TUBA1A-GLI1 fusion in a soft tissue myoepithelial neoplasm

Q4 Medicine
Yajuan J. Liu , Michael J. Wagner , Edward Y. Kim , Eleanor Y. Chen
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引用次数: 3

Abstract

Several types of benign and malignant neoplasms harboring GLI1 gene fusions with various partner genes, including ACTB, MALAT1 and PTCH1, have been described. These neoplasms show a spectrum of morphologic features and immunohistochemical profiles. However, the GLI1 gene fusion has not been described in soft tissue myoepithelial neoplasms previously. In this study, we reported a novel TUBA1A-GLI1 gene fusion in soft tissue neoplasm occurring in the chest wall of a 35-year-old male. The neoplasm shows morphologic features and immunophenotype of myoepithelial differentiation. FusionPlex analysis detected TUBA1A-GLI1 fusion in the neoplasm. The fusion transcript is comprised of 3′ end of exon 1 of TUBA1A and 5′ end of exon 6 of GLI1, retaining the FOXP coiled-coil domain and the DNA-binding zinc finger domains of GLI1. Promoter swapping with the TUBA1A (tubulin alpha 1a) gene likely leads to deregulation of GLI1 expression and its downstream targets. Despite the clinical presentation of multifocal disease and regional lymph node metastasis, the neoplasm in our case study appeared to be stable in a 10-month follow-up, suggesting that this neoplasm likely pursues an indolent clinical course. This study expands the morphologic and immunohistochemical spectrum of the neoplasms with GLI1 gene fusions and identifies a novel fusion in soft tissue myoepithelial neoplasms. As the TUBA1A-GLI1 fusion event likely results in activated GLI1 expression, targeting the Hedgehog pathway is a potential therapeutic option for treatment of patients with this neoplasm.

TUBA1A-GLI1在软组织肌上皮肿瘤中的融合
已经报道了几种类型的良恶性肿瘤,其中GLI1基因与各种伙伴基因融合,包括ACTB、MALAT1和PTCH1。这些肿瘤表现出一系列的形态特征和免疫组织化学特征。然而,GLI1基因融合在软组织肌上皮肿瘤中尚未见报道。在这项研究中,我们报道了一种新的TUBA1A-GLI1基因融合在一名35岁男性胸壁软组织肿瘤中。肿瘤表现为肌上皮分化的形态学特征和免疫表型。FusionPlex分析在肿瘤中检测到TUBA1A-GLI1融合。该融合转录物由TUBA1A外显子1的3 '端和GLI1外显子6的5 '端组成,保留了GLI1的FOXP卷曲结构域和dna结合锌指结构域。启动子与TUBA1A(微管蛋白α 1a)基因交换可能导致GLI1表达及其下游靶点的失调。尽管临床表现为多灶性疾病和局部淋巴结转移,但在我们的病例研究中,肿瘤在10个月的随访中表现稳定,这表明该肿瘤可能具有惰性临床病程。本研究扩展了GLI1基因融合肿瘤的形态学和免疫组化谱,并在软组织肌上皮肿瘤中发现了一种新的融合。由于TUBA1A-GLI1融合事件可能导致GLI1表达激活,因此靶向Hedgehog通路是治疗该肿瘤患者的潜在治疗选择。
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
Human Pathology: Case Reports
Human Pathology: Case Reports Medicine-Pathology and Forensic Medicine
CiteScore
0.50
自引率
0.00%
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0
审稿时长
16 weeks
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