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默克尔细胞多瘤病毒状态与默克尔细胞癌的临床病程无关。

Merkel cell polyomavirus status is not associated with clinical course of Merkel cell carcinoma.

机构信息

Department of Dermatology, Division of General Dermatology, Medical University of Graz, Graz, Austria.

出版信息

J Invest Dermatol. 2011 Aug;131(8):1631-8. doi: 10.1038/jid.2011.115. Epub 2011 May 12.

Abstract

The majority of Merkel cell carcinomas (MCCs) are associated with the recently identified Merkel cell polyomavirus (MCV). However, as it is still unclear to which extent the presence of MCV impacts tumor characteristics or clinical outcome, we correlated the MCV status of tumor lesions obtained from 174 MCC patients including 38 MCC patients from Australia and 138 MCC patients from Germany with clinical characteristics, histomorphology, immunohistochemistry, and course of the disease. MCV DNA was present in 86% of MCCs and, in contrast to previous reports, no significant difference in MCV prevalence was present between Australian and German MCC cases. When patients were stratified according to their MCV status, only tumor localization (P=0.001), gender (P=0.024), and co-morbidity, i.e., frequency of patients with previous skin tumors (P=0.024), were significantly different factors. In contrast, year of birth and diagnosis, age at diagnosis, or histological type and features representing the oncogenic phenotype such as mitotic rate or expression of p16, p53, RB1, and Ki67 were not significantly different between MCV-positive and MCV-negative MCCs. MCV status also did not influence recurrence-free, overall, and MCC-specific survival significantly. In summary, although MCV-positive and MCV-negative MCCs may have different etiologies, these tumors have comparable clinical behaviors and prognosis.

摘要

大多数 Merkel 细胞癌 (MCC) 与最近发现的 Merkel 细胞多瘤病毒 (MCV) 有关。然而,由于 MCV 的存在对肿瘤特征或临床结果的影响程度尚不清楚,我们将从 174 例 MCC 患者中获得的肿瘤病变的 MCV 状态与临床特征、组织形态学、免疫组织化学和疾病过程相关联,这些患者包括 38 例来自澳大利亚的 MCC 患者和 138 例来自德国的 MCC 患者。MCV DNA 存在于 86%的 MCC 中,与之前的报道相比,澳大利亚和德国 MCC 病例中 MCV 的流行率没有显著差异。当根据 MCV 状态对患者进行分层时,只有肿瘤定位(P=0.001)、性别(P=0.024)和合并症,即有先前皮肤肿瘤的患者的频率(P=0.024)是显著不同的因素。相比之下,MCV 阳性和 MCV 阴性 MCC 之间的 MCV 阳性和 MCV 阴性 MCC 之间的发病年份和诊断、诊断时的年龄或代表致癌表型的组织学类型和特征,如有丝分裂率或 p16、p53、RB1 和 Ki67 的表达,没有显著差异。MCV 状态也没有显著影响无复发生存、总生存和 MCC 特异性生存。总之,尽管 MCV 阳性和 MCV 阴性的 MCC 可能具有不同的病因,但这些肿瘤具有相似的临床行为和预后。

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