NTRK融合型中枢神经系统肿瘤:临床病理学和遗传学见解以及对TRK抑制剂的反应。

IF 6.2 2区 医学 Q1 NEUROSCIENCES
Eric Eunshik Kim, Chul-Kee Park, Seung-Ki Kim, Ji Hoon Phi, Sun Ha Paek, Jung Yoon Choi, Hyoung Jin Kang, Joo Ho Lee, Jae Kyung Won, Hongseok Yun, Sung-Hye Park
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NTRK2 fusions were found in ten cerebral diffuse low-grade and high-grade gliomas (DLGGs and DHGGs, respectively), and NTRK1 fusions were found in one cerebral desmoplastic infantile ganglioglioma and one spinal DHGG. In this series, the fusion partners of NTRK2 were HOOK3, KIF5A, GKAP1, LHFPL3, SLMAP, ZBTB43, SPECC1L, FKBP15, KANK1, and BCR, while the NTRK1 fusion partners were TPR and TPM3. DLGGs tended to harbour only an NTRK fusion, while DHGGs exhibited further genetic alterations, such as TERT promoter/TP53/PTEN mutation, CDKN2A/2B homozygous deletion, PDGFRA/KIT/MDM4/AKT3 amplification, or multiple chromosomal copy number aberrations. Four patients received adjuvant TRK inhibitor therapy (larotrectinib, repotrectinib, or entrectinib), among which three also received chemotherapy (n = 2) or proton therapy (n = 1). The treatment outcomes for patients receiving TRK inhibitors varied: one child who received larotrectinib for residual DLGG maintained stable disease. 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引用次数: 0

摘要

背景 神经营养性肌球蛋白受体激酶(NTRK)基因融合在1%的儿童和成人胶质瘤中被发现。TRK 抑制剂是治疗 NTRK 融合型胶质瘤的有前途的药物,因为它们与组织无关,并能穿过血脑屏障 (BBB)。方法 我们调查了来自首尔国立大学医院一家研究所的 12 例经 NGS 验证的 NTRK 融合型胶质瘤。结果 患者队列包括六名儿童(1-15 岁)和六名成人(27-72 岁)。在10例脑弥漫性低级别和高级别胶质瘤(分别为DLGGs和DHGGs)中发现了NTRK2融合,在1例脑去势婴儿神经节胶质瘤和1例脊髓DHGGs中发现了NTRK1融合。在这个系列中,NTRK2的融合伙伴是HOOK3、KIF5A、GKAP1、LHFPL3、SLMAP、ZBTB43、SPECC1L、FKBP15、KANK1和BCR,而NTRK1的融合伙伴是TPR和TPM3。DLGG往往只存在NTRK融合,而DHGG则表现出进一步的基因改变,如TERT启动子/TP53/PTEN突变、CDKN2A/2B同源缺失、PDGFRA/KIT/MDM4/AKT3扩增或多染色体拷贝数畸变。四名患者接受了TRK抑制剂辅助治疗(拉罗替尼、雷贝替尼或entrectinib),其中三人还接受了化疗(n = 2)或质子治疗(n = 1)。接受TRK抑制剂治疗的患者的治疗结果各不相同:一名患儿因残留的DLGG接受了拉罗替尼治疗,病情保持稳定。相比之下,另一名脊髓DHGG患儿则经历了多次肿瘤复发。尽管接受了拉罗替尼治疗,但该患儿最终还是因肿瘤进展而死亡。一名接受 entrectinib 治疗的胶质母细胞瘤(GBM)成年患者也经历了肿瘤进展并最终死亡。不过,一名患有 DHGG 的儿童患者取得了成功,在第二次肿瘤全部切除并接受repotrectinib 治疗后,患者没有出现任何疾病迹象。这名患者曾在初次手术后复发,并接受了卡铂/硫替帕和质子治疗的自体外周血干细胞疗法。结论 我们的研究阐明了 NTRK 融合的 LGG 和 HGG 在病理和 TRK 抑制剂反应方面的明显差异。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
NTRK-fused central nervous system tumours: clinicopathological and genetic insights and response to TRK inhibitors.

Background Neurotrophic tropomyosin receptor kinase (NTRK) gene fusions are found in 1% of gliomas across children and adults. TRK inhibitors are promising therapeutic agents for NTRK-fused gliomas because they are tissue agnostic and cross the blood-brain barrier (BBB). Methods We investigated twelve NGS-verified NTRK-fused gliomas from a single institute, Seoul National University Hospital. Results The patient cohort included six children (aged 1-15 years) and six adults (aged 27-72 years). NTRK2 fusions were found in ten cerebral diffuse low-grade and high-grade gliomas (DLGGs and DHGGs, respectively), and NTRK1 fusions were found in one cerebral desmoplastic infantile ganglioglioma and one spinal DHGG. In this series, the fusion partners of NTRK2 were HOOK3, KIF5A, GKAP1, LHFPL3, SLMAP, ZBTB43, SPECC1L, FKBP15, KANK1, and BCR, while the NTRK1 fusion partners were TPR and TPM3. DLGGs tended to harbour only an NTRK fusion, while DHGGs exhibited further genetic alterations, such as TERT promoter/TP53/PTEN mutation, CDKN2A/2B homozygous deletion, PDGFRA/KIT/MDM4/AKT3 amplification, or multiple chromosomal copy number aberrations. Four patients received adjuvant TRK inhibitor therapy (larotrectinib, repotrectinib, or entrectinib), among which three also received chemotherapy (n = 2) or proton therapy (n = 1). The treatment outcomes for patients receiving TRK inhibitors varied: one child who received larotrectinib for residual DLGG maintained stable disease. In contrast, another child with DHGG in the spinal cord experienced multiple instances of tumour recurrence. Despite treatment with larotrectinib, ultimately, the child died as a result of tumour progression. An adult patient with glioblastoma (GBM) treated with entrectinib also experienced tumour progression and eventually died. However, there was a successful outcome for a paediatric patient with DHGG who, after a second gross total tumour removal followed by repotrectinib treatment, showed no evidence of disease. This patient had previously experienced relapse after the initial surgery and underwent autologous peripheral blood stem cell therapy with carboplatin/thiotepa and proton therapy. Conclusions Our study clarifies the distinct differences in the pathology and TRK inhibitor response between LGG and HGG with NTRK fusions.

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来源期刊
Acta Neuropathologica Communications
Acta Neuropathologica Communications Medicine-Pathology and Forensic Medicine
CiteScore
11.20
自引率
2.80%
发文量
162
审稿时长
8 weeks
期刊介绍: "Acta Neuropathologica Communications (ANC)" is a peer-reviewed journal that specializes in the rapid publication of research articles focused on the mechanisms underlying neurological diseases. The journal emphasizes the use of molecular, cellular, and morphological techniques applied to experimental or human tissues to investigate the pathogenesis of neurological disorders. ANC is committed to a fast-track publication process, aiming to publish accepted manuscripts within two months of submission. This expedited timeline is designed to ensure that the latest findings in neuroscience and pathology are disseminated quickly to the scientific community, fostering rapid advancements in the field of neurology and neuroscience. The journal's focus on cutting-edge research and its swift publication schedule make it a valuable resource for researchers, clinicians, and other professionals interested in the study and treatment of neurological conditions.
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