在深部侵袭性痣中未发现 HRAS 突变和 GNAQ 或 GNA11 突变。
Identification of HRAS mutations and absence of GNAQ or GNA11 mutations in deep penetrating nevi.
机构信息
Caris Life Sciences, Phoenix, AZ, USA.
出版信息
Mod Pathol. 2013 Oct;26(10):1320-8. doi: 10.1038/modpathol.2013.77. Epub 2013 Apr 19.
HRAS is mutated in ∼15% of Spitz nevi, and GNAQ or GNA11 is mutated in blue nevi (46-83% and ∼7% respectively). Epithelioid blue nevi and deep penetrating nevi show features of both blue nevi (intradermal location, pigmentation) and Spitz nevi (epithelioid morphology). Epithelioid blue nevi and deep penetrating nevi can also show overlapping features with melanoma, posing a diagnostic challenge. Although epithelioid blue nevi are considered blue nevic variants, no GNAQ or GNA11 mutations have been reported. Classification of deep penetrating nevi as blue nevic variants has also been proposed, however, no GNAQ or GNA11 mutations have been reported and none have been tested for HRAS mutations. To better characterize these tumors, we performed mutational analysis for GNAQ, GNA11, and HRAS, with blue nevi and Spitz nevi as controls. Within deep penetrating nevi, none demonstrated GNAQ or GNA11 mutations (0/38). However, 6% revealed HRAS mutation (2/32). Twenty percent of epithelioid blue nevi contained a GNAQ mutation (2/10), while none displayed GNA11 or HRAS mutation. Eighty-seven percent of blue nevi contained a GNAQ mutation (26/30), 4% a GNA11 mutation (1/28), and none an HRAS mutation. Within Spitz nevi, none demonstrated GNAQ or GNA11 mutations (0/30). Seventeen percent contained an HRAS mutation (5/30). All GNAQ and GNA11 mutations were p.Q209L (c.626A>T) point mutations, except 2 GNAQ mutations, which contained novel c.625_626CA>TT double mutations. Four HRAS mutations were in exon 2, and three in exon 3. This is the first study to identify HRAS mutations in deep penetrating nevi. The presence of HRAS mutations and absence of GNAQ or GNA11 mutations in deep penetrating nevi suggests classification of these unusual nevi within the Spitz nevus category of melanocytic tumors, rather than the blue nevus category.
HRAS 在 ∼15% 的 Spitz 痣中发生突变,GNAQ 或 GNA11 在蓝色痣中发生突变(分别为 46-83%和 ∼7%)。上皮样蓝色痣和深部穿透痣同时具有蓝色痣(真皮内位置、色素沉着)和 Spitz 痣(上皮样形态)的特征。上皮样蓝色痣和深部穿透痣也可能与黑色素瘤重叠,这给诊断带来了挑战。尽管上皮样蓝色痣被认为是蓝色痣的变异体,但尚未报道 GNAQ 或 GNA11 突变。也有人提出将深部穿透痣归类为蓝色痣的变异体,但尚未报道 GNAQ 或 GNA11 突变,也未对 HRAS 突变进行检测。为了更好地描述这些肿瘤,我们对 GNAQ、GNA11 和 HRAS 进行了突变分析,并以蓝色痣和 Spitz 痣作为对照。在深部穿透痣中,没有发现 GNAQ 或 GNA11 突变(0/38)。然而,6%的 HRAS 突变(2/32)。20%的上皮样蓝色痣含有 GNAQ 突变(2/10),而没有 GNA11 或 HRAS 突变。87%的蓝色痣含有 GNAQ 突变(26/30),4%的 GNA11 突变(1/28),无一例 HRAS 突变。在 Spitz 痣中,没有发现 GNAQ 或 GNA11 突变(0/30)。17%含有 HRAS 突变(5/30)。所有 GNAQ 和 GNA11 突变均为 p.Q209L(c.626A>T)点突变,除 2 个 GNAQ 突变外,均为 c.625_626CA>TT 双突变。4 个 HRAS 突变位于外显子 2,3 个位于外显子 3。这是首次在深部穿透痣中发现 HRAS 突变。深部穿透痣中存在 HRAS 突变而缺乏 GNAQ 或 GNA11 突变,提示这些不寻常的痣应归类于 Spitz 痣黑色素瘤类别,而不是蓝色痣类别。
Zotero 插件