epiquinamide and lupinine

epiquinamide has been researched along with lupinine* in 2 studies

Other Studies

2 other study(ies) available for epiquinamide and lupinine

Article	Year
Short access to (+)-lupinine and (+)-epiquinamide via double hydroformylation. Organic letters, 2010, Feb-05, Volume: 12, Issue:3 Short and efficient access to (+)-lupinine and (+)-epiquinamide by means of an unprecedented double hydroformylation of a bis-homoallylic azide followed by a tandem catalytic hydrogenation/reductive bis-amination is reported. Topics: Alkaloids; Amination; Azides; Catalysis; Hydrogenation; Molecular Structure; Quinolizines; Sparteine; Stereoisomerism	2010
Epiquinamide: a poison that wasn't from a frog that was. Journal of natural products, 2009, Feb-27, Volume: 72, Issue:2 In 2003, we reported the isolation, structure elucidation, and pharmacology of epiquinamide (1), a novel alkaloid isolated from an Ecuadoran poison frog, Epipedobates tricolor. Since then, several groups, including ours, have undertaken synthetic efforts to produce this compound, which appeared initially to be a novel, beta2-selective nicotinic acetylcholine receptor agonist. Based on prior chiral GC analysis of synthetic and natural samples, the absolute structure of this alkaloid was established as (1S,9aS)-1-acetamidoquinolizidine. We have synthesized the (1R,9aS)-isomer (epi-epiquinamide) using an iminium ion nitroaldol reaction as the key step. We have also synthesized ent-1 semisynthetically from (-)-lupinine. Synthetic epiquinamide is inactive at nicotinic receptors, in accord with recently published reports. We have determined that the activity initially reported is due to cross-contamination from co-occurring epibatidine in the isolated material. Topics: Alkaloids; Amphibian Venoms; Animals; Gas Chromatography-Mass Spectrometry; Molecular Structure; Quinolizines; Ranidae; Receptors, Nicotinic; Sparteine; Stereoisomerism	2009

Article

Year

Short access to (+)-lupinine and (+)-epiquinamide via double hydroformylation.

Organic letters, 2010, Feb-05, Volume: 12, Issue:3

Short and efficient access to (+)-lupinine and (+)-epiquinamide by means of an unprecedented double hydroformylation of a bis-homoallylic azide followed by a tandem catalytic hydrogenation/reductive bis-amination is reported.

Topics: Alkaloids; Amination; Azides; Catalysis; Hydrogenation; Molecular Structure; Quinolizines; Sparteine; Stereoisomerism

2010

Epiquinamide: a poison that wasn't from a frog that was.

Journal of natural products, 2009, Feb-27, Volume: 72, Issue:2

In 2003, we reported the isolation, structure elucidation, and pharmacology of epiquinamide (1), a novel alkaloid isolated from an Ecuadoran poison frog, Epipedobates tricolor. Since then, several groups, including ours, have undertaken synthetic efforts to produce this compound, which appeared initially to be a novel, beta2-selective nicotinic acetylcholine receptor agonist. Based on prior chiral GC analysis of synthetic and natural samples, the absolute structure of this alkaloid was established as (1S,9aS)-1-acetamidoquinolizidine. We have synthesized the (1R*,9aS*)-isomer (epi-epiquinamide) using an iminium ion nitroaldol reaction as the key step. We have also synthesized ent-1 semisynthetically from (-)-lupinine. Synthetic epiquinamide is inactive at nicotinic receptors, in accord with recently published reports. We have determined that the activity initially reported is due to cross-contamination from co-occurring epibatidine in the isolated material.

Topics: Alkaloids; Amphibian Venoms; Animals; Gas Chromatography-Mass Spectrometry; Molecular Structure; Quinolizines; Ranidae; Receptors, Nicotinic; Sparteine; Stereoisomerism

2009