Person: Vujic, Ana
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Publication Structural basis for potency differences between GDF8 and GDF11
(BioMed Central, 2017) Walker, Ryan G.; Czepnik, Magdalena; Goebel, Erich J.; McCoy, Jason C.; Vujic, Ana; Cho, Miook; Oh, Juhyun; Aykul, Senem; Walton, Kelly L.; Schang, Gauthier; Bernard, Daniel J.; Hinck, Andrew P.; Harrison, Craig A.; Martinez-Hackert, Erik; Wagers, Amy; Lee, Richard; Thompson, Thomas B.Background: Growth/differentiation factor 8 (GDF8) and GDF11 are two highly similar members of the transforming growth factor β (TGFβ) family. While GDF8 has been recognized as a negative regulator of muscle growth and differentiation, there are conflicting studies on the function of GDF11 and whether GDF11 has beneficial effects on age-related dysfunction. To address whether GDF8 and GDF11 are functionally identical, we compared their signaling and structural properties. Results: Here we show that, despite their high similarity, GDF11 is a more potent activator of SMAD2/3 and signals more effectively through the type I activin-like receptor kinase receptors ALK4/5/7 than GDF8. Resolution of the GDF11:FS288 complex, apo-GDF8, and apo-GDF11 crystal structures reveals unique properties of both ligands, specifically in the type I receptor binding site. Lastly, substitution of GDF11 residues into GDF8 confers enhanced activity to GDF8. Conclusions: These studies identify distinctive structural features of GDF11 that enhance its potency, relative to GDF8; however, the biological consequences of these differences remain to be determined. Electronic supplementary material The online version of this article (doi:10.1186/s12915-017-0350-1) contains supplementary material, which is available to authorized users.
Publication Exercise induces new cardiomyocyte generation in the adult mammalian heart
(Nature Publishing Group UK, 2018) Vujic, Ana; Lerchenmüller, Carolin; Wu, Ting-Di; Guillermier, Christelle; Rabolli, Charles P.; Gonzalez, Emilia; Senyo, Samuel E.; Liu, Xiaojun; Guerquin-Kern, Jean-Luc; Steinhauser, Matthew; Lee, Richard; Rosenzweig, AnthonyLoss of cardiomyocytes is a major cause of heart failure, and while the adult heart has a limited capacity for cardiomyogenesis, little is known about what regulates this ability or whether it can be effectively harnessed. Here we show that 8 weeks of running exercise increase birth of new cardiomyocytes in adult mice (~4.6-fold). New cardiomyocytes are identified based on incorporation of 15N-thymidine by multi-isotope imaging mass spectrometry (MIMS) and on being mononucleate/diploid. Furthermore, we demonstrate that exercise after myocardial infarction induces a robust cardiomyogenic response in an extended border zone of the infarcted area. Inhibition of miR-222, a microRNA increased by exercise in both animal models and humans, completely blocks the cardiomyogenic exercise response. These findings demonstrate that cardiomyogenesis can be activated by exercise in the normal and injured adult mouse heart and suggest that stimulation of endogenous cardiomyocyte generation could contribute to the benefits of exercise.