P3 optimization of functional potency, in vivo efficacy and oral bioavailability in 3-aminopyrazinone thrombin inhibitors bearing non-charged groups at the P1 position

Richard C.A. Isaacs,Christina L. Newton,Kellie J. Cutrona,Swati P. Mercer,Bruce D. Dorsey,Colleen McDonough,Jacquelynn J. Cook,Julie A. Krueger,S. Dale Lewis,Bobby J. Lucas,Elizabeth A. Lyle,Joseph J. Lynch,Cynthia Miller-Stein,Maria T. Michener,Audrey A. Wallace,Rebecca B. White,Bradley K. Wong

P3 optimization of functional potency, in vivo efficacy and oral bioavailability in 3-aminopyrazinone thrombin inhibitors bearing non-charged groups at the P1 position

2011

Richard C.A. Isaacs
Christina L. Newton
Kellie J. Cutrona
Swati P. Mercer
Bruce D. Dorsey
Colleen McDonough
Jacquelynn J. Cook
Julie A. Krueger
S. Dale Lewis
Bobby J. Lucas
Elizabeth A. Lyle
Joseph J. Lynch
Cynthia Miller-Stein
Maria T. Michener
Audrey A. Wallace
Rebecca B. White
Bradley K. Wong

Although the S3 pocket of the thrombin active site is lined with lipophilic amino acid residues, the accommodation of polarity within the lipophilic P3 moiety of small molecule inhibitors is possible provided that the polar functionality is capable of pointing away from the binding pocket outwards toward solvent while simultaneously allowing the lipophilic portion of the P3 ligand to interact with the S3 amino acid residues. Manipulation of this motif provided the means to effect optimization of functional potency, in vivo antithrombotic efficacy and oral bioavailability in a series of 3-aminopyrazinone thrombin inhibitors which contained non-charged groups at the P1 position.

Keywords:

Small molecule
Moiety
Thrombin
Organic chemistry
Discovery and development of direct thrombin inhibitors
Bioavailability
Amino acid
Stereochemistry
In vivo
Active site
Biochemistry
Chemistry
Enzyme inhibitor

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