| Literature DB >> 16902412 |
Weiguang Zhong1, Songyan Mao, Scott Tobis, Ekaterini Angelis, Maria C Jordan, Kenneth P Roos, Michael C Fishbein, Ignacio Moreno de Alborán, W Robb MacLellan.
Abstract
c-Myc (Myc) is highly expressed in developing embryos where it regulates body size by controlling proliferation but not cell size. However, Myc is also induced in many postmitotic tissues, including adult myocardium, in response to stress where the predominant form of growth is an increase in cell size (hypertrophy) and not number. The function of Myc induction in this setting is unproven. Therefore, to explore Myc's role in hypertrophic growth, we created mice where Myc can be inducibly inactivated, specifically in adult myocardium. Myc-deficient hearts demonstrated attenuated stress-induced hypertrophic growth, secondary to a reduction in cell growth of individual myocytes. To explore the dependence of Myc-induced cell growth on CycD2, we created bigenic mice where Myc can be selectively activated in CycD2-null adult myocardium. Myc-dependent hypertrophic growth and cell cycle reentry is blocked in CycD2-deficient hearts. However, in contrast to Myc-induced DNA synthesis, hypertrophic growth is independent of CycD2-induced Cdk2 activity. These data suggest that Myc is required for a normal hypertrophic response and that its growth-promoting effects are also mediated through a CycD2-dependent pathway.Entities:
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Year: 2006 PMID: 16902412 PMCID: PMC1553193 DOI: 10.1038/sj.emboj.7601252
Source DB: PubMed Journal: EMBO J ISSN: 0261-4189 Impact factor: 11.598