Title of article
Global Sequencing of Proteolytic Cleavage Sites in Apoptosis by Specific Labeling of Protein N Termini
Author/Authors
Sami Mahrus، نويسنده , , Jonathan C. Trinidad، نويسنده , , David T. Barkan، نويسنده , , Andrej Sali، نويسنده , , Alma L. Burlingame، نويسنده , , James A. Wells، نويسنده ,
Issue Information
هفته نامه با شماره پیاپی سال 2008
Pages
11
From page
866
To page
876
Abstract
The nearly 600 proteases in the human genome regulate a diversity of biological processes, including programmed cell death. Comprehensive characterization of protease signaling in complex biological samples is limited by available proteomic methods. We have developed a general approach for global identification of proteolytic cleavage sites using an engineered enzyme to selectively biotinylate free protein N termini for positive enrichment of corresponding N-terminal peptides. Using this method to study apoptosis, we have sequenced 333 caspase-like cleavage sites distributed among 292 protein substrates. These sites are generally not predicted by in vitro caspase substrate specificity but can be used to predict other physiological caspase cleavage sites. Structural bioinformatic studies show that caspase cleavage sites often appear in surface-accessible loops and even occasionally in helical regions. Strikingly, we also find that a disproportionate number of caspase substrates physically interact, suggesting that these dimeric proteases target protein complexes and networks to elicit apoptosis.
Journal title
CELL
Serial Year
2008
Journal title
CELL
Record number
1019407
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