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Citation |
Mazaleyrat JP, Rage I, Xie J, Savrda J, Wakselman M. Tetrahedron Letters 1992; 33(31): 4453-4456. |
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Copyright |
(Copyright © 1992) |
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DOI |
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PMID |
unavailable |
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Abstract |
Coupling of (D,L)-baikiain methyl ester with Boc-(L)-phenylalanine, followed by saponification, idolactonization and aminolysis of the diastereoisomeric iodolactones by (L)-isoleucyl-(L)-valine methyl ester gave two diastereoisomeric peptides incorporating either a 3S-hydroxy-4S-iodo-(L)-pipecolic acid or a 3R-hydroxy-4R-iodo-(D)-pipecolic acid residue, which were separated by thin layer chromatography. Assignment of configuration was unambiguous when the synthesis was repeated with (L)-baikiain as starting material. All compounds exhibited conformational isomerism in their1H NMR spectra, attributed to the existence of boths-cis ands-trans configurations of the Phe-NR2 peptide bond. Acetylation of each of the two separated diastereoisomers gave Boc-(L)-Phe-3S-OAc-4S-I-(L)-Pip-(L)-Ile-(L)-Val-OMe and Boc-(L)-Phe-3R-OAc-4R-I-(D)-Pip-(L)-Ile-(L)-Val-OMe. N-deprotection and coupling of the former with Boc-(L)-Ser-(L)-Ala-(L)-Ala-OH by the DCC/HOBt method or stepwise elongation of the peptidic chain, gave Boc-(L)-Ser-(L)-Ala-(L)-Ala-(L)-Phe-3S-OAc-4S-I-(L)-Pip-(L)-Ile-(L)-Val-OMe. Dehydroiodination of this compound on treatment with DBU gave Boc-(L)-Ser-(L)-Ala-(L)-Ala-(L)-Phe-3S-OAc-Δ-4,5-(L)-Pip-(L)-Ile-(L)-Val-OMe, a potential "suicide substrate" of the HIV-1 protease. © 1992 Pergamon Press Ltd. Language: en |
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Keywords |
article; priority journal; thin layer chromatography; enzyme inhibitor; peptide; drug synthesis; antivirus agent; enantiomer; nuclear magnetic resonance; proteinase inhibitor |