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部分肢端和皮肤黑色素瘤中意外的紫外线辐射(UVR)和非紫外线辐射突变负担

Unexpected UVR and non-UVR mutation burden in some acral and cutaneous melanomas.

作者信息

Rawson Robert V, Johansson Peter A, Hayward Nicholas K, Waddell Nicola, Patch Ann-Marie, Lo Serigne, Pearson John V, Thompson John F, Mann Graham J, Scolyer Richard A, Wilmott James S

机构信息

Melanoma Institute Australia, The University of Sydney, North Sydney, NSW, Australia.

Sydney Medical School, The University of Sydney, Sydney, NSW, Australia.

出版信息

Lab Invest. 2017 Feb;97(2):130-145. doi: 10.1038/labinvest.2016.143. Epub 2017 Jan 9.

Abstract

Ultraviolet radiation (UVR) mutagenesis causes nearly all cutaneous melanomas, however, since UVR signatures are largely absent in acral melanoma, as well as melanoma in sun-protected sites, the cause of these melanomas is unknown. Whole-genome sequencing data generated as part of the Australian Melanoma Genome Project was supplemented with a detailed histopathological assessment with the melanomas then classified as UVR or non-UVR related, based on their mutation signatures. The clinicopathological characteristics of melanomas with mutation signatures for their subtype were compared. Three (of 35=8.6%) acral melanomas, all clinically and pathologically verified as arising from acral or subungual locations, had predominant UVR mutation burden, whereas four (of 140=2.9%) cutaneous melanomas showed predominant non-UVR mutations. Among the acral melanomas, the few that were UVR dominant occurred in younger patients, had a higher mutation load and a proportion of mutation burden due to UVR, which was similar to that in melanomas from intermittently UVR-exposed skin. Acral melanomas with a UVR signature occurred most frequently in subungual sites and included tumors harboring BRAF or NF1 mutations. Cutaneous melanomas dominated by non-UVR signatures had lower mutation burdens counts and their primary tumors were thicker and had more mitoses than in other cutaneous melanomas. No histopathological features predicted UVR dominance in acral melanomas or non-UVR dominance in cutaneous melanomas. Our finding of acral/subungual melanomas with predominant UVR mutagenesis suggests that the nail plate and acral skin do not provide complete protection from UVR. Our data also confirm that cutaneous melanomas not caused by UVR are infrequent. Identifying where mutation burden is discordant with primary tumor anatomical site is likely to be clinically significant when determining treatment options for metastatic acral and cutaneous melanoma patients.

摘要

紫外线辐射(UVR)诱变是几乎所有皮肤黑色素瘤的病因,然而,由于肢端黑色素瘤以及受阳光保护部位的黑色素瘤中基本不存在UVR特征,这些黑色素瘤的病因尚不清楚。作为澳大利亚黑色素瘤基因组计划一部分生成的全基因组测序数据,辅以详细的组织病理学评估,然后根据黑色素瘤的突变特征将其分类为与UVR相关或与非UVR相关。比较了具有其亚型突变特征的黑色素瘤的临床病理特征。35例肢端黑色素瘤中有3例(占8.6%)——所有病例均经临床和病理证实起源于肢端或甲下部位——具有主要的UVR突变负荷,而140例皮肤黑色素瘤中有4例(占2.9%)表现出主要的非UVR突变。在肢端黑色素瘤中,少数UVR占主导的病例发生在年轻患者中,具有较高的突变负荷以及因UVR导致的一定比例的突变负担,这与间歇性暴露于UVR的皮肤中黑色素瘤的情况相似。具有UVR特征的肢端黑色素瘤最常发生在甲下部位,包括携带BRAF或NF1突变的肿瘤。以非UVR特征为主的皮肤黑色素瘤的突变负荷较低,其原发肿瘤比其他皮肤黑色素瘤更厚且有更多的核分裂象。没有组织病理学特征能够预测肢端黑色素瘤中的UVR主导或皮肤黑色素瘤中的非UVR主导。我们发现具有主要UVR诱变的肢端/甲下黑色素瘤表明甲板和肢端皮肤并不能完全抵御UVR。我们的数据还证实,非UVR引起的皮肤黑色素瘤并不常见。在为转移性肢端和皮肤黑色素瘤患者确定治疗方案时,确定突变负担与原发肿瘤解剖部位不一致的情况可能具有临床意义。

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