PRKC 融合性黑色素细胞肿瘤，一类更接近蓝痣而非 PRKAR1A 失活的色素性上皮样黑素细胞瘤的黑色素细胞肿瘤亚组。

PRKC Fusion Melanocytic Tumors, a Subgroup of Melanocytic Tumors More Closely Aligned to Blue Nevi Than to PRKAR1A-inactivated Pigmented Epithelioid Melanocytomas.

机构信息

Department of Dermatology, Feinberg School of Medicine, Northwestern University, Chicago, IL.

出版信息

Am J Surg Pathol. 2024 Nov 1;48(11):1349-1358. doi: 10.1097/PAS.0000000000002262. Epub 2024 Jun 12.

Abstract

Tumors morphologically classified as pigmented epithelioid melanocytomas (PEMs) are genomically diverse, with the 2 most common genomic subtypes being PRKC fusions or PRKAR1A inactivating mutations. PRKC fusions activate the Gα q/11 pathway similar to blue nevi. Conversely, inactivating mutations in PRKAR1A activate the Gα s pathway. We hypothesize that PRKC fusions have greater genomic overlap with blue nevi compared with PRKAR1A-inactivated PEMs. We characterized the clinical and morphologic features of 21 PRKC and PRKACB fusion melanocytic tumors and compared this to PRKAR1A mutated PEMs. To test our hypothesis regarding greater genomic overlap between PRKC fusions and blue nevi relative to PRKAR1A mutated PEMs, we performed a principal component analysis (PCA) using mRNA expression data. Lastly, we performed a meta-analysis focusing on the outcome data of PRKC fusions. PRKC fusions occur at a younger median age than PRKAR1A mutated PEMs (16 vs. 27). Histologically, PRKC fusions have solid aggregates of epithelioid melanocytes not typical of PRKAR1A mutated PEMs. The PCA plot showed no overlap between the PRKC fusion group and the PRKAR1A-mutated PEMs. There was a significant overlap between PRKC fusions and blue nevi. A meta-analysis of PRKC fusion cases in the literature suggests melanoma is uncommon, but the loss of BAP-1 nuclear expression may be associated with an adverse prognosis as in tumors from the blue nevus family. PRKC fusion melanocytic tumors have greater genomic overlap with blue nevi compared with PRKAR1A mutated PEMs. We recommend categorizing benign PRKC fusion melanocytic tumors as blue fusion nevi/tumors.

摘要

组织学上形态分类为色素性上皮样黑素细胞瘤（PEMs）的肿瘤具有多种基因组改变，其中最常见的两种基因组亚型为 PRKC 融合或 PRKAR1A 失活突变。PRKC 融合通过激活 Gα q/11 途径类似于蓝色痣。相反，PRKAR1A 失活突变激活 Gα s 途径。我们假设 PRKC 融合与蓝色痣相比与 PRKAR1A 失活 PEMs 具有更大的基因组重叠。我们描述了 21 例 PRKC 和 PRKACB 融合性黑素细胞瘤的临床和形态特征，并将其与 PRKAR1A 突变的 PEMs 进行了比较。为了验证我们关于 PRKC 融合与蓝色痣相比与 PRKAR1A 失活 PEMs 具有更大的基因组重叠的假设，我们使用 mRNA 表达数据进行了主成分分析（PCA）。最后，我们进行了一项荟萃分析，重点关注 PRKC 融合的结局数据。PRKC 融合发生的中位年龄比 PRKAR1A 突变的 PEMs 更年轻（16 岁比 27 岁）。组织学上，PRKC 融合具有上皮样黑素细胞的实性聚集，这与 PRKAR1A 突变的 PEMs 不同。PCA 图显示 PRKC 融合组与 PRKAR1A 突变的 PEMs 之间没有重叠。PRKC 融合与蓝色痣之间存在显著重叠。文献中 PRKC 融合病例的荟萃分析表明黑色素瘤并不常见，但 BAP-1 核表达缺失可能与预后不良相关，类似于来自蓝色痣家族的肿瘤。与 PRKAR1A 突变的 PEMs 相比，PRKC 融合黑素细胞瘤与蓝色痣具有更大的基因组重叠。我们建议将良性 PRKC 融合黑素细胞瘤归类为蓝色融合痣/肿瘤。