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非色素性弥漫性神经纤维瘤中存在显著比例的黑色素细胞分化:一个潜在的诊断陷阱。

Melanocytic differentiation is present in a significant proportion of nonpigmented diffuse neurofibromas: a potential diagnostic pitfall.

机构信息

Medical Faculty, Institute of Pathology, University of Ljubljana, Ljubljana, Slovenia.

出版信息

Am J Surg Pathol. 2013 Aug;37(8):1182-91. doi: 10.1097/PAS.0b013e31828950a3.

DOI:10.1097/PAS.0b013e31828950a3
PMID:23715161
Abstract

Whereas the pigmented (melanotic) variant of diffuse neurofibroma (DNF) with positivity for melanocytic markers is well recognized, expression of melanocytic markers in nonpigmented DNF has not been systematically studied. We analyzed 28 unselected consecutive DNFs for expression of melanocytic markers, including melan A, microphthalmia transcription factor (MITF), and HMB-45 antigen. For comparison, we also analyzed 40 localized skin neurofibromas and 7 intraneural neurofibromas. One case of nonpigmented DNF was analyzed by electron microscopy. Of the 28 DNFs studied by immunohistochemistry, 3 were pigmented and 25 nonpigmented. The 3 pigmented DNFs and 9 of 25 (36%) nonpigmented DNFs expressed melan A, MITF, and HMB-45 antigen. These markers were expressed either focally or more diffusely, typically in a minority of the lesional cells, and usually both in the dermal and subcutaneous portion of the DNF. Melan A was expressed in the largest number of the lesional cells (up to 50%), whereas only a small fraction of the melan A-positive cells (from 5% to 10% in most cases) also expressed HMB-45 antigen. None of the 47 non-DNFs expressed these markers. Ultrastructurally, melanosomes were present in some cells in nonpigmented DNF that expressed the melanocytic markers. Twenty-three of 28 (82%) DNFs, including 10 of 12 (83%) DNFs with melanocytic differentiation, were associated with neurofibromatosis type 1. Expression of melanocytic markers, including melan A, HMB-45 antigen, and MITF in DNF is a potential pitfall in differential diagnosis with melanocytic lesions that may clinically or histopathologically resemble DNF, in particular congenital melanocytic nevus with neurotization and neurofibroma-like melanoma.

摘要

虽然弥漫性神经纤维瘤(DNF)的色素性(黑色素性)变体伴有黑色素细胞标志物的阳性表达已得到广泛认可,但非色素性 DNF 中黑色素细胞标志物的表达尚未得到系统研究。我们分析了 28 例未经选择的连续 DNF,以检测黑色素细胞标志物的表达,包括黑色素 A、小眼畸形转录因子(MITF)和 HMB-45 抗原。为了比较,我们还分析了 40 例局部皮肤神经纤维瘤和 7 例神经内神经纤维瘤。对 1 例非色素性 DNF 进行了电子显微镜分析。在免疫组织化学研究的 28 例 DNF 中,3 例为色素性,25 例为非色素性。3 例色素性 DNF 和 25 例(36%)非色素性 DNF 中的 9 例表达黑色素 A、MITF 和 HMB-45 抗原。这些标志物的表达要么是局灶性的,要么是弥漫性的,通常在少数病变细胞中表达,通常在 DNF 的真皮和皮下部分都有表达。黑色素 A 在病变细胞中表达的数量最多(高达 50%),而在大多数情况下,只有一小部分黑色素 A 阳性细胞(5%至 10%)也表达 HMB-45 抗原。47 例非 DNF 均未表达这些标志物。超微结构显示,在表达黑色素细胞标志物的非色素性 DNF 中的一些细胞中存在黑色素体。28 例 DNF 中有 23 例(82%),包括 12 例有黑色素细胞分化的 DNF 中有 10 例(83%),与 1 型神经纤维瘤病有关。黑色素细胞标志物(包括黑色素 A、HMB-45 抗原和 MITF)在 DNF 中的表达是与黑色素细胞病变进行鉴别诊断的潜在陷阱,这些病变在临床上或组织病理学上可能与 DNF 相似,特别是伴有神经化的先天性黑色素细胞痣和神经纤维瘤样黑色素瘤。

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