原发性眼眶黑色素瘤的基因谱分析:6 例临床病理相关性分析。
Genetic Profiling of Primary Orbital Melanoma: An Analysis of 6 Cases with Clinicopathologic Correlation.
机构信息
National Specialist Ophthalmic Pathology Service (NSOPS), Department of Histopathology, Royal Hallamshire Hospital, Sheffield, United Kingdom.
Department of Oncology & Metabolism, Medical School, University of Sheffield, Sheffield, United Kingdom.
出版信息
Ophthalmology. 2019 Jul;126(7):1045-1052. doi: 10.1016/j.ophtha.2018.12.047. Epub 2018 Dec 31.
PURPOSE
To analyze the genetic profile of 6 cases of primary orbital melanoma with clinicopathologic correlation.
DESIGN
Retrospective noninterventional study to analyze the genetic profile of 6 cases of primary orbital melanoma and to correlate the genetic findings with prognosis and clinicopathologic features. Inclusion criteria were patients with primary orbital melanoma with no evidence of primary eyelid skin, conjunctival, uveal, or remote melanoma at extraocular sites.
PARTICIPANTS
The study involved 6 primary orbital melanomas from 6 patients. Four patients were exenterated and 2 had incisional biopsies performed.
METHODS
Clinical notes and radiologic records were assessed to ascertain clinical tumor behavior. Sections were stained with hematoxylin-eosin and exposed to immunohistochemistry for S100, MelA, HMB45, Sox10, and BAP1. Melanoma DNA was exposed to array comparative genomic hybridization to assess gross chromosomal copy number changes. Point mutation assessment and Sanger sequencing were performed for GNAQ, GNA11, BRAF, NRAS, pTERT, SF3B1, and EIF1AX.
MAIN OUTCOME MEASURES
These were the presence of gross chromosomal copy number changes and the presence of mutations in GNAQ, GNA11, BRAF, NRAS, pTERT, SF3B1, and EIF1AX; the presence of metastases and time period between diagnosis and death from melanoma; and correlation between the tumor genetic profile and the clinical behavior of the tumor.
RESULTS
One of the 6 cases was clinically associated with oculodermal melanocytosis. Of the 6 patients, 3 died of melanoma metastases and 1 of unrelated causes; 2 remain alive at last review. Three of the 6 cases were histologically associated with a benign precursor lesion. All melanomas expressed S100, MelA, HMB45, and Sox10. One patient showed loss of BAP1 nuclear staining. The most frequent chromosomal gains across the 6 cases, in order of frequency, were 6p, 8q, 17q, 6q, and 20p. The most frequently lost regions were 1p, 9p, 16q, and 17p. One patient showed monsomy 3 and gain of 8q (and showed the BAP1 loss). Mutations were found in GNAQ (1 case), GNA11 (1 case), SF3B1 (2 cases), NRAS (2 cases), and pTERT (2 cases).
CONCLUSIONS
The data point to 2 genetic groups for primary orbital conjunctiva melanoma-like and a uveal melanoma-like group. A larger study would help confirm this suggestion.
目的
分析 6 例原发性眼眶黑色素瘤的遗传特征,并与临床病理相关联。
设计
回顾性非干预性研究,分析 6 例原发性眼眶黑色素瘤的遗传特征,并将遗传发现与预后和临床病理特征相关联。纳入标准为无原发性眼脸皮肤、结膜、葡萄膜或眼外部位远处黑色素瘤的原发性眼眶黑色素瘤患者。
参与者
该研究涉及 6 名原发性眼眶黑色素瘤患者,共 6 例。4 例患者接受了眼眶内容剜除术,2 例患者接受了切开活检。
方法
评估临床记录和影像学记录以确定临床肿瘤行为。对组织切片进行苏木精-伊红染色,并进行 S100、MelA、HMB45、Sox10 和 BAP1 的免疫组织化学染色。对黑色素瘤 DNA 进行阵列比较基因组杂交,以评估大体染色体拷贝数变化。对 GNAQ、GNA11、BRAF、NRAS、pTERT、SF3B1 和 EIF1AX 进行点突变评估和 Sanger 测序。
主要观察指标
大体染色体拷贝数变化的存在情况,GNAQ、GNA11、BRAF、NRAS、pTERT、SF3B1 和 EIF1AX 突变的存在情况;转移的存在情况,以及诊断和黑色素瘤死亡之间的时间间隔;肿瘤遗传特征与肿瘤临床行为的相关性。
结果
6 例患者中有 1 例与眼皮肤黑色素增多症临床相关。6 例患者中,3 例死于黑色素瘤转移,1 例死于非相关原因,2 例仍存活。6 例中有 3 例组织学上与良性前体病变相关。所有黑色素瘤均表达 S100、MelA、HMB45 和 Sox10。1 例患者出现 BAP1 核染色缺失。在 6 例患者中,最常见的染色体增益依次为 6p、8q、17q、6q 和 20p。最常见的缺失区域为 1p、9p、16q 和 17p。1 例患者表现为 3 号单体和 8q 增益(并表现出 BAP1 缺失)。发现 GNAQ(1 例)、GNA11(1 例)、SF3B1(2 例)、NRAS(2 例)和 pTERT(2 例)有突变。
结论
数据表明,原发性眼眶结膜黑色素瘤样和葡萄膜黑色素瘤样有 2 个遗传群。更大的研究将有助于证实这一建议。
Zotero 插件