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桥粒芯糖蛋白2在恶性皮肤癌中的表达增加:一项基于组织芯片的研究。

Increased expression of Dsg2 in malignant skin carcinomas: A tissue-microarray based study.

作者信息

Brennan Donna, Mahoney Mÿ G

机构信息

Department of Dermatology and Cutaneous Biology, Thomas Jefferson University, Philadelphia, Pennsylvania, USA.

出版信息

Cell Adh Migr. 2009 Apr-Jun;3(2):148-54. doi: 10.4161/cam.3.2.7539. Epub 2009 Apr 4.

Abstract

Desmoglein 2 (Dsg2), a transmembrane cadherin of the desmosomal cell-cell adhesion structure, is downregulated with epithelial differentiation. We recently demonstrated that overexpression of Dsg2 in epidermal keratinocytes deregulates multiple signaling pathways associated with increased growth rate, anchorage-independent cell survival, and the development of skin tumors. While changes in Dsg2 expression have been observed in neoplastic lesions, the correlation of expression levels and localization of Dsg2 and the state of tumor development has not been fully established. Here we generated a highly sensitive Dsg2 antibody (Ab10) and characterized that antibody along with a previously developed Dsg2 specific antibody 10D2. Using these antibodies in immunostaining of tissue microarrays, we show a dramatic upregulation of Dsg2 expression in certain human epithelial malignancies including basal cell carcinomas (BCC; n = 12), squamous cell carcinomas (SCC; n = 57), carcinomas of sebaceous and sweat glands (n = 12), and adenocarcinomas (n = 3). Dsg2 expression was completely absent in malignant fibrosarcomas (n = 16) and melanomas (n = 15). While Dsg2 expression was consistently strong in BCC, it varied in SCC with a minor correlation between a decrease of Dsg2 expression and tumor differentiation. In summary, we have identified Dsg2 as a potential novel marker for epithelial-derived malignancies.

摘要

桥粒芯糖蛋白2(Dsg2)是桥粒细胞间黏附结构的一种跨膜钙黏蛋白,其表达随上皮分化而下调。我们最近证明,在表皮角质形成细胞中过表达Dsg2会使与生长速率增加、不依赖贴壁的细胞存活以及皮肤肿瘤发生相关的多种信号通路失调。虽然在肿瘤性病变中已观察到Dsg2表达的变化,但Dsg2的表达水平和定位与肿瘤发展状态之间的相关性尚未完全明确。在此,我们制备了一种高灵敏度的Dsg2抗体(Ab10),并对该抗体以及先前开发的Dsg2特异性抗体10D2进行了特性鉴定。通过使用这些抗体对组织微阵列进行免疫染色,我们发现Dsg2在某些人类上皮恶性肿瘤中显著上调,包括基底细胞癌(BCC;n = 12)、鳞状细胞癌(SCC;n = 57)、皮脂腺癌和汗腺癌(n = 12)以及腺癌(n = 3)。在恶性纤维肉瘤(n = 16)和黑色素瘤(n = 15)中完全不存在Dsg2表达。虽然Dsg2在BCC中始终呈强表达,但在SCC中其表达存在差异,Dsg2表达降低与肿瘤分化之间存在轻微相关性。总之,我们已将Dsg2鉴定为上皮源性恶性肿瘤的一种潜在新型标志物。

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