James Joseph Erdei

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Featured researches published by James Joseph Erdei.

Journal of Medicinal Chemistry | 2011

Michael S. Malamas; Yike Ni; James Joseph Erdei; Hans Stange; Rudolf Schindler; Hans-Joachim Lankau; Christian Grunwald; Kristi Fan; Kevin Parris; Barbara Langen; Ute Egerland; Thorsten Hage; Karen L. Marquis; Steve Grauer; Rachel Navarra; Radka Graf; Boyd L. Harrison; Albert Jean Robichaud; Thomas Kronbach; Menelas N. Pangalos; Norbert Hoefgen; Nicholas J. Brandon

The identification of highly potent and orally active phenylpyrazines for the inhibition of PDE10A is reported. The new analogues exhibit subnanomolar potency for PDE10A, demonstrate high selectivity against all other members of the PDE family, and show desired druglike properties. Employing structure-based drug design approaches, we methodically explored two key regions of the binding pocket of the PDE10A enzyme to alter the planarity of the parent compound 1 and optimize its affinity for PDE10A. Bulky substituents at the C9 position led to elimination of the mutagenicity of 1, while a crucial hydrogen bond interaction with Glu716 markedly enhanced its potency and selectivity. A systematic assessment of the ADME and PK properties of the new analogues led to druglike development candidates. One of the more potent compounds, 96, displayed an IC(50) for PDE10A of 0.7 nM and was active in predictive antipsychotic animal models.

Bioorganic & Medicinal Chemistry Letters | 2012

Michael S. Malamas; Hans Stange; Rudolf Schindler; Hans-Joachim Lankau; Christian Grunwald; Barbara Langen; Ute Egerland; Thorsten Hage; Yike Ni; James Joseph Erdei; Kristi Fan; Kevin Parris; Karen L. Marquis; Steve Grauer; Rachel Navarra; Radka Graf; Boyd L. Harrison; Albert J. Robichaud; Thomas Kronbach; Menelas N. Pangalos; Nicholas J. Brandon; Norbert Hoefgen

The identification of highly potent and orally active triazines for the inhibition of PDE10A is reported. The new analogs exhibit low-nanomolar potency for PDE10A, demonstrate high selectivity against all other members of the PDE family, and show desired drug-like properties. Employing structure-based drug design approaches, we investigated the selectivity of PDE10A inhibitors against other known PDE isoforms, by methodically exploring the various sub-regions of the PDE10A ligand binding pocket. A systematic assessment of the ADME and pharmacokinetic properties of the newly synthesized compounds has led to the design of drug-like candidates with good brain permeability and desirable drug kinetics (t(1/2), bioavailability, clearance). Compound 66 was highly potent for PDE10A (IC(50)=1.4 nM), demonstrated high selectivity (>200×) for the other PDEs, and was efficacious in animal models of psychoses; reversal of MK-801 induced hyperactivity (MED=0.1mg/kg) and conditioned avoidance responding (CAR; ID(50)=0.2 mg/kg).

Archive | 2005

Michael Sotirios Malamas; James Joseph Erdei; Iwan Gunawan; Ping Zhou; Yinfa Yan; Dominick Anthony Quagliato

Archive | 2005

Michael Sotirios Malamas; James Joseph Erdei; Iwan Gunawan; Keith Douglas Barnes; Matthew Robert Johnson; Yu Hui

Archive | 2006

Michael Sotirios Malamas; Iwan Gunawan; James Joseph Erdei; Pawel Wojciech Nowak; Joseph Raymond Stock; Yinfa Yan

Archive | 2006

Michael Sotirios Malamas; Ping Zhou; William Floyd Fobare; William Ronald Solvibile; Iwan Gunawan; James Joseph Erdei; Yinfa Yan; Patrick Michael Andrae; Dominick Anthony Quagliato

Archive | 2006