Optimization of a Tertiary Alcohol Series of Phosphodiesterase-4 (PDE4) Inhibitors:  Structure−Activity Relationship Related to PDE4 Inhibition and Human Ether-a-go-go Related Gene Potassium Channel Binding Affinity

Friesen, Richard W.; Ducharme, Yves; Ball, Richard G.; Blouin, Marc; Boulet, Louise; Côté, Bernard; Frenette, Richard; Girard, M. Fusco; Guay, Daniel; Huang, Zheng; Jones, Thomas R.; Lynch, Joseph J.; Mancini, Joseph A.; Martins, Evelyn; Masson, P.; Muise, Eric S.; Pon, D. J.; Siegl, P. K. S.; Styhler, Angela; Tsou, Nancy N.; Turner, Mervyn J.; Young, Robert N.; Girard, Yves

doi:10.1021/jm0204542

Cited by 64 publications

(48 citation statements)

References 39 publications

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“…For example, compounds 21 and 23, as the pure Z-isomers, afforded the expected product with only a slight decrease in yields (entries 12 and 13) using our standard procedure, while compound 25 provided an excellent yield of 26 (entry 14). Introducing a bulky t-Bu group (27) into the alkynone provided a quantitative yield of the desired isoxazole 28 (entry 15). Compounds 29 and 31 introduce steric bulk at the ortho positions of the parent phenyl rings.…”

Section: (2)mentioning

confidence: 99%

The Synthesis of Highly Substituted Isoxazoles by Electrophilic Cyclization: An Efficient Synthesis of Valdecoxib

2007

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Section: (2)mentioning

confidence: 99%

The Synthesis of Highly Substituted Isoxazoles by Electrophilic Cyclization: An Efficient Synthesis of Valdecoxib

2007

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“…It binds away from the bimetallic ion center, thus rendering its insensitivity towards Mg 2+ ion with a K d of 4700 nM with the apoenzyme [28]. Over the years, several thousands of catechol-ether based PDE4 inhibitors have been synthesized including the prototypical rolipram, and the more advanced second generation compounds such as roflumilast, cilomilast and L-869,298 [29]. Studies of over 30 of their published PDE4 cocrystals revealed that they all rely on a hydrogen bonding interaction between the invariant glutamine and their common catechol-ether oxygens, and a hydrogen bond Fig.…”

Section: Two-point Anchoring Model For Most Catechol-ether Based Inhimentioning

confidence: 99%

Phosphodiesterase 4 Inhibitors for the Treatment of Asthma and COPD

Huang¹,

Mancini²

2006

CMC

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Type 4 cyclic nucleotide phosphodiesterases (PDE4s) are metallo-hydrolases which specifically hydrolyze cAMP to AMP in various cells types. The catalytic core is a bimetallic ion center composed of a tightly bound Zn(2+) and a loosely bound Mg(2+), which plays a dictating role in eliciting cAMP binding and catalysis activation. An invariant glutamine positioned opposite to the ion center serves as the substrate recognition determinant and synergizes the transient Mg-oxo-phosphate interaction in the substrate complex. The Mg(2+) binding is activated by a PKA-mediated serine phosphorylation and modulated through protein-protein interactions, thus, providing efficient mechanisms in the temporal regulation of cAMP signaling. Several PDE4 inhibitors including roflumilast, cilomilast and rolipram also rely on the interaction with the glutamine and metallic ion center for binding, with their affinity enhanced dramatically by the presence of the Mg(2+) ion. Recent studies have provided new insights into the role of this enzyme in inflammatory settings, CFTR regulation, long term potentiation, and its importance in immune surveillance. The major inflammatory cytokines which are modulated with PDE4 inhibitors include TNFalpha, IL-2, IFNgamma, IL-12, GM-CSF and LTB(4). The role of PDE4 inhibitors in modulating cytokines, lipid mediators and in mucociliary clearance, along with clinical efficacy in asthma and/or COPD demonstrated with roflumilast and cilomilast, suggest a broad anti-inflammatory spectrum for these compounds. Presently, the major impediment to approval of these novel therapies has been the mechanism based gastrointestinal adverse events which has limited the dosing and the ultimate efficacy with these novel therapeutic agents.

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“…11 Candidate 3 was identified as a potent, selective PDE-IV inhibitor 12 and a 14 C-labeled tracer was needed for drug metabolism studies. Thanks to the effort of Merck process research, a 13-step synthesis of 3 was developed, and the compound 4 is an advanced intermediate from the 9th step of that very …”

Section: Introductionmentioning

confidence: 99%

Cu(I)Br‐mediated preparation of ¹⁴C‐labeled 3‐pyridineacetate derivatives and synthesis of a novel ¹⁴C‐labeled PDE‐IV inhibitor

Braun

2007

Labelled Comp Radiopharmac

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An efficient protocol for the synthesis of 14C‐labeled 3‐pyridineacetate (1) and its N‐oxide ([14C]2) is described. Oxidation of this pyridine ([14C]1) to its N‐oxide ([14C]2) proceeded in high yield using H2O2 with MeReO3 as a catalyst. The reaction employs readily available diethyl [2‐14C]malonate. This method has proven to be general in preparation of other pyridineacetate derivatives and their N‐oxides which have been typically difficult to prepare by other means. Our development of the Cu(I)Br‐coupling methodology as well as application to the synthesis of a 14C‐labeled phosphodiesterase‐IV (PDE‐IV) inhibitor, [14C]3, are also reported. Copyright © 2007 John Wiley & Sons, Ltd.

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Optimization of a Tertiary Alcohol Series of Phosphodiesterase-4 (PDE4) Inhibitors: Structure−Activity Relationship Related to PDE4 Inhibition and Human Ether-a-go-go Related Gene Potassium Channel Binding Affinity

Cited by 64 publications

References 39 publications

The Synthesis of Highly Substituted Isoxazoles by Electrophilic Cyclization: An Efficient Synthesis of Valdecoxib

The Synthesis of Highly Substituted Isoxazoles by Electrophilic Cyclization: An Efficient Synthesis of Valdecoxib

Phosphodiesterase 4 Inhibitors for the Treatment of Asthma and COPD

Cu(I)Br‐mediated preparation of ¹⁴C‐labeled 3‐pyridineacetate derivatives and synthesis of a novel ¹⁴C‐labeled PDE‐IV inhibitor

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Optimization of a Tertiary Alcohol Series of Phosphodiesterase-4 (PDE4) Inhibitors: Structure−Activity Relationship Related to PDE4 Inhibition and Human Ether-a-go-go Related Gene Potassium Channel Binding Affinity

Cited by 64 publications

References 39 publications

The Synthesis of Highly Substituted Isoxazoles by Electrophilic Cyclization: An Efficient Synthesis of Valdecoxib

The Synthesis of Highly Substituted Isoxazoles by Electrophilic Cyclization: An Efficient Synthesis of Valdecoxib

Phosphodiesterase 4 Inhibitors for the Treatment of Asthma and COPD

Cu(I)Br‐mediated preparation of 14C‐labeled 3‐pyridineacetate derivatives and synthesis of a novel 14C‐labeled PDE‐IV inhibitor

Contact Info

Product

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About

Cu(I)Br‐mediated preparation of ¹⁴C‐labeled 3‐pyridineacetate derivatives and synthesis of a novel ¹⁴C‐labeled PDE‐IV inhibitor