1. Downregulation of lamin A by tumor suppressor AIMP3/p18 leads to a progeroid phenotype in mice
- Author
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Yousin Suh, Brian K. Kennedy, Gyuyoup Kim, Sunghoon Kim, Dae Gyu Kim, Eung Chil Choi, Young Sun Oh, and Bum Joon Park
- Subjects
Senescence ,Gene isoform ,Genetically modified mouse ,congenital, hereditary, and neonatal diseases and abnormalities ,Aging ,Progeria ,integumentary system ,Cell Biology ,Biology ,Progerin ,medicine.disease ,Molecular biology ,Phenotype ,Cell biology ,Downregulation and upregulation ,medicine ,Lamin - Abstract
Summary Although AIMP3 ⁄p18 is normally associated with the macromolecular tRNA synthetase complex, recent reports have revealed a new role of AIMP3 in tumor suppression. In this study, we generated a transgenic mouse that overexpresses AIMP3 and characterized the associated phenotype in vivo and in vitro. Surprisingly, the AIMP3 transgenic mouse exhibited a progeroid phenotype, and the cells that overexpressed AIMP3 showed accelerated senescence and defects in nuclear morphology. We found that overexpression of AIMP3 resulted in proteasomedependent degradation of mature lamin A, but not of lamin C, prelamin A, or progerin. The resulting imbalance in the protein levels of lamin A isoforms, namely altered stoichiometry of prelamin A and progerin to lamin A, appeared to be responsible for a phenotype that resembled progeria. An increase in the level of endogenous AIMP3 has been observed in aged human tissues and cells. The findings in this report suggest that AIMP3 is a specific regulator of mature lamin A and imply that enhanced expression of AIMP3 might be a factor driving cellular and ⁄or organismal aging.
- Published
- 2010