Florence Jovic
Neurocrine Biosciences
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Publication
Featured researches published by Florence Jovic.
Journal of Medicinal Chemistry | 2009
Wilna J. Moree; Bin-Feng Li; Florence Jovic; Timothy Coon; Jinghua Yu; Raymond S. Gross; Fabio C. Tucci; Dragan Marinkovic; Said Zamani-Kord; Siobhan Malany; Margaret J. Bradbury; Lisa M. Hernandez; Zhihong O’Brien; Jianyun Wen; Hua Wang; Samuel R.J. Hoare; Robert E. Petroski; Aida Sacaan; Ajay Madan; Paul D. Crowe; Graham Beaton
Analogues of the known H(1)-antihistamine R-dimethindene were profiled as potential agents for the treatment of insomnia. Several highly selective compounds were efficacious in rodent sleep models. On the basis of overall profile, indene 1d and benzothiophene 2a had pharmacokinetic properties suitable for evaluation in night time dosing. Compound 2a did not show an in vivo cardiovascular effect from weak hERG channel inhibition.
Bioorganic & Medicinal Chemistry Letters | 2008
Chen Chen; Brian Dyck; Beth A. Fleck; Alan C. Foster; Jonathan Grey; Florence Jovic; Michael Mesleh; Kasey Phan; Junko Tamiya; Troy Vickers; Mingzhu Zhang
Derivatives of milnacipran were synthesized and studied as monoamine transporter inhibitors. Potent analogs were discovered at NET (9k) and at both NET and SERT (9s and 9u). A pharmacophore model was established based on the conformational analysis of milnacipran in aqueous solution using NMR techniques and was consistent with the SAR results.
Bioorganic & Medicinal Chemistry Letters | 2008
Junko Tamiya; Brian Dyck; Mingzhu Zhang; Kasey Phan; Beth A. Fleck; Anna Aparicio; Florence Jovic; Joe A. Tran; Troy Vickers; Jonathan Grey; Alan C. Foster; Chen Chen
A series of milnacipran analogs were synthesized and studied as monoamine transporter inhibitors, and several potent compounds with moderate lipophilicity were identified from the 1S,2R-isomers. Thus, 15l exhibited IC(50) values of 1.7nM at NET and 25nM at SERT, which were, respectively, 20- and 13-fold more potent than 1S,2R-milnacipran 1-II.
Bioorganic & Medicinal Chemistry Letters | 2008
Mingzhu Zhang; Florence Jovic; Troy Vickers; Brian Dyck; Junko Tamiya; Jonathan Grey; Joe A. Tran; Beth A. Fleck; Rebecca R. Pick; Alan C. Foster; Chen Chen
Compounds with various activities and selectivities were discovered through structure-activity relationship studies of bicifadine analogs as monoamine transporter inhibitors. The norepinephrine-selective 2-thienyl compound S-6j was efficacious in a rodent pain model.
Bioorganic & Medicinal Chemistry Letters | 2010
Wilna J. Moree; Florence Jovic; Timothy Coon; Jinghua Yu; Bin-Feng Li; Fabio C. Tucci; Dragan Marinkovic; Raymond S. Gross; Siobhan Malany; Margaret J. Bradbury; Lisa M. Hernandez; Zhihong O’Brien; Jianyun Wen; Hua Wang; Samuel R.J. Hoare; Robert E. Petroski; Aida Sacaan; Ajay Madan; Paul D. Crowe; Graham Beaton
SAR of lead benzothiophene H(1)-antihistamine 2 was explored to identify backup candidates with suitable pharmacokinetic profiles for an insomnia program. Several potent and selective H(1)-antihistamines with a range of projected half-lives in humans were identified. Compound 16d had a suitable human half-life as demonstrated in a human microdose study, but variability in pharmacokinetic profile, attributed to metabolic clearance, prevented further development of this compound. Compound 28b demonstrated lower predicted clearance in preclinical studies, and may represent a more suitable backup compound.
Journal of Medicinal Chemistry | 2008
Brian Dyck; Junko Tamiya; Florence Jovic; Rebecca R. Pick; Margaret J. Bradbury; Julie A. O'Brien; Jenny Wen; Michael Johns; Ajay Madan; Beth A. Fleck; Alan C. Foster; Bin-Feng Li; Mingzhu Zhang; Joe A. Tran; Troy Vickers; Jonathan Grey; John Saunders; Chen Chen
Thien-2-yl 1S,2R-milnacipran analogues were synthesized and characterized as norepinephrine/serotonin transporter inhibitors. These compounds possessed higher potencies than 1S,2R-milnacipran (2R-1) while maintaining low molecular weight and moderate lipophilicity, which are the important features for the pharmacological and pharmacokinetic characteristics of milnacipran (1). Thus, compound 5c exhibited IC50 values of 2.3 and 32 nM, respectively, at NET and SERT, which were more than 10-fold better than those of 1 (NET IC50 = 77 nM, SERT IC50 = 420 nM). Moreover, 5c achieved the same efficacy as 1, but with much lower doses, in a rodent spinal nerve ligation pain model. In addition, 5c displayed desirable pharmacokinetic properties in several species, including high oral availability and significant brain penetration.
Bioorganic & Medicinal Chemistry Letters | 2008
Troy Vickers; Brian Dyck; Junko Tamiya; Mingzhu Zhang; Florence Jovic; Jonathan Grey; Beth A. Fleck; Anna Aparicio; Michael Johns; Liping Jin; Hui Tang; Alan C. Foster; Chen Chen
A series of milnacipran analogs containing a heteroaromatic group were synthesized and studied as monoamine transporter inhibitors. Many compounds exhibited higher potency than milnacipran at NET and NET/SERT with no significant change in lipophilicity. For example, compound R-26f was about 10-fold more potent than milnacipran with IC(50) values of 8.7 and 26nM at NET and SERT, respectively.
Organic Process Research & Development | 2008
Timothy D. Gross; Shine Chou; Daniel Bonneville; Raymond S. Gross; Peng Wang; Onorato Campopiano; Michael Ouellette; Scott E. Zook; Jayachandra P. Reddy; Wilna J. Moree; Florence Jovic; Shubham Chopade
Archive | 2010
Brian Dyck; Joe A. Tran; Junko Tamiya; Florence Jovic; Troy Vickers; Chen Chen; Nicole Harriott; Timothy Coon; Neil J. Ashweek
Organic Process Research & Development | 2012
Bernie M. Choudary; Robert Gordon Giles; Florence Jovic; Norman G. Lewis; Steve Moore; Michael Urquhart
