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人类皮肤黑色素瘤中通过微阵列显示的整合素表达模式改变。

Altered integrin expression patterns shown by microarray in human cutaneous melanoma.

作者信息

Vizkeleti Laura, Kiss Timea, Koroknai Viktoria, Ecsedi Szilvia, Papp Orsolya, Szasz Istvan, Adany Roza, Balazs Margit

机构信息

aDepartment of Preventive Medicine, Faculty of Public Health bMTA-DE Public Health Research Group, University of Debrecen, Debrecen, Hungary.

出版信息

Melanoma Res. 2017 Jun;27(3):180-188. doi: 10.1097/CMR.0000000000000322.

DOI:10.1097/CMR.0000000000000322
PMID:28234767
Abstract

A large variety of molecular pathways in melanoma progression suggests that no individual molecular alteration is crucial in itself. Our aim was to define the molecular alterations underlying metastasis formation. Gene expression profiling was performed using microarray and qRT-PCR to define alterations between matched primary and metastatic melanoma cell lines. These data were integrated with publicly available unmatched tissue data. The invasiveness of cell lines was determined by Matrigel invasion assays and invasive clones from primary melanoma-derived cell lines were also selected. Two metastatic cell line models were created: the regional lymph node WM983A-WM983A-WM983B and the distant lung WM793B-WM793B-1205Lu metastatic models. The majority of metastasis genes were downregulated and enriched in adhesion and ITGA6-B4 pathways. Upregulation of immune pathways was characteristic of distant metastases, whereas increased Rap1 signaling was specific for regional (sub)cutaneous metastases. qRT-PCR analysis of selected integrins (A2, A3, A4, A9, B5, B8, A6, B1, and B3) highlighted the possible importance of ITGA3/4 and B8 in the metastatic process, distinguishing regional and distant metastases. We identified functionally relevant gene clusters that influenced metastasis formation. Our data provide further evidence that integrin expression patterns may be important in distant metastasis formation.

摘要

黑色素瘤进展过程中存在多种分子途径,这表明单个分子改变本身并非至关重要。我们的目的是确定转移形成背后的分子改变。使用微阵列和qRT-PCR进行基因表达谱分析,以确定匹配的原发性和转移性黑色素瘤细胞系之间的改变。这些数据与公开可用的不匹配组织数据相结合。通过基质胶侵袭试验确定细胞系的侵袭性,并从原发性黑色素瘤衍生的细胞系中选择侵袭性克隆。创建了两种转移细胞系模型:区域淋巴结WM983A-WM983A-WM983B和远处肺WM793B-WM793B-1205Lu转移模型。大多数转移基因下调,并在黏附及ITGA6-B4途径中富集。免疫途径的上调是远处转移的特征,而Rap1信号增加是区域(皮下)转移所特有的。对选定整合素(A2、A3、A4、A9、B5、B8、A6、B1和B3)的qRT-PCR分析突出了ITGA3/4和B8在转移过程中的可能重要性,可区分区域转移和远处转移。我们确定了影响转移形成的功能相关基因簇。我们的数据进一步证明整合素表达模式可能在远处转移形成中起重要作用。

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