AI Article Synopsis
- Soft tissue tumors can range from benign to highly aggressive and metastatic, and understanding the molecular differences among them is crucial for treatment decisions.
- Researchers analyzed 102 tumor samples and identified 12 key genes that exhibited opposite expression patterns in locally aggressive versus metastatic tumors.
- These genes are linked to interactions between cells and their environment, as well as cell growth, which could improve tumor classification, diagnosis, and lead to new drug development.
Article Abstract
Soft tissue tumors represent a group of neoplasia with different histologic and biological presentations varying from benign, locally confined to very aggressive and metastatic tumors. The molecular mechanisms responsible for such differences are still unknown. The understanding of these molecular alterations mechanism will be critical to discriminate patients who need systemic treatment from those that can be treated only locally and could also guide the development of new drugs' against this tumors. Using 102 tumor samples representing a large spectrum of these tumors, we performed expression profiling and defined differentially expression genes that are likely to be involved in tumors that are locally aggressive and in tumors with metastatic potential. We described a set of 12 genes (SNRPD3, MEGF9, SPTAN-1, AFAP1L2, ENDOD1, SERPIN5, ZWINTAS, TOP2A, UBE2C, ABCF1, MCM2, and ARL6IP5) showing opposite expression when these two conditions were compared. These genes are mainly related to cell-cell and cell-extracellular matrix interactions and cell proliferation and might represent helpful tools for a more precise classification and diagnosis as well as potential drug targets.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2822450 | PMC |
| http://dx.doi.org/10.1593/tlo.09166 | DOI Listing |
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