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具有真皮梭形细胞形态的皮肤黑素细胞性病变亚组中NRAS的突变和扩增:两例耳部小儿病例报告

Mutated and amplified NRAS in a subset of cutaneous melanocytic lesions with dermal spitzoid morphology: report of two pediatric cases located on the ear.

作者信息

Dubruc Estelle, Balme Brigitte, Dijoud Frédérique, Disant Francois, Thomas Luc, Wang Qing, Pissaloux Daniel, de la Fouchardiere Arnaud

机构信息

Département de Biopathologie, Centre Léon Bérard, Lyon, France.

出版信息

J Cutan Pathol. 2014 Nov;41(11):866-72. doi: 10.1111/cup.12389. Epub 2014 Oct 21.

Abstract

Extensive cytogenetic testing is slowly unveiling the complexity of the genomics of melanocytic tumors. NRAS mutations have been the first genetic abnormality described in malignant melanomas. We report the cases of two children, presenting a melanocytic lesion located on the ear. One appeared as a combined dermal clone inside a congenital nevus and the other as a centimetric purely dermal tumor. Both tumors were composed of spindled spitzoid melanocytes with atypical histologic features. aCGH and FISH revealed an amplification of the NRAS gene. Sequencing showed an exon 3 NRAS mutation. In the combined case, the amplification was limited to the spitzoid component, underscoring a possible phenotypic shift induced by the alteration. Similarly an overexpression of CyclinD1 and elevation of ki-67 was found in the spitzoid component confirming a raise in proliferation. Such combination of mutation and copy number increase has been previously reported for the HRAS gene in a subset of Spitz nevi. Further studies must evaluate if mutated NRAS is also amplified in melanomas arising in this clinical setting. These combined alterations could represent an early event ultimately leading to malignancy.

摘要

广泛的细胞遗传学检测正在逐步揭示黑素细胞肿瘤基因组学的复杂性。NRAS突变是恶性黑色素瘤中最早描述的基因异常。我们报告了两名儿童的病例,他们耳部出现黑素细胞病变。一例表现为先天性痣内的混合性真皮克隆,另一例为厘米级的单纯真皮肿瘤。两种肿瘤均由具有非典型组织学特征的梭形斯皮茨样黑素细胞组成。阵列比较基因组杂交(aCGH)和荧光原位杂交(FISH)显示NRAS基因扩增。测序显示NRAS基因第3外显子突变。在混合性病例中,扩增仅限于斯皮茨样成分,强调了这种改变可能引起的表型转变。同样,在斯皮茨样成分中发现细胞周期蛋白D1过表达和ki-67升高,证实增殖增加。先前在一部分斯皮茨痣中报道过HRAS基因存在这种突变和拷贝数增加的组合。进一步的研究必须评估在这种临床情况下发生的黑色素瘤中,突变的NRAS是否也会扩增。这些联合改变可能代表了最终导致恶性肿瘤的早期事件。

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