Terry Patrick Finn
Janssen Pharmaceutica
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Publication
Featured researches published by Terry Patrick Finn.
Journal of Pharmacology and Experimental Therapeutics | 2013
Mikhail Kalinichev; Mélanie Rouillier; Françoise Girard; Isabelle Royer-Urios; Bruno Bournique; Terry Patrick Finn; Delphine Charvin; Brice Campo; Emmanuel Le Poul; Vincent Mutel; Sonia Maria Poli; Stuart A. Neale; T.E. Salt; Robert Johannes Lütjens
Metabotropic glutamate receptor 7 (mGlu7) has been suggested to be a promising novel target for treatment of a range of disorders, including anxiety, post-traumatic stress disorder, depression, drug abuse, and schizophrenia. Here we characterized a potent and selective mGlu7 negative allosteric modulator (NAM) (+)-6-(2,4-dimethylphenyl)-2-ethyl-6,7-dihydrobenzo[d]oxazol-4(5H)-one (ADX71743). In vitro, Schild plot analysis and reversibility tests at the target confirmed the NAM properties of the compound and attenuation of l-(+)-2-amino-4-phosphonobutyric acid–induced synaptic depression confirmed activity at the native receptor. The pharmacokinetic analysis of ADX71743 in mice and rats revealed that it is bioavailable after s.c. administration and is brain penetrant (cerebrospinal fluid concentration/total plasma concentration ratio at Cmax = 5.3%). In vivo, ADX71743 (50, 100, 150 mg/kg, s.c.) caused no impairment of locomotor activity in rats and mice or activity on rotarod in mice. ADX71743 had an anxiolytic-like profile in the marble burying and elevated plus maze tests, dose-dependently reducing the number of buried marbles and increasing open arm exploration, respectively. Whereas ADX71743 caused a small reduction in amphetamine-induced hyperactivity in mice, it was inactive in the mouse 2,5-dimethoxy-4-iodoamphetamine–induced head twitch and the rat conditioned avoidance response tests. In addition, the compound was inactive in the mouse forced swim test. These data suggest that ADX71743 is a suitable compound to help unravel the physiologic role of mGlu7 and to better understand its implication in central nervous system diseases. Our in vivo tests using ADX71743, reported here, suggest that pharmacological inhibition of mGlu7 is a valid approach for developing novel pharmacotherapies to treat anxiety disorders, but may not be suitable for treatment of depression or psychosis.
ACS Chemical Neuroscience | 2010
José M. Cid; Guillaume Albert Jacques Duvey; Philippe Cluzeau; Vanthea Nhem; Karim Macary; Alexandre Raux; Nicolas Poirier; Jessica Muller; Christelle Bolea; Terry Patrick Finn; Sonia Poli; Mark Epping-Jordan; Emilie Chamelot; Francis Derouet; Françoise Girard; Gregor James Macdonald; Juan Antonio Vega; Ana Isabel de Lucas; Encarnación Matesanz; Hilde Lavreysen; María Lourdes Linares; Daniel Oehlrich; Julen Oyarzabal; Gary Tresadern; Andrés A. Trabanco; José Ignacio Andrés; Emmanuel Le Poul; Hassan Julien Imogai; Robert Johannes Lütjens; Jean-Philippe Rocher
A series of 1,5-disubstituted pyridones was identified as positive allosteric modulators (PAMs) of the metabotropic glutamate receptor 2 (mGluR2) via high throughput screening (HTS). Subsequent SAR exploration led to the identification of several compounds with improved in vitro activity. Lead compound 8 was further profiled and found to attenuate the increase in PCP induced locomotor activity in mice.
Journal of Medicinal Chemistry | 2014
José M. Cid; Gary Tresadern; Guillaume Albert Jacques Duvey; Robert Johannes Lütjens; Terry Patrick Finn; Jean-Philippe Rocher; Sonia Maria Poli; Juan Antonio Vega; Ana Isabel de Lucas; Encarnación Matesanz; María Lourdes Linares; José Ignacio Andrés; Jesús Alcázar; José Manuel Alonso; Gregor James Macdonald; Daniel Oehlrich; Hilde Lavreysen; Abdelah Ahnaou; Wilhelmus Drinkenburg; Claire Mackie; Stefan Pype; David Gallacher; Andrés A. Trabanco
We previously reported the discovery of 4-aryl-substituted pyridones with mGlu2 PAM activity starting from the HTS hit 5. In this article, we describe a different exploration from 5 that led to the discovery of a novel subseries of phenylpiperidine-substituted pyridones. The optimization strategy involved the introduction of different spacers between the pyridone core and the phenyl ring of 5. The fine tuning of metabolism and hERG followed by differentiation of advanced leads that were identified on the basis of PK profiles and in vivo potency converged on lead compound 36 (JNJ-40411813). Full in vitro and in vivo profiles indicate that 36 displayed an optimal interplay between potency, selectivity, favorable ADMET/PK and cardiovascular safety profile, and central EEG activity. Compound 36 has been investigated in the clinic for schizophrenia and anxious depression disorders.
Bioorganic & Medicinal Chemistry Letters | 2011
Andrés A. Trabanco; Guillaume Albert Jacques Duvey; José María Cid; Gregor James Macdonald; Philippe Cluzeau; Vanthea Nhem; Rocco Furnari; Nadia Behaj; Géraldine Poulain; Terry Patrick Finn; Hilde Lavreysen; Sonia Maria Poli; Alexandre Raux; Yves Thollon; Nicolas Poirier; David D’Addona; José Ignacio Andrés; Robert Johannes Lütjens; Emmanuel Le Poul; Hassan Julien Imogai; Jean-Philippe Rocher
A series of N-propyl-8-chloro-6-substituted isoquinolones was identified as positive allosteric modulators of metabotropic glutamate receptor 2 (mGluR2 PAM) via high throughput screening (HTS). The subsequent synthesis and initial SAR exploration that led to the identification of compound 28 is described.
MedChemComm | 2011
Andrés A. Trabanco; Guillaume Albert Jacques Duvey; José María Cid; Gregor James Macdonald; Philippe Cluzeau; Vanthea Nhem; Rocco Furnari; Nadia Behaj; Géraldine Poulain; Terry Patrick Finn; Sonia Maria Poli; Hilde Lavreysen; Alexandre Raux; Yves Thollon; Nicolas Poirier; David D'Addona; José Ignacio Andrés; Robert Johannes Lütjens; Emmanuel Le Poul; Hassan Julien Imogai; Jean-Philippe Rocher
A series of N-propyl-5-substituted isoquinolones was identified as positive allosteric modulators (PAM) of metabotropic glutamate receptor 2 (mGluR2) via high-throughput screening (HTS). The subsequent synthesis and preliminary SAR exploration that led to the identification of compound 20 are described.
Archive | 2005
Hassan Julien Imogai; Jose Maria Cid-Nunez; Guillaume Albert Jacques Duvey; Christelle Bolea; Vanthea Nhem; Terry Patrick Finn; Emmanuel Christian Le Poul; Jean-Philippe Rocher; Robert Johannes Lütjens
Archive | 2007
Hassan Julien Imogai; Jose Maria Cid-Nunez; Jose Ignacio Andres-Gil; Andrés Avelino Trabanco-Suárez; Julen Oyarzabal Santamarina; Frank Matthias Dautzenberg; Gregor James Macdonald; Shriley Elizabeth Pullan; Robert Johannes Lütjens; Guillaume Albert Jacques Duvey; Vanthea Nhem; Terry Patrick Finn; Gagik Melikyan
Archive | 2008
Jose Maria Cid-Nunez; Andrés Avelino Trabanco-Suárez; Gregor James Macdonald; Guillaume Albert Jacques Duvey; Robert Johannes Lütjens; Terry Patrick Finn
Archive | 2017
Andrés Avelino Trabanco-Suárez; Gregor James Macdonald; Guillaume Albert Jacques Duvey; Jose Maria Cid-Nunez; Robert Johannes Lütjens; Terry Patrick Finn
Archive | 2017
Andrés Avelino Trabanco-Suárez; Gregor James Macdonald; Guillaume Albert Jacques Duvey; Jose Maria Cid-Nunez; Robert Johannes Lütjens; Terry Patrick Finn
