Ketomethylureas. A New Class of Angiotensin Converting Enzyme Inhibitors

Sesha I Natarajan,Eric M. Gordon,Emily F. Sabo,Jollie D. Godfrey,Harold N. Weller,Jelka Pluscec,M.B. Rom,J. Engebrecht,David W. Cushman,Jack M. DeForrest,James R. Powell

Ketomethylureas. A New Class of Angiotensin Converting Enzyme Inhibitors

1988

Sesha I Natarajan
Eric M. Gordon
Emily F. Sabo
Jollie D. Godfrey
Harold N. Weller
Jelka Pluscec
M.B. Rom
J. Engebrecht
David W. Cushman
Jack M. DeForrest
James R. Powell

AbstractThe design rationale for a new series of tripeptide derived angiotensin converting enzyme (ACE) inhibitors, which we term “ketomethylureas”, is described. Analogs of tripeptide substrates (i.e. N-benzoyl-Phe-Ala-Pro) in which the nitrogen atom of the scissile amide bond and the adjacent asymmetric carbon atom of the penultimate amino acid residue are formally transposed give rise to this novel class of inhibitors. The most potent ketomethylureas inhibit ACE wtih I50 values in the nM range.

Keywords:

Organic chemistry
Nitrogen
Biochemistry
Amino acid
Chemistry
Tripeptide
Asymmetric carbon
Peptide bond
Angiotensin-converting enzyme
amino acid residue
Stereochemistry
nitrogen atom

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