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      Global Gene Expression Profiling Of Human Pleural Mesotheliomas: Identification of Matrix Metalloproteinase 14 (MMP-14) as Potential Tumour Target

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          Abstract

          Background

          The goal of our study was to molecularly dissect mesothelioma tumour pathways by mean of microarray technologies in order to identify new tumour biomarkers that could be used as early diagnostic markers and possibly as specific molecular therapeutic targets.

          Methodology

          We performed Affymetrix HGU133A plus 2.0 microarray analysis, containing probes for about 39,000 human transcripts, comparing 9 human pleural mesotheliomas with 4 normal pleural specimens. Stringent statistical feature selection detected a set of differentially expressed genes that have been further evaluated to identify potential biomarkers to be used in early diagnostics. Selected genes were confirmed by RT-PCR. As reported by other mesothelioma profiling studies, most of genes are involved in G2/M transition. Our list contains several genes previously described as prognostic classifier. Furthermore, we found novel genes, never associated before to mesotheliom that could be involved in tumour progression. Notable is the identification of MMP-14, a member of matrix metalloproteinase family. In a cohort of 70 mesothelioma patients, we found by a multivariate Cox regression analysis, that the only parameter influencing overall survival was expression of MMP14. The calculated relative risk of death in MM patients with low MMP14 expression was significantly lower than patients with high MMp14 expression (P = 0.002).

          Conclusions

          Based on the results provided, this molecule could be viewed as a new and effective therapeutic target to test for the cure of mesothelioma.

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          Most cited references64

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          Cancer genes and the pathways they control.

          Bert Vogelstein, Kenneth W. Kinzler (2004)
          The revolution in cancer research can be summed up in a single sentence: cancer is, in essence, a genetic disease. In the last decade, many important genes responsible for the genesis of various cancers have been discovered, their mutations precisely identified, and the pathways through which they act characterized. The purposes of this review are to highlight examples of progress in these areas, indicate where knowledge is scarce and point out fertile grounds for future investigation.
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            Tumour microenvironment - opinion: validating matrix metalloproteinases as drug targets and anti-targets for cancer therapy.

            Christopher Overall, Oded Kleifeld (2006)
            The matrix metalloproteinases (MMPs) mediate homeostasis of the extracellular environment. They have multiple signalling activities that are commonly altered during tumorigenesis and that might serve as intervention points for anticancer drugs. However, there are many criteria to consider in validating MMPs as drug targets and for the development of MMP inhibitors. The inhibition of some MMPs could have pro-tumorigenic effects (making them anti-targets), counterbalancing the benefits of target inhibition. These effects might partially account for the failure of MMP inhibitors in clinical trials. What are the major challenges in MMP target validation and MMP-inhibitor-drug development?
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              ERK promotes tumorigenesis by inhibiting FOXO3a via MDM2-mediated degradation.

              Jer-Yen Yang, Cong Zong, Weiya Xia (2008)
              The RAS-ERK pathway is known to play a pivotal role in differentiation, proliferation and tumour progression. Here, we show that Erk downregulates Forkhead box O 3a (FOXO3a) by directly interacting with and phosphorylating FOXO3a at Ser 294, Ser 344 and Ser 425, which consequently promotes cell proliferation and tumorigenesis. The ERK-phosphorylated FOXO3a degrades via an MDM2-mediated ubiquitin-proteasome pathway. However, the non-phosphorylated FOXO3a mutant is resistant to the interaction and degradation by murine double minute 2 (MDM2), thereby resulting in a strong inhibition of cell proliferation and tumorigenicity. Taken together, our study elucidates a novel pathway in cell growth and tumorigenesis through negative regulation of FOXO3a by RAS-ERK and MDM2.
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                Author and article information

                Contributors
                : Role: Editor
                Journal
                Journal ID (nlm-ta): PLoS One
                Journal ID (publisher-id): plos
                Journal ID (pmc): plosone
                Title: PLoS ONE
                Publisher: Public Library of Science (San Francisco, USA )
                ISSN (Electronic): 1932-6203
                Publication date Collection: 2009
                Publication date (Electronic): 15 September 2009
                Volume: 4
                Issue: 9
                Electronic Location Identifier: e7016
                Affiliations
                [1 ]Gene Expression Core - Human Molecular Genetics Laboratory, Institute of Genetics and Biophysics, Naples, Italy
                [2 ]Bioinformatics and Genomics Unit, Department of Clinical and Biological Science, University of Turin, Turin, Italy
                [3 ]Department of Thoracic Surgery, Second University of Naples, Naples, Italy
                [4 ]Department of Biochemistry, Sect. Pathology, Second University of Naples, Naples, Italy
                [5 ]Campus BioMedico University, Section of Oncology, Rome, Italy
                [6 ]SAFU Department, CRS, Regina Elena Cancer Institute, Rome, Italy
                [7 ]Department of Experimental Medicine, Second University of Naples, Naples, Italy
                [8 ]Campania Regional Operating Center (COR) of the National Mesothelioma Registry (ReNaM) - Department of Experimental Medicine, Second University of Naples, Naples, Italy
                [9 ]Department of Thoracic Surgery, Regina Elena Cancer Institute, Rome, Italy
                Oregon Health & Science University, United States of America
                Author notes

                Conceived and designed the experiments: SC RAC AB MM. Performed the experiments: SC PM RM GC. Analyzed the data: SC RAC MS BV GV SF SM RP FF AB. Contributed reagents/materials/analysis tools: MS GC GV RP FF. Wrote the paper: SC RAC AB MM.

                Article
                Publisher ID: 09-PONE-RA-09802R2
                DOI: 10.1371/journal.pone.0007016
                PMC ID: 2737627
                PubMed ID: 19753302
                SO-VID: 82badd48-d5ca-4985-b2ba-9fc733e98d58
                Copyright © Crispi et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
                History
                Date received : 16 April 2009
                Date accepted : 29 July 2009
                Page count
                Pages: 13
                Categories
                Subject: Research Article
                Subject: Computational Biology/Genomics
                Subject: Computational Biology/Transcriptional Regulation
                Subject: Genetics and Genomics/Cancer Genetics
                Subject: Genetics and Genomics/Gene Expression
                Subject: Respiratory Medicine/Pleural Diseases, including Mesothelioma

                ScienceOpen disciplines: Uncategorized
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                ScienceOpen disciplines: Uncategorized

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