Griewank Klaus G, Müller Hansgeorg, Jackett Louise A, Emberger Michael, Möller Inga, van de Nes Johannes Ap, Zimmer Lisa, Livingstone Elisabeth, Wiesner Thomas, Scholz Simone L, Cosgarea Ioana, Sucker Antje, Schimming Tobias, Hillen Uwe, Schilling Bastian, Paschen Annette, Reis Henning, Mentzel Thomas, Kutzner Heinz, Rütten Arno, Murali Rajmohan, Scolyer Richard A, Schadendorf Dirk
Department of Dermatology, University Hospital Essen, West German Cancer Center, University Duisburg-Essen and the German Cancer Consortium (DKTK), Essen, Germany.
Dermatopathologie bei Mainz, Nieder-Olm, Germany.
Mod Pathol. 2017 Jul;30(7):928-939. doi: 10.1038/modpathol.2017.23. Epub 2017 Apr 14.
Blue nevi are melanocytic tumors originating in the cutaneous dermis. Malignant tumors may arise in association with or resembling blue nevi, so called 'blue nevus-like melanoma', which can metastasize and result in patient death. Identifying which tumors will behave in a clinically aggressive manner can be challenging. Identifying genetic alterations in such tumors may assist in their diagnosis and prognostication. Blue nevi are known to be genetically related to uveal melanomas (eg, both harboring GNAQ and GNA11 mutations). In this study, we analyzed a large cohort (n=301) of various morphologic variants of blue nevi and related tumors including tumors diagnosed as atypical blue nevi (n=21), and blue nevus-like melanoma (n=12), screening for all gene mutations known to occur in uveal melanoma. Similar to published reports, we found the majority of blue nevi harbored activating mutations in GNAQ (53%) or GNA11 (15%). In addition, rare CYSLTR2 (1%) and PLCB4 (1%) mutations were identified. EIF1AX, SF3B1, and BAP1 mutations were also detected, with BAP1 and SF3B1 R625 mutations being present only in clearly malignant tumors (17% (n=2) and 25% (n=3) of blue nevus-like melanoma, respectively). In sequencing data from a larger cohort of cutaneous melanomas, this genetic profile was also identified in tumors not originally diagnosed as blue nevus-like melanoma. Our findings suggest that the genetic profile of coexistent GNAQ or GNA11 mutations with BAP1 or SF3B1 mutations can aid the histopathological diagnosis of blue nevus-like melanoma and distinguish blue nevus-like melanoma from conventional epidermal-derived melanomas. Future studies will need to further elucidate the prognostic implications and appropriate clinical management for patients with tumors harboring these mutation profiles.
蓝痣是起源于皮肤真皮层的黑素细胞肿瘤。恶性肿瘤可能与蓝痣相关或类似蓝痣出现,即所谓的“蓝痣样黑色素瘤”,它可发生转移并导致患者死亡。确定哪些肿瘤会表现出临床侵袭性行为可能具有挑战性。确定此类肿瘤中的基因改变可能有助于其诊断和预后评估。已知蓝痣与葡萄膜黑色素瘤存在遗传关联(例如,两者都存在GNAQ和GNA11突变)。在本研究中,我们分析了一大组(n = 301)蓝痣及相关肿瘤的各种形态学变体,包括诊断为非典型蓝痣(n = 21)和蓝痣样黑色素瘤(n = 12)的肿瘤,筛查了已知在葡萄膜黑色素瘤中发生的所有基因突变。与已发表的报告相似,我们发现大多数蓝痣存在GNAQ(53%)或GNA11(15%)的激活突变。此外,还鉴定出罕见的CYSLTR2(1%)和PLCB4(1%)突变。还检测到EIF1AX、SF3B1和BAP1突变,其中BAP1和SF3B1 R625突变仅存在于明确的恶性肿瘤中(分别占蓝痣样黑色素瘤的17%(n = 2)和25%(n = 3))。在来自更大一组皮肤黑色素瘤的测序数据中,这种基因特征在最初未诊断为蓝痣样黑色素瘤的肿瘤中也被发现。我们的研究结果表明,共存的GNAQ或GNA11突变与BAP1或SF3B1突变的基因特征有助于蓝痣样黑色素瘤的组织病理学诊断,并将蓝痣样黑色素瘤与传统表皮来源的黑色素瘤区分开来。未来的研究需要进一步阐明具有这些突变特征的肿瘤患者的预后意义和适当的临床管理。
