S100 protein expression in PKC-fused blue naevi, cellular blue naevi and PRKAR1A-inactivated pigmented epithelioid melanocytomas.

IF 3.6 3区 医学 Q1 PATHOLOGY Pathology Pub Date : 2024-09-18 DOI:10.1016/j.pathol.2024.06.014
Pauline Hayenne, Daniel Pissaloux, Franck Tirode, Arnaud de la Fouchardiere
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Abstract

Recent data have redefined the genetic spectrum of pigmented epithelioid melanocytomas (PEMs). PEM is now defined by a secondary genetic event, a protein kinase cAMP-dependent type I regulatory subunit alpha (PRKAR1A) inactivation, that confers the specific cytomorphology of the entity, but this event can arise within a naevus with a genetic background of common, blue or Spitz type. PKC-fused melanocytic proliferations, although they can exhibit PEM-like morphological features, have now been regrouped within the blue group of tumours. Past studies have shown that the latter group tends to lose S100 expression. Herein, we studied the nuclear expression of S100 by immunohistochemistry in 73 PKC-fused benign blue naevi. Histologically, the most frequent pattern found in PKC-fused blue naevi (51%) was a dermal biphasic architecture associated with a horizontal band of medium-sized bland melanocytes in the upper papillary dermis, with a deeper dermal expansion combining spindled and dendritic melanocytes with occasional small nests of bland melanocytes within a fibrous background. A PEM-like hyperpigmented hyperplasia of the epidermis was seen in 32% of cases. The immunohistochemical study found in 31 of the 37 (84%) dermal biphasic PKC-fused melanocytic tumour cases a significant loss of nuclear expression of S100 (in more than 50% of cells) in the superficial horizontal dermal band area and in 68% of the biphasic dermal component. However, the hyperpigmented PEM-like junctional components were not assessable by immunohistochemistry. An exploratory analysis of S100 expression in 21 blue naevi and in 25 PEM with confirmed PRKAR1A inactivation was also performed. In blue naevi, a loss of nuclear S100 expression in more than 50% of melanocytes was found in over 70% of these lesions both in the dendritic and epithelioid dermal components. By contrast, nuclear expression of S100 was most often preserved in PEM with PRKAR1A inactivation (85% preservation in the epithelioid component). These results suggest that searching for S100 expression loss by immunohistochemistry may be helpful in the diagnosis of PKC-fused blue naevus similarly as in dendritic and cellular blue naevi. This simple test, especially if a band-like structure is present in the upper dermis, can effectively support this diagnosis, as a genetic confirmation of these benign tumours is not warranted.

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PKC融合蓝痣、细胞蓝痣和PRKAR1A失活的色素上皮样黑素细胞瘤中S100蛋白的表达。
最新数据重新定义了色素上皮样黑色素细胞瘤(PEM)的遗传谱。现在,PEM 是由一个次要遗传事件(蛋白激酶 cAMP 依赖性 I 型调节亚基 alpha (PRKAR1A)失活)定义的,该事件赋予了该实体特殊的细胞形态学,但该事件可能发生在具有普通型、蓝色型或 Spitz 型遗传背景的痣中。PKC融合型黑素细胞增生虽然可以表现出与PEM相似的形态特征,但现在已被重新归入蓝色肿瘤组。过去的研究表明,后一类肿瘤往往失去 S100 的表达。在此,我们通过免疫组化方法研究了 73 例融合 PKC 的良性蓝痣的 S100 核表达情况。从组织学角度看,PKC 融合型蓝痣最常见的形态(51%)是真皮双相结构,在真皮乳头上部有一条中等大小的平淡无奇的黑素细胞水平带,真皮深部扩张,结合了纺锤形和树枝状黑素细胞,偶尔在纤维背景内有平淡无奇的黑素细胞小巢。32%的病例表皮出现 PEM 样色素沉着增生。免疫组化研究发现,37 例真皮双相 PKC 融合型黑素细胞瘤病例中有 31 例(84%)在真皮浅层水平带区域和 68% 的真皮双相成分中,S100 的核表达明显丧失(超过 50% 的细胞)。不过,免疫组化无法评估色素沉着的 PEM 样交界成分。此外,还对 21 个蓝色痣和 25 个证实 PRKAR1A 失活的 PEM 中的 S100 表达进行了探索性分析。在蓝痣中,超过50%的黑色素细胞核S100表达缺失,其中70%以上的病变在树枝状和上皮样真皮成分中都有S100表达。相比之下,在PRKAR1A失活的PEM中,S100的核表达最常得到保留(在上皮样成分中保留了85%)。这些结果表明,用免疫组化方法检测 S100 表达缺失可能有助于诊断 PKC 融合型蓝痣,就像诊断树突状蓝痣和细胞状蓝痣一样。这种简单的检测方法,尤其是当真皮上部出现带状结构时,可有效支持这一诊断,因为这些良性肿瘤无需进行基因确诊。
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来源期刊
Pathology
Pathology 医学-病理学
CiteScore
6.50
自引率
2.20%
发文量
459
审稿时长
54 days
期刊介绍: Published by Elsevier from 2016 Pathology is the official journal of the Royal College of Pathologists of Australasia (RCPA). It is committed to publishing peer-reviewed, original articles related to the science of pathology in its broadest sense, including anatomical pathology, chemical pathology and biochemistry, cytopathology, experimental pathology, forensic pathology and morbid anatomy, genetics, haematology, immunology and immunopathology, microbiology and molecular pathology.
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