| Literature DB >> 33908663 |
Christian Fernandez1, Andres Burgos1, Diego Morales1, Roberto Rosales-Rojas2, Javiera Canelo1, Ariela Vergara-Jaque2,3, Gabriel Viliod Vieira4, Rodrigo Alberto Alves da Silva4, Katiuchia Uzzun Sales4, Michael J Conboy5, Eun Ji Bae6, Kang-Sik Park6, Vicente A Torres7, Mauricio Garrido8, Oscar Cerda1,3,9, Irina M Conboy5, Mónica Cáceres1,3,9.
Abstract
Aging is a gradual biological process characterized by a decrease in cellular and organism functions. Aging-related processes involve changes in the expression and activity of several proteins. Here, we identified the transmembrane protease serine 11a (TMPRSS11a) as a new age-specific protein that plays an important role in skin wound healing. TMPRSS11a levels increased with age in rodent and human skin and gingival samples. Strikingly, overexpression of TMPRSS11a decreased cell migration and spreading, and inducing cellular senescence. Mass spectrometry, bioinformatics, and functional analyses revealed that TMPRSS11a interacts with integrin β1 through an RGD sequence contained within the C-terminal domain and that this motif was relevant for cell migration. Moreover, TMPRSS11a was associated with cellular senescence, as shown by overexpression and downregulation experiments. In agreement with tissue-specific expression of TMPRSS11a, shRNA-mediated downregulation of this protein improved wound healing in the skin, but not in the skeletal muscle of old mice, where TMPRSS11a is undetectable. Collectively, these findings indicate that TMPRSS11a is a tissue-specific factor relevant for wound healing, which becomes elevated with aging, promoting cellular senescence and inhibiting cell migration and skin repair.Entities:
Keywords: RGD motif; aging; beta1 integrin; cell migration
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Year: 2021 PMID: 33908663 DOI: 10.1096/fj.202002253RRR
Source DB: PubMed Journal: FASEB J ISSN: 0892-6638 Impact factor: 5.191