Title of article
Proteasome-Mediated Degradation of p21 via N-Terminal Ubiquitinylation
Author/Authors
Joanna Bloom، نويسنده , , Virginia Amador، نويسنده , , Francesca Bartolini، نويسنده , , George DeMartino، نويسنده , , Michele Pagano، نويسنده ,
Issue Information
هفته نامه با شماره پیاپی سال 2003
Pages
12
From page
71
To page
82
Abstract
We examined the mechanism responsible for the degradation of p21, a negative regulator of the cell division cycle. We found that p21 proteolysis requires functional ubiquitin and Nedd8 systems. Ubiquitinylated forms of p21 and p21(K0), a p21 mutant missing all lysines, are detected in vivo and in vitro, showing that the presence of lysines is dispensable for p21 ubiquitinylation. Instead, the free amino group of the N-terminal methionine of p21 is a site for ubiquitinylation in vivo. Although wild-type p21 is more abundantly ubiquitinylated than p21(K0) mutant due to the presence of internal lysine residues, their rates of proteolysis are indistinguishable. These results demonstrate that proteasomal degradation of p21 is regulated by the ubiquitin pathway and suggest that the site of the ubiquitin chain is critical in making p21 a competent substrate for the proteasome.
Journal title
CELL
Serial Year
2003
Journal title
CELL
Record number
1018376
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