| Literature DB >> 15099520 |
Brigitte Goulet1, Amos Baruch, Nam-Sung Moon, Madeleine Poirier, Laurent L Sansregret, Ann Erickson, Matthew Bogyo, Alain Nepveu.
Abstract
The subclass of cysteine proteases termed lysosomal cathepsins has long been thought to be primarily involved in end-stage protein breakdown within lysosomal compartments. Furthermore, few specific protein substrates for these proteases have been identified. We show here that cathepsin L functions in the regulation of cell cycle progression through proteolytic processing of the CDP/Cux transcription factor. CDP/Cux processing in situ was increased following ectopic expression of cathepsin L but was reduced in Cat L(-/-) cells. Furthermore, catalytically active cathepsin L was localized to the nucleus during the G1-S transition as detected by immunofluorescence imaging and labeling using activity-based probes. Trafficking of cathepsin L to the nucleus is accomplished through a mechanism involving translation initiation at downstream AUG sites and the synthesis of proteases that are devoid of a signal peptide. Overall, these results uncover an as yet unsuspected role for cysteine proteases in the control of cell cycle progression.Entities:
Mesh:
Substances:
Year: 2004 PMID: 15099520 DOI: 10.1016/s1097-2765(04)00209-6
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970