101 例结膜黑色素瘤的突变特征和预后分析。
Mutational Landscape and Outcomes of Conjunctival Melanoma in 101 Patients.
机构信息
Ocular Oncology Service, Wills Eye Hospital, Sidney Kimmel Medical College at Thomas Jefferson University, Philadelphia, Pennsylvania.
Department of Pathology, Wills Eye Hospital, Sidney Kimmel Medical College at Thomas Jefferson University, Philadelphia, Pennsylvania.
出版信息
Ophthalmology. 2022 Jun;129(6):679-693. doi: 10.1016/j.ophtha.2022.01.016. Epub 2022 Jan 24.
PURPOSE
To evaluate targetable mutations and molecular genetic pathways in conjunctival melanoma with clinical correlation.
DESIGN
Observational case series.
PARTICIPANTS
Patients with conjunctival melanoma.
MAIN OUTCOME MEASURES
Mutational profile of the tumor by next-generation sequencing (NGS), alternative lengthening of telomeres (ALT) by fluorescence in situ hybridization (FISH), and ATRX immunohistochemistry. Outcomes at 2 years and 5 years of tumor-related metastasis and death were recorded.
RESULTS
Of the 101 patients, mean age at presentation was 60 years, 52% were male, and 88% were White. The NGS panels initially targeted BRAF only (n = 6, 6%), BRAF/NRAS (n = 17, 17%), and BRAF/NRAS/NF1 (n = 10, 10%). Sixty-eight tumors were tested with the expanded 592-gene panel. Next-generation sequencing identified high-frequency mutations in NF1 (29/74, 39%), BRAF (31/101, 31%), NRAS (25/95, 26%), and ATRX (17/68, 25%). Of those with an ATRX mutation, 12 (71%) had an additional NF1 mutation. A subset analysis of 21 melanomas showed that the ATRX mutation was associated with loss of ATRX protein expression and ALT. Loss of ATRX expression and ALT were present in both intraepithelial and invasive tumors, suggesting that an ATRX mutation is an early event in conjunctival melanoma progression. The NF1 and ATRX mutations were associated with tarsal (vs. nontarsal) tumors (NF1: 28% vs. 9%, P = 0.035, ATRX: 41% vs. 14%, P = 0.021) and orbital (vs. nonorbital) tumors (ATRX: 24% vs. 2%, P = 0.007). ATRX (vs. ATRX) tumors were associated with a lower 2-year rate of metastasis (0% vs. 24%, P = 0.005). NRAS (vs. NRAS) tumors were associated with a greater 2-year rate of metastasis (28% vs. 14%, P = 0.07) and death (16% vs. 4%, P = 0.04), with a 5-fold increased risk of death (relative risk, 5.45 [95% confidence interval, 1.11-26.71], P = 0.039).
CONCLUSIONS
This study confirms the high frequency of previously documented BRAF and NRAS mutations and recently reported ATRX and NF1 mutations in conjunctival melanoma. An NRAS mutation implied increased risk for metastasis and death. Loss of ATRX and ALT may be early events in conjunctival melanoma development.
目的
通过临床相关性评估结膜黑色素瘤中的靶向突变和分子遗传途径。
设计
观察性病例系列。
参与者
结膜黑色素瘤患者。
主要观察指标
通过下一代测序(NGS)、荧光原位杂交(FISH)的端粒延长替代(ALT)和 ATRX 免疫组织化学检测肿瘤的突变情况。记录 2 年和 5 年肿瘤相关转移和死亡的结果。
结果
在 101 名患者中,平均发病年龄为 60 岁,52%为男性,88%为白人。NGS 面板最初仅靶向 BRAF(n=6,6%)、BRAF/NRAS(n=17,17%)和 BRAF/NRAS/NF1(n=10,10%)。68 个肿瘤用扩展的 592 个基因进行了检测。下一代测序确定 NF1(29/74,39%)、BRAF(31/101,31%)、NRAS(25/95,26%)和 ATRX(17/68,25%)高频突变。在有 ATRX 突变的患者中,12 例(71%)有额外的 NF1 突变。对 21 例黑色素瘤的亚组分析表明,ATRX 突变与 ATRX 蛋白表达缺失和 ALT 有关。ATR 缺失表达和 ALT 存在于上皮内和侵袭性肿瘤中,提示 ATRX 突变是结膜黑色素瘤进展的早期事件。NF1 和 ATRX 突变与跗骨(与非跗骨)肿瘤有关(NF1:28%与 9%,P=0.035,ATRX:41%与 14%,P=0.021)和眶内(与非眶内)肿瘤(ATRX:24%与 2%,P=0.007)。ATRX(与 ATRX)肿瘤与较低的 2 年转移率(0%与 24%,P=0.005)有关。NRAS(与 NRAS)肿瘤与更高的 2 年转移率(28%与 14%,P=0.07)和死亡率(16%与 4%,P=0.04)有关,死亡风险增加 5 倍(相对风险,5.45[95%置信区间,1.11-26.71],P=0.039)。
结论
本研究证实了先前报道的 BRAF 和 NRAS 突变以及最近报道的 ATRX 和 NF1 突变在结膜黑色素瘤中高频发生。NRAS 突变提示转移和死亡的风险增加。ATR 和 ALT 的缺失可能是结膜黑色素瘤发生的早期事件。
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