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pHH3、Ki-67和存活素在良性和恶性黑素细胞性病变中的免疫反应性比较。

Comparison of pHH3, Ki-67, and survivin immunoreactivity in benign and malignant melanocytic lesions.

作者信息

Nasr Michel R, El-Zammar Ola

机构信息

Department of Pathology, State University of New York Upstate Medical University, Syracuse, NY, USA.

出版信息

Am J Dermatopathol. 2008 Apr;30(2):117-22. doi: 10.1097/DAD.0b013e3181624054.

Abstract

Differentiating malignant melanoma from benign melanocytic lesions can be challenging. We undertook this study to evaluate the use of the immunohistochemical mitosis marker phospho-Histone H3 (pHH3) and the proliferation markers Ki-67 and survivin in separating malignant melanoma from benign nevi. Sixty-six melanocytic lesions (18 malignant melanomas, 8 Spitz nevi, 20 dysplastic nevi, and 20 compound nevi) were stained with antibodies to pHH3, Ki-67, and survivin. No pHH3 expression was detected in the dermis of compound and dysplastic nevi. Rare mitoses were observed in the superficial dermis in 3 of 8 Spitz nevi (37%). Staining for pHH3 was higher in malignant melanomas [average 25 per 10 high-power field (HPF), range 2-75 per 10 HPF] than in Spitz nevi (average 0.5 per 10 HPF, range 0-2 per 10 HPF) and was heterogeneously distributed in the malignant melanomas compared with a superficial dermal location in Spitz nevi. There was no cytoplasmic staining for survivin in any of the 66 melanocytic lesions and no nuclear staining in any of the benign ones. Survivin nuclear staining was present in 12 of 18 cases of malignant melanoma (67%) with an average index of 7% (range 0%-15%). In benign melanocytic lesions, the Ki-67 index was less than 5% (range 0%-4%) and staining was present close to the dermo-epidermal junction compared with an average index of 27% in melanomas (range 5%-50%) and a generally heterogeneous pattern of staining throughout the dermis. pHH3 and Ki-67 can be useful adjuncts to histopathology to separate malignant melanoma from benign nevi. pHH3 is especially useful to highlight mitoses and to rapidly assess the mitotic activity in melanocytic lesions.

摘要

鉴别恶性黑色素瘤与良性黑素细胞病变具有挑战性。我们开展这项研究以评估免疫组化有丝分裂标志物磷酸化组蛋白H3(pHH3)以及增殖标志物Ki-67和生存素在区分恶性黑色素瘤与良性痣方面的应用。66例黑素细胞病变(18例恶性黑色素瘤、8例Spitz痣、20例发育异常痣和20例复合痣)用抗pHH3、Ki-67和生存素的抗体进行染色。在复合痣和发育异常痣的真皮层未检测到pHH3表达。8例Spitz痣中有3例(37%)在真皮浅层观察到罕见的有丝分裂。恶性黑色素瘤中pHH3染色[平均每10个高倍视野(HPF)有25个,范围为每10个HPF 2 - 75个]高于Spitz痣(平均每10个HPF 0.5个,范围为每10个HPF 0 - 2个),且与Spitz痣真皮浅层分布不同,pHH3在恶性黑色素瘤中呈异质性分布。66例黑素细胞病变中任何一例均未观察到生存素的胞质染色,良性病变中也均未观察到核染色。18例恶性黑色素瘤中有12例(67%)存在生存素核染色,平均指数为7%(范围为0% - 15%)。在良性黑素细胞病变中,Ki-67指数小于5%(范围为0% - 4%),染色位于真皮 - 表皮交界处附近,而黑色素瘤的平均指数为27%(范围为5% - 50%),且在整个真皮层的染色模式通常呈异质性。pHH3和Ki-67可作为组织病理学的有用辅助手段,用于区分恶性黑色素瘤与良性痣。pHH3在突出有丝分裂以及快速评估黑素细胞病变的有丝分裂活性方面尤其有用。

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