Human Gene Set: ALONSO_METASTASIS_EMT_DN

Standard name

ALONSO_METASTASIS_EMT_DN

Systematic name

M3029

Brief description

EMT (epithelial-mesenchymal transition) genes down-regulated genes in melanoma tumous that developed metastatic disease compared to primary melanoma that did not.

Full description or abstract

Metastatic disease is the primary cause of death in cutaneous malignant melanoma (CMM) patients. To understand the mechanisms of CMM metastasis and identify potential predictive markers, we analyzed gene-expression profiles of 34 vertical growth phase melanoma cases using cDNA microarrays. All patients had a minimum follow-up of 36 months. Twenty-one cases developed nodal metastatic disease and 13 did not. Comparison of gene expression profiling of metastatic and nonmetastatic melanoma cases identified 243 genes with a >2-fold differential expression ratio and a false discovery rate of <0.2 (206 up-regulated and 37 down-regulated). This set of genes included molecules involved in cell cycle and apoptosis regulation, epithelial-mesenchymal transition (EMT), signal transduction, nucleic acid binding and transcription, protein synthesis and degradation, metabolism, and a specific group of melanoma- and neural-related proteins. Validation of these expression data in an independent series of melanomas using tissue microarrays confirmed that the expression of a set of proteins included in the EMT group (N-cadherin, osteopontin, and SPARC/osteonectin) were significantly associated with metastasis development. Our results suggest that EMT-related genes contribute to the promotion of the metastatic phenotype in primary CMM by supporting specific adhesive, invasive, and migratory properties. These data give a better understanding of the biology of this aggressive tumor and may provide new prognostic and patient stratification markers in addition to potential therapeutic targets.

Collection

C2: Curated
CGP: Chemical and Genetic Perturbations

Source publication

Pubmed 17409456 Authors: Alonso SR,Tracey L,Ortiz P,Pérez-Gómez B,Palacios J,Pollán M,Linares J,Serrano S,Sáez-Castillo AI,Sánchez L,Pajares R,Sánchez-Aguilera A,Artiga MJ,Piris MA,Rodríguez-Peralto JL

Exact source

Table 3

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Source species

Homo sapiens

Contributed by

Jessica Robertson (MSigDB Team)

Source platform or
identifier namespace

HUMAN_GENE_SYMBOL

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The contents of this gene set are protected by copyright (c) 2004-2026 Broad Institute, Inc., Massachusetts Institute of Technology, and Regents of the University of California, subject to the terms and conditions of the Creative Commons Attribution 4.0 International License.

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