Alexey B. Dyatkin
Johnson & Johnson Pharmaceutical Research and Development
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Publication
Featured researches published by Alexey B. Dyatkin.
Bioorganic & Medicinal Chemistry Letters | 2012
Henry J. Breslin; Craig J. Diamond; Robert W. Kavash; Chaozhong Cai; Alexey B. Dyatkin; Tamara A. Miskowski; Sui-Po Zhang; Paul R. Wade; Pamela J. Hornby; Wei He
A small set of acyclic analogs 5 were prepared to explore their structure-activity relationships (SARs) relative to heterocyclic core, opioid receptor (OR) agonists 4. Compound 5l was found to have very favorable OR binding affinities at the δ and μ ORs (r K(i) δ=1.3 nM; r K(i) μ=0.9 nM; h K(i) μ=1.7 nM), with less affinity for the κ OR (gp K(i) κ=55 nM). The OR functional profile for 5l varied from the previously described dual δ/μ OR agonists 4, with 5l being a potent, mixed dual δ OR antagonist/μ OR agonist [δ IC(50)=89 nM (HVD); μ EC(50)=1 nM (GPI); κ EC(50)=1.6 μM (GPC)]. Compound 5l has progressed through a clinical Phase II Proof of Concept study on 800 patients suffering from diarrhea-predominant Irritable Bowel Syndrome (IBS-d). This Phase II study was recently completed successfully, with 5l demonstrating statistically significant efficacy over placebo.
Bioorganic & Medicinal Chemistry Letters | 2008
Yong Gong; J. Kent Barbay; Edward S. Kimball; Rosemary J. Santulli; M. Carolyn Fisher; Alexey B. Dyatkin; Tamara A. Miskowski; Pamela J. Hornby; Wei He
Structural modification and cellular adhesion inhibition activities of pyridazinone-substituted phenylalanine amide alpha(4) integrin antagonists are described. Functionality requirements for the arylamide moiety and the carboxylic acid group were demonstrated. The study also revealed novel structure-activity relationships (SAR) for arylated pyridazinones. A correlation between bioavailability and permeability was also explored. A selected compound showed effectiveness in a mouse leukocytosis study.
Bioorganic & Medicinal Chemistry Letters | 2002
Alexey B. Dyatkin; William J. Hoekstra; Dennis J. Hlasta; Patricia Andrade-Gordon; Lawrence de Garavilla; Keith T. Demarest; Joseph Gunnet; William Hageman; Richard Look; Bruce E. Maryanoff
The synthesis and biological testing of a novel series of nonpeptide vasopressin receptor antagonists, containing a bridged bicyclic nucleus, are reported. Variation of substituents (R(1)-R(3)) in general formula 3, and the configuration of the stereocenter, resulted in potent V(2)-selective (e.g., 5) and balanced dual V(1a)/V(2) (e.g., 10) compounds. Data from receptor binding, cell-based functional, and in vivo assays are presented [corrected]
Bioorganic & Medicinal Chemistry Letters | 2009
Janet L. Ralbovsky; Joseph Lisko; Jeffrey M. Palmer; John R. Mabus; Kristen M. Chevalier; Mark Schulz; Alexey B. Dyatkin; Tamara A. Miskowski; Steven J. Coats; Pamela J. Hornby; Wei He
A series of guanidine triazinediones were identified as potent PK1 receptor antagonists. A compound in this series inhibited the PK1 invoked prosecretory response in rat ileum tissue.
Chirality | 2002
Alexey B. Dyatkin; Teresa B. Freedman; Xiaolin Cao; Rina K. Dukor; Bruce E. Maryanoff; Cynthia A. Maryanoff; Jay M. Matthews; Rekha D. Shah; Laurence A. Nafie
Archive | 2001
Alexey B. Dyatkin; Bruce E. Maryanoff; William J. Hoekstra; Wei He; William A. Kinney
Archive | 2006
Steven J. Coats; Alexey B. Dyatkin; Wei He; Joseph Lisko; Tamara A. Miskowski; Janet L. Ralbovsky; Mark Schulz
Archive | 2005
Kent Barbay; Alexey B. Dyatkin; Yong Gong; Wei He; Tamara A. Miskowski
Archive | 1999
William J. Hoekstra; Alexey B. Dyatkin; Bruce E. Maryanoff; Jay M. Matthews
Tetrahedron-asymmetry | 2004
Jay M. Matthews; Alexey B. Dyatkin; Mary Evangelisto; Diane A. Gauthier; Leonard R. Hecker; William J. Hoekstra; Fuqiang Liu; Brenda L. Poulter; Kirk L. Sorgi; Bruce E. Maryanoff
