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SMARCB1 ‐deficient malignant melanocytic uveal tumours: a new neural crest‐derived tumour entity with SMARCB1 ‐related germline predisposition

SMARCB1型 生物 病理 恶性肿瘤 癌症研究 生殖系 上皮样肉瘤 免疫组织化学 医学 表观遗传学 遗传学 染色质重塑 基因
作者
Joanna Cyrta,Julien Masliah‐Planchon,Owen Hoare,Riwan Brillet,Mamy Andrianteranagna,Pierre Sohier,Liesbeth Cardoen,Yassine Bouchoucha,Mathilde Filser,Andreia Gonçalves,Martial Caly,Paul Fréneaux,Kalliopi Stefanaki,Maria Pefkianaki,Maria Moschovi,Alexandre Matet,Nathalie Cassoux,Livia Lumbroso-Le Rouïc,Marion Gauthier‐Villars,Marc‐Henri Stern
标识
DOI:10.1002/path.6390
摘要

Abstract Rhabdoid tumours (RT) are an aggressive malignancy affecting <2‐year‐old infants, characterised by biallelic loss‐of‐function alterations in SWI/SNF‐related BAF chromatin remodelling complex subunit B1 ( SMARCB1 ) in nearly all cases. Germline SMARCB1 alterations are found in ~30% of patients and define the RT Predisposition Syndrome type 1 (RTPS1). Uveal melanoma (UVM), the most common primary intraocular cancer in adults, does not harbour SMARCB1 alterations. We report two cases of a previously undescribed intraocular malignancy that shared some features with UVM and RT, but was also distinct from these entities. Both female patients, aged 23 and 14 years, underwent enucleation, and the tumours were subjected to comprehensive genomic, DNA methylation, and transcriptomic profiling. Pathological examination showed large, amelanotic intraocular tumours with epithelioid features, expressing melanocytic markers [S100P, SOX10, Melan‐A, PMEL (HMB45), TYR] as seen using immunohistochemistry (IHC), but with little or no melanin production. Both tumours harboured biallelic loss‐of‐function SMARCB1 alterations, associated with loss of SMARCB1 (BAF47/INI1) expression on IHC. Their genomic profiles were atypical both for UVM and for RT, and no pathogenic variants were found in other genes tested, including those recurrently altered in UVM. In both patients, a germline SMARCB1 variant was found. However, there was no relevant family history of cancer. Transcriptome and methylome profiling suggested that these tumours were distinct from RT, UVM, and skin melanomas. RNAseq confirmed expression of early and late genes related to melanocytic differentiation. The first patient died of metastatic disease 16 months after diagnosis, the second was disease‐free 10 months after completion of treatment. In summary, we report two cases of a previously undescribed, aggressive SMARCB1 ‐deficient intraocular malignancy with melanocytic differentiation, which occurs in young patients, is distinct from UVM and RT, and expands the RTPS1 spectrum. © 2025 The Author(s). The Journal of Pathology published by John Wiley & Sons Ltd on behalf of The Pathological Society of Great Britain and Ireland.
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