A cyclopent-2-enecarbonyl group mimics proline at the P2 position of prolyl oligopeptidase inhibitors.

Elina M. Jarho,Jarkko I. Venäläinen,Juhani Huuskonen,Johannes A. M. Christiaans,J. Arturo García-Horsman,Markus M. Forsberg,Tomi Järvinen,Jukka Gynther,Pekka T. Männistö,Erik A.A. Wallén

A cyclopent-2-enecarbonyl group mimics proline at the P2 position of prolyl oligopeptidase inhibitors.

2004

Elina M. Jarho
Jarkko I. Venäläinen
Juhani Huuskonen
Johannes A. M. Christiaans
J. Arturo García-Horsman
Markus M. Forsberg
Tomi Järvinen
Jukka Gynther
Pekka T. Männistö
Erik A.A. Wallén

With the aim to replace the natural amino acid proline by a proline mimetic structure, a cyclopent-2-enecarbonyl moiety was studied at the P2 position of prolyl oligopeptidase (POP) inhibitors. The cyclopent-2-enecarbonyl moiety proved to be an excellent proline mimetic at the P2 position of POP inhibitors. The replacement is particularly useful when increased lipophilicity is needed.

Keywords:

Enzyme
Lipophilicity
Proline
Moiety
Organic chemistry
Oligopeptidase
Biochemistry
Amino acid
Chemistry
Enzyme inhibitor
Chemical synthesis
Stereochemistry

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