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Increased expression of stem cell markers in malignant melanoma

机译:恶性黑色素瘤中干细胞标志物的表达增加

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The potential role of stem cells in neoplasia is a subject of recent interest. Three markers of melanocytic stem cells have been described recently. CD166 is expressed on the surface of mesenchymal stem cells and has been found on human melanoma cell lines. CD133 is expressed on the surface of dermal-derived stem cells that are capable of differentiating into neural cells. Nestin is an intermediate filament expressed in the cytoplasm of neuroepithelial stem cells. In this study, we evaluate the expression of these markers and possible differences among banal nevi, primary melanoma, and metastastic melanoma. Tissue microarrays containing normal tissue and 226 melanocytic lesions (71 banal nevi, 71 in situ and invasive melanomas, and 84 metastatic melanomas) were studied by immunohistochemistry using monoclonal antibodies CD166, CD133, and nestin. A significantly greater percentage of melanomas (combined primary and metastatic) contained cells that expressed CD166 (P=0.005), CD133 (P=0.003), and nestin (P=0.03) than banal nevi. Only nestin showed a statistical difference when comparing primary and metastatic melanoma (P=0.05). A stepwise increase in the proportion of lesions expressing all three markers was observed from banal nevi (2/19) to primary melanomas (8/17) to metastatic melanoma (19/28), P=0.0005. All cases of metastatic melanoma expressed at least one stem cell marker. The increased expression of CD166, CD133, and nestin in melanoma suggests that progression to malignant melanoma likely involves genetic pathways instrumental to stem cell biology and normal tissue development. Further studies and characterization of these pathways may also reveal new prognostic markers for a disease whose prognosis in advanced stages is dismal.
机译:干细胞在瘤形成中的潜在作用是最近引起关注的主题。最近已经描述了黑素细胞干细胞的三个标记。 CD166在间充质干细胞的表面表达,并已在人黑素瘤细胞系中发现。 CD133在能够分化为神经细胞的真皮干细胞表面表达。巢蛋白是在神经上皮干细胞的细胞质中表达的中间丝。在这项研究中,我们评估了这些标志物的表达以及正常痣,原发性黑色素瘤和转移性黑色素瘤之间的可能差异。使用单克隆抗体CD166,CD133和nestin,通过免疫组织化学研究了包含正常组织和226个黑素细胞病变(71个班纳痣,71个原位和浸润性黑色素瘤以及84个转移性黑色素瘤)的组织微阵列。黑色素瘤(合并原发性和转移性)的百分比明显高于正常痣,所表达的细胞表达CD166(P = 0.005),CD133(P = 0.003)和Nestin(P = 0.03)。比较原发性和转移性黑色素瘤时,只有巢蛋白显示出统计学差异(P = 0.05)。从全部痣(2/19)到原发性黑色素瘤(8/17)到转移性黑色素瘤(19/28)观察到表达所有三种标记物的病变比例逐步增加,P = 0.0005。所有转移性黑色素瘤病例均表达至少一种干细胞标记。黑色素瘤中CD166,CD133和Nestin的表达增加表明向恶性黑色素瘤的发展可能涉及对干细胞生物学和正常组织发育有帮助的遗传途径。这些途径的进一步研究和表征也可能揭示出疾病的新的预后标志物,其晚期预后不良。

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