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Nuclear expression of survivin portends a poor prognosis in Merkel cell carcinoma

机译:Survivin的核表达预示默克尔细胞癌预后不良

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Inhibition of apoptosis is a critical step in tumorigenesis in many cancers, including Merkel cell carcinoma; however, the exact regulatory mechanisms are not fully understood. Survivin is an inhibitor of apoptosis that is undetectable in most terminally differentiated normal human tissues, strongly expressed in embryonic and fetal organs and is strongly expressed in many different human cancers. In this study, we investigated the expression of survivin in cutaneous Merkel cell carcinoma using immunohistochemistry and correlated the findings with long-term clinical follow-up. We collected and immunostained 19 cases of Merkel cell carcinoma with antibodies to survivin. The median patient age was 79 years, with an average follow-up of 17 months, and a male/female ratio of 7:11. All but one sample represented primary lesions and two cases were obtained from one patient. Clinical follow-up was obtained in 15 cases (79%). All 19 cases of Merkel cell carcinoma demonstrated strong immunoreactivity for survivin. Survivin protein was localized and classified into predominately nuclear (N=8) or cytoplasmic (N=4) compartments. A mixed pattern of survivin expression was also seen in three cases. Cases with a nuclear staining pattern were distinguished by an aggressive clinical course, with seven of eight patients developing metastases or dead of disease on follow-up. Furthermore, all of the cases with predominately cytoplasmic survivin localization (N=4) were free of disease on follow-up. Merkel cell carcinomas represent aggressive malignancies regulated by apoptotic pathways. We demonstrate that survivin, a protein with a dual role in inhibition of apoptosis and regulation of cellular proliferation is expressed in Merkel cell carcinoma. Moreover, nuclear subcellular localization of survivin in Merkel cell carcinomas may portend a poor prognosis and identification of these cases may assist clinical management.
机译:抑制细胞凋亡是许多癌症(包括默克尔细胞癌)中肿瘤发生的关键步骤。但是,确切的监管机制尚未完全了解。 Survivin是凋亡的抑制剂,在大多数终末分化的正常人体组织中无法检测到,在胚胎和胎儿器官中强烈表达,在许多不同的人类癌症中强烈表达。在这项研究中,我们使用免疫组织化学研究了Survivin在皮肤默克尔细胞癌中的表达,并将该发现与长期临床随访相关联。我们收集和免疫染色的19例默克细胞癌中含有survivin抗体。患者平均年龄为79岁,平均随访17个月,男女比例为7:11。除一个样本外,所有样本均代表原发灶,其中两个病例来自一名患者。 15例(79%)获得了临床随访。默克尔细胞癌的所有19例病例均显示出对生存素的强免疫反应性。 Survivin蛋白被定位并主要分为核(N = 8)或胞质(N = 4)区域。在三例中也观察到了survivin表达的混合模式。具有核染色模式的病例以积极的临床过程为特征,八名患者中有七名在随访中出现转移或死亡。此外,所有以细胞质survivin定位为主(N = 4)的病例在随访时均无疾病。默克尔细胞癌代表由凋亡途径调节的侵袭性恶性肿瘤。我们证明survivin,一种在抑制凋亡和调节细胞增殖中具有双重作用的蛋白质,在默克尔细胞癌中表达。此外,默克尔细胞癌中survivin的核亚细胞定位可能预示不良预后,这些病例的鉴定可能有助于临床管理。

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