dinoprost and 3-hydroxybutanal

dinoprost has been researched along with 3-hydroxybutanal* in 2 studies

Other Studies

2 other study(ies) available for dinoprost and 3-hydroxybutanal

Article	Year
Synthesis of prostaglandin analogues, latanoprost and bimatoprost, using organocatalysis via a key bicyclic enal intermediate. Organic letters, 2015, Feb-06, Volume: 17, Issue:3 Two antiglaucoma drugs, bimatoprost and latanoprost, which are analogues of the prostaglandin, PGF2α, have been synthesized in just 7 and 8 steps, respectively. The syntheses employ an organocatalytic aldol reaction that converts succinaldehyde into a key bicyclic enal intermediate, which is primed for attachment of the required lower and upper side chains. By utilizing the crystalline lactone, the drug molecules were prepared in >99% ee. Topics: Aldehydes; Amides; Bimatoprost; Cloprostenol; Dinoprost; Latanoprost; Molecular Structure; Prostaglandins F, Synthetic; Prostaglandins, Synthetic	2015
Stereocontrolled organocatalytic synthesis of prostaglandin PGF2α in seven steps. Nature, 2012, Sep-13, Volume: 489, Issue:7415 Prostaglandins are hormone-like chemical messengers that regulate a broad range of physiological activities, including blood circulation, digestion and reproduction. Their biological activities and their complex molecular architectures have made prostaglandins popular targets for synthetic organic chemists for over 40 years. Prostaglandin analogues are widely used as pharmaceuticals and some, such as latanoprost, which is used to treat glaucoma, have become billion-dollar drugs. Previously reported syntheses of these compounds are quite lengthy, and every chemical step costs time and energy, generates waste and is accompanied by material losses. Using a new bond disconnection, here we report a concise synthesis of the most complex prostaglandin, PGF2α, with high levels of control of relative and absolute stereochemistry, and fewer steps. The key step is an aldol cascade reaction of succinaldehyde using proline organocatalysis to create a bicyclic enal in one step and an enantiomeric excess of 98%. This intermediate bicyclic enal is fully primed with the appropriate functionality for attachment of the remaining groups. Access to this bicyclic enal will not only render existing prostaglandin-based drugs more affordable, but will also facilitate the rapid exploration of related chemical structures around the ubiquitous five-membered ring motif, such as potentially therapeutic prostaglandin analogues. Topics: Aldehydes; Catalysis; Chemistry Techniques, Synthetic; Dinoprost; Molecular Structure; Proline; Prostaglandins F, Synthetic; Stereoisomerism	2012

Article

Year

Synthesis of prostaglandin analogues, latanoprost and bimatoprost, using organocatalysis via a key bicyclic enal intermediate.

Organic letters, 2015, Feb-06, Volume: 17, Issue:3

Two antiglaucoma drugs, bimatoprost and latanoprost, which are analogues of the prostaglandin, PGF2α, have been synthesized in just 7 and 8 steps, respectively. The syntheses employ an organocatalytic aldol reaction that converts succinaldehyde into a key bicyclic enal intermediate, which is primed for attachment of the required lower and upper side chains. By utilizing the crystalline lactone, the drug molecules were prepared in >99% ee.

Topics: Aldehydes; Amides; Bimatoprost; Cloprostenol; Dinoprost; Latanoprost; Molecular Structure; Prostaglandins F, Synthetic; Prostaglandins, Synthetic

2015

Stereocontrolled organocatalytic synthesis of prostaglandin PGF2α in seven steps.

Nature, 2012, Sep-13, Volume: 489, Issue:7415

Prostaglandins are hormone-like chemical messengers that regulate a broad range of physiological activities, including blood circulation, digestion and reproduction. Their biological activities and their complex molecular architectures have made prostaglandins popular targets for synthetic organic chemists for over 40 years. Prostaglandin analogues are widely used as pharmaceuticals and some, such as latanoprost, which is used to treat glaucoma, have become billion-dollar drugs. Previously reported syntheses of these compounds are quite lengthy, and every chemical step costs time and energy, generates waste and is accompanied by material losses. Using a new bond disconnection, here we report a concise synthesis of the most complex prostaglandin, PGF2α, with high levels of control of relative and absolute stereochemistry, and fewer steps. The key step is an aldol cascade reaction of succinaldehyde using proline organocatalysis to create a bicyclic enal in one step and an enantiomeric excess of 98%. This intermediate bicyclic enal is fully primed with the appropriate functionality for attachment of the remaining groups. Access to this bicyclic enal will not only render existing prostaglandin-based drugs more affordable, but will also facilitate the rapid exploration of related chemical structures around the ubiquitous five-membered ring motif, such as potentially therapeutic prostaglandin analogues.

Topics: Aldehydes; Catalysis; Chemistry Techniques, Synthetic; Dinoprost; Molecular Structure; Proline; Prostaglandins F, Synthetic; Stereoisomerism

2012