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Literature summary extracted from
- Labeling and protecting N-terminal protein positions by beta-peptidyl aminopeptidase-catalyzed attachment of beta-amino-acid residues - insulin as a first example (2018), Helv. Chim. Acta, 101, e1700259 .
No PubMed abstract available
Application
| EC Number | Application | Comment | Organism |
|---|---|---|---|
| 3.4.11.25 | synthesis | BapA catalyzes reversible protein acylation at the N-terminus. The selective modification can also be applied for protein labeling and tagging and should be generally useful, also to protect peptides and proteins from attack by common aminopeptidase | Sphingosinicella xenopeptidilytica |
Organism
| EC Number | Organism | UniProt | Comment | Textmining |
|---|---|---|---|---|
| 3.4.11.25 | Sphingosinicella xenopeptidilytica | Q52VH2 | - |
- |
Substrates and Products (Substrate)
| EC Number | Substrates | Comment Substrates | Organism | Products | Comment (Products) | Rev. | Reac. |
|---|---|---|---|---|---|---|---|
| 3.4.11.25 | insulin + rac-3-aminobutanamide | enatioselectivity for beta-alanine is more than 300:1 | Sphingosinicella xenopeptidilytica | ? | - |
r |  |
Synonyms
| EC Number | Synonyms | Comment | Organism |
|---|---|---|---|
| 3.4.11.25 | BapA | - |
Sphingosinicella xenopeptidilytica |
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Release 2023.1 (January 2023)
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