Department of Dermatology, University of Regensburg, Regensburg, Germany.
Nat Genet. 2012 Jun 10;44(7):783-7. doi: 10.1038/ng.2316.
Nevus sebaceous is a common congenital cutaneous malformation. Affected individuals may develop benign and malignant secondary tumors in the nevi during life. Schimmelpenning syndrome is characterized by the association of nevus sebaceous with extracutaneous abnormalities. We report that of 65 sebaceous nevi studied, 62 (95%) had mutations in the HRAS gene and 3 (5%) had mutations in the KRAS gene. The HRAS c.37G>C mutation, which results in a p.Gly13Arg substitution, was present in 91% of lesions. Nonlesional tissues from 18 individuals had a wild-type sequence, confirming genetic mosaicism. The HRAS c.37G>C mutation was also found in 8 of 8 associated secondary tumors. Mosaicism for HRAS c.37G>C and KRAS c.35G>A mutations was found in two individuals with Schimmelpenning syndrome. Functional analysis of HRAS c.37G>C mutant cells showed constitutive activation of the MAPK and PI3K-Akt signaling pathways. Our results indicate that nevus sebaceous and Schimmelpenning syndrome are caused by postzygotic HRAS and KRAS mutations. These mutations may predispose individuals to the development of secondary tumors in nevus sebaceous.
皮脂腺痣是一种常见的先天性皮肤畸形。受影响的个体在其一生中可能会在痣中发展出良性和恶性的继发性肿瘤。Schimmelpenning 综合征的特征是皮脂腺痣与皮肤外异常相关联。我们报告在研究的 65 个皮脂腺痣中,62 个(95%)有 HRAS 基因突变,3 个(5%)有 KRAS 基因突变。导致 p.Gly13Arg 取代的 HRAS c.37G>C 突变存在于 91%的病变中。18 个个体的非病变组织具有野生型序列,证实了遗传镶嵌现象。HRAS c.37G>C 突变也存在于 8 个相关的继发性肿瘤中。Schimmelpenning 综合征的 2 名个体中存在 HRAS c.37G>C 和 KRAS c.35G>A 突变的镶嵌现象。HRAS c.37G>C 突变细胞的功能分析显示 MAPK 和 PI3K-Akt 信号通路的组成性激活。我们的结果表明,皮脂腺痣和 Schimmelpenning 综合征是由合子后 HRAS 和 KRAS 突变引起的。这些突变可能使个体易患皮脂腺痣中继发性肿瘤的发生。
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