Your search keyword '"Prostaglandins, Synthetic chemical synthesis"' showing total 98 results

1. New β-ketophosphonates for the synthesis of prostaglandin analogues. 1. Phosphonates with a bicyclo[3.3.0]octene scaffold spaced by a methylene group from the β-ketone.

Author

Tănase C, Căproiu MT, and Drăghici C

Subjects

Bridged Bicyclo Compounds chemistry, Ketones chemical synthesis, Ketones chemistry, Organophosphonates chemistry, Organophosphorus Compounds chemistry, Organophosphonates chemical synthesis, Prostaglandins, Synthetic chemical synthesis

Abstract

The synthesis of β-ketophosphonates, linked by a methylene group to a bicyclo[3.3.0]octene fragment, was performed by the reaction of dimethyl methanephosphonate with the ester group of two intermediates with this scaffold. Starting from a diol, protected with good leaving groups (mesyl and tosyl), we performed a sequence of reactions with good yields: the carbon chain lengthening by reaction with KCN, the hydrolysis of the nitrile groups to carboxyl, the esterification of carboxyl to ester and finally the phosphonate synthesis, which gave one bis-β-ketophosphonate and two mono β-ketophosphonates. The new β-ketophosphonates are key intermediates for obtaining new prostaglandin analogues with a bicyclo[3.3.0]octene fragment in the ω-side chain. The bicyclo[3.3.0]octane scaffold, found in natural products and in anticancer compounds, are expected to keep their activity in PG analogs; the bulky scaffold, separated by a methylene group from the C-15 carbon atom, is expected to diminish the inactivation of the PG analog by enzyme oxidation of 15α-OH oxidation to 15-Keto via PGDH pathway., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2021

2. β-Ketophosphonates with Pentalenofuran Scaffolds Linked to the Ketone Group for the Synthesis of Prostaglandin Analogs.

Author

Tănase CI, Drăghici C, Căproiu MT, Hanganu A, Borodi G, Maganu M, Gal E, and Pintilie L

Subjects

Chemistry Techniques, Synthetic, Crystallography, X-Ray, Models, Molecular, Molecular Conformation, Molecular Structure, Prostaglandins, Synthetic chemistry, Sesquiterpenes chemistry, Ketones chemistry, Organophosphonates chemistry, Prostaglandins, Synthetic chemical synthesis

Abstract

β-Ketophosphonates with pentalenofurane fragments linked to the keto group were synthesized. The bulky pentalenofurane skeleton is expected to introduce more hindrance in the prostaglandin analogues of type III , greater than that obtained with the bicyclo[3.3.0]oct(a)ene fragments of prostaglandin analogues I and II , to slow down (retard) the inactivation of the prostaglandin analogues by oxidation of 15α-OH to the 15-keto group via the 15-PGDH pathway. Their synthesis was performed by a sequence of three high yield reactions, starting from the pentalenofurane alcohols 2 , oxidation of alcohols to acids 3 , esterification of acids 3 to methyl esters 4 and reaction of the esters 4 with lithium salt of dimethyl methanephosphonate at low temperature. The secondary compounds 6b and 6c were formed in small amounts in the oxidation reactions of 2b and 2c , and the NMR spectroscopy showed that their structure is that of an ester of the acid with the starting alcohol. Their molecular structures were confirmed by single crystal X-ray determination method for 6c and XRPD powder method for 6b .

Published

2021

3. Lactones in the Synthesis of Prostaglandins and Prostaglandin Analogs.

Author

Tănase C, Pintilie L, and Tănase RE

Subjects

Catalysis, Molecular Structure, Lactones chemistry, Prostaglandins chemical synthesis, Prostaglandins, Synthetic chemical synthesis

Abstract

In the total stereo-controlled synthesis of natural prostaglandins (PGs) and their structural analogs, a vast class of compounds and drugs, known as the lactones, are encountered in a few key steps to build the final molecule, as: δ-lactones, γ-lactones, and 1,9-, 1,11-, and 1,15-macrolactones. After the synthesis of 1,9-PGF 2α and 1,15-PGF 2α lactones, many 1,15-lactones of E 2 , E 3 , F 2 , F 3 , A 2 , and A 3 were found in the marine mollusc Tethys fimbria and the quest for understanding their biological role stimulated the research on their synthesis. Then 1,9-, 1,11-, and 1,15-PG lactones of the drugs were synthesized as an alternative to the corresponding esters, and the first part of the paper describes the methods used for their synthesis. The efficient Corey procedure for the synthesis of prostaglandins uses the key δ-lactone and γ-lactone intermediates with three or four stereocenters on the cyclopentane fragment to link the PG side chains. The paper describes the most used procedures for the synthesis of the milestone δ-Corey-lactones and γ-Corey-lactones, their improvements, and some new promising methods, such as interesting, new stereo-controlled and catalyzed enantioselective reactions, and methods based on the chemical/enzymatic resolution of the compounds in different steps of the sequences. The many uses of δ-lactones not only for the synthesis of γ-lactones, but also for obtaining 9β-halogen-PGs and halogen-substituted cyclopentane intermediates, as synthons for new 9β-PG analogs and future applications, are also discussed.

Published

2021

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

Author

Prévost S, Thai K, Schützenmeister N, Coulthard G, Erb W, and Aggarwal VK

Subjects

Aldehydes chemistry, Amides chemistry, Bimatoprost, Cloprostenol chemical synthesis, Cloprostenol chemistry, Dinoprost analogs & derivatives, Dinoprost chemistry, Latanoprost, Molecular Structure, Prostaglandins F, Synthetic chemistry, Prostaglandins, Synthetic chemistry, Amides chemical synthesis, Cloprostenol analogs & derivatives, Dinoprost chemical synthesis, Prostaglandins F, Synthetic chemical synthesis, Prostaglandins, Synthetic chemical synthesis

Abstract

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.

Published

2015

5. Discovery of novel prostaglandin analogs as potent and selective EP2/EP4 dual agonists.

Author

Kambe T, Maruyama T, Nakai Y, Yoshida H, Oida H, Maruyama T, Abe N, Nishiura A, Nakai H, and Toda M

Subjects

Administration, Topical, Animals, CHO Cells, Cricetinae, Cricetulus, Drug Evaluation, Preclinical, Fractures, Bone drug therapy, Isomerism, Mice, Prostaglandins, Synthetic chemical synthesis, Prostaglandins, Synthetic therapeutic use, Rats, Receptors, Prostaglandin E, EP2 Subtype genetics, Receptors, Prostaglandin E, EP2 Subtype metabolism, Receptors, Prostaglandin E, EP4 Subtype genetics, Receptors, Prostaglandin E, EP4 Subtype metabolism, Structure-Activity Relationship, Thiazolidines chemical synthesis, Thiazolidines therapeutic use, Prostaglandins, Synthetic chemistry, Receptors, Prostaglandin E, EP2 Subtype agonists, Receptors, Prostaglandin E, EP4 Subtype agonists, Thiazolidines chemistry

Abstract

To identify potent EP2/EP4 dual agonists with excellent subtype selectivity, a series of γ-lactam prostaglandin E analogs bearing a 16-phenyl ω-chain were synthesized and evaluated. Structural hybridization of 1 and 2, followed by more detailed chemical modification of the benzoic acid moiety, led us to the discovery of a 2-mercaptothiazole-4-carboxylic acid analog 3 as the optimal compound in the series. An isomer of this compound, the 2-mercaptothiazole-5-carboxylic acid analog 13, showed 34-fold and 13-fold less potent EP2 and EP4 receptor affinities, respectively. Structure activity relationship data from an in vitro mouse receptor binding assay are presented. Continued evaluation in an in vivo rat model of another 2-mercaptothiazole-4-carboxylic acid analog 17, optimized for sustained compound release from PLGA microspheres, demonstrated its effectiveness in a rat bone fracture-healing model following topical administration., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012

6. Synthesis of neuroprotective cyclopentenone prostaglandin analogs: suppression of manganese-induced apoptosis of PC12 cells.

Author

Furuta K, Maeda M, Hirata Y, Shibata S, Kiuchi K, and Suzuki M

Subjects

Animals, DNA Fragmentation drug effects, Indicators and Reagents, PC12 Cells, Rats, Apoptosis drug effects, Manganese antagonists & inhibitors, Manganese pharmacology, Neuroprotective Agents chemical synthesis, Neuroprotective Agents pharmacology, Prostaglandins, Synthetic chemical synthesis, Prostaglandins, Synthetic pharmacology

Abstract

The synthesis and evaluation for anti- and proapoptotic properties of cyclopentenone prostaglandin analogs are described. Novel J-type analogs of NEPP11 with a cross-conjugated cyclopentadienone moiety and a lipophilic omega-side chain suppressed manganese ion-induced apoptosis of PC12 cells at comparable levels to NEPP11, while monoenone derivatives were inactive. The proapoptotic activities of J-type analogs were much lower than that of NEPP11. Natural 15-deoxy-Delta(12,14)-PGJ(2) and Delta(7)-PGA(1) methyl ester were highly toxic, inducing apoptosis at lower concentrations.

Published

2007

7. Novel synthetic strategies for the preparation of prostacyclin and prostaglandin analogues--off the beaten track.

Author

Sheddan NA, Czybowski M, and Mulzer J

Subjects

Epoprostenol chemistry, Molecular Structure, Prostaglandins, Synthetic chemistry, Epoprostenol analogs & derivatives, Epoprostenol chemical synthesis, Prostaglandins, Synthetic chemical synthesis

Abstract

The recent increase in activity in the fields of neuroscience and life sciences has been mirrored by the design and synthesis of novel chemically and metabolically stable prostaglandin and prostacyclin analogues. Consequently, convenient and practical access to these important classes of compounds is greatly coveted. Various strategies for the preparation of prostacyclin, prostaglandin and isoprostane analogues are discussed, with particular focus on novel approaches developed in our own laboratories.

Published

2007

8. Prostacyclin, atherothrombosis, and cardiovascular disease.

Author

Arehart E, Gleim S, Kasza Z, Fetalvero KM, Martin KA, and Hwa J

Subjects

Animals, Cyclooxygenase 2 drug effects, Epoprostenol genetics, Epoprostenol therapeutic use, Humans, Hypertension, Pulmonary drug therapy, Mice, Mice, Transgenic, Prostaglandins, Synthetic chemical synthesis, Prostaglandins, Synthetic therapeutic use, Receptors, Epoprostenol chemistry, Receptors, Epoprostenol genetics, Cardiovascular Diseases drug therapy, Drug Design, Epoprostenol analogs & derivatives, Prostaglandins, Synthetic chemistry, Receptors, Epoprostenol agonists, Thrombosis drug therapy

Abstract

Prostacyclin (PGI(2)) is a major product of COX-2 catalyzed metabolism of arachidonic acid in the endothelium. Recent studies have demonstrated that PGI(2) protects against atherothrombosis. The prostacyclin receptor knockout mice exhibit increased atherosclerosis, enhanced thrombosis, and enhanced proliferative response to carotid vascular injury with increased intima to media ratios [1-3]. Moreover, the recent withdrawal of rofecoxib (Vioxx) due to increased cardiovascular events further supports the critical role of prostacyclin in inhibiting atherothrombosis in humans. Such studies have paralleled intense chemical biology studies to develop more stable prostacyclin analogues. Indeed a number of these analogues are currently being successfully used for the treatment of pulmonary hypertension. In this review we will summarize the current literature on some principles of prostacyclin analogue development, our current understanding of the receptor, and recent developments which implicate prostacyclin in atherothrombotic protection. More than 68 million Americans suffer from cardiovascular disease, which causes more deaths, disability and economic loss than any other group of diseases. Further clinical investigations of orally stable prostacyclin analogues for treatment of cardiovascular diseases other than pulmonary hypertension may now be warranted.

Published

2007

9. Development of a common fully stereocontrolled access to the medicinally important and promising prostacyclin analogues iloprost, 3-oxa-iloprost and cicaprost.

Author

Gais HJ, Kramp GJ, Wolters D, and Reddy LR

Subjects

Epoprostenol chemical synthesis, Stereoisomerism, Vasodilator Agents chemical synthesis, Epoprostenol analogs & derivatives, Iloprost analogs & derivatives, Iloprost chemical synthesis, Prostaglandins, Synthetic chemical synthesis

Abstract

We describe new fully stereocontrolled syntheses of the prostacyclin analogues iloprost (2), the most active component of the drugs Ilomedin and Ventavis, and 3-oxa-iloprost (3), a derivative that is expected to have a significantly higher metabolic stability than 2 perhaps allowing an oral application. The syntheses are based on the same strategy and chiral bicyclic building block as used in the synthesis of cicaprost (4), the third most potent analogue that exhibits, besides prostacyclin-like activities, antimetastatic activities. Reaction of the enantiopure C6-C13 bicyclic aldehyde 17 with Cl(3)CCOOH/Cl(3)CCOONa afforded trichlorocarbinol 24 which was converted via mesylate 25 to the C6-C14 bicyclic alkyne 9. The palladium-catalysed hydrostannylation of alkyne 9 gave with high regio- and stereoselectivity the alkenylstannane 26, Sn/Li exchange of which afforded the E-configured alkenyllithium derivative 8. Coupling of the C6-C14 building block 8 with the enantiopure C15-C20 building block, the N-methoxyamide 7, gave the C6-C20 bicyclic ketone 6 in high yield without epimerisation at C16. The configuration at C15 of iloprost (2) and 3-oxa-iloprost (3) was established through a highly diastereoselective reduction of ketone 6 with catecholborane and the chiral oxazaborolidine 28 which furnished alcohol (15S)-29. The highly stereoselective conversions of alcohol (15S)-29 to iloprost (2) and 3-oxa-iloprost (3), which include as key stereoselective steps an olefination with a chiral phosphonoacetate and a copper-mediated allylic alkylation, have already been described.

Published

2006

10. Chemical transformation of prostaglandin-A2: a novel series of C-10 halogenated, C-12 hydroxylated prostaglandin-A2 analogues.

Author

Ratnayake AS, Bugni TS, Veltri CA, Skalicky JJ, and Ireland CM

Subjects

Hydrocarbons, Halogenated chemistry, Molecular Structure, Nuclear Magnetic Resonance, Biomolecular, Stereoisomerism, Hydrocarbons, Halogenated chemical synthesis, Prostaglandins A chemical synthesis, Prostaglandins A chemistry, Prostaglandins, Synthetic chemical synthesis

Abstract

[reaction: see text] Synthesis of a novel class of C-10 halogenated and C-12 oxygenated prostaglandin-A(2) derivatives (6a-6c) has been accomplished. (15S)-Prostaglandin-A(2) (1), from the gorgonian Plexaura homomalla, served as the starting material for the synthesis. The absolute configuration was determined using NMR.

Published

2006

11. A convergent synthesis of the 11-oxa prostaglandin analogue AL-12182.

Author

Fox ME, Jackson M, Lennon IC, and McCague R

Subjects

Cyclization, Molecular Structure, Prostaglandins chemistry, Prostaglandins, Synthetic chemistry, Prostaglandins, Synthetic chemical synthesis

Abstract

[reaction: see text] The 11-oxa prostaglandin analogue AL-12182 1 has potent topical ocular hypotensive activity. A convergent and concise general synthesis of this class of prostanoid was developed employing a stereoselective coupling reaction between a tetrahydrofuran core electrophile and a nucleophilic omega side chain component, providing a route that should be suitable for commercial scale production. The tetrahydrofuran core was assembled from dimethyl d-malate using a stereoselective beta-hydroxy ester dianion alkylation reaction.

Published

2005

12. Cyclooxygenase isozymes: the biology of prostaglandin synthesis and inhibition.

Author

Simmons DL, Botting RM, and Hla T

Subjects

Amino Acid Sequence, Animals, Cyclooxygenase 1, Cyclooxygenase 2, Humans, Isoenzymes chemistry, Isoenzymes genetics, Membrane Proteins, Models, Genetic, Molecular Sequence Data, Prostaglandin-Endoperoxide Synthases chemistry, Prostaglandin-Endoperoxide Synthases genetics, Prostaglandins, Synthetic therapeutic use, Isoenzymes pharmacology, Prostaglandin-Endoperoxide Synthases pharmacology, Prostaglandins, Synthetic antagonists & inhibitors, Prostaglandins, Synthetic chemical synthesis

Abstract

Nonsteroidal anti-inflammatory drugs (NSAIDs) represent one of the most highly utilized classes of pharmaceutical agents in medicine. All NSAIDs act through inhibiting prostaglandin synthesis, a catalytic activity possessed by two distinct cyclooxygenase (COX) isozymes encoded by separate genes. The discovery of COX-2 launched a new era in NSAID pharmacology, resulting in the synthesis, marketing, and widespread use of COX-2 selective drugs. These pharmaceutical agents have quickly become established as important therapeutic medications with potentially fewer side effects than traditional NSAIDs. Additionally, characterization of the two COX isozymes is allowing the discrimination of the roles each play in physiological processes such as homeostatic maintenance of the gastrointestinal tract, renal function, blood clotting, embryonic implantation, parturition, pain, and fever. Of particular importance has been the investigation of COX-1 and -2 isozymic functions in cancer, dysregulation of inflammation, and Alzheimer's disease. More recently, additional heterogeneity in COX-related proteins has been described, with the finding of variants of COX-1 and COX-2 enzymes. These variants may function in tissue-specific physiological and pathophysiological processes and may represent important new targets for drug therapy.

Published

2004

13. Studies on ocular inflammation and development of a prostaglandin analogue for glaucoma treatment.

Author

Stjernschantz J

Subjects

Dose-Response Relationship, Drug, Eye Color drug effects, Humans, Intraocular Pressure drug effects, Latanoprost, Melanosis, Neurogenic Inflammation physiopathology, Prostaglandins F, Synthetic adverse effects, Prostaglandins F, Synthetic therapeutic use, Prostaglandins, Synthetic adverse effects, Prostaglandins, Synthetic therapeutic use, Glaucoma drug therapy, Neurogenic Inflammation etiology, Prostaglandins F, Synthetic chemical synthesis, Prostaglandins, Synthetic chemical synthesis

Abstract

This review summarizes the Ernst H. Bárány Prize Lecture given at the meeting of the International Society of Eye Research in Geneva 2002. In the paper the path from the author's early studies on neurogenic inflammation in the eye to the search for a suitable prostaglandin analogue for glaucoma treatment, and the development of latanoprost are described. In particular the solution to the nociceptive and hyperemic side-effects of naturally occurring prostaglandins in the eye, the mechanism of action of FP prostanoid receptor agonists as well as the selection of dose for glaucoma treatment are discussed. In addition, pharmacokinetical aspects of latanoprost, and the melanogenic side-effect of prostaglandins in the iris are addressed. The paper is primarily focused on studies performed by the author and complete reference to other previous, or contemporary studies is therefore not always given as the purpose is not to present a comprehensive review article.

Published

2004

14. Asymmetric synthesis of the highly potent anti-metastatic prostacyclin analogue cicaprost and its isomer isocicaprost.

Author

Lerm M, Gais HJ, Cheng K, and Vermeeren C

Subjects

Antineoplastic Agents chemical synthesis, Isomerism, Models, Molecular, Molecular Structure, Epoprostenol analogs & derivatives, Epoprostenol chemical synthesis, Prostaglandins, Synthetic chemical synthesis

Abstract

An asymmetric synthesis of the anti-metastatic prostacyclin analogue cicaprost and a formal one of its isomer isocicaprost by a new route are described. A key step of these syntheses is the coupling of a chiral bicyclic C6-C14 ethynyl building block with a chiral C15-C21 omega-side chain amide building block with formation of the C14-C15 bond of the target molecules. A highly stereoselective reduction of the thereby obtained C6-C21 intermediate carrying a carbonyl group at C15 of the side chain was accomplished by the chiral oxazaborolidine method. The chiral phosphono acetate method was used for the highly stereoselective attachment of the alpha-side chain to the bicyclic C6-C21 intermediate carrying a carbonyl group at C6. Asymmetric syntheses of the bicyclic C6-C14 ethynyl building blocks were carried out starting from achiral bicyclic C6-C12 ketones by using the chiral lithium amide method. In the course of these syntheses, a new method for the introduction of an ethynyl group at the alpha-position of the carbonyl group of a ketone with formation of the corresponding homopropargylic alcohol was devised. Its key steps are an aldol reaction of the corresponding silyl enol ether with chloral and the elimination of a trichlorocarbinol derivative with formation of the ethynyl group. In addition, a new aldehyde to terminal alkyne transformation has been realized. Its key steps are the conversion of an aldehyde to the corresponding 1-alkenyl dimethylaminosulfoxonium salt and the elimination of the latter with a strong base. Two basically different routes have been followed for the synthesis of the enantiomerically pure C15-C21 omega-side chain amide building block. The first is based on the chiral oxazolidinone method and features a highly stereoselective alkylation of (4R)-N-acetyl-4-benzyloxazolidin-2-one, and the second encompasses a malonate synthesis of the racemic amide and its efficient preparative scale resolution by HPLC on a chiral stationary phase containing column.

Published

2003

15. A new strategy for the enantioselective synthesis of carba-prostacyclin analogues based on organocopper conjugate addition to a bicyclic azoene and its application to the synthesis of 13,14-dinor-inter-p-phenylene carbacyclin.

Author

van Bergen M and Gais HJ

Subjects

Azo Compounds chemistry, Epoprostenol analogs & derivatives, Epoprostenol chemistry, Prostaglandins, Synthetic chemistry, Stereoisomerism, Copper chemistry, Epoprostenol chemical synthesis, Organometallic Compounds chemistry, Prostaglandins, Synthetic chemical synthesis

Abstract

An enantioselective synthesis of E/Z-13,14-dinor-inter-p-phenylene carbacyclin (E/Z-2d) by a new strategy has been realized that holds the prospect of serving as a general route for carba-prostacyclin analogues. The key intermediate in this synthesis is the bicyclic azoene Ts-9, and the key step is the regio- and stereoselective conjugate addition of the chiral arylcopper compound Cu-8d/P-n-Bu3 to the azoene with formation of hydrazone 7d. Enantioselective synthesis of azoene Ts-9 of 95% ee from ketone 4 was accomplished in four and five steps, respectively. Thus, enantioselective deprotonation of bicyclic ketone 4 with chiral base Li-10 and trapping of lithium enolate 11 with ClSiMe3 gave enol ether 12, which was chlorinated with N-chlorosuccinimide (NCS) to afford chloro ketone 13. Alternatively, chloro ketone 13 was also prepared upon chlorination of 11 with NCS. Chloro ketone 13 was converted to chloro hydrazone 14, which upon treatment with a mild base furnished azoene Ts-9. Arylcopper compound 8d of 98% ee was obtained in two steps from alcohol 16, which was prepared by enantioselective reduction of ketone 17 with (-)-diisopinocampheylchloroborane. Carbacyclin derivative E/Z-2d was found to be essentially inactive as an inhibitor of ADP induced human platelet aggregation, having an IC50 of >10 micromol/L.

Published

2002

16. The design and synthesis of selective prostaglandin analogs as bone anabolic agents for the potential treatment of osteoporosis.

Author

Soper DL, Wang Y, De B, deLong MA, Dirr MJ, Soehner ME, Lundy MW, Mieling GE, and Wos JA

Subjects

Bone and Bones drug effects, Bone and Bones physiopathology, Drug Design, Humans, Models, Molecular, Molecular Structure, Prostaglandins F, Synthetic therapeutic use, Structure-Activity Relationship, Bone and Bones physiology, Osteoporosis drug therapy, Prostaglandins, Synthetic chemical synthesis, Prostaglandins, Synthetic therapeutic use

Abstract

A series of prostaglandins selective for the human FP receptor have been synthesized and evaluated as potential therapeutics for the treatment of osteoporosis. The compounds proved to be potent (nanomolar binding affinity) and selective (> 100x) ligands for the human FP receptor in vitro, and increased bone volume in the ovariectomized rat in vivo.

Published

2002

17. A new strategy for cyclopentenone synthesis.

Author

Trost BM and Pinkerton AB

Subjects

Anti-Infective Agents chemical synthesis, Anti-Infective Agents chemistry, Anti-Ulcer Agents chemical synthesis, Anti-Ulcer Agents chemistry, Antihypertensive Agents chemical synthesis, Antihypertensive Agents chemistry, Bryopsida chemistry, Cyclopentanes chemical synthesis, Esters chemical synthesis, Esters chemistry, Expectorants chemical synthesis, Expectorants chemistry, Gastrointestinal Agents chemical synthesis, Gastrointestinal Agents chemistry, Prostaglandins, Synthetic chemical synthesis, Prostaglandins, Synthetic chemistry, Prostanoic Acids chemical synthesis, Prostanoic Acids chemistry, Cyclopentanes chemistry

Abstract

[reaction--see text] A new strategy for the synthesis of 2,3-disubstituted cyclopentenones emerges from two key reactions-the ruthenium-catalyzed three-component coupling of an equivalent of HBr, an alkyne, and a vinyl ketone and the Ni-Cr Barbier type reaction. As a result, these important structures are readily accessed from an alkyne and a vinyl ketone (which derive directly from carboxylic acids). Syntheses of tetrahydrodicranenone B and rosaprostol illustrate the new strategy.

Published

2000

18. Synthesis of bicyclic ketones in prostaglandins and their antimitotic activity.

Author

Domínguez JN, Zapata AJ, Lobo GM, and Blanca I

Subjects

Antineoplastic Agents pharmacology, Humans, Mitosis drug effects, Prostaglandins pharmacology, Prostaglandins, Synthetic pharmacology, Structure-Activity Relationship, Tumor Cells, Cultured, Antineoplastic Agents chemical synthesis, Prostaglandins chemical synthesis, Prostaglandins, Synthetic chemical synthesis

Abstract

The synthesis of a second ring in the prostaglandin structure, located at positions C-11 and C-13, has been accomplished starting from prostaglandin A2. Also an efficient enantioselectivity was obtained through the conjugate addition of carbanions at position C-11, together with the stereospecificity of a Claisen rearrangement at position C-13. Evaluation of the inhibitory effects on the proliferation of the K-562 cell line, in vitro, is presented. A structure-activity relationship indicated that alterations of the functional groups incorporated in the second ring of the prostaglandin structure affected their hydrophobicity. The antimitotic activity for prostanoids 7b, 7c and 7e have shown substantial improvements in their activities according to their ID50 values (12.5, 9.0 and 1.12 micrograms/ml), respectively). Attention is called to the importance of derivative 7a in terms of its high potency, determined by its ID50 values (0.35 micrograms/ml).

Published

1995

19. Synthesis of C(10)-halogenated prostaglandins.

Author

Dominguez JN, Taddei A, Cordero M, and Blanca I

Subjects

Acetylation, Animals, Antineoplastic Agents chemical synthesis, Antineoplastic Agents pharmacology, Catalysis, Cell Division drug effects, Chromatography, Thin Layer, Drug Screening Assays, Antitumor, Humans, Hydroxylation, Leukemia, Erythroblastic, Acute physiopathology, Magnetic Resonance Spectroscopy, Prostaglandins, Synthetic pharmacology, Stereoisomerism, Tumor Cells, Cultured, Cnidaria chemistry, Prostaglandins, Synthetic chemical synthesis

Abstract

The synthesis of halogenated prostaglandins at position C(10), starting from prostaglandin A2, has been accomplished, as well as an efficient regioselective hydroxylation of the upper chain of the prostanoid structure. Evaluation of the inhibitory effects on the proliferation of the K-562 cell line in vitro is presented. When the prostaglandin was modified in the upper chain, the antimitotic activity for bromo derivatives 4b, c and iodo derivative 5b had shown substantial improvements in their activities according to their ID50 values (28, 25, and 22 micrograms/mL, respectively). Attention is called to the significance of chloro derivative 3a in terms of its high potency, determined by its ID50 value (0.06 micrograms/mL).

Published

1994

20. Synthesis of (+/-)-homosarkomycin and (+/-)-rosaprostol.

Author

Tanimori S, Kainuki T, and Nakayama M

Subjects

Biotechnology, Cyclopentanes chemistry, Cyclopropanes, Indicators and Reagents, Magnetic Resonance Spectroscopy, Methods, Prostaglandins, Synthetic chemical synthesis, Prostaglandins, Synthetic chemistry, Prostanoic Acids chemistry, Stereoisomerism, Cyclopentanes chemical synthesis, Prostanoic Acids chemical synthesis

Published

1992

21. Synthesis of a 11-deoxyprostanoid in the area of preclavulones: (+-)-8,12-trans-(5Z-14Z)-9-oxo-prosta-5,14-dienoic acid from 2-allyl-2-cyclopenten-1-one.

Author

Di Giacomo M, Leggeri P, Papeo G, Pirillo D, and Traverso G

Subjects

Animals, Cnidaria chemistry, Magnetic Resonance Spectroscopy, Prostaglandins, Synthetic analysis, Spectrophotometry, Infrared, Eicosanoids analysis, Prostaglandins, Synthetic chemical synthesis

Abstract

Following our research on the arachidonic acid metabolites and their derivatives with potential biological activity, we describe the synthesis of the (+-)-8,12-trans-(5Z, 14Z)-9-oxo-prosta-5,14-dienoic acid, a 11-deoxyprostanoid correlated to the class of Preclavulones, one of the unusual families of marine eicosanoids from the coral Clavularia Viridis with considerable biological interest.

Published

1992

22. Imidazolidin-2-one prostaglandin analogues.

Author

Barraclough P, Jackson WP, and Harris CJ

Subjects

Cyclohexanes pharmacology, Humans, Hydantoins chemical synthesis, Hydantoins chemistry, Hydantoins pharmacology, Imidazoles pharmacology, In Vitro Techniques, Platelet Aggregation drug effects, Platelet Aggregation Inhibitors chemical synthesis, Prostaglandins, Synthetic chemistry, Prostaglandins, Synthetic pharmacology, Structure-Activity Relationship, Cyclohexanes chemical synthesis, Imidazoles chemical synthesis, Prostaglandins, Synthetic chemical synthesis

Abstract

The 5-desoxy analogue of BW245C, imidazolidin-2-one 3, has been synthesized by reduction of the N-benzyl hydantoin derivative 6. Compound 3 was found to be approximately equipotent with BW245C as an inhibitor of platelet aggregation and this result indicates that the 5-keto group of BW245C is not essential for platelet inhibitory activity.

Published

1991

23. Antiulcer activity of some PG-like derivatives and their intermediates.

Author

Passarotti C, Bandi GL, Citerio L, and Valenti M

Subjects

Animals, Anti-Inflammatory Agents, Non-Steroidal, Prostaglandins, Synthetic chemical synthesis, Rats, Rats, Inbred Strains, Anti-Ulcer Agents chemical synthesis, Prostaglandins, Synthetic pharmacology

Abstract

During a search on PG-like compounds as antiulcer drugs we synthetized some hetherocyclic derivatives. Some compounds of this series were found to be effective after oral administration in inhibiting restraint induced ulcers in the rat. Three of the most active compounds showed fairly good antiinflammatory activity in the carrageenin-induced rat paw oedema test and in the RPAR test.

Published

1991

24. Prostaglandins intermediates. Reduction of (E)-oxolactone by means of a chiral phase transfer catalyst.

Author

Passarotti C, Bandi GL, Fossati A, Valenti M, and Dal Bo L

Subjects

Catalysis, Magnetic Resonance Spectroscopy, Prostaglandins, Synthetic chemistry, Biphenyl Compounds chemistry, Cyclopentanes chemistry, Lactones, Prostaglandins, Synthetic chemical synthesis

Abstract

Preparation of (15 S)-hydroxy derivative (1-b), a key intermediate in the synthesis of PG like compounds, by reduction the corresponding enone (2), is described. High yields in (S)-isomer was obtained by means of chiral phase-transfer catalyst: (-)-N-(1-dodecyl)-N-methylephedrinium bromide. Eleven ammonium quaternary salts derived from (-)-N-methylephedrine were prepared and tested as catalyst in the reduction of enone (2) with NaBH4. Synthesis of enone (2), from phosphonate (6) (via Wadsworth-Emmons reaction) is also described.

Published

1990

25. (+/-)-11-oxo-10,11,13,14-tetrahydro-12-azaprostaglandin A1 methyl ester.

Author

Scribner RM

Subjects

Chemical Phenomena, Chemistry, Molecular Conformation, Prostaglandins A chemical synthesis, Prostaglandins, Synthetic chemical synthesis

Published

1977

26. Synthesis of prostaglandin H2 methyl ester.

Author

Johnson RA, Nidy EG, Baczynskyj L, and Gorman RR

Subjects

Prostaglandins F, Prostaglandin Endoperoxides chemical synthesis, Prostaglandins H chemical synthesis, Prostaglandins, Synthetic chemical synthesis

Published

1977

27. Prostaglandins and congeners. 25. Inhibition of gastric acid secretion. Replacement of the carboxylate moiety of a prostaglandin with a hydroxymethylketo functional group.

Author

Wissner A, Birnbaum JE, and Wilson DE

Subjects

Animals, Depression, Chemical, Dogs, Ketones, Methanol analogs & derivatives, Prostaglandins, Synthetic pharmacology, Rats, Gastric Juice metabolism, Prostaglandins, Synthetic chemical synthesis

Published

1980

28. Synthesis and platelet aggregation inhibiting activity of prostaglandin D analogues.

Author

Bundy GL, Morton DR, Peterson DC, Nishizawa EE, and Miller WL

Subjects

Animals, Blood Pressure drug effects, Colon drug effects, Cricetinae, Diarrhea chemically induced, Fertility drug effects, Gerbillinae, Humans, Prostaglandins D chemical synthesis, Prostaglandins D pharmacology, Prostaglandins, Synthetic pharmacology, Rats, Platelet Aggregation drug effects, Prostaglandins, Synthetic chemical synthesis

Abstract

Several prostaglandin D (PGD) analogues have been synthesized, incorporating the following variations: (a) varying degrees of side-chain unsaturation, (b) C-9 hydroxy removed or in the unnatural 9 beta configuration, (c) metabolically stabilized analogues (e.g., 15-methyl, 16,16-dimethyl, 17-phenyl, etc.), and (d) delta 12 isomers resulting from decomposition of PGD2. With regard to their ability to inhibit adenosine diphosphate (ADP) induced human platelet aggregation: (a) PGD3 greater than or equal to PGD2 greater than PGD1 greater than 13,14-dihydro-PGD1, (b) the 9 beta- and 9-deoxy-PGD2 analogues are more potent than PGD2, (c) metabolically stabilized analogues with bulky substituents at or near C-15 have substantially reduced antiaggregatory activity relative to PGD2 and (d) the delta 12 isomers of PGD2 are much less active than PGD2.

Published

1983

29. Synthesis of 11C-labeled prostaglandins and positron emission tomography studies using the rhesus monkey.

Author

Watanabe Y, Långström B, Stålnacke CG, Gullberg P, Svärd H, Halldin C, and Hayaishi O

Subjects

Animals, Brain metabolism, Carbon Radioisotopes, Macaca mulatta, Muscles metabolism, Prostaglandins D chemical synthesis, Prostaglandins D metabolism, Prostaglandins, Synthetic metabolism, Tomography, Emission-Computed, Prostaglandin D2 analogs & derivatives, Prostaglandins, Synthetic chemical synthesis

Published

1987

30. Prostaglandin prodrugs. II: New method for synthesizing prostaglandin C1-aliphatic esters.

Author

Morozowich W, Oesterling TO, Miller WL, and Douglas SL

Subjects

Animals, Contraceptive Agents, Female, Cricetinae, Female, Methods, Prostaglandins, Synthetic pharmacology, Prostaglandins, Synthetic chemical synthesis

Abstract

A new method for synthesizing C1-aliphatic esters of dinoprost and dinoprostone without using hydroxyl protective groups is described. Reaction of the prostaglandin with an alkyl halide in the presence of the sterically hindered amine N,N-diisopropylethylamine proceeds smoothly to give C1-esters in various solvents at ambient or slightly elevated temperatures. Polar solvents were strongly catalytic, and even the hindered tert-butyl esters were synthesized by employing solvents such as dimethylformamide or dimethyl sulfoxide. Biological evaluation in the hamster antifertility assay showed that some esters maintained high bioactivity.

Published

1979

31. Syntheses and biological activities of some prostacyclin analogs.

Author

Ohuchida S, Hashimoto S, Wakatsuka H, Arai Y, and Hayashi M

Subjects

Animals, Biological Assay, Dogs, Epoprostenol pharmacology, Heart drug effects, Heart physiology, Indicators and Reagents, Methods, Platelet Aggregation drug effects, Prostaglandins E pharmacology, Prostaglandins, Synthetic pharmacology, Rabbits, Rats, Structure-Activity Relationship, Vasodilation, Epoprostenol chemical synthesis, Prostaglandins chemical synthesis, Prostaglandins, Synthetic chemical synthesis

Published

1980

32. Synthesis of 13,14-dehydroprostacyclin methyl ester: a potent inhibitor of platelet aggregation.

Author

Fried J and Barton J

Subjects

Animals, Biological Assay, Dogs, Epoprostenol analogs & derivatives, Isomerism, Kidney blood supply, Magnetic Resonance Spectroscopy, Methods, Prostaglandins, Synthetic pharmacology, Regional Blood Flow drug effects, Platelet Aggregation drug effects, Prostaglandins, Synthetic chemical synthesis

Abstract

The structure of the most recently discovered, biologically highly active prostaglandin, PGI2 or prostacyclin, is correctly predicted on biogenetic grounds, and a general synthesis starting with prostaglandins of the F2alpha series is reported. Starting with the biologically active 13,14-dehydro-PGF2alpha, the synthesis involves formation of a 5-bromo-6,9alpha-epoxy derivative, followed by esterification and dehydrobromination of the methyl ester to form the prostacyclin structure. The stereochemistry at C-5 and C-6 of all reported products is assigned on the basis of experimental findings and mechanistic reasoning. 13,14-Dehydroprostacyclin methyl ester is considerably more stable at pH 7.5 than prostacyclin. It inhibits platelet aggregation induced by a variety of agents and causes an increase in renal blood flow in the dog at nanomolar levels.

Published

1977

33. [Synthesis of fluoroprostacyclins].

Author

Bezuglov VV and Bergel'son LD

Subjects

Epoprostenol, Fluorine, Methods, Prostaglandins, Synthetic chemical synthesis

Published

1980

34. 15,15-Ketals of natural prostaglandins and prostaglandin analogues. Synthesis and biological activities.

Author

Skuballa W, Radüchel B, Loge O, Elger W, and Vorbrüggen H

Subjects

Abortifacient Agents, Nonsteroidal chemical synthesis, Animals, Female, Guinea Pigs, In Vitro Techniques, Luteolytic Agents chemical synthesis, Methods, Muscle Contraction drug effects, Muscle, Smooth drug effects, Pregnancy, Prostaglandins, Synthetic pharmacology, Rats, Uterine Contraction drug effects, Prostaglandins, Synthetic chemical synthesis

Abstract

The synthesis is described of new 15,15-ethylene ketals of natural prostaglandins and prostaglandin analogues. Especially the crystalline trisamine salt of the 15,15-ethylene ketal of 15-dehydro-16-phenoxy-17,18,19,20-tetranorprostaglandin F2alpha is a very active inducer of luteolysis in laboratory animals and cattle.

Published

1978

35. Properties of prostaglandin derivatives on a phospholipid basis.

Author

Lekim D, Sieck A, Betzing H, and Kunze H

Subjects

Animals, Blood Pressure drug effects, Cats, Dose-Response Relationship, Drug, Guinea Pigs, Hydrolysis, In Vitro Techniques, Muscle Contraction drug effects, Phosphatidylethanolamines pharmacology, Prostaglandins E pharmacology, Prostaglandins E, Synthetic metabolism, Rats, Phospholipids chemical synthesis, Prostaglandins E, Synthetic pharmacology, Prostaglandins, Synthetic chemical synthesis

Published

1978

36. Stability of prostacyclin analogues: an unusual lack of reactivity in acid-catalyzed alkene hydration.

Author

Magill A, O'Yang C, and Powell MF

Subjects

Acids, Alkenes, Catalysis, Drug Stability, Epoprostenol pharmacology, Hydrogen-Ion Concentration, Kinetics, Lactones chemical synthesis, Prostaglandins, Synthetic chemical synthesis, Protons, Stereoisomerism, Temperature, Prostaglandins, Synthetic pharmacology

Abstract

Prostacyclin analogue 5 undergoes specific acid-catalyzed hydration (kH+ = 1.9 x 10(-7)M-1 sec-1 at 25 degrees C) and a pH-independent oxidation reaction (k0 = 1.2 x 10(-10) sec-1 at 25 degrees C) above pH approximately 5. The hydration reaction for 5 is much slower than for other structurally similar exocyclic alkenes, even though the rate-determining step is proton transfer. This slowness of reaction and an analysis of the pH-rate profile show that 5 does not exhibit significant intramolecular general acid catalysis, as does prostacyclin.

Published

1988

37. Uterine stimulant action of some omega-chain modified (+)-11-deoxyprostaglandins.

Author

Broughton BJ, Caton MP, Christmas AJ, Coffee EC, and Hambling DJ

Subjects

Animals, Constipation chemically induced, Cricetinae, Female, Gastrointestinal Motility drug effects, Luteolytic Agents, Male, Mice, Morphine antagonists & inhibitors, Prostaglandins, Synthetic chemical synthesis, Rats, Rats, Inbred Strains, Prostaglandins, Synthetic pharmacology, Uterine Contraction drug effects

Abstract

Rat uterine stimulant activity has been determined in vivo for a series of (+)-11-deoxyprostaglandins. The most active members of the series. 11-deoxy-15 methyl-PGE1, 11-deoxy-16,16-dimethyl - PGE1 and its 1-alcohol were 2-3 times more potent than PGE1. Gastrointestinal side effects assessed by the antagonism of morphine-induced constipation in the mouse, were generally relatively low with these compounds and consequently several members of the series had a more favourable relative selectivity than 16,16-dimethyl-PGE2 methyl ester.

Published

1981

38. New prostacyclin analogues.

Author

Bartmann W, Beck G, Knolle J, and Rupp RH

Subjects

Animals, Blood Pressure drug effects, Epoprostenol, Humans, Platelet Aggregation drug effects, Prostaglandins, Synthetic chemical synthesis

Published

1980

39. Designing prostacyclin analogues.

Author

Flohé L, Böhlke H, Frankus E, Kim SM, Lintz W, Loschen G, Michel G, Müller B, Schneider J, and Seipp U

Subjects

Adenosine Diphosphate antagonists & inhibitors, Anesthesia, Animals, Arachidonic Acid, Arachidonic Acids antagonists & inhibitors, Blood Pressure drug effects, Chemical Phenomena, Chemistry, Pharmaceutical, Chemistry, Physical, Cyclic AMP blood, Drug Stability, Horses, Humans, Hydroxyprostaglandin Dehydrogenases metabolism, In Vitro Techniques, Platelet Aggregation drug effects, Rats, Epoprostenol chemical synthesis, Prostaglandins, Synthetic chemical synthesis

Abstract

A series of prostacyclin analogues were synthesized and investigated for influence on blood pressure in rats, in vivo inhibition of platelet aggregation in rats, and in vitro inhibition of platelet aggregation in human platelet-rich plasma. The common feature of the analogues described is a replacement of C1-C4 of prostacyclin by a carboxyphenylene residue. The following structure-activity relationships were obtained. Only the meta-carboxyphenylene derivatives yield substantial prostacyclin activity. The 2,3,4-trinor-1,5-inter-m-phenylene prostacyclin analogues in contrast to the natural prototype are reasonably stable against hydrolysis of the enolether bond. The corresponding 2,3,4-trinor-1,5-inter-m-phenylene analogues of carbaprostacyclin have a somewhat lower specific activity but are superior in stability at acid pH values. With regard to the stereoisomerism at the delta 5 double bond, the Z-isomers of the oxa-cyclic prostacyclin series and the E-isomers of the carba-cyclic prostacyclin series are substantially more active than their counterparts. As with natural prostacyclin, the OH group at C15 has to be present in S-configuration. The "wrong" isomers do not inhibit prostacyclin-dependent effects. Resistance against 15-hydroxyprostaglandin dehydrogenase is achieved by substitutions at or near C15. Optimum specific activity combined with resistance against all known prostaglandin-activating enzymes is observed in prostacyclin and carbaprostacyclin analogues, in which the terminal n-pentyl residue is replaced by cyclohexyl. Duration of action, i.e. lowering of blood pressure in anaesthesized rats and inhibition of platelet aggregation in anaesthesized rats, was investigated with selected analogues in order to check the consequences of chemical and metabolic stabilization.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1983

40. 11,12-Secoprostaglandins. 3. 8-Alkylthio(sulfinyl and sulfonyl)-12-hydroxyalkanoic acids and related compounds.

Author

Smith RL, Bicking JB, Gould NP, Lee T, Robb CM, Kuehl FA Jr, Mandel LR, and Cragoe EJ Jr

Subjects

Animals, Binding, Competitive, Blood Pressure drug effects, Cyclic AMP biosynthesis, Dogs, Female, Gastric Juice metabolism, Humans, In Vitro Techniques, Lymphocytes drug effects, Mice, Ovary drug effects, Ovary metabolism, Prostaglandins E metabolism, Prostaglandins E pharmacology, Prostaglandins, Synthetic metabolism, Prostaglandins, Synthetic pharmacology, Psoriasis metabolism, Receptors, Prostaglandin metabolism, Skin drug effects, Skin metabolism, Structure-Activity Relationship, Prostaglandins, Synthetic chemical synthesis

Abstract

A series of 8-alkylthio(sulfinyl and sulfonyl)-12-hydroxyalkanoic acids which embody structural features of 11,12-secoprostaglandins was synthesized and evaluated for their ability to mimic the E series prostaglandins in stimulating cAMP formation in the mouse ovary and in binding to the rat lipocyte prostaglandin receptor. A key member of the series, 8-methylsulfonyl-12-hydroxyheptadecanoic acid, markedly stimulated cAMP formation at reasonable pharmacological concentrations, shows significant affinity for a prostaglandin receptor, and effectively inhibits antigen-induced lymphocyte transformation. In contrast, this compound is not a substrate for 15-hydroxyprostaglandin dehydrogenase, the major prostaglandin-metabolizing enzyme.

Published

1977

41. [Progress in modified prostaglandins].

Author

Wu YL

Subjects

Animals, Humans, Prostaglandins biosynthesis, Prostaglandins physiology, Structure-Activity Relationship, Prostaglandins, Synthetic chemical synthesis

Published

1984

42. N-(Methanesulfonyl)-16-phenoxyprostaglandincarboxamides: tissue-selective, uterine stimulants.

Author

Schaaf TK, Bindra JS, Eggler JF, Plattner JJ, Nelson AJ, Johnson MR, Constantine JW, Hess HJ, and Elger W

Subjects

Abortifacient Agents, Nonsteroidal chemical synthesis, Animals, Chemical Phenomena, Chemistry, Female, Guinea Pigs, Haplorhini, Hydroxyprostaglandin Dehydrogenases antagonists & inhibitors, In Vitro Techniques, Lung enzymology, Organ Specificity, Pregnancy, Prostaglandins, Synthetic pharmacology, Stimulation, Chemical, Structure-Activity Relationship, Prostaglandins, Synthetic chemical synthesis, Uterine Contraction drug effects

Abstract

In an effort to develop tissue-selective prostaglandin analogues resistant to the metabolic inactivating pathways of the natural materials, hybrid compounds modified both at C-1 with a sulfonimide moiety and in the n-amylcarbinol side chain with substituted phenoxy groups were synthesized and evaluated in a variety of in vitro models. Several of these analogues exhibited potent, tissue-selective, uterine stimulant activity, a finding subsequently confirmed in clinical studies with one member of this series, N-(methanesulfonyl)-16-phenoxy-omega-tetranor-PGE2-carboxamide (CP-34089/ZK-57671, sulprostone).

Published

1981

43. Synthesis of 11-deoxy-8-azaprostaglandin E1.

Author

Zoretic PA, Branchaud B, and Sinha ND

Subjects

Aza Compounds chemical synthesis, Methods, Oxidation-Reduction, Prostaglandins E, Prostaglandins, Synthetic chemical synthesis

Published

1977

44. Synthesis of (19r)-19-hydroxy-PGE and -PGF prostaglandins.

Author

Sih JC

Subjects

Methods, Molecular Conformation, Prostaglandins E chemical synthesis, Prostaglandins F chemical synthesis, Prostaglandins, Synthetic chemical synthesis

Published

1977

45. Synthesis of a highly potent analogue of prostacyclin, (-)-5-methyleneisocarbacyclin.

Author

Amemiya S, Koyama K, Saito S, and Kojima K

Subjects

Epoprostenol pharmacology, Humans, Platelet Aggregation drug effects, Prostaglandins, Synthetic pharmacology, Epoprostenol chemical synthesis, Prostaglandins, Synthetic chemical synthesis

Published

1986

46. Synthesis of putative prostaglandin D2 metabolites.

Author

Prakash C, Roberts LJ 2nd, Saleh S, Taber DF, and Blair IA

Subjects

Chemical Phenomena, Chemistry, Gas Chromatography-Mass Spectrometry, Methods, Prostaglandin D2, Prostaglandins D chemical synthesis, Prostaglandins D metabolism, Prostaglandins, Synthetic chemical synthesis

Published

1987

47. Synthesis of prostaglandin H2 (PGH2) and prostacyclin (PGI2) analogs: tetrathia-PGH2 and PGI2-ketal methyl ester.

Author

Nicolaou KC, Barnette WE, and Magolda RL

Subjects

Prostaglandins H chemical synthesis, Prostaglandins, Synthetic chemical synthesis, Epoprostenol chemical synthesis, Prostaglandin Endoperoxides, Synthetic chemical synthesis, Prostaglandins chemical synthesis

Published

1978

48. A new stable prostacyclin mimic, 7-oxoprostaglandin I2.

Author

Kovács G, Simonidesz V, Tömösközi I, Körmöczy P, Székely I, Papp-Behr A, Stadler I, Szekeres L, and Papp G

Subjects

Adenylyl Cyclase Inhibitors, Animals, Cattle, Chemical Phenomena, Chemistry, Dogs, Drug Stability, Epoprostenol pharmacology, Hemodynamics drug effects, Humans, In Vitro Techniques, Muscle Relaxation drug effects, Muscle, Smooth, Vascular drug effects, Platelet Aggregation drug effects, Prostaglandins, Synthetic pharmacology, Epoprostenol chemical synthesis, Prostaglandins chemical synthesis, Prostaglandins, Synthetic chemical synthesis

Published

1982

49. 11- and 15-deoxy-carboprostacyclins: hypothetic prostacyclin antagonists.

Author

Mongelli N, Magni O, Gandolfi C, Grossoni M, and Ceserani R

Subjects

Animals, Blood Pressure drug effects, Epoprostenol chemical synthesis, Epoprostenol pharmacology, Guinea Pigs, Hypertension physiopathology, Muscle Relaxation drug effects, Platelet Aggregation drug effects, Prostaglandins, Synthetic pharmacology, Rats, Rats, Inbred Strains, Structure-Activity Relationship, Epoprostenol antagonists & inhibitors, Prostaglandin Antagonists, Prostaglandins, Synthetic chemical synthesis

Published

1983

50. Stereocontrolled synthesis of 7-oxabicyclo (2.2.1) heptane prostaglandin analogs as thromboxane A2 antagonists.

Author

Sprague PW, Heikes JE, Harris DN, and Greenberg R

Subjects

Animals, Arachidonic Acids pharmacology, Blood Platelets enzymology, Bridged Bicyclo Compounds pharmacology, Guinea Pigs, Humans, Lung drug effects, Methods, Platelet Aggregation drug effects, Prostaglandins, Synthetic pharmacology, Structure-Activity Relationship, Thromboxane-A Synthase antagonists & inhibitors, Bridged Bicyclo Compounds chemical synthesis, Bridged-Ring Compounds chemical synthesis, Prostaglandins, Synthetic chemical synthesis, Thromboxane A2 pharmacology, Thromboxanes pharmacology

Published

1980