Mouse Gene Set: GALIE_TUMOR_STEMNESS_GENES

For the Human gene set with the same name, see GALIE_TUMOR_STEMNESS_GENES

Standard name GALIE_TUMOR_STEMNESS_GENES
Systematic name MM546
Brief description Stemness-related genes changed in A17 carcinomas (MTC, mesenchymal tumor cells) compared with the mesenchymal stem cells (MSC).
Full description or abstract Tumor microenvironment in carcinomas recruits mesenchymal cells with an abnormal proangiogenic and invasive phenotype. It is not clear whether mesenchymal tumor cells (MTCs) derive from the activation of mature fibroblasts or from their stem cell precursors. However, stromal cell activation in tumors resembles in several aspects the mesenchymal rearrangement which normally occurs during reparative processes such as wound healing. Mesenchymal stem cells (MSCs) play a crucial role in developmental and reparative processes and have extraordinary proangiogenic potential, on the basis of which they are thought to show great promise for the treatment of ischemic disorders. Here, we show that MTCs have proangiogenic potential and that they share the transcriptional expression of the best-known proangiogenic factors with MSCs. We also found that MTCs and MSCs have the same molecular signature for stemness-related genes, and that when co-implanted with cancer cells in syngeneic animals MSCs determine early tumor appearance, probably by favoring the angiogenic switch. Our data (1) reveal crucial aspects of the proangiogenic phenotype of MTCs, (2) strongly suggest their stem origin and (3) signal the risk of therapeutic use of MSCs in tumor-promoting conditions.
Collection M2: Curated
      CGP: Chemical and Genetic Perturbations
Source publication Pubmed 17998939   Authors: Galič M,Konstantinidou G,Peroni D,Scambi I,Marchini C,Lisi V,Krampera M,Magnani P,Merigo F,Montani M,Boschi F,Marzola P,Orrų R,Farace P,Sbarbati A,Amici A
Exact source Table 4
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Source species Mus musculus
Contributed by Jessica Robertson (MSigDB Team)
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Mouse_RefSeq
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Version history 2022.1.Mm: First Introduced.

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