Your search keyword '"Bubert C"' showing total 22 results

1. ChemInform Abstract: Novel Strategies for the Synthesis of Peptides Containing cis- or trans-β-Aminocyclopropanecarboxylic Acids.

Author

BUBERT, C., primary, CABRELE, C., additional, and REISER, O., additional

Published

2010

2. ChemInform Abstract: Exceptionally High Felkin-Anh Control for the Addition of Nucleophiles to a β-Aminocyclopropylcarbaldehyde.

Author

BUBERT, C., primary and REISER, O., additional

Published

2010

3. ChemInform Abstract: A New Approach to β‐ and γ‐Amino Esters (III) and Amino Aldehydes (IV) by Regioselective Ozonolysis of 2,3‐Dihydropyrroles and 1,2,3,4‐Tetrahydropyridines (I).

Author

BUBERT, C., primary, VOIGT, J., additional, BIASETTON, S., additional, and REISER, O., additional

Published

1994

4. E-Ring Modified Steroids as Novel Potent Inhibitors of 17β-Hydroxysteroid Dehydrogenase Type 1

Author

Fischer, D. S., Allan, G. M., Bubert, C., Vicker, N., Smith, A., Tutill, H. J., Purohit, A., Wood, L., Packham, G., Mahon, M. F., Reed, M. J., and Potter, B. V. L.

Abstract

17β-Hydroxysteroid dehydrogenases (17β-HSDs) are an important class of steroidogenic enzymes that regulate the bioavailability of active estrogens and androgens and are as yet a relatively unexploited therapeutic target. Based on our investigations and those of others, E-ring modified steroids were identified as a useful template for the design of inhibitors of 17β-HSD type 1, an enzyme involved in the conversion of estrone into estradiol. The synthesis and biological evaluation of a new series of N- and C-substituted 1,3,5(10)-estratrien-[17,16-c]-pyrazoles and the corresponding SAR are discussed. Among the N-alkylated analogues, the most potent inhibitor was the 1‘-methoxyethyl derivative, 41, with an IC50 of 530 nM in T47-D human breast cancer cells. The X-ray crystal structure of the 1‘-isobutyl derivative, 37, was determined. Further optimization of the template using parallel synthesis resulted in a library of C5‘-linked amides from which 73 emerged. This pyridylethyl amide had an IC50 of 300 nM and its activity, with that of 41, suggests the importance of hydrogen bond acceptor groups in the pyrazole side chain. Both 41 and 73 displayed selectivity over 17β-HSD type 2, and preliminary investigations showed 41 to be nonestrogenic in vitro in a luciferase reporter gene assay in contrast to the parent pyrazole 25. Molecular modeling studies, which support these findings, and a QSAR, the predictive power of which was demonstrated, are also presented.

Published

2005

5. First Dual Aromatase-Steroid Sulfatase Inhibitors

Author

Woo, L. W. L., Sutcliffe, O. B., Bubert, C., Grasso, A., Chander, S. K., Purohit, A., Reed, M. J., and Potter, B. V. L.

Abstract

Aromatase inhibitors in clinical use block the biosynthesis of estrogens. Hydrolysis of estrone 3-sulfate by steroid sulfatase is an important additional source of tumor estrogen, and blockade of both enzymes should provide a more effective endocrine therapy. Sulfamoylated derivatives of the aromatase inhibitor YM511 inhibited sulfatase and aromatase in JEG-3 cells with respective IC50 values of 20−227 and 0.82−100 nM (cf. letrozole, 0.89 nM). One dual inhibitor was potent against both enzymes in vivo, validating the concept.

Published

2003

6. ChemInform Abstract: Novel Strategies for the Synthesis of Peptides Containing cis- or trans-β-Aminocyclopropanecarboxylic Acids.

Author

BUBERT, C., CABRELE, C., and REISER, O.

Published

1997

7. ChemInform Abstract: Exceptionally High Felkin-Anh Control for the Addition of Nucleophiles to a β-Aminocyclopropylcarbaldehyde.

Author

BUBERT, C. and REISER, O.

Published

1997

8. Synthesis of water-soluble aminosulfonamide ligands and their application in enantioselective transfer hydrogenation

Author

Bubert, C

Published

2001

9. Exceptionally high Felkin-Anh control for the addition of nucleophiles to a β-aminocyclopropylcarbaldehyde

Author

Bubert, C

Published

1997

10. Binding mode and structure-activity relationships around direct inhibitors of the Nrf2-Keap1 complex.

Author

Jnoff E, Albrecht C, Barker JJ, Barker O, Beaumont E, Bromidge S, Brookfield F, Brooks M, Bubert C, Ceska T, Corden V, Dawson G, Duclos S, Fryatt T, Genicot C, Jigorel E, Kwong J, Maghames R, Mushi I, Pike R, Sands ZA, Smith MA, Stimson CC, and Courade JP

Subjects

Animals, Crystallography, X-Ray, Dose-Response Relationship, Drug, Humans, Isoquinolines chemical synthesis, Isoquinolines chemistry, Kelch-Like ECH-Associated Protein 1, Mice, Models, Molecular, Molecular Structure, Phthalimides chemical synthesis, Phthalimides chemistry, Structure-Activity Relationship, Adaptor Proteins, Signal Transducing antagonists & inhibitors, Cytoskeletal Proteins antagonists & inhibitors, Intracellular Signaling Peptides and Proteins antagonists & inhibitors, Isoquinolines pharmacology, NF-E2-Related Factor 2 antagonists & inhibitors, Phthalimides pharmacology

Abstract

An X-ray crystal structure of Kelch-like ECH-associated protein (Keap1) co-crystallised with (1S,2R)-2-[(1S)-1-[(1,3-dioxo-2,3-dihydro-1H-isoindol-2-yl)methyl]-1,2,3,4-tetrahydroisoquinolin-2-carbonyl]cyclohexane-1-carboxylic acid (compound (S,R,S)-1 a) was obtained. This X-ray crystal structure provides breakthrough experimental evidence for the true binding mode of the hit compound (S,R,S)-1 a, as the ligand orientation was found to differ from that of the initial docking model, which was available at the start of the project. Crystallographic elucidation of this binding mode helped to focus and drive the drug design process more effectively and efficiently., (© 2014 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2014

11. Synthesis and structure-activity relationship studies of derivatives of the dual aromatase-sulfatase inhibitor 4-{[(4-cyanophenyl)(4H-1,2,4-triazol-4-yl)amino]methyl}phenyl sulfamate.

Author

Woo LW, Wood PM, Bubert C, Thomas MP, Purohit A, and Potter BV

Subjects

Cell Line, Dose-Response Relationship, Drug, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Humans, Models, Molecular, Molecular Structure, Steryl-Sulfatase metabolism, Structure-Activity Relationship, Sulfonamides chemical synthesis, Sulfonamides chemistry, Triazoles chemical synthesis, Triazoles chemistry, Aromatase metabolism, Enzyme Inhibitors pharmacology, Steryl-Sulfatase antagonists & inhibitors, Sulfonamides pharmacology, Triazoles pharmacology

Abstract

4-{[(4-Cyanophenyl)(4H-1,2,4-triazol-4-yl)amino]methyl}phenyl sulfamate and its ortho-halogenated (F, Cl, Br) derivatives are first-generation dual aromatase and sulfatase inhibitors (DASIs). Structure-activity relationship studies were performed on these compounds, and various modifications were made to their structures involving relocation of the halogen atom, introduction of more halogen atoms, replacement of the halogen with another group, replacement of the methylene linker with a difluoromethylene linker, replacement of the para-cyanophenyl ring with other ring structures, and replacement of the triazolyl group with an imidazolyl group. The most potent in vitro DASI discovered is an imidazole derivative with IC50 values against aromatase and steroid sulfatase in a JEG-3 cell preparation of 0.2 and 2.5 nM, respectively. The parent phenol of this compound inhibits aromatase with an IC50 value of 0.028 nM in the same assay., (Copyright © 2013 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2013

12. Hybrid dual aromatase-steroid sulfatase inhibitors with exquisite picomolar inhibitory activity.

Author

Woo LW, Bubert C, Purohit A, and Potter BV

Abstract

Single agents against multiple drug targets are highly topical. Hormone-dependent breast cancer (HDBC) may be more effectively treated by dual inhibition of aromatase and steroid sulfatase (STS), and several dual aromatase-sulfatase inhibitors (DASIs) have been recently reported. The best compounds from two leading classes of DASI, 3 and 9, are low nanomolar inhibitors. In search of a novel class of DASI, core motifs of two leading classes were combined to give a series of hybrid structures, with several compounds showing markedly improved dual inhibitory activities in the picomolar range in JEG-3 cells. Thus, DASIs 14 (IC50: aromatase, 15 pM; STS, 830 pM) and 15 (IC50: aromatase, 18 pM; STS, 130 pM) are the first examples of an exceptional new class of highly potent dual inhibitor that should encourage further development toward multitargeted therapeutic intervention in HDBC.

Published

2010

13. Effects of C-17 heterocyclic substituents on the anticancer activity of 2-ethylestra-1,3,5(10)-triene-3-O-sulfamates: synthesis, in vitro evaluation and computational modelling.

Author

Jourdan F, Bubert C, Leese MP, Smith A, Ferrandis E, Regis-Lydi S, Newman SP, Purohit A, Reed MJ, and Potter BV

Subjects

Antineoplastic Agents chemistry, Antineoplastic Agents metabolism, Binding Sites, Cell Line, Tumor, Cell Proliferation drug effects, Electrons, Humans, Hydrogen Bonding, Sulfonic Acids chemistry, Sulfonic Acids metabolism, Tubulin metabolism, Antineoplastic Agents chemical synthesis, Antineoplastic Agents pharmacology, Computer Simulation, Heterocyclic Compounds chemistry, Models, Molecular, Sulfonic Acids chemical synthesis, Sulfonic Acids pharmacology

Abstract

The potent activity of 2-substituted estra-1,3,5(10)-triene-3-O-sulfamates against the proliferation of cancer cells in vitro and tumours in vivo highlights the therapeutic potential of such compounds. Optimal activity is derived from a combination of a 2-XMe group (where X = CH(2), O or S), a 3-O-sulfamate group in the steroidal A-ring and a H-bond acceptor around C-17 of the D-ring. Herein, we describe the synthesis and anti-proliferative activities of a series of novel 2-substituted estra-1,3,5(10)-triene-3-O-sulfamates bearing heterocyclic substituents (oxazole, tetrazole, triazole) tethered to C-17. In vitro evaluation of these molecules revealed that high anti-proliferative activity in breast and prostate cancer cells lines (GI(50) of 340-850 nM) could be retained when the heterocyclic substituent possesses H-bond acceptor properties. A good correlation between the calculated electron density of the heterocyclic ring and anti-proliferative activity was observed. Docking of the most active compounds into their putative site of action, the colchicine binding site of tubulin, suggests that they bind through a different mode to the previously described bis-sulfamate derivatives and 1 and 2, which possess similar in vitro activity.

Published

2008

14. Synthesis of aromatase inhibitors and dual aromatase steroid sulfatase inhibitors by linking an arylsulfamate motif to 4-(4H-1,2,4-triazol-4-ylamino)benzonitrile: SAR, crystal structures, in vitro and in vivo activities.

Author

Bubert C, Woo LW, Sutcliffe OB, Mahon MF, Chander SK, Purohit A, Reed MJ, and Potter BV

Subjects

Amino Acid Motifs, Aromatase metabolism, Aromatase Inhibitors chemistry, Cell Line, Tumor, Crystallography, X-Ray methods, Drug Design, Estradiol chemistry, Humans, In Vitro Techniques, Inhibitory Concentration 50, Molecular Conformation, Structure-Activity Relationship, Sulfonamides chemistry, Aromatase Inhibitors chemical synthesis, Aromatase Inhibitors pharmacology, Chemistry, Pharmaceutical methods, Nitriles chemistry, Steryl-Sulfatase antagonists & inhibitors, Triazoles chemistry

Abstract

4-(((4-Cyanophenyl)(4H-1,2,4-triazol-4-yl)amino)methyl)phenyl sulfamate (6 a) was the first dual aromatase-sulfatase inhibitor (DASI) reported. Several series of its derivatives with various linker systems between the steroid sulfatase (STS) and the aromatase inhibitory pharmacophores were synthesised and evaluated in JEG-3 cells. The X-ray crystal structures of the aromatase inhibitors, DASI precursors 42 d and 60, and DASI 43 h were determined. Nearly all derivatives show improved in vitro aromatase inhibition over 6 a but decreased STS inhibition. The best aromatase inhibitor is 42 e (IC(50)=0.26 nM) and the best DASI is 43 e (IC(50 aromatase)=0.45 nM, IC(50 STS)=1200 nM). SAR for aromatase inhibition shows that compounds containing an alkylene- and thioether-based linker system are more potent than those that are ether-, sulfone-, or sulfonamide-based, and that the length of the linker has a limited effect on aromatase inhibition beyond two methylene units. Compounds 43 d-f were studied in vivo (10 mg kg(-1), single, p.o.). The most potent DASI is 43 e, which inhibited PMSG-induced plasma estradiol levels by 92 % and liver STS activity by 98 % 3 h after dosing. These results further strengthen the concept of designing and developing DASIs for potential treatment of hormone-related cancers.

Published

2008

15. A new therapeutic strategy against hormone-dependent breast cancer: the preclinical development of a dual aromatase and sulfatase inhibitor.

Author

Foster PA, Chander SK, Newman SP, Woo LW, Sutcliffe OB, Bubert C, Zhou D, Chen S, Potter BV, Reed MJ, and Purohit A

Subjects

Administration, Oral, Animals, Azasteroids therapeutic use, Breast Neoplasms enzymology, Breast Neoplasms surgery, Cell Proliferation drug effects, Estrogens blood, Female, Humans, Letrozole, Mice, Mice, Nude, Neoplasms, Hormone-Dependent enzymology, Neoplasms, Hormone-Dependent surgery, Nitriles therapeutic use, Ovariectomy, Rats, Rats, Wistar, Steryl-Sulfatase metabolism, Treatment Outcome, Triazoles therapeutic use, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, Aromatase Inhibitors therapeutic use, Breast Neoplasms drug therapy, Neoplasms, Hormone-Dependent drug therapy, Steryl-Sulfatase antagonists & inhibitors

Abstract

Purpose: The production of E2 is paramount for the growth of estrogen receptor-positive breast cancer. Various strategies have been used, including the use of enzyme inhibitors against either aromatase (AROM) or steroid sulfatase (STS), in an attempt to ablate E2 levels. Both these enzymes play a critical role in the formation of estrogenic steroids and their inhibitors are now showing success in the clinic., Experimental Design: We show here, in a xenograft nude mouse model, that the inhibition of both enzymes using STX681, a dual AROM and STS inhibitor (DASI), is a potential new therapeutic strategy against HDBC. MCF-7 cells stably expressing either AROM cDNA (MCF-7(AROM)) or STS cDNA (MCF-7(STS)) were generated. Ovariectomized MF-1 female nude mice receiving s.c. injections of either androstenedione (A(4)) or E2 sulfate and bearing either MCF-7(AROM) or MCF-7(STS) tumors were orally treated with STX64, letrozole, or STX681. Treatment was administered for 28 days. Mice were weighed and tumor measurements were taken weekly., Results: STX64, a potent STS inhibitor, completely blocked MCF-7(STS) tumor growth but failed to attenuate MCF-7(AROM) tumor growth. In contrast, letrozole inhibited MCF-7(AROM) tumors but had no effect on MCF-7(STS) tumors. STX681 completely inhibited the growth of both tumors. AROM and STS activity was also completely inhibited by STX681, which was accompanied by a significant reduction in plasma E2 levels., Conclusions: This study indicates that targeting both the AROM and the STS enzyme with a DASI inhibits HDBC growth and is therefore a potentially novel treatment for this malignancy.

Published

2008

16. 3,17-disubstituted 2-alkylestra-1,3,5(10)-trien-3-ol derivatives: synthesis, in vitro and in vivo anticancer activity.

Author

Bubert C, Leese MP, Mahon MF, Ferrandis E, Regis-Lydi S, Kasprzyk PG, Newman SP, Ho YT, Purohit A, Reed MJ, and Potter BV

Subjects

Animals, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Carbamates pharmacology, Cell Line, Tumor, Crystallography, X-Ray, Drug Screening Assays, Antitumor, Estradiol pharmacology, Female, Humans, Male, Mice, Mice, Nude, Models, Molecular, Molecular Structure, Neoplasm Transplantation, Structure-Activity Relationship, Sulfonic Acids pharmacology, Antineoplastic Agents chemical synthesis, Carbamates chemical synthesis, Estradiol analogs & derivatives, Estradiol chemical synthesis, Sulfonic Acids chemical synthesis

Abstract

Estradiol-3,17-O,O-bis-sulfamates inhibit steroid sulfatase (STS), carbonic anhydrase (CA), and, when substituted at C-2, cancer cell proliferation and angiogenesis. C-2 Substitution and 17-sulfamate replacement of the estradiol-3,17-O,O-bis-sulfamates were explored with efficient and practical syntheses developed. Evaluation against human cancer cell lines revealed the 2-methyl derivative 27 (DU145 GI(50) = 0.38 microM) as the most active novel bis-sulfamate, while 2-ethyl-17-carbamate derivative 52 (GI(50) = 0.22 microM) proved most active of its series (cf. 2-ethylestradiol-3,17-O,O-bis-sulfamate 4 GI(50) = 0.21 microM). Larger C-2 substituents were deleterious to activity. 2-Methoxy-17-carbamate 50 was studied by X-ray crystallography and was surprisingly 13-fold weaker as an STS inhibitor compared to parent bis-sulfamate 3. The potential of 4 as an orally dosed anti-tumor agent is confirmed using breast and prostate cancer xenografts. In the MDA-MB-231 model, dramatic reduction in tumor growth or regression was observed, with effects sustained after cessation of treatment. 3-O-Sulfamoylated 2-alkylestradiol-17-O-carbamates and sulfamates have considerable potential as anticancer agents.

Published

2007

17. Dual aromatase-steroid sulfatase inhibitors.

Author

Woo LW, Bubert C, Sutcliffe OB, Smith A, Chander SK, Mahon MF, Purohit A, Reed MJ, and Potter BV

Subjects

Animals, Aromatase Inhibitors chemistry, Aromatase Inhibitors pharmacology, Cell Line, Tumor, Crystallography, X-Ray, Female, Humans, Protein Conformation, Rats, Rats, Wistar, Steryl-Sulfatase chemistry, Structure-Activity Relationship, Sulfonamides chemistry, Sulfonamides pharmacology, Triazoles chemistry, Triazoles pharmacology, Aromatase Inhibitors chemical synthesis, Models, Molecular, Steryl-Sulfatase antagonists & inhibitors, Sulfonamides chemical synthesis, Triazoles chemical synthesis

Abstract

By introducting the steroid sulfatase inhibitory pharmacophore into aromatase inhibitor 1 (YM511), two series of single agent dual aromatase-sulfatase inhibitors (DASIs) were generated. The best DASIs in vitro (JEG-3 cells) are 5, (IC50(aromatase) = 0.82 nM; IC50(sulfatase) = 39 nM), and 14, (IC50(aromatase) = 0.77 nM; IC50(sulfatase) = 590 nM). X-ray crystallography of 5, and docking studies of selected compounds into an aromatase homology model and the steroid sulfatase crystal structure are presented. Both 5 and 14 inhibit aromatase and sulfatase in PMSG pretreated adult female Wistar rats potently 3 h after a single oral 10 mg/kg dose. Almost complete dual inhibition is observed for 5 but the levels were reduced to 85% (aromatase) and 72% (sulfatase) after 24 h. DASI 5 did not inhibit aldosterone synthesis. The development of a potent and selective DASI should allow the therapeutic potential of dual aromatase-sulfatase inhibition in hormone-dependent breast cancer to be assessed.

Published

2007

18. Focused libraries of 16-substituted estrone derivatives and modified e-ring steroids: inhibitors of 17beta-hydroxysteroid dehydrogenase type 1.

Author

Vicker N, Lawrence HR, Allan GM, Bubert C, Smith A, Tutill HJ, Purohit A, Day JM, Mahon MF, Reed MJ, and Potter BV

Subjects

Chromatography, High Pressure Liquid, Estrone chemistry, Magnetic Resonance Spectroscopy, Mass Spectrometry methods, Models, Molecular, 17-Hydroxysteroid Dehydrogenases antagonists & inhibitors, Enzyme Inhibitors pharmacology, Estrone pharmacology

Abstract

17beta-hydroxysteroid dehydrogenase type 1 (17beta-HSD1), an oxidoreductase which has a preferential reductive activity using NADPH as cofactor, converts estrone to estradiol and is expressed in many steroidogenic tissues including breast and in malignant breast cells. As estradiol stimulates the growth and development of hormone-dependent breast cancer, inhibition of the final step of its synthesis is an attractive target for the treatment of this disease. The parallel synthesis of novel focused libraries of 16-substituted estrone derivatives and modified E-ring pyrazole steroids as new potent 17beta-HSD1 inhibitors is described. Substituted 3-O-sulfamoylated estrone derivatives were used as templates and were immobilised on 2-chlorotrityl chloride resin to give resin-bound scaffolds with a multi-detachable linker. Novel focused libraries of 16-substituted estrone derivatives and new modified E-ring steroids were assembled from these immobilised templates using solid-phase organic synthesis and solution-phase methodologies. Among the derivatives synthesised, the most potent 17beta-HSD1 inhibitors were 25 and 26 with IC50 values in T-47D human breast cancer cells of 27 and 165 nm, respectively. Parallel synthesis resulting in a library of C5'-linked amides from the pyrazole E-ring led to the identification of 62 with an IC50 value of 700 nM. These potent inhibitors of 17beta-HSD1 have a 2-ethyl substituent which will decrease their estrogenic potential. Several novel 17beta-HSD1 inhibitors emerged from these libraries and these provide direction for further template exploration in this area. A new efficient diastereoselective synthesis of 25 has also been developed to facilitate supply for in vivo evaluation, and an X-ray crystal structure of this inhibitor is presented.

Published

2006

19. Novel, potent inhibitors of 17beta-hydroxysteroid dehydrogenase type 1.

Author

Allan GM, Bubert C, Vicker N, Smith A, Tutill HJ, Purohit A, Reed MJ, and Potter BV

Subjects

Amides chemical synthesis, Amides chemistry, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Estrone chemistry, Estrone pharmacology, Humans, Pyrazoles chemical synthesis, Pyrazoles chemistry, Structure-Activity Relationship, Tumor Cells, Cultured, Amides pharmacology, Enzyme Inhibitors pharmacology, Estradiol Dehydrogenases antagonists & inhibitors, Estrone analogs & derivatives, Pyrazoles pharmacology

Abstract

Many breast tumours are hormone-responsive and rely on estrogens for their sustained growth and development. The enzyme 17beta-hydroxysteroid dehydrogenase type 1 (17beta-HSD1) is primarily responsible for the conversion of estrone (E1) into the most potent of the human estrogens 17beta-estradiol (E2). Here we report the syntheses, inhibitory activities and docking studies for a novel series of pyrazole amides which have been discovered with the aim of probing the structure activity relationships (SAR) for such a template and of using this template to mimic the potent inhibitor 1 (Fig. 1). Amides containing an aromatic pyridyl moiety have been found to give the best inhibition, indicating that the pyridyl group interacts beneficially in the active site. This work has shown that extension from this position on the pyrazole template is well tolerated and the optimization of such systems is under investigation.

Published

2006

20. Modification of estrone at the 6, 16, and 17 positions: novel potent inhibitors of 17beta-hydroxysteroid dehydrogenase type 1.

Author

Allan GM, Lawrence HR, Cornet J, Bubert C, Fischer DS, Vicker N, Smith A, Tutill HJ, Purohit A, Day JM, Mahon MF, Reed MJ, and Potter BV

Subjects

Amides chemical synthesis, Amides pharmacology, Antineoplastic Agents pharmacology, Breast Neoplasms, Cell Line, Tumor, Crystallography, X-Ray, Estradiol analogs & derivatives, Estradiol chemical synthesis, Estradiol pharmacology, Estrone pharmacology, Female, Humans, Models, Molecular, Neoplasms, Hormone-Dependent, Oximes chemical synthesis, Oximes pharmacology, Pyrazolones chemical synthesis, Pyrazolones pharmacology, Pyridines pharmacology, Quantitative Structure-Activity Relationship, 17-Hydroxysteroid Dehydrogenases antagonists & inhibitors, 17-Hydroxysteroid Dehydrogenases chemistry, Antineoplastic Agents chemical synthesis, Estrone analogs & derivatives, Estrone chemical synthesis, Pyridines chemical synthesis

Abstract

The 17beta-hydroxysteroid dehydrogenases (17beta-HSDs) catalyze the interconversion between the oxidized and reduced forms of androgens and estrogens at the 17 position. The 17beta-HSD type 1 enzyme (17beta-HSD1) catalyzes the reduction of estrone to estradiol and is expressed in malignant breast cells. Inhibitors of this enzyme thus have potential as treatments for hormone dependent breast cancer. Here we report the syntheses and biological evaluation of novel inhibitors based on the estrone or estradiol template. These have been investigated by modification at the 6, 16 or 17 positions or combinations of these in order to gain information about structure-activity relationships by probing different areas in the enzyme active site. Activity data have been incorporated into a QSAR with predictive power, and the X-ray crystal structures of compounds 15 and 16c have been determined. Compound 15 has an IC50 of 320 nM for 17beta-HSD1 and is selective for 17beta-HSD1 over 17beta-HSD2. Three libraries of amides are also reported that led to the identification of inhibitors 19e and 20a, which have IC50 values of 510 and 380 nM respectively, and 20 h which, having an IC50 value of 37 nM, is the most potent inhibitor of 17beta-HSD1 reported to date. These amides are also selective for 17beta-HSD1 over 17beta-HSD2.

Published

2006

21. Analogues of neuropeptide Y containing beta-aminocyclopropane carboxylic acids are the shortest linear peptides that are selective for the Y1 receptor.

Author

Koglin N, Zorn C, Beumer R, Cabrele C, Bubert C, Sewald N, Reiser O, and Beck-Sickinger AG

Subjects

Amino Acid Sequence, Carboxylic Acids, Neuropeptide Y metabolism, Protein Conformation, Structure-Activity Relationship, Substrate Specificity, Neuropeptide Y analogs & derivatives, Peptides chemistry, Peptides metabolism, Receptors, Neuropeptide Y metabolism

Published

2003

22. The synthesis of diastereo- and enantiomerically pure beta-aminocyclopropanecarboxylic acids.

Author

Beumer R, Bubert C, Cabrele C, Vielhauer O, Pietzsch M, and Reiser O

Subjects

Carboxylic Acids chemistry, Chromatography, High Pressure Liquid, Cyclopropanes chemistry, Hydrolysis, Indicators and Reagents, Kinetics, Lipase chemistry, Stereoisomerism, Carboxylic Acids chemical synthesis, Cyclopropanes chemical synthesis

Abstract

The synthesis of diastereo- and enantiomerically pure beta-aminocyclopropanecarboxylic acids (beta-ACCs) is described. Starting from pyrrole, (rac)-4 is readily obtained, which was kinetically resolved by enzymatic hydrolysis. Subsequent oxidation of (-)-4 and deformylation gives rise to the cis-beta-ACC derivative (ent)-9, while (+)-10 was converted to the trans-beta-ACC derivative 8. Both 8 and (ent)-9 and their benzyl esters 13 and 16, being conformationally restricted beta-alanine or gamma-aminobutyric acid (GABA) derivatives, represent useful building blocks for peptides containing unnatural amino acids.

Published

2000