AI Article Synopsis
- * Napsin A is weakly inhibited by a polypeptide from Ascaris lumbricoides but strongly inhibited by isovaleryl and lactoyl-pepstatins.
- * Synthetic inhibitors with specific dipeptide analogues reveal that napsin A's active site is distinct from other human aspartic proteinases.
Article Abstract
The newly-discovered human aspartic proteinase, napsin A was not susceptible to protein inhibitors from potato, squash or yeast but was weakly inhibited by the 17 kDa polypeptide from Ascaris lumbricoides and potently by isovaleryl and lactoyl-pepstatins. A series of synthetic inhibitors was also investigated which contained in the P(1)-P(1)' positions the dipeptide analogue statine or its phenylalanine or cyclohexylalanine homologues and in which the residues occupying P(4)-P(3)' were varied systematically. On this basis, the active site of napsin A can be readily distinguished from other human aspartic proteinases.
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| http://dx.doi.org/10.2174/0929866033408237 | DOI Listing |
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