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伴有AKAP9-BRAF基因融合的未分类硬化性恶性黑色素瘤:两例报告及黑素细胞肿瘤中BRAF融合的综述

Unclassified sclerosing malignant melanomas with AKAP9-BRAF gene fusion: a report of two cases and review of BRAF fusions in melanocytic tumors.

作者信息

Perron Emilie, Pissaloux Daniel, Neub Angela, Hohl Daniel, Tartar Marie Dominique, Mortier Laurent, Alberti Laurent, de la Fouchardiere Arnaud

机构信息

Département de Biopathologie, Centre Leon Bérard, Lyon, France.

Département de Biologie médicale, Service d'anatomopathologie, Centre hospitalier universitaire de Québec-Université Laval, 11 Côte du Palais, Québec, QC, G1R 2J6, Canada.

出版信息

Virchows Arch. 2018 Mar;472(3):469-476. doi: 10.1007/s00428-017-2290-0. Epub 2018 Feb 21.

DOI:10.1007/s00428-017-2290-0
PMID:29464327
Abstract

The current classification of melanocytic tumors includes clinical, pathological, and molecular data. A subset of lesions remains difficult to classify according to these complex multilayer schemes. We report two cases of deeply infiltrating melanomas with a sclerosing background. The first case occurred on the back of a middle-aged man appearing clinically as a dermatofibroma. The architectural and cytological aspects resembled those of a desmoplastic melanoma but the strong expression of both melanA and HMB45, two stainings usually reported as negative in this entity, raised the question of an alternate diagnosis. The second case was a large, slowly growing, perivulvar tumor in a middle-aged woman. The morphology was complex with a central junctional spitzoid pattern associating an epidermal hyperplasia with large nests of large spindled melanocytes. The dermal component was made of deeply invasive strands and nests of nevoid unpigmented melanocytes surrounded by fibrosis; a perineural invasion was present at the periphery of the lesion. In both cases, aCGH found, among many other anomalies, a chromosomal breakpoint at the BRAF locus. RNA sequencing identified in both an AKAP9-BRAF gene fusion. A complementary resection was performed and no relapses have been observed in the respectively 15 and 6 months of follow-up. Both of these melanomas remained unclassified. We further review the variety of melanocytic tumors associated with such BRAF fusions.

摘要

黑色素细胞肿瘤的当前分类包括临床、病理和分子数据。根据这些复杂的多层方案,仍有一部分病变难以分类。我们报告了两例具有硬化背景的深部浸润性黑色素瘤。第一例发生在一名中年男性的背部,临床上表现为皮肤纤维瘤。其结构和细胞学特征类似于促结缔组织增生性黑色素瘤,但MelanA和HMB45这两种通常在该实体中呈阴性的染色均呈强阳性表达,这就引发了关于另一种诊断的问题。第二例是一名中年女性外阴周围的一个大的、生长缓慢的肿瘤。其形态复杂,中央为交界性梭形细胞样模式,伴有表皮增生以及大的梭形黑色素细胞大巢。真皮成分由深部浸润的条索和无色素痣样黑色素细胞巢组成,周围有纤维化;病变周边存在神经周围浸润。在这两例中,阵列比较基因组杂交(aCGH)在许多其他异常中发现BRAF基因座处有一个染色体断点。RNA测序在两例中均鉴定出AKAP9 - BRAF基因融合。进行了补充切除,在分别15个月和6个月的随访中均未观察到复发。这两例黑色素瘤仍未分类。我们进一步回顾了与这种BRAF融合相关的各种黑色素细胞肿瘤。

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本文引用的文献

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Oncogenic BRAF fusions in mucosal melanomas activate the MAPK pathway and are sensitive to MEK/PI3K inhibition or MEK/CDK4/6 inhibition.黏膜黑色素瘤中的致癌 BRAF 融合会激活 MAPK 通路,并对 MEK/PI3K 抑制或 MEK/CDK4/6 抑制敏感。
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