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利用靶向下一代测序鉴定樱桃状血管瘤中的激活热点突变。

Use of Targeted Next-Generation Sequencing to Identify Activating Hot Spot Mutations in Cherry Angiomas.

机构信息

Medical student, Wellman Center for Photomedicine at Massachusetts General Hospital, Harvard Medical School, Boston.

Department of Dermatology, Massachusetts General Hospital, Boston.

出版信息

JAMA Dermatol. 2019 Feb 1;155(2):211-215. doi: 10.1001/jamadermatol.2018.4231.

Abstract

IMPORTANCE

Shared gene variants in benign-malignant process pairs, such as BRAF mutations common to benign nevi and melanoma, are associated with differing phenotypic manifestations. Study of gene mechanisms underlying cherry angioma may uncover previously unknown disease relationships.

OBJECTIVE

To identify somatic mutations present in cherry angioma specimens by using targeted next-generation sequencing.

DESIGN, SETTING, AND PARTICIPANTS: In a single-center case series, 10 formalin-fixed, paraffin-embedded cherry angioma specimens from biopsies performed at Massachusetts General Hospital in Boston from July 10, 2016, to January 23, 2018, were obtained and underwent sequencing across a panel of 323 genes most relevant to cancer. Somatic mutations were curated by excluding variants that were presumed to be germline or of low mapping quality.

MAIN OUTCOMES AND MEASURES

Identification of somatic mutations associated with cherry angiomas.

RESULTS

In 10 cherry angioma tissue samples originating from 6 female and 4 male patients with a median (range) age of 54 (26-79) years, 5 samples (50%) revealed somatic missense mutations in GNAQ (Q209H, Q209R, and R183G) and GNA11 (Q209H). Individually, these mutational hot spots are known to be involved in entities that include congenital and anastomosing hemangiomas, hepatic small-vessel neoplasms (Q209), port-wine stains, and Sturge-Weber syndrome (R183). Both hot spots are associated with blue nevi, melanoma associated with blue nevus, and uveal melanoma.

CONCLUSIONS AND RELEVANCE

In this case series study, the high prevalence of 5 known genetic drivers within the benign cherry angioma entity appears to support the context-dependent role of gene alterations in both benign and malignant proliferations from various cellular origins.

摘要

重要性

良性-恶性过程对(如 BRAF 突变,它常见于良性痣和黑色素瘤)中的共享基因变异与不同的表型表现相关。研究樱桃状血管瘤的基因机制可能会揭示以前未知的疾病关系。

目的

通过靶向下一代测序鉴定樱桃状血管瘤标本中的体细胞突变。

设计、地点和参与者:在单中心病例系列研究中,我们从 2016 年 7 月 10 日至 2018 年 1 月 23 日在波士顿马萨诸塞州综合医院进行的活检中获得了 10 例福尔马林固定、石蜡包埋的樱桃状血管瘤标本,并对与癌症最相关的 323 个基因进行了测序。通过排除被认为是种系或低映射质量的变体来对体细胞突变进行策展。

主要结果和措施

鉴定与樱桃状血管瘤相关的体细胞突变。

结果

在 10 例源自 6 名女性和 4 名男性患者的樱桃状血管瘤组织样本中(中位年龄 54 岁[26-79 岁]),有 5 例(50%)样本发现 GNAQ(Q209H、Q209R 和 R183G)和 GNA11(Q209H)的体细胞错义突变。这些突变热点单独参与包括先天性和吻合性血管瘤、肝小血管肿瘤(Q209)、葡萄酒色斑和 Sturge-Weber 综合征(R183)等实体。这两个热点都与蓝痣、蓝痣相关黑色素瘤和葡萄膜黑色素瘤有关。

结论和相关性

在本病例系列研究中,良性樱桃状血管瘤实体中已知的 5 个遗传驱动因素的高患病率似乎支持基因改变在来自不同细胞起源的良性和恶性增殖中的上下文相关作用。

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