Your search keyword '"Androstadienes chemistry"' showing total 25 results

1. New steroidal oxazolines, benzoxazoles and benzimidazoles related to abiraterone and galeterone.

Author

Latysheva AS, Zolottsev VA, Veselovsky AV, Scherbakov KA, Morozevich GE, Pokrovsky VS, Novikov RA, Timofeev VP, Tkachev YV, and Misharin AY

Subjects

Androstadienes chemical synthesis, Androstadienes chemistry, Androstenes chemical synthesis, Androstenes chemistry, Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Benzimidazoles chemical synthesis, Benzimidazoles chemistry, Benzoxazoles chemistry, Cell Proliferation drug effects, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Humans, Models, Molecular, Molecular Conformation, Oxazoles chemistry, PC-3 Cells, Stereoisomerism, Structure-Activity Relationship, Tumor Cells, Cultured, Androstadienes pharmacology, Androstenes pharmacology, Antineoplastic Agents pharmacology, Benzimidazoles pharmacology, Benzoxazoles pharmacology, Oxazoles pharmacology

Abstract

Seven new oxazoline, benzoxazole and benzimidazole derivatives were synthesized from 3β-acetoxyandrosta-5,16-dien-17-carboxylic, 3β-acetoxyandrost-5-en-17β-carboxylic and 3β-acetoxypregn-5-en-21-oic acids. Docking to active site of human 17α-hydroxylase/17,20-lyase revealed that all oxazolines, as well as benzoxazoles and benzimidazoles comprising Δ 16 could form stable complexes with enzyme, in which steroid moiety is positioned similarly to that of abiraterone and galeterone, and nitrogen atom coordinates heme iron, while 16,17-saturated benzoxazoles and benzimidazoles could only bind in a position where heterocycle is located nearly parallel to heme plane. Modeling of the interaction of new benzoxazole and benzimidazole derivatives with androgen receptor revealed the destabilization of helix 12, constituting activation function 2 (AF2) site, by mentioned compounds, similar to one induced by known antagonist galeterone. The synthesized compounds inhibited growth of prostate carcinoma LNCaP and PC-3 cells at 96 h incubation; the potency of 2'-(3β-hydroxyandrosta-5,16-dien-17-yl)-4',5'-dihydro-1',3'-oxazole and 2'-(3β-hydroxyandrosta-5,16-dien-17-yl)-benzimidazole was superior and could inspire further investigations of these compounds as potential anti-cancer agents., (Copyright © 2019 Elsevier Inc. All rights reserved.)

Published

2020

2. Quinone-related hexacyclic by-products in the production process of exemestane.

Author

Giovenzana GB, Masciocchi N, Negri R, Palmisano G, Penoni A, and Toma L

Subjects

Magnetic Resonance Spectroscopy, Mass Spectrometry, Molecular Structure, X-Ray Diffraction, Androstadienes chemistry, Benzoquinones chemistry

Abstract

Exemestane, a 3rd-generation aromatase inhibitor, is clinically used in the treatment of breast cancer in postmenopausal women. The key step of the industrial synthetic process, i.e., a dehydrogenation to introduce the Δ 1 -unsaturation, is normally performed with quinones such as p-chloranil or DDQ. We observed the formation of two different hexacyclic by-products, depending on the quinone used in the oxidation step. These compounds arise from an initial [4+2] cycloaddition between the precursor 6-methylenandrost-4-ene-3,17-dione and the quinone reagent, followed by a twofold dehydrohalogenation (with p-chloranil) or dehydrogenation (with DDQ). The structures of these unprecedented hexacyclic adducts were determined by a combination of mass spectrometry, NMR techniques and crystallographic analysis., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017

3. Synthetic approaches towards the multi target drug spironolactone and its potent analogues/derivatives.

Author

Larik FA, Saeed A, Shahzad D, Faisal M, El-Seedi H, Mehfooz H, and Channar PA

Subjects

Aldosterone chemistry, Androstadienes chemistry, Androstenes chemistry, Animals, Canrenone chemistry, Chloranil chemistry, Dehydroepiandrosterone chemistry, Eplerenone, Humans, Molecular Structure, Receptors, Mineralocorticoid metabolism, Spironolactone metabolism, Aldosterone chemical synthesis, Canrenone chemical synthesis, Spironolactone analogs & derivatives, Spironolactone chemical synthesis, Spironolactone chemistry

Abstract

Spironolactone is a well-known multi-target drug and is specifically used for the treatment of high blood pressure and heart failure. It is also used for the treatment of edema, cirrhosis of the liver, malignant, pediatric, nephrosis and primary hyperaldosteronism. Spironolactone in association with thiazide diuretics treats hypertension and in association with furosemide treats bronchopulmonary dyspepsia. The therapeutic mechanism of action of spironolactone involves binding to intracellular mineralocorticoids receptors (MRs) in kidney epithelial cells, thereby inhibiting the binding of aldosterone. Since its first synthesis in 1957 there are several synthetic approaches have been reported throughout the years, Synthetic community has devoted efforts to improve the synthesis of spironolactone and to synthesize its analogues and derivatives. This review aims to provide comprehensive insight for the synthetic endeavors devoted towards the synthesis of a versatile drug spironolactone and its analogues/derivatives., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017

4. Microbial-catalysed derivatization of anti-cancer drug exemestane and cytotoxicity of resulting metabolites against human breast adenocarcinoma cell line (MCF-7) in vitro.

Author

Baydoun S, Wahab AT, Bano S, Imad R, and Choudhary MI

Subjects

Androstadienes chemistry, Antineoplastic Agents chemistry, Aspergillus niger metabolism, Cell Survival drug effects, Cunninghamella metabolism, Fermentation, Gibberella metabolism, Humans, MCF-7 Cells, Molecular Structure, Androstadienes metabolism, Androstadienes pharmacology, Antineoplastic Agents metabolism, Antineoplastic Agents pharmacology, Breast Neoplasms metabolism

Abstract

Structural transformation of anticancer drug exemestane (1) with fungi Cunninghamella blakesleeana (ATCC 8688A), Curvularia lunata (ATCC 12017), Aspergillus niger (ATCC 10549), and Gibberella fujikuroi (ATCC 10704) yielded eleven metabolites 2-12, in which 2 and 8 were identified as new. Their structures were characterized as 6-methylene-5α-androstane-3β,16β,17β-triol (2), 17β-hydroxy-6-methyleneandrosta-4-ene-3-one (3), 6α-spiroxirandrost-4-ene-3,17-dione (4), 6-methyleneandrosta-4-ene-3,17-dione (5), 6β,17β-dihydroxyandrost-4-en-3-one (6), 17β-hydroxy-6α-spiroxirandrost-1,4-diene-3-one (7), 17β-hydroxy-6α-hydroxymethylandrosta-1,4-dien-3-one (8), 6α-hydroxymethylandrosta-1,4-diene-3,17-dione (9), 17β-hydroxy-6-methyleneandrosta-1,4-diene-3,16-dione (10), 6α-hydroxy-4-androstene-3,17-dione (11), and 6α-hydroxymethylandrost-4-ene-3,17-dione (12). Substrate 1, and its transformed products were evaluated for their cytotoxicity against breast cancer cell line (MCF-7). Compound 3 was found to be moderately active with an IC 50 of 33.43±4.01μM, in comparison to the standard anti-cancer drug, doxorubicin (IC 50 =0.92±0.1μM)., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016

5. Increased yield of biotransformation of exemestane with β-cyclodextrin complexation technique.

Author

Li G, Li F, Deng L, Fang X, Zou H, Xu K, Li T, and Tan G

Subjects

2-Hydroxypropyl-beta-cyclodextrin, Arthrobacter metabolism, Biotransformation, Solubility, Water chemistry, Androstadienes chemistry, Androstadienes metabolism, Antineoplastic Agents chemistry, Antineoplastic Agents metabolism, beta-Cyclodextrins chemistry

Abstract

In this study, 6-methylenandrosta-4-ene-3,17-dione and Hydroxypropyl-β-cyclodextrin (HP-β-CD) were used to form a complex, which could be then biotransformed by Arthrobacter simplex ATCC6946 to obtain the antitumor drug exemestane. The complex was analyzed by UV, DSC and TG techniques, while the products were analyzed by HPLC, NMR and MS. These results confirmed that the β-cyclodextrin not only improved the water-solubility of 6-methylenandrosta-4-ene-3,17-dione, but also greatly enhanced the biocompatibility during the biotransformation process. This result may be applied to other precursors which have poor aqueous solubility in the biotransformation processes., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

6. Detection, synthesis and characterization of metabolites of steroid hormones conjugated with cysteine.

Author

Fabregat A, Kotronoulas A, Marcos J, Joglar J, Alfonso I, Segura J, Ventura R, and Pozo OJ

Subjects

Androstadienes blood, Androstadienes chemistry, Biotransformation physiology, Chromatography, Liquid, Cysteine blood, Cysteine chemistry, Glutathione blood, Glutathione chemistry, Humans, Hydrocortisone blood, Hydrocortisone chemistry, Hydroxides chemistry, Metabolic Detoxication, Phase II physiology, Models, Molecular, Potassium Compounds chemistry, Progesterone blood, Progesterone chemistry, Tandem Mass Spectrometry, Testosterone blood, Testosterone chemistry, Androstadienes urine, Cysteine urine, Glutathione urine, Hydrocortisone urine, Progesterone urine, Testosterone urine

Abstract

The occurrence of several polyunsaturated testosterone related compounds (including 4,6-androstadien-3,17-dione and 4,6-androstadien-17β-ol-3-one) in urine after alkaline treatment of the sample has been recently reported. Although several experiments seem to indicate that they are testosterone metabolites, their origin is still unknown. In this study, it is demonstrated that these metabolites are produced from the degradation of cysteine conjugates. Several testosterone metabolites conjugated with cysteine have been synthesized and characterized by NMR techniques. Their detection in human urine has been performed by LC-MS/MS. The acquisition of several transitions in the SRM mode and the comparison between ion ratios and retention times allowed for the unequivocal confirmation of the presence of cysteine conjugates in urine. The analysis of urine samples collected after testosterone administration confirmed that synthesized cysteine conjugates are testosterone metabolites. The fact that these conjugates result in polyunsaturated compounds in urine after alkaline treatment was demonstrated by fraction collection and alkaline treatment of each fraction. Besides, the presence of these metabolites was also confirmed in human plasma. The formation of these metabolites implies an unreported metabolic biotransformation: 6,7-dehydrogenation as phase I metabolism followed by conjugation with glutathione and subsequent transformation to cysteine conjugates. Finally, the existence of similar metabolites for cortisol and progesterone was also confirmed by LC-MS/MS indicating that the presented metabolic pathway is not exclusively active in androgens, but common to progestagens and glucocorticoids., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2013

7. Synthesis and biological evaluations of putative metabolically stable analogs of VN/124-1 (TOK-001): head to head anti-tumor efficacy evaluation of VN/124-1 (TOK-001) and abiraterone in LAPC-4 human prostate cancer xenograft model.

Author

Bruno RD, Vasaitis TS, Gediya LK, Purushottamachar P, Godbole AM, Ates-Alagoz Z, Brodie AM, and Njar VC

Subjects

Androstenes, Animals, Antineoplastic Agents chemistry, Cell Line, Tumor, Cell Proliferation drug effects, Clinical Trials, Phase III as Topic, Drug Combinations, Estradiol analogs & derivatives, Estradiol pharmacology, Humans, Male, Mice, Mice, SCID, Norethindrone pharmacology, Receptors, Androgen metabolism, Steroid 17-alpha-Hydroxylase antagonists & inhibitors, Structure-Activity Relationship, Testosterone analogs & derivatives, Testosterone pharmacology, Xenograft Model Antitumor Assays, Androstadienes chemistry, Androstadienes therapeutic use, Androstenols chemistry, Androstenols therapeutic use, Antineoplastic Agents chemical synthesis, Antineoplastic Agents therapeutic use, Benzimidazoles chemistry, Benzimidazoles therapeutic use, Prostatic Neoplasms drug therapy

Abstract

In a continuing study of our clinical candidate 5 VN/124-1 (TOK-001) and analogs as potential agents for prostate cancer therapy, putative metabolites (10, 15 and 18) of compound 5 were rationally designed and synthesized. However, none of these agents were as efficacious as 5 in several in vitro studies. Using western blot analysis, we have generated a preliminary structure-activity relationship (SAR) of 5 and related analogs as androgen receptor ablative agents (ARAAs). In vivo using the androgen-dependent LAPC-4 prostate cancer xenograft model, we demonstrated for the first time that 5 is more efficacious than the 17-lyase inhibitor 3 (abiraterone)/4 (abiraterone acetate) that is currently in phase III clinical trials. In our desire to optimize the potency of 5, compounds 6 (3ξ-fluoro-) and 9 (3β-sulfamate-) designed to increase the stability and oral bioavailability of 5, respectively were evaluated in vivo. We showed, that on equimolar basis, compound 6 was ∼2-fold more efficacious versus LAPC-4 xenografts than 5, but the toxicity observed with 6 is of concern. These studies further demonstrate the efficacy of 5 in a clinically relevant prostate cancer model and justify its current clinical development as a potential treatment of prostate cancer., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

8. Binding features of steroidal and nonsteroidal inhibitors.

Author

Hong Y, Rashid R, and Chen S

Subjects

Amino Acids chemistry, Androgens chemistry, Androstadienes chemistry, Androstenedione chemistry, Aromatase genetics, Binding Sites, Breast Neoplasms chemistry, Catalytic Domain, Estrogens biosynthesis, Estrone chemistry, Female, Humans, Letrozole, Mutagenesis, Site-Directed, NADPH-Ferrihemoprotein Reductase chemistry, Neoplasms, Hormone-Dependent chemistry, Nitriles chemistry, Protein Conformation, Structure-Activity Relationship, Triazoles chemistry, Aromatase chemistry, Aromatase Inhibitors chemistry

Abstract

Aromatase is the rate-limiting enzyme in estrogen biosynthesis. As a cytochrome P450, it utilizes electrons from NADPH-cytochrome P450 reductase (CPR) to produce estrogen from androgen. Estrogen is a key factor in the promotion of hormone-dependent breast cancer growth. Aromatase inhibitors (AIs) are drugs that block estrogen synthesis, and are widely used to treat estrogen-dependent breast cancer. Structure-function experiments have been performed to study how CPR and AIs interact with aromatase to further the understanding of how these drugs elicit their effects. Our studies have revealed a strong interaction between aromatase and CPR, and that the residue K108 is situated in a region important to the interaction of aromatase with CPR. The published X-ray structure of aromatase indicates that the F221, W224 and M374 residues are located in the active site. Our site-directed mutagenesis experiments confirm their importance in the binding of the androgen substrate as well as AIs, but these residues interact differently with steroidal inhibitors (exemestane) and non-steroidal inhibitors (letrozole and anastrozole). Furthermore, our results predict that the residue W224 also participates in the mechanism-based inhibition of exemestane, as time-dependent inhibition is eliminated with mutation on this residue. Together with previous research from our laboratory, this study confirms that W224, E302, D309 and S478 are important active site residues involved in the suicide mechanism of exemestane against aromatase., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

9. The reaction of azoles with 17-chloro-16-formylandrosta-5,16-dien-3β-yl-acetate: synthesis and structural elucidation of novel 16-azolylmethylene-17-oxoandrostanes.

Author

Moreira VM, Salvador JA, Beja AM, and Paixão JA

Subjects

Androsterone chemical synthesis, Androsterone chemistry, Crystallography, X-Ray, Indoles chemical synthesis, Isomerism, Molecular Conformation, Molecular Structure, Pyrroles chemical synthesis, Androstadienes chemistry, Androsterone analogs & derivatives, Azoles chemistry, Indoles chemistry, Pyrroles chemistry

Abstract

The synthesis and structural elucidation, by 1D and 2D NMR and X-ray diffraction techniques, of novel E/Z 16-azolylmethylene-17-oxoandrostanes 2-9 prepared from the Vilsmeier-Hack reaction product 17-chloro-16-formylandrosta-5,16-dien-3β-yl acetate 1 is reported. The reaction proceeds with pyrrole and pyrrole-alike nitrogen heterocycles such as 7-azaindole, indole, and 3-methylindole, in DMF, at 80°C, in the presence of K(2)CO(3), and allowed the attachment of privileged heterocyclic moieties, through the nitrogen atom to the steroid core at C16 via a methine carbon bridge, which is unprecedented in the literature and of potential synthetic and biological interest. Considerations on the possible reaction mechanism are included. All the synthesized compounds are new and are currently being tested for biological activities., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

10. Probing the binding pocket of the active site of aromatase with 2-phenylaliphatic androsta-1,4-diene-3,17-dione steroids.

Author

Takahashi M, Yamashita K, and Numazawa M

Subjects

Androstadienes chemistry, Androstenedione chemistry, Androstenedione metabolism, Aromatase Inhibitors chemistry, Enzyme Activation drug effects, Humans, Kinetics, Models, Molecular, Substrate Specificity drug effects, Time Factors, Androstadienes pharmacology, Aromatase chemistry, Aromatase metabolism, Aromatase Inhibitors pharmacology, Catalytic Domain

Abstract

A series of 2-phenylaliphatic-substituted androsta-1,4-diene-3,17-diones (6) as well as their androstenedione derivatives (5) were synthesized as aromatase inhibitors to gain insights of structure-activity relationships of varying the alkyl moiety (C(1) to C(4)) of the 2-phenylaliphatic substituents as well as introducing a methyl- or trifluoromethyl function to p-position of a phenethyl moiety to the inhibitory activity. The inhibitors examined showed a competitive type inhibition. The 2-phenpropylandrosta-1,4-diene 6c was the most powerful inhibitor (K(i): 16.1nM) among them. Compounds 6c along with the phenethyl derivative 6b caused a time-dependent inactivation of aromatase (k(inact): 0.0293 and 0.0454min(-1) for 6b and 6c, respectively). The inactivation was prevented by the substrate androstenedione, and no significant effect of l-cysteine on the inactivation was observed in each case. Molecular docking of the phenpropyl compound 6c to aromatase was conducted to demonstrate that the phenpropyl group orients to a hydrophobic binding pocket in the active site to result in the formation of thermodynamically stable enzyme-inhibitor complex.

Published

2010

11. A new steroidal 5,7-diene derivative, 3beta-hydroxyandrosta-5,7-diene-17beta-carboxylic acid, shows potent anti-proliferative activity.

Author

Kim TK, Chen J, Li W, Zjawiony J, Miller D, Janjetovic Z, Tuckey RC, and Slominski A

Subjects

Androstadienes chemical synthesis, Androstadienes chemistry, Animals, Cells, Cultured, Cricetinae, Cricetulus, Cyclin E genetics, Cyclin E metabolism, ErbB Receptors genetics, ErbB Receptors metabolism, HL-60 Cells, Humans, Keratinocytes cytology, Keratinocytes drug effects, Keratinocytes metabolism, Melanocytes cytology, Melanocytes drug effects, Melanocytes metabolism, Molecular Structure, Nuclear Magnetic Resonance, Biomolecular, Oncogene Proteins genetics, Oncogene Proteins metabolism, Protein Precursors genetics, Protein Precursors metabolism, Proto-Oncogene Proteins c-bcl-2 genetics, Proto-Oncogene Proteins c-bcl-2 metabolism, Androstadienes pharmacology, Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Carboxylic Acids chemical synthesis, Carboxylic Acids chemistry, Carboxylic Acids pharmacology, Cell Proliferation drug effects, Steroids chemical synthesis, Steroids chemistry, Steroids pharmacology

Abstract

The new steroidal 5,7-diene, 3beta-hydroxyandrosta-5,7-diene-17beta-carboxylic acid (17-COOH-7DA), was synthesized from 21-acetoxypregnenolone, with the oxidative cleavage of the side chain being dependent on the presence of oxygen. In human epidermal (HaCaT) keratinocytes, 17-COOH-7DA inhibited proliferation in a dose-dependent manner, starting at a dose as low as 10(-11) M. This inhibition was accompanied by decreased expression of epidermal growth factor receptor, bcl2 and cyclin E2 mRNAs and by increased expression of involucrin mRNA. Inhibition of proliferation was associated with slowing of the cell cycle in G1/G0 phases but not with cell death. 17-COOH-7DA was significantly more potent than pregnenolone, 17-COOH-pregnenolone, 17-COOCH(3)-7DA and calcitriol. 17-COOH-7DA also inhibited proliferation of normal human epidermal melanocytes and human and hamster melanoma lines, however, with lower potency than for keratinocytes. In normal human dermal fibroblasts 17-COOH-7DA stimulated proliferation in serum-free media but inhibited it in the presence of 5% serum. 17-COOH-7DA inhibited cell colony formation of human and hamster melanoma cells, and induced monocyte-like differentiation of human HL60 leukemia cells. Thus, the new steroidal 5,7-diene, 17-COOH-7DA, can serve as an inhibitor of proliferation of normal keratinocytes and normal and malignant melanocytes, as a condition-dependent regulator of fibroblast proliferation and a stimulator of leukemia cell differentiation., (Copyright 2009 Elsevier Inc. All rights reserved.)

Published

2010

12. Computer-aided structure analysis of an epimerized dehydroepiandrosterone derivative and its biological effect in a model of reactive gliosis.

Author

Hoyk Z, Csákvári E, Szájli A, Kóti J, Paragi G, Gyenes A, Wölfling J, Pfoh R, Rühl S, and Párducz A

Subjects

Androstadienes chemistry, Androstadienes metabolism, Androstenedione analogs & derivatives, Androstenedione chemistry, Androstenedione metabolism, Animals, Aromatase chemistry, Aromatase metabolism, Aromatase Inhibitors chemistry, Aromatase Inhibitors metabolism, Crystallography, X-Ray, Dehydroepiandrosterone chemistry, Dehydroepiandrosterone pharmacology, Glial Fibrillary Acidic Protein metabolism, Gliosis pathology, Male, Molecular Sequence Data, Molecular Structure, Rats, Rats, Wistar, Dehydroepiandrosterone analogs & derivatives, Dehydroepiandrosterone therapeutic use, Gliosis drug therapy

Abstract

The naturally occurring steroid dehydroepiandrosterone (DHEA) is reported to reduce glial fibrillary acidic protein (GFAP) overexpression in a model of reactive gliosis due to its conversion to estradiol by the enzyme aromatase. In the present study we examined the biological effect of a new epimerized derivative of DHEA, 16alpha-iodomethyl-13alpha-dehydroepiandrosterone derivative (16alpha-iodomethyl-13alpha-DHEAd, 16alpha-iodomethyl-13alpha-androst-5-en-3beta,17beta-diol), using the same model system, and compared the 3D structure of this molecule with that of DHEA and two steroidal type aromatase inhibitors, formestane and exemestane. The synthetic compound, in contrast to the reported effect of DHEA, was able to reduce GFAP overexpression only if the enzyme aromatase was inhibited. Data obtained from computational calculations fortified by X-ray crystallography revealed that contrary to the nearly planar sterane framework of DHEA, the synthetic derivative 16alpha-iodomethyl-13alpha-DHEAd has a bent sterane skeleton, resulting in a 3D structure that is similar to that of formestane or exemestane. Moreover, 16alpha-iodomethyl-13alpha-DHEAd resulted to be metabolically more stable than DHEA. The results suggest that epimerization of the sterane skeleton of DHEA inclines the plane of the D ring, leading to a significantly altered biological activity. The synthetic molecule has a DHEA-like effect on GFAP overexpression when the enzyme aromatase is inhibited and the naturally occurring DHEA is ineffective in this respect. On the other hand, based on their structural similarity it can be hypothesized that 16alpha-iodomethyl-13alpha-DHEAd applied alone might have a biological effect similar to that of formestane or exemestane., (Copyright 2010 Elsevier Inc. All rights reserved.)

Published

2010

13. Liquid chromatography-tandem mass spectrometry analysis of urinary fluticasone propionate-17beta-carboxylic acid for monitoring compliance with inhaled-fluticasone propionate therapy.

Author

Korpi-Steiner NL, Netzel BC, Seegmiller JC, Hagan JB, and Singh RJ

Subjects

Adult, Androstadienes chemistry, Androstadienes metabolism, Androstadienes pharmacokinetics, Anti-Allergic Agents administration & dosage, Anti-Allergic Agents chemistry, Anti-Allergic Agents urine, Drug Monitoring, Female, Fluticasone, Humans, Male, Metabolic Clearance Rate, Middle Aged, Molecular Structure, Reproducibility of Results, Androstadienes urine, Asthma drug therapy, Chromatography, Liquid methods, Tandem Mass Spectrometry methods

Abstract

Background: Inhaled corticosteroids including fluticasone propionate (FP) are the most effective treatment for persistent-asthma. Noncompliance ranging from 20% to 80% of treated patients is associated with substantial health care costs, morbidity and fatalities. A noninvasive test to assess FP treatment compliance is needed. The major metabolite of FP is FP-17beta-carboxylic acid (FP17betaCA) and is excreted in urine. This study demonstrates the development of a liquid chromatography-tandem mass spectrometry (LC-MS/MS) assay to measure FP17betaCA in urine and evaluation of FP17betaCA urinary elimination., Experimental: Fluorometholone was used as the internal standard. After acetonitrile precipitation, samples were extracted with dichloromethane, washed and dried. Reconstituted extract (60 microL) was subjected to reversed-phase chromatography and positive-ion mode LC-MS/MS analysis. Assay precision, linearity, recovery and sample stability were determined. Elimination evaluation included measurement of FP17betaCA in urine collected daily from human subjects before (day 1), during treatment (days 2-5; dose FP-110 microg 2 puffs/day), and following cessation of FP therapy (days 6-14; n=4)., Results: Linear range of the FP17betaCA assay was 10.3-9510pg/mL. Limit of quantitation (LOQ) was 10.3 pg/mL and recovery ranged from 85.8% to 111.9%. Inter-assay CVs were 7.4-12.0% for FP17betaCA concentrations of 11.1-5117 pg/mL. Urine FP17betaCA was absent in subjects prior to FP therapy, detectable (180-1991 ng FP17betaCA/g creatinine) throughout the dosing period and reached below the LOQ at 6 days after therapy cessation., Conclusions: Measurement of FP17betaCA by LC-MS/MS has acceptable analytical performance for clinical use. These data support the clinical utility of measuring FP17betaCA in urine to monitor patient compliance with FP therapy.

Published

2010

14. New-D-homoandrost-4,6-diene derivatives as potent progesterone receptor antagonist.

Author

Cabeza M, García-Lorenzana M, Garcés M, Heuze I, Teran N, and Bratoeff E

Subjects

Androgen Receptor Antagonists, Androstadienes metabolism, Androstenedione analogs & derivatives, Androstenedione chemistry, Androstenedione pharmacology, Animals, Binding, Competitive, Corpus Luteum drug effects, Corpus Luteum metabolism, Endometrium drug effects, Endometrium metabolism, Female, Gonadotropin-Releasing Hormone pharmacology, Homosteroids chemistry, Homosteroids pharmacology, Hormone Antagonists chemistry, Hormone Antagonists metabolism, Hormone Antagonists pharmacology, Male, Mice, Mifepristone chemistry, Mifepristone metabolism, Mifepristone pharmacology, Molecular Structure, Ovary drug effects, Ovary metabolism, Phenylacetates chemistry, Progesterone chemistry, Progesterone metabolism, Progesterone pharmacology, Rabbits, Rats, Receptors, Androgen metabolism, Receptors, Progesterone metabolism, Structure-Activity Relationship, Uterus drug effects, Uterus metabolism, Androstadienes chemistry, Androstadienes pharmacology, Receptors, Progesterone antagonists & inhibitors

Abstract

The aim of this study was to synthesize three different D-homoandrostadiene derivatives (2-4) and study their biological activity. We carried out in vivo and in vitro experiments using female cycling mice, which were synchronized for estrus with luteinizing hormone-releasing hormone (LHRH) and injected with the steroidal compounds. It was also determined the binding of these compounds to the progesterone receptors (PR). Since these steroids have a new D-homoandrostandienone skeleton in their molecular structure, it was of interest also to study their binding to the androgen receptors (AR). After LHRH treatment, the mice of the control group showed the presence of 14+/-4 corpus lutea in the ovary whereas the animals treated with steroids 2-4, with RBAs of 100%, exhibited 11+/-7, 12+/-2, and 10+/-4 respectively. As a result of this study, it is evident that these steroids did not inhibit the ovulation in these animals. The uterus of the control group, showed the typical progestational activity with an enlarged endometrial thickness with a secretory activity. However, the endometrium of the mice treated with steroids 2-4 did not show an enlargement of the endometrium and no secretory activity could be detected. This fact indicates that compounds 2-4 had antagonistic activity in this tissue. The overall data show that steroids 2-4 are antagonists of the PR. However, they do not bind to the AR. These results also demonstrate that 2-4 have an antiprogestational activity in vivo, but do not decrease the number of corpus lutea in the ovary of mice treated with LHRH.

Published

2010

15. Criteria to distinguish between natural situations and illegal use of boldenone, boldenone esters and boldione in cattle 2. Direct measurement of 17beta-boldenone sulpho-conjugate in calf urine by liquid chromatography--high resolution and tandem mass spectrometry.

Author

Destrez B, Bichon E, Rambaud L, Courant F, Monteau F, Pinel G, Antignac JP, and Le Bizec B

Subjects

Anabolic Agents chemistry, Anabolic Agents metabolism, Anabolic Agents pharmacokinetics, Androstadienes chemistry, Androstadienes metabolism, Androstadienes pharmacokinetics, Animal Feed, Animals, Chromatography, High Pressure Liquid, Glucuronides metabolism, Horses, Humans, Male, Metabolic Clearance Rate, Reproducibility of Results, Solid Phase Extraction, Sulfates administration & dosage, Sulfates chemistry, Sulfates metabolism, Tandem Mass Spectrometry, Testosterone administration & dosage, Testosterone chemistry, Testosterone metabolism, Testosterone pharmacokinetics, Testosterone urine, Anabolic Agents urine, Androstadienes urine, Cattle urine, Esters chemistry, Substance Abuse Detection, Sulfates urine, Testosterone analogs & derivatives

Abstract

Boldenone is banned in the European Union (Directive 96/22/EC) as growth promoter for meat producing animals. Boldione (ADD), boldenone and boldenone esters (mainly the undecylenate form) are commercially available as anabolic preparations, either to the destination of human, horse or cattle. Since the late 90s, the natural occurrence of boldenone metabolites has been reported in cattle. According to EU regulation, the unambiguous demonstration of boldenone administration in bovine urine should be provided on the basis of boldenone identification in the corresponding conjugate fraction. An analytical method has been developed and validated according to current standards with main concern to the measurement of intact 17beta-boldenone-sulphate. The analytical procedure included direct extraction-purification of target analyte on octadecylsilyl cartridges and direct detection of phase II metabolite by liquid chromatography (negative electrospray), tandem mass spectrometry (QqQ) or high resolution mass spectrometry (Orbitrap). Decision limit (CCalpha) and detection capability (CCbeta) were respectively 0.2 microg L(-1) and 0.4 microg L(-1) on triple quadrupole and 0.1 microg L(-1) and 0.2 microg L(-1) on hybrid system. The method was successfully applied to the analysis of incurred samples collected in different experiments. 17beta-Boldenone-sulphate was measurable up to 36h after oral administration of boldione, and 30 days after 17beta-boldenone undecylenate intra-muscular injection. This conjugate form was never detected in non-treated animals, confirming its status of definitive candidate marker for boldenone administration in calf.

Published

2009

16. The synthesis of 13alpha-androsta-5,16-diene derivatives with carboxylic acid, ester and carboxamido functionalities at position-17 via palladium-catalyzed carbonylation.

Author

Acs P, Takács A, Szilágyi A, Wölfling J, Schneider G, and Kollár L

Subjects

Catalysis, Amides chemistry, Androstadienes chemical synthesis, Androstadienes chemistry, Carboxylic Acids chemistry, Esters chemistry, Palladium chemistry

Abstract

17-Alkoxycarbonyl- and 17-carboxamido-3beta-hydroxy-13alpha-androsta-5,16-diene derivatives were synthetized in high yields in the palladium-catalyzed carbonylation reactions of the corresponding 3beta-hydroxy-17-iodo-13alpha-androsta-5,16-diene. This substrate with a 17-iodo-16-ene functionality was obtained from the 17-keto derivative via its 17-hydrazone, which was treated with iodine in the presence of a base (1,1,3,3-tetramethylguanidine). 17-Carboxamides were obtained by chemoselective aminocarbonylation through the use of amines, including amino acid esters, as N-nucleophiles. The 17-methoxycarbonyl-16-ene derivative was synthetized by using methanol as O-nucleophile. The parent compound of this series, the 17-carboxylic acid derivative, was formed in the presence of water via hydroxycarbonylation.

Published

2009

17. Synthesis of exemestane labelled with (13)C.

Author

Fontana E, Pignatti A, Giribone D, and Di Salle E

Subjects

Androstadienes chemistry, Androstadienes isolation & purification, Testosterone chemistry, Androstadienes chemical synthesis, Carbon Isotopes, Isotope Labeling methods

Abstract

The synthesis of exemestane Aromasin, an irreversible steroidal aromatase inhibitor, specifically labelled with (13)C is reported. The preparation of [(13)C(3)]exemestane was achieved according to an eight-step procedure starting from the commercially available testosterone.

Published

2008

18. Facile synthesis of 11-carboxamido-androst-4,9(11)-dienes via palladium-catalyzed aminocarbonylation.

Author

Acs P, Jakab B, Takács A, and Kollár L

Subjects

Alkenes, Androstadienes chemistry, Catalysis, Molecular Conformation, Molecular Structure, Polyenes chemistry, Steroids chemistry, Androstadienes chemical synthesis, Carbon chemistry, Palladium chemistry, Polyenes chemical synthesis, Steroids chemical synthesis

Abstract

11-Carboxamido-androst-4,9(11)-dienes were synthesized from the corresponding 11-iodo-androst-4,9(11)-diene derivative in palladium-catalyzed aminocarbonylation reaction under mild reaction conditions. The synthesis of the iodo-alkene substrate is based on the transformation of the 11-keto derivative to hydrazone, which was treated with iodine in the presence of a base (1,1,3,3-tetramethyl guanidine). The 11-carboxamides were synthesized in moderate to high isolated yields by using simple alkyl/arylamines or amino acid methylesters as N-nucleophiles. The highly active palladium catalysts enable the homogeneous catalytic functionalization at one of the most hindered position (C-11) of the steroidal skeleton.

Published

2007

19. Microbial transformation of 17alpha-ethynyl- and 17alpha-ethylsteroids, and tyrosinase inhibitory activity of transformed products.

Author

Choudhary MI, Sultan S, Khan MT, and Rahman AU

Subjects

Androstadienes chemistry, Androstadienes pharmacology, Biotransformation drug effects, Cosmetics chemistry, Cosmetics metabolism, Cosmetics pharmacology, Enzyme Activation drug effects, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Ethisterone chemistry, Ethisterone pharmacology, Fungal Proteins metabolism, Humans, Hyperpigmentation drug therapy, Melanins biosynthesis, Monophenol Monooxygenase metabolism, Oxidation-Reduction drug effects, Testosterone metabolism, Testosterone pharmacology, Acremonium enzymology, Androstadienes metabolism, Enzyme Inhibitors metabolism, Ethisterone metabolism, Fungal Proteins antagonists & inhibitors, Monophenol Monooxygenase antagonists & inhibitors, Mucorales enzymology, Testosterone analogs & derivatives

Abstract

The microbial transformation of the 17alpha-ethynyl-17beta-hydroxyandrost-4-en-3-one (1) (ethisterone) and 17alpha-ethyl-17beta-hydroxyandrost-4-en-3-one (2) by the fungi Cephalosporium aphidicola and Cunninghamella elegans were investigated. Incubation of compound 1 with C. aphidicola afforded oxidized derivative, 17alpha-ethynyl-17beta-hydroxyandrosta-1,4-dien-3-one (3), while with C. elegans afforded a new hydroxy derivative, 17alpha-ethynyl-11alpha,17beta-dihydroxyandrost-4-en-3-one (4). On the other hand, the incubation of compound 2 with the fungus C. aphidicola afforded 17alpha-ethyl-17beta-hydroxyandrosta-1,4-dien-3-one (5). Two new hydroxylated derivatives, 17alpha-ethyl-11alpha,17beta-dihydroxyandrost-4-en-3-one (6) and 17alpha-ethyl-6alpha,17beta-dihydroxy-5alpha-androstan-3-one (7) were obtained from the incubation of compound 2 with C. elegans. Compounds 1-6 exhibited tyrosinase inhibitory activity, with compound 6 being the most potent member (IC(50)=1.72 microM).

Published

2005

20. Isolation and structure elucidation of the major photodegradation products of loteprednol etabonate.

Author

Shirasaki Y, Inada K, Inoue J, and Nakamura M

Subjects

Androstadienes chemistry, Chromatography, High Pressure Liquid, Loteprednol Etabonate, Magnetic Resonance Spectroscopy, Molecular Structure, Photolysis, Ultraviolet Rays, Androstadienes radiation effects

Abstract

Photodegradation of loteprednol etabonate (5), a steroid anti-inflammatory drug, in the solid state, in aqueous suspension, and in aqueous acetonitrile solution has been investigated. Analysis by HPLC showed that the profile of photodegradation products in the solid state was qualitatively similar to that in the aqueous suspension, although the profile in the aqueous acetonitrile solution was considerably different. The major photodegradation products were isolated from the aqueous suspension and the aqueous acetonitrile solution by using preparative reversed-phase HPLC and their structures were elucidated on the basis of spectroscopic data. Photolysis in the solid state and in aqueous suspension yielded three rearrangement products, chloromethyl 17alpha-ethoxycarbonyloxy-11beta-hydroxy-5alpha-methyl-2-oxo-19-norandrosta-1(10),3-diene-17beta-carboxylate (8), chloromethyl 17alpha-ethoxycarbonyloxy-11beta-hydroxy-1-methyl-3-oxo-6(5-->10alpha)-abeo-19-norandrosta-1,4-diene-17beta-carboxylate (9), and chloromethyl 1beta,11beta-epoxy-17alpha-ethoxycarbonyloxy-2-oxo-10alpha-androsta-4-ene-17beta-carboxylate (10). In aqueous acetonitrile solution, 10 was the major product, however, 8 and 9 were not obtained. Pathways for the formation of these compounds from loteprednol etabonate (5) are proposed.

Published

2004

21. Chemistry of loteprednol etabonate and related steroids. II. Reactions at ring C and NMR structural studies of the resulting compounds.

Author

Rachwal S, Druzgala P, Liu ZZ, Vlasak J, Brewster ME, and Pop E

Subjects

Chromatography, High Pressure Liquid, Loteprednol Etabonate, Magnetic Resonance Spectroscopy, Mass Spectrometry, Androstadienes chemistry, Anti-Inflammatory Agents chemistry, Steroids chemistry

Abstract

Several derivatives of lotoprednol etabonate (1), a soft corticosteroid antiinflammatory drug, are formed during the synthesis and sterilization process. Some of these contaminants of 1 result from side reactions taking place on the steroid ring C including oxidation, dehydration, chlorination and chlorohydroxylation. The products have been identified, synthesized, and fully characterized by 1H and 13C NMR spectroscopy.

Published

1998

22. Structural studies of loteprednol etabonate and other analogs of prednisolone using NMR techniques.

Author

Rachwal S, Pop E, and Brewster ME

Subjects

Androstadienes chemical synthesis, Loteprednol Etabonate, Magnetic Resonance Spectroscopy, Molecular Structure, Structure-Activity Relationship, Androstadienes chemistry, Prednisolone analogs & derivatives, Prednisolone chemistry

Abstract

Several structural analogs of prednisolone, prepared by esterification of the carboxylic and/or the C(17)-hydroxy group of 11 beta, 17 alpha-dihydroxy-3-oxo-androsta-1,4-diene-17 beta-carboxylic acid, were investigated by NMR. Step-by-step analysis of the 1H and 13C NMR spectra of these steroids, including proton-proton selective decoupling, nuclear Overhauser effect difference spectra, attached proton test, proton-carbon correlation (HETCOR), proton-proton correlation (COSY), and long-range proton-carbon decoupling (INAPT) techniques, led to unequivocal assignments of all their proton and carbon resonances. The stereochemical structure of loteprednol etabonate (chloromethyl 17 alpha-ethoxycarbonyloxy-11 beta-hydroxy-3-oxoandrosta-1,4-diene-17 beta-carboxylate, 1), a soft corticosteroid antiinflammatory drug, was proved to be analogous to prednisolone.

Published

1996

23. 15 beta-hydroxysteroids (Part VI). steroids of the human perinatal period: the preparation and reactions of 3 beta-hydroxy-5,15-androstadien-17-one. The synthesis of 3 beta,15 beta-dihydroxy-5-androsten-17-one and derivatives.

Author

Reeder AY and Joannou GE

Subjects

Androstenediols, Female, Humans, Magnetic Resonance Spectroscopy, Mass Spectrometry methods, Pregnancy, Androstadienes chemistry, Androstenes chemical synthesis, Hydrogen-Ion Concentration

Abstract

A successful approach to the synthesis of 3 beta,15 beta-dihydroxy-5-androsten-17-one (14d) has been developed using trichloroethoxy ethers as intermediates in the synthesis of the corresponding alcohols. 3 beta-Methoxymethoxy-5,15-androstadien-17-one (10c) was prepared by a selenation/dehydroselenation strategy from 3 beta-methoxymethoxy-5-androsten-17-one (14c). Base-catalyzed reaction of trichloroethanol with 10c gave 3 beta-methoxymethoxy-15 beta-trichloroethoxy-5-androsten-17-one (14g). Under the same conditions, 3 beta-acetoxy-5,15-androstadien-17-one (10b) gave 3 beta-hydroxy-15 beta-trichloroethoxy-5-androsten-17-one (14f) which was characterized after conversion to 14g. Cleavage of the trichloroethoxy group in 14f with zinc or zinc/copper couple gave 14d. The acid-catalyzed hydrolysis of 17,17-ethylenedioxy-5,15-androstadien-3 beta-ol (15) gave 3 beta-hydroxy-5,15-androstadien-17-one (10a) as the major product along with 14d. However, addition of water to 10a in the presence of acid gave the desired product 14d in poor yield (15%).

Published

1996

24. Synthesis and aromatase inhibition by potential metabolites of exemestane (6-methylenandrosta-1,4-diene-3,17-dione).

Author

Buzzetti F, Di Salle E, Longo A, and Briatico G

Subjects

Androstadienes metabolism, Antineoplastic Agents pharmacology, Female, Humans, Molecular Structure, Placenta enzymology, Structure-Activity Relationship, Androstadienes chemistry, Antineoplastic Agents chemical synthesis, Aromatase Inhibitors

Abstract

Exemestane (6-methylenandrosta-1,4-diene-3,17-dione; FCE 24304) is an orally active irreversible aromatase inhibitor which is in phase II clinical evaluation for the potential therapy of postmenopausal breast cancer. A series of exemestane analogs, with modifications at the 6-methylene group and with additional reduction at the 17-keto group, were synthesized as potential metabolites and tested in vitro for their effect on human placental aromatase. All these new analogs were found to be less potent in inhibiting aromatase than exemestane. The most effective compound was the 17 beta-hydroxy-derivative (compound 2), which is 2.6-fold less potent than exemestane [50% inhibitory concentration (IC50) 69 and 27 nM, respectively]. The various C-6 modified derivatives of the 17-oxo series were found to inhibit the aromatase enzyme in the following descending order: 6-methylene (exemestane) > 6-spirooxirane (6) > 6 beta-hydroxymethyl (11) > 6-hydroxymethyl (7) > 6 beta-carboxy (13), showing IC50 values of 27, 206, 295, 2,300, and 7,200 nM, respectively. The 17 beta-hydroxy analogs of some of the above mentioned compounds were also synthesized (3,4,12) and found to be 3-8-fold less potent than the corresponding 17-keto analogs.

Published

1993

25. The identification of 14 alpha,17 beta-dihydroxyandrost-4-en-3-one monohydrate and 14 alpha,17 beta-dihydroxyandrosta-1,4-dien-3-one monohydrate, metabolites of androstenedione in Mucor piriformis.

Author

Krishnan R, Madyastha KM, Seshadri TP, and Viswamitra MA

Subjects

Androstadienes chemistry, Chemical Phenomena, Chemistry, Physical, Crystallization, Hydrogen Bonding, Hydroxytestosterones chemistry, Molecular Structure, X-Ray Diffraction, Androstadienes analysis, Androstenedione metabolism, Hydroxytestosterones analysis, Mucor chemistry

Abstract

The microorganism Mucor piriformis transforms androst-4-ene-3,17-dione into a major and several minor metabolites. X-ray crystallographic analysis of two of these metabolites was undertaken to determine unambiguously their composition and chirality. Crystals belong to the orthorhombic space-group P2(1)2(1)2(1), with a = 7.199(4) A and a = 6.023(3) A, b = 11.719(3) A and b = 13.455(4) A, c = 20.409(3) A and c = 20.702(4) A for the two title compounds, respectively. The structures have been refined to final R values of 0.060 and 0.040, respectively.

Published

1991