Division of Surgical Oncology, Department of Surgery, Moores Cancer Center, University of California, San Diego, UC San Diego Health Sciences, 3855 Health Sciences Drive, Room 2313, Mail Code 0987, La Jolla, CA, 92093-0987, USA.
Department of Surgery, David Geffen School of Medicine at UCLA, Los Angeles, CA, USA.
J Transl Med. 2019 Jul 30;17(1):246. doi: 10.1186/s12967-019-1995-z.
Plexiform fibromyxoma (PF) is a rare gastric tumor often confused with gastrointestinal stromal tumor. These so-called "benign" tumors often present with upper GI bleeding and gastric outlet obstruction. It was recently demonstrated that approximately one-third of PF have activation of the GLI1 oncogene, a transcription factor in the hedgehog (Hh) pathway, via a MALAT1-GLI1 fusion protein or GLI1 up-regulation. Despite this discovery, the biology of most PFs remains unknown.
Next generation sequencing (NGS) was performed on formalin-fixed paraffin-embedded (FFPE) samples of PF specimens collected from three institutions (UCSD, NCI and OHSU). Fresh frozen tissue from one tumor was utilized for in vitro assays, including quantitative RT-PCR and cell viability assays following drug treatment.
Eight patients with PF were identified and 5 patients' tumors were analyzed by NGS. An index case had a mono-allelic PTCH1 deletion of exons 15-24 and a second case, identified in a validation cohort, also had a PTCH1 gene loss associated with a suspected long-range chromosome 9 deletion. Building on the role of Hh signaling in PF, PTCH1, a tumor suppressor protein, functions upstream of GLI1. Loss of PTCH1 induces GLI1 activation and downstream gene transcription. Utilizing fresh tissue from the index PF case, RT-qPCR analysis demonstrated expression of Hh pathway components, SMO and GLI1, as well as GLI1 transcriptional targets, CCND1 and HHIP. In turn, short-term in vitro treatment with a Hh pathway inhibitor, sonidegib, resulted in dose-dependent cell killing.
For the first time, we report a novel association between PTCH1 inactivation and the development of plexiform fibromyxoma. Hh pathway inhibition with SMO antagonists may represent a target to study for treating a subset of plexiform fibromyxomas.
丛状纤维黏液瘤(PF)是一种罕见的胃肿瘤,常与胃肠道间质瘤混淆。这些所谓的“良性”肿瘤常表现为上消化道出血和胃出口梗阻。最近的研究表明,大约三分之一的 PF 中存在 Hedgehog(Hh)通路转录因子 GLI1 的激活,其通过 MALAT1-GLI1 融合蛋白或 GLI1 上调实现。尽管有了这一发现,但大多数 PF 的生物学特性仍不清楚。
对来自三个机构(加州大学圣地亚哥分校、美国国家癌症研究所和俄勒冈健康与科学大学)的 PF 标本进行了福尔马林固定石蜡包埋(FFPE)样本的下一代测序(NGS)。利用一个肿瘤的新鲜冷冻组织进行了体外实验,包括定量 RT-PCR 和药物处理后的细胞活力测定。
共鉴定出 8 例 PF 患者,对 5 例患者的肿瘤进行了 NGS 分析。1 例患者的 PTCH1 外显子 15-24 存在单等位基因缺失,另 1 例患者在验证队列中也发现了与疑似长距离 9 号染色体缺失相关的 PTCH1 基因缺失。基于 Hh 信号通路在 PF 中的作用,肿瘤抑制蛋白 PTCH1 位于 GLI1 的上游。PTCH1 的缺失会诱导 GLI1 的激活和下游基因的转录。利用索引 PF 病例的新鲜组织,RT-qPCR 分析显示 Hh 通路成分 SMO 和 GLI1 以及 GLI1 转录靶标 CCND1 和 HHIP 的表达。相反,短期的体外 Hh 通路抑制剂 sonidegib 治疗会导致剂量依赖性的细胞杀伤。
我们首次报道了 PTCH1 失活与丛状纤维黏液瘤发生之间的新关联。SMO 拮抗剂的 Hh 通路抑制可能是研究治疗丛状纤维黏液瘤亚群的一个靶点。
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