Novel Apoptotic Mediators Identified by Conservation of Vertebrate Caspase Targets
Novel Apoptotic Mediators Identified by Conservation of Vertebrate Caspase Targets
Caspases are proteases conserved throughout Metazoans and responsible for initiating and executing the apoptotic program. Currently, there are over 1800 known apoptotic caspase substrates, many of them known regulators of cell proliferation and death, which makes them attractive therapeutic targets. However, most caspase substrates are by-standers, and identifying novel apoptotic mediators amongst all caspase substrates remains an unmet need. Here, we conducted an in silico search for significant apoptotic caspase targets across different species within the Vertebrata subphylum, using different criteria of conservation combined with structural features of cleavage sites. We observed that P1 aspartate is highly conserved while the cleavage sites are extensively variable and found that cleavage sites are located primarily in coiled regions composed of hydrophilic amino acids. Using the combination of these criteria, we determined the final list of the 107 most relevant caspase substrates including 30 novel targets previously unknown for their role in apoptosis and cancer. These newly identified substrates can be potential regulators of apoptosis and candidates for anti-tumor therapy.
- Keldysh Institute of Applied Mathematics Russian Federation
- Department of Biological Sciences Russian Federation
- Skolkovo Institute of Science and Technology Russian Federation
- Russian Academy of Sciences Russian Federation
- Institute of Theoretical and Experimental Biophysics Russian Federation
Proteome, Apoptosis, N-degron pathway, cleavage site, Microbiology, Article, Protein Structure, Secondary, Neoplasms, evolution, Animals, Humans, Conserved Sequence, Aspartic Acid, apoptosis, conservation, regulation, QR1-502, caspases, Caspases, Proteolysis, Vertebrates, Hydrophobic and Hydrophilic Interactions
Proteome, Apoptosis, N-degron pathway, cleavage site, Microbiology, Article, Protein Structure, Secondary, Neoplasms, evolution, Animals, Humans, Conserved Sequence, Aspartic Acid, apoptosis, conservation, regulation, QR1-502, caspases, Caspases, Proteolysis, Vertebrates, Hydrophobic and Hydrophilic Interactions
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