Comprehensive Genomic Assessment of Advanced-Stage GI Stromal Tumors Using the Japanese National Center for Cancer Genomics and Advanced Therapeutics Database.

IF 5.3 2区 医学 Q1 ONCOLOGY JCO precision oncology Pub Date : 2024-10-01 Epub Date: 2024-10-24 DOI:10.1200/PO.24.00284
Hiroyuki Fujii, Hidekazu Hirano, Kouya Shiraishi, Hirokazu Shoji, Toshiharu Hirose, Natsuko Okita, Atsuo Takashima, Takafumi Koyama, Ken Kato
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Abstract

Purpose: Clinical utility of comprehensive genomic profiling (CGP) for precision medicine has become evident. Although there are several reports on the genomic landscape of GI stromal tumors (GISTs), large-scale data specific to GIST are limited, especially in Asia. Additionally, the applicability of molecular-targeted agents identified using CGP has not been extensively examined. We investigated the status of genomic alterations in Japanese patients with advanced GISTs using the National Center for Cancer Genomics and Advanced Therapeutics (C-CAT) database to identify novel treatment strategies and drug development.

Materials and methods: We retrospectively reviewed the clinical and CGP data of patients with advanced-stage GIST registered in the C-CAT database to assess the genomic landscape and potential actionable alterations.

Results: Data from 144 patients were reviewed. Oncogenic alterations were detected frequently in KIT (78%), CDKN2A (37%), CDKN2B (29%), RB1 (11%), STK11 (10%), TP53 (9%), PDGFRA (6%), and SDHB (6%). Loss of CDKN2A/CDKN2B was only observed in KIT/PDGFRA-mutated GISTs, while alterations in SDHA/SDHB were only detected in KIT/PDGFRA wild-type GISTs. Among 119 KIT/PDGFRA-mutated GISTs, 95 (80%) had oncogenic genomic alterations and 29 (24%) had actionable alterations, excluding KIT and PDGFRA. However, among 25 KIT/PDGFRA wild-type GISTs, 22 (88%) had oncogenic alterations and 11 (44%) had actionable alterations. Representative candidate drugs for genome-matched therapies in KIT/PDGFRA-mutated and wild-type GISTs were as follows: pembrolizumab for tumor mutation burden-high in one and two patients, respectively; poly-adenosine diphosphate ribose polymerase inhibitors for alterations related to homologous recombination deficiency in 12 and one patient, respectively; NTRK inhibitor for ETV6-NTRK3 fusion in one with KIT/PDGFRA wild-type GIST; and human epidermal growth factor receptor 2-antibody-drug conjugate in one with KIT/PDGFRA-mutated GIST.

Conclusion: This study highlights the genomic landscape of advanced GISTs and the important role of CGP in identifying rational molecular-targeted therapeutic options.

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利用日本国家癌症基因组学和先进疗法中心数据库对晚期消化道间质瘤进行全面基因组评估
目的:综合基因组图谱(CGP)在精准医疗方面的临床实用性已显而易见。虽然有一些关于消化道间质瘤(GIST)基因组图谱的报道,但专门针对 GIST 的大规模数据却很有限,尤其是在亚洲。此外,利用 CGP 确定的分子靶向药物的适用性尚未得到广泛研究。我们利用国家癌症基因组学和先进治疗中心(C-CAT)数据库调查了日本晚期 GIST 患者的基因组改变状况,以确定新的治疗策略和药物开发:我们回顾性地审查了C-CAT数据库中登记的晚期GIST患者的临床和CGP数据,以评估基因组状况和潜在的可操作改变:结果:我们回顾了144例患者的数据。在KIT(78%)、CDKN2A(37%)、CDKN2B(29%)、RB1(11%)、STK11(10%)、TP53(9%)、PDGFRA(6%)和SDHB(6%)中经常检测到致癌基因的改变。CDKN2A/CDKN2B的缺失仅在KIT/PDGFRA突变的GIST中观察到,而SDHA/SDHB的改变仅在KIT/PDGFRA野生型GIST中检测到。在119例KIT/PDGFRA突变的GIST中,95例(80%)有致癌基因组改变,29例(24%)有可操作的改变,其中不包括KIT和PDGFRA。然而,在 25 例 KIT/PDGFRA 野生型 GIST 中,22 例(88%)有致癌基因组改变,11 例(44%)有可操作的改变。KIT/PDGFRA突变型和野生型GIST基因组匹配疗法的代表性候选药物如下:pembrolizumab分别用于1例和2例肿瘤突变负担较高的患者;多聚腺苷二磷酸核糖聚合酶抑制剂分别用于12例和1例与同源重组缺陷相关的改变;NTRK抑制剂用于1例KIT/PDGFRA野生型GIST患者的ETV6-NTRK3融合;人表皮生长因子受体2-抗体-药物结合物用于1例KIT/PDGFRA突变型GIST患者。结论本研究强调了晚期 GIST 的基因组情况以及 CGP 在确定合理的分子靶向治疗方案中的重要作用。
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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