Publication | Closed Access
Genome-wide analysis of organ-preferential metastasis of human small cell lung cancer in mice.
114
Citations
22
References
2003
Year
Biological MicroenvironmentsPathologyCancer MetastasisCancer BiologyTumor BiologyOncologyTumor HeterogeneityCancer Cell BiologyRadiation OncologyCancer ResearchHealth SciencesOrgan SpecificityCancer GeneticsMetastasis ModelCell BiologyTumor MicroenvironmentLung CancerOrgan-preferential MetastasisCancer GenomicsMedicineGenome-wide Analysis
Although a number of molecules have been implicated in the process of cancer metastasis, the organ-selective nature of cancer cells is still poorly understood. To investigate this issue, we established a metastasis model in mice with multiple organ dissemination by i.v. injection of human small cell lung cancer (SBC-5) cells. We analyzed gene-expression profiles of 25 metastatic lesions from four organs (lung, liver, kidney, and bone) using a cDNA microarray representing 23,040 genes and extracted 435 genes that seemed to reflect the organ specificity of the metastatic cells and the cross-talk between cancer cells and microenvironment. Furthermore, we discovered 105 genes that might be involved in the incipient stage of secondary-tumor formation by comparing the gene-expression profiles of metastatic lesions classified according to size (<1 or >2 mm) as either "micrometastases" or "macrometastases." This genome-wide analysis should contribute to a greater understanding of molecular aspects of the metastatic process in different microenvironments, and provide indicators for new strategies to predict and prevent metastasis.
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