticancer Drugs Predicted by the CNS-TAP Tool Versus Those Selected by a Molecularly Driven Tumor Board in Children With DIPG.

IF 0.9 4区 医学 Q4 HEMATOLOGY
Holly J Roberts, Karthik Ravi, Bernard L Marini, Allison Schepers, Cassie Kline, Lindsay Kilburn, Michael Prados, Sara A Byron, Julie Sturza, Sabine Mueller, Carl Koschmann, Andrea T Franson
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Abstract

The recent trial Pediatric Neuro-Oncology Consortium 003 (PNOC003) utilized a molecular tumor board to recommend personalized treatment regimens based on tumor sequencing results in children with DIPG. We separately developed the Central Nervous System Targeted Agent Prediction (CNS-TAP) tool, which numerically scores targeted anticancer agents using preclinical, clinical, and patient-specific data. We hypothesized that highly scored agents from CNS-TAP would overlap with the PNOC003 tumor board's recommendations. For each of the 28 participants, actionable genetic alterations were derived from PNOC003 genomic reports and input to CNS-TAP to identify the highest scoring agents. These agents were then compared with PNOC003 recommendations, with a resultant concordance percentage calculated. Overall, 38% of the total agents recommended by the tumor board were also selected by CNS-TAP, with higher concordance (63%) in a subanalysis including only targeted anticancer agents. Furthermore, nearly all patients (93%) had at least 1 drug chosen by both methods. We demonstrate overlap between agents recommended by CNS-TAP and PNOC003 tumor board, though this does not appear to improve survival. We do observe some discordance, highlighting strengths and limitations of each method. We propose that a combination of expert opinion and data-driven tools may improve targeted treatment recommendations for children with DIPG.

中枢神经系统靶向治疗工具(CNS-TAP)预测的靶向抗癌药物与分子驱动肿瘤委员会(Molecularly Driven Tumor Board)为 DIPG 儿童患者选择的靶向抗癌药物的回顾性比较。
最近进行的儿科神经肿瘤联盟 003(PNOC003)试验利用分子肿瘤委员会根据 DIPG 儿童的肿瘤测序结果推荐个性化治疗方案。我们单独开发了中枢神经系统靶向药物预测(CNS-TAP)工具,该工具利用临床前、临床和患者特异性数据对靶向抗癌药物进行数字评分。我们假设 CNS-TAP 中得分较高的药物将与 PNOC003 肿瘤委员会的建议重叠。我们从 PNOC003 基因组报告中为 28 位参与者中的每一位提取了可操作的基因改变,并将其输入 CNS-TAP,以确定得分最高的药物。然后将这些药物与 PNOC003 的建议进行比较,计算出一致性百分比。总体而言,在肿瘤委员会推荐的所有药物中,CNS-TAP 也选择了 38% 的药物,在仅包括靶向抗癌药物的子分析中,一致性更高(63%)。此外,几乎所有患者(93%)都在两种方法中至少选择了一种药物。我们发现 CNS-TAP 和 PNOC003 肿瘤委员会推荐的药物之间存在重叠,但这似乎并没有提高生存率。我们确实发现了一些不一致之处,凸显了每种方法的优势和局限性。我们建议将专家意见与数据驱动工具相结合,以改进针对 DIPG 儿童的靶向治疗建议。
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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来源期刊
CiteScore
1.90
自引率
8.30%
发文量
415
审稿时长
2.5 months
期刊介绍: ​Journal of Pediatric Hematology/Oncology (JPHO) reports on major advances in the diagnosis and treatment of cancer and blood diseases in children. The journal publishes original research, commentaries, historical insights, and clinical and laboratory observations.
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