Your search keyword '"Dong Jin Hwang"' showing total 37 results

1. Exploration and Biological Evaluation of Basic Heteromonocyclic Propanamide Derivatives as SARDs for the Treatment of Enzalutamide-Resistant Prostate Cancer

Author

Michael L. Mohler, Ramesh Narayanan, Duane D. Miller, Dong Jin Hwang, Yali He, Thirumagal Thiyagarajan, and Suriyan Ponnusamy

Subjects

Male, medicine.drug_class, Antineoplastic Agents, Antiandrogen, Article, Rats, Sprague-Dawley, Mice, Structure-Activity Relationship, Prostate cancer, chemistry.chemical_compound, Prostate, Nitriles, Phenylthiohydantoin, Drug Discovery, LNCaP, Androgen Receptor Antagonists, medicine, Animals, Humans, Enzalutamide, Cell Proliferation, Dose-Response Relationship, Drug, Molecular Structure, Prostatic Neoplasms, Neoplasms, Experimental, medicine.disease, Amides, Propanamide, Rats, Androgen receptor, HEK293 Cells, medicine.anatomical_structure, chemistry, Drug Resistance, Neoplasm, Receptors, Androgen, Benzamides, Cancer research, Molecular Medicine, Drug Screening Assays, Antitumor, Pharmacophore

Abstract

A series of propanamide derivatives were designed, synthesized, and pharmacologically characterized as selective androgen receptor degraders (SARDs) and pan-antagonists that exert a broad-scope androgen receptor (AR) antagonism. Incorporating different basic heteromonocyclic B-ring structural elements in the common A-ring–linkage–B-ring nonsteroidal antiandrogen general pharmacophore contributed to a novel scaffold of small molecules with SARD and pan-antagonist activities even compared to our recently published AF-1 binding SARDs such as UT-69 (11), UT-155 (12), and UT-34 (13). Compound 26f exhibited inhibitory and degradation effects in vitro in a wide array of wtAR, point mutant, and truncation mutant-driven prostate cancers (PCs). Further, 26f inhibited tumor cell growth in a xenograft model composed of enzalutamide-resistant (EnzR) LNCaP cells. These results demonstrate an advancement toward the development of novel SARDs and pan-antagonists with efficacy against EnzR prostate cancers.

Published

2021

2. Pyrazol-1-yl-propanamides as SARD and Pan-Antagonists for the Treatment of Enzalutamide-Resistant Prostate Cancer

Author

Duane D. Miller, Michael L. Mohler, Dong Jin Hwang, Yali He, Thirumagal Thiyagarajan, Ramesh Narayanan, and Suriyan Ponnusamy

Subjects

Male, Antiandrogens, Antineoplastic Agents, Pharmacology, Pyrazole, 01 natural sciences, Article, Rats, Sprague-Dawley, 03 medical and health sciences, chemistry.chemical_compound, Prostate cancer, Mice, Structure-Activity Relationship, In vivo, Cell Line, Tumor, Drug Discovery, Nitriles, Phenylthiohydantoin, medicine, Androgen Receptor Antagonists, Enzalutamide, Animals, Humans, 030304 developmental biology, Cell Proliferation, 0303 health sciences, Antagonist, Prostatic Neoplasms, medicine.disease, Xenograft Model Antitumor Assays, 0104 chemical sciences, Rats, Androgen receptor, 010404 medicinal & biomolecular chemistry, chemistry, Drug Resistance, Neoplasm, Receptors, Androgen, Drug Design, Benzamides, Microsomes, Liver, Molecular Medicine, Pyrazoles, Pharmacophore, Half-Life

Abstract

We report herein the design, synthesis, and pharmacological characterization of a library of novel aryl pyrazol-1-yl-propanamides as selective androgen receptor degraders (SARDs) and pan-antagonists that exert broad-scope AR antagonism. Pharmacological evaluation demonstrated that introducing a pyrazole moiety as the B-ring structural element in the common A-ring-linkage-B-ring nonsteroidal antiandrogens' general pharmacophore allowed the development of a new scaffold of small molecules with unique SARD and pan-antagonist activities even compared to our recently published AF-1 binding SARDs such as UT-155 (9) and UT-34 (10). Novel B-ring pyrazoles exhibited potent AR antagonist activities, including promising distribution, metabolism, and pharmacokinetic properties, and broad-spectrum AR antagonist properties, including potent in vivo antitumor activity. 26a was able to induce an 80% tumor growth inhibition of xenografts derived from the enzalutamide-resistant (Enz-R) VCaP cell line. These results represent an advancement toward the development of novel AR antagonists for the treatment of Enz-R prostate cancer.

Published

2020

3. Colchicine Binding Site Agent DJ95 Overcomes Drug Resistance and Exhibits Antitumor Efficacy

Author

Zi-Ning Lei, Deanna N. Parke, Tiffany N. Seagroves, Dong Jin Hwang, Zhe-Sheng Chen, Wei Li, Qiang Chen, Miller Duane D, Stephen W. White, Gyanendra Kumar, Jinliang Yang, Kinsie E. Arnst, Dejian Ma, and Yuxi Wang

Subjects

0301 basic medicine, Male, Cell Survival, Pyridines, Mice, Nude, Crystallography, X-Ray, Small Molecule Libraries, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Microtubule, Cell Movement, Tubulin, Cell Line, Tumor, medicine, Human Umbilical Vein Endothelial Cells, Colchicine, Animals, Humans, Mitosis, Melanoma, Pharmacology, biology, Chemistry, HEK 293 cells, Imidazoles, Cancer, Articles, Cell cycle, medicine.disease, Xenograft Model Antitumor Assays, Tubulin Modulators, 030104 developmental biology, HEK293 Cells, Paclitaxel, Drug Resistance, Neoplasm, Cancer research, biology.protein, Molecular Medicine, ATP-Binding Cassette Transporters, Female, 030217 neurology & neurosurgery

Abstract

Interfering with microtubule dynamics is a well-established strategy in cancer treatment; however, many microtubule-targeting agents are associated with drug resistance and adverse effects. Substantial evidence points to ATP-binding cassette (ABC) transporters as critical players in the development of resistance. Herein, we demonstrate the efficacy of DJ95 (2-(1H-indol-6-yl)-4-(3,4,5-trimethoxyphenyl)-1H-imidazo[4,5-c]pyridine), a novel tubulin inhibitor, in a variety of cancer cell lines, including malignant melanomas, drug-selected resistant cell lines, specific ABC transporter-overexpressing cell lines, and the National Cancer Institute 60 cell line panel. DJ95 treatment inhibited cancer cell migration, caused morphologic changes to the microtubule network foundation, and severely disrupted mitotic spindle formation of mitotic cells. The high-resolution crystal structure of DJ95 in complex with tubulin protein and the detailed molecular interactions confirmed its direct binding to the colchicine site. In vitro pharmacological screening of DJ95 using SafetyScreen44 (Eurofins Cerep-Panlabs) revealed no significant off-target interactions, and pharmacokinetic analysis showed that DJ95 was maintained at therapeutically relevant plasma concentrations for up to 24 hours in mice. In an A375 xenograft model in nude mice, DJ95 inhibited tumor growth and disrupted tumor vasculature in xenograft tumors. These results demonstrate that DJ95 is potent against a variety of cell lines, demonstrated greater potency to ABC transporter-overexpressing cell lines than existing tubulin inhibitors, directly targets the colchicine binding domain, exhibits significant antitumor efficacy, and demonstrates vascular-disrupting properties. Collectively, these data suggest that DJ95 has great potential as a cancer therapeutic, particularly for multidrug resistance phenotypes, and warrants further development. SIGNIFICANCE STATEMENT: Paclitaxel is a widely used tubulin inhibitor for cancer therapy, but its clinical efficacy is often limited by the development of multidrug resistance. In this study, we reported the preclinical characterization of a new tubulin inhibitor DJ95, and demonstrated its abilities to overcome paclitaxel resistance, disrupt tumor vasculature, and exhibit significant antitumor efficacy.

Published

2019

4. Orally Bioavailable Androgen Receptor Degrader, Potential Next-Generation Therapeutic for Enzalutamide-Resistant Prostate Cancer

Author

Robert H. Getzenberg, Vera Bocharova, Miller Duane D, Iain J. McEwan, René Houtman, Daniel L. Johnson, Suriyan Ponnusamy, Yali He, Elias J. Fernandez, Dong Jin Hwang, Thirumagal Thiyagarajan, Lawrence M. Pfeffer, Bobby G. Sumpter, Ramesh Narayanan, and Ziyun Du

Subjects

0301 basic medicine, Oncology, Male, Cancer Research, Administration, Oral, Gene Expression, Neoplasm genetics, chemistry.chemical_compound, Prostate cancer, Mice, 0302 clinical medicine, User Facility, Receptors, Androgen, 030220 oncology & carcinogenesis, Benzamides, Protein Binding, Signal Transduction, medicine.medical_specialty, Proteasome Endopeptidase Complex, Antineoplastic Agents, 03 medical and health sciences, Internal medicine, Cell Line, Tumor, Nitriles, Phenylthiohydantoin, medicine, Androgen Receptor Antagonists, Biomarkers, Tumor, Enzalutamide, Animals, Humans, Dose-Response Relationship, Drug, business.industry, Ubiquitin, Prostatic Neoplasms, Differential regulation, Oak Ridge National Laboratory, medicine.disease, Xenograft Model Antitumor Assays, Rats, Androgen receptor, Abiraterone, Disease Models, Animal, 030104 developmental biology, chemistry, Drug Resistance, Neoplasm, Mutation, Proteolysis, business

Abstract

Purpose: Androgen receptor (AR)-targeting prostate cancer drugs, which are predominantly competitive ligand-binding domain (LBD)-binding antagonists, are inactivated by common resistance mechanisms. It is important to develop next-generation mechanistically distinct drugs to treat castration- and drug-resistant prostate cancers. Experimental Design: Second-generation AR pan antagonist UT-34 was selected from a library of compounds and tested in competitive AR binding and transactivation assays. UT-34 was tested using biophysical methods for binding to the AR activation function-1 (AF-1) domain. Western blot, gene expression, and proliferation assays were performed in various AR-positive enzalutamide-sensitive and -resistant prostate cancer cell lines. Pharmacokinetic and xenograft studies were performed in immunocompromised rats and mice. Results: UT-34 inhibits the wild-type and LBD-mutant ARs comparably and inhibits the in vitro proliferation and in vivo growth of enzalutamide-sensitive and -resistant prostate cancer xenografts. In preclinical models, UT-34 induced the regression of enzalutamide-resistant tumors at doses when the AR is degraded; but, at lower doses, when the AR is just antagonized, it inhibits, without shrinking, the tumors. This indicates that degradation might be a prerequisite for tumor regression. Mechanistically, UT-34 promotes a conformation that is distinct from the LBD-binding competitive antagonist enzalutamide and degrades the AR through the ubiquitin proteasome mechanism. UT-34 has a broad safety margin and exhibits no cross-reactivity with G-protein–coupled receptor kinase and nuclear receptor family members. Conclusions: Collectively, UT-34 exhibits the properties necessary for a next-generation prostate cancer drug.

Published

2019

5. New Generation of Selective Androgen Receptor Degraders: Our Initial Design, Synthesis, and Biological Evaluation of New Compounds with Enzalutamide-Resistant Prostate Cancer Activity

Author

Duane D. Miller, Suriyan Ponnusamy, Ramesh Narayanan, Dong Jin Hwang, Thirumagal Thiyagarajan, Michael L. Mohler, Yali He, and Iain J. McEwan

Subjects

Agonist, Male, Indoles, medicine.drug_class, Protein degradation, 01 natural sciences, 03 medical and health sciences, chemistry.chemical_compound, Prostate cancer, Mice, Structure-Activity Relationship, Cell Line, Tumor, Drug Discovery, Nitriles, Phenylthiohydantoin, medicine, Androgen Receptor Antagonists, Enzalutamide, Structure–activity relationship, Animals, Humans, Receptor, 030304 developmental biology, Cell Proliferation, 0303 health sciences, Prostatic Neoplasms, Biological activity, medicine.disease, Amides, Xenograft Model Antitumor Assays, 0104 chemical sciences, Rats, Androgen receptor, 010404 medicinal & biomolecular chemistry, chemistry, Drug Resistance, Neoplasm, Receptors, Androgen, Drug Design, Benzamides, Proteolysis, Cancer research, Androgens, Molecular Medicine

Abstract

In our effort to find small-molecule treatments of advanced prostate cancers (PCs), a novel series of indolyl and indolinyl propanamides (series II and III) were discovered as selective androgen receptor degraders (SARDs). Initial studies of androgen receptor (AR) antagonist (1) and agonist (2) propanamides yielded a tertiary aniline (3) with novel SARD activity but poor metabolic stability. Cyclization to II and III produced submicromolar AR antagonism and protein degradation selective to AR and AR splice variant (AR SV). II and III maintained potency against enzalutamide-resistant (Enz-R) mutant ARs and PC cells and were efficacious in Enz-R xenografts, suggesting their potential to treat advanced PCs. Design, synthesis, and biological activity of novel SARDs that could potentially be used for the treatment of a wide spectrum of PCs including castration-resistant, Enz-R, and/or AR SV-dependent advanced PCs that are often untreatable with known hormone therapies are discussed.

Published

2018

6. Structural Optimization of Indole Derivatives Acting at Colchicine Binding Site as Potential Anticancer Agents

Author

Wei Li, Dong Jin Hwang, Jin Wang, and Duane D. Miller

Subjects

Indole test, Stereochemistry, Melanoma, Organic Chemistry, Biology, Inhibitory postsynaptic potential, medicine.disease, Biochemistry, Multiple drug resistance, chemistry.chemical_compound, chemistry, Drug Discovery, Pyridine, medicine, Microsome, Lead compound, IC50

Abstract

A new series of indole analogues based on our earlier lead compound, 2-(1H-indol-5-yl)-4-(3,4,5-trimethoxyphenyl)-1H-imidazo[4,5-c]pyridine (42), was prepared as tubulin inhibitors in an effort to find a molecule with improved cytotoxic potency and metabolic stability. A series of indolyl-imidazopyridines (IIP) were synthesized and exhibited potent tubulin polymerization inhibitory activity with potent IC50 values ranging from 3 to 175 nM against a panel of human melanoma and prostate cancer cell lines. Among these compounds, the 6-indolyl compound 43 showed improved cytotoxic potency (average IC50 of 9.75 nM vs 55.75 nM) and metabolic stability in human liver microsomes (half-life time was 56.3 min vs. 45.4 min) as compared to previously reported 42. It was also shown to be effective against P-glycoprotein (P-gp) mediated multiple drug resistance (MDR) and taxol resistance.

Published

2015

7. Novel selective agents for the degradation of androgen receptor variants to treat castration-resistant prostate cancer

Author

Robert W. Wake, James T. Dalton, Duane D. Miller, Dong Jin Hwang, Christopher C. Coss, Yali He, Charles B. Duke, Wayne D. Tilley, Iain J. McEwan, Tudor Moldoveanu, Christopher Ledbetter, Jayaprakash Pagadala, Luke A. Selth, Ramesh Narayanan, Thirumagal Thiyagarajan, Kate Watts, Geetika Singh, and Suriyan Ponnusamy

Subjects

0301 basic medicine, Gene isoform, Male, Cancer Research, Indoles, Mice, SCID, Pharmacology, Article, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Mice, Inbred NOD, Cell Line, Tumor, medicine, Androgen Receptor Antagonists, Animals, Humans, Anilides, Receptor, Cell Proliferation, Mice, Knockout, Molecular Structure, Cell growth, Chemistry, Gene Expression Profiling, Cancer, medicine.disease, Xenograft Model Antitumor Assays, Androgen receptor, Gene Expression Regulation, Neoplastic, Alternative Splicing, Prostatic Neoplasms, Castration-Resistant, 030104 developmental biology, Oncology, Proteasome, Receptors, Androgen, 030220 oncology & carcinogenesis

Abstract

Androgen receptor (AR) mediates the growth of prostate cancer throughout its course of development, including in abnormal splice variants (AR-SV)-driven advanced stage castration-resistant disease. AR stabilization by androgens makes it distinct from other steroid receptors, which are typically ubiquitinated and degraded by proteasomes after ligand binding. Thus, targeting AR in advanced prostate cancer requires the development of agents that can sustainably degrade variant isoforms for effective therapy. Here we report the discovery and characterization of potent selective AR degraders (SARD) that markedly reduce the activity of wild-type and splice variant isoforms of AR at submicromolar doses. Three SARDs (UT-69, UT-155, and (R)-UT-155) bind the amino-terminal transcriptional activation domain AF-1, which has not been targeted for degradation previously, with two of these SARD (UT-69 and UT-155) also binding the carboxy-terminal ligand binding domain. Despite different mechanisms of action, all three SARDs degraded wild-type AR and inhibited AR function, exhibiting greater inhibitory potency than the approved AR antagonists. Collectively, our results introduce a new candidate class of next-generation therapeutics to manage advanced prostate cancer. Cancer Res; 77(22); 6282–98. ©2017 AACR.

Published

2017

8. MP57-03 IDENTIFICATION AND CHARACTERIZATION OF SELECTIVE ANDROGEN RECEPTOR DEGRADERS (SARDS) FOR THE TREATMENT OF ENZALUTAMIDE UNRESPONSIVE AND/OR RESISTANT PROSTATE CANCER

Author

Carolyn Watt, Suriyan Ponnusamy, Tudor Moldoveanu, Yali He, Iain J. McEwan, Ramesh Narayanan, Dong Jin Hwang, Thirumagal Thiyagarajan, Duane D. Miller, and Robert H. Getzenberg

Subjects

Androgen receptor, Prostate cancer, chemistry.chemical_compound, chemistry, business.industry, Urology, medicine, Cancer research, Enzalutamide, Identification (biology), medicine.disease, business

Published

2017

9. A Potent, Metabolically Stable Tubulin Inhibitor Targets the Colchicine Binding Site and Overcomes Taxane Resistance

Author

Terry Costello, Frank Park, Jinliang Yang, Dong Jin Hwang, Yi Xue, Wei Li, James T. Dalton, Duane D. Miller, Kinsie E. Arnst, Yuxi Wang, David J. Hamilton, and Qiang Chen

Subjects

0301 basic medicine, Bridged-Ring Compounds, Cancer Research, Indoles, Lung Neoplasms, Pyridines, Melanoma, Experimental, Mice, Nude, Drug resistance, Biology, Pharmacology, Crystallography, X-Ray, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Microtubule, Cell Movement, Tubulin, Cell Line, Tumor, medicine, Animals, Humans, Binding Sites, Melanoma, Imidazoles, Cancer, medicine.disease, Xenograft Model Antitumor Assays, Tubulin Modulators, Multiple drug resistance, Mice, Inbred C57BL, 030104 developmental biology, Oncology, Paclitaxel, chemistry, Mechanism of action, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, biology.protein, Taxoids, medicine.symptom, Drug Screening Assays, Antitumor, Colchicine

Abstract

Antimitotics that target tubulin are among the most useful chemotherapeutic drugs, but their clinical activity is often limited by the development of multidrug resistance. We recently discovered the novel small-molecule DJ101 as a potent and metabolically stable tubulin inhibitor that can circumvent the drug efflux pumps responsible for multidrug resistance of existing tubulin inhibitors. In this study, we determined the mechanism of action of this drug. The basis for its activity was illuminated by solving the crystal structure of DJ101 in complex with tubulin at a resolution of 2.8Å. Investigations of the potency of DJ101 in a panel of human metastatic melanoma cell lines harboring major clinically relevant mutations defined IC50 values of 7–10 nmol/L. In cells, DJ101 disrupted microtubule networks, suppressed anchorage-dependent melanoma colony formation, and impaired cancer cell migration. In melanoma-bearing mice, DJ101 administration inhibited tumor growth and reduced lung metastasis in the absence of observable toxicity. DJ101 also completely inhibited tumor growth in a paclitaxel-resistant xenograft mouse model of human prostate cancer (PC-3/TxR), where paclitaxel was minimally effective. Our findings offer preclinical proof of concept for the continued development of DJ101 as a next-generation tubulin inhibitor for cancer therapy. Significance: These findings offer preclinical proof of concept for the continued development of DJ101 as a next-generation antitubulin drug for cancer therapy. Cancer Res; 78(1); 265–77. ©2017 AACR.

Published

2017

10. Abstract B037: Potential next-generation androgen receptor-targeted therapeutic for enzalutamide-resistant prostate cancer; In vivo characterization in immune-compromised SRG rats

Author

Suriyan Ponnusamy, Dong Jin Hwang, Sam Moody, Yali He, Fallon K. Noto, Ramesh Narayanan, Bisoye Towobola Adedeji, Tseten Yeshi Jamling, Thirumagal Thiyagarajan, and Duane D. Miller

Subjects

Cancer Research, medicine.drug_class, business.industry, Cancer, medicine.disease, Androgen, Androgen receptor, chemistry.chemical_compound, Prostate cancer, medicine.anatomical_structure, Oncology, chemistry, Nuclear receptor, Prostate, In vivo, medicine, Cancer research, Enzalutamide, business

Abstract

Current treatment options for advanced castration-resistant prostate cancers (CRPC) are effective for a brief period before becoming refractory. It is important to use relevant in vivo models for candidate selection in the development of next-generation mechanistically-distinct drugs to treat castration- and drug- resistant prostate cancers. Here, we describe a series of AR pan-antagonists (selective AR degraders (SARDs)) that degrade the AR and AR splice variants. SARDs inhibit the wild-type and LBD mutant ARs comparably and inhibit the in vitro proliferation and in vivo growth of enzalutamide-sensitive and resistant prostate cancer xenografts. Xenograft studies conducted in immune-compromised SRG rats (Sprague Dawley Rag2-/- Il2rg -/-; Hera Biolabs) with three lead SARDs demonstrated regression of enzalutamide-sensitive and -resistant VCaP tumors both in castrated and in intact rats. SRG rats provide the benefit of abundant blood samples for weekly evaluation of rising PSA, which also indicated that the SARDs inhibit the rising PSA, while enzalutamide was inactive in enzalutamide-resistant model. Drug metabolism and pharmacokinetic (DMPK) studies, also conducted with SRG and wild-type rats and in combination with efficacy, indicate that the molecules possess all the necessary drug-like properties. The molecules exhibit a broad safety margin with no cross-reactivity with G-Protein Coupled Receptor, kinase, and nuclear receptor family members. Collectively, the SARDs exhibit the properties necessary for a next-generation prostate cancer drug and that use of SRG rats facilitated thorough characterization of their in vivo properties. Citation Format: Suriyan Udhayasuriyan Ponnusamy, Fallon K Noto, Bisoye Towobola Adedeji, Yali He, Dong-Jin Hwang, Sam Moody, Thirumagal Thiyagarajan, Tseten Yeshi Jamling, Duane D Miller, Ramesh Narayanan. Potential next-generation androgen receptor-targeted therapeutic for enzalutamide-resistant prostate cancer; In vivo characterization in immune-compromised SRG rats [abstract]. In: Proceedings of the AACR-NCI-EORTC International Conference on Molecular Targets and Cancer Therapeutics; 2019 Oct 26-30; Boston, MA. Philadelphia (PA): AACR; Mol Cancer Ther 2019;18(12 Suppl):Abstract nr B037. doi:10.1158/1535-7163.TARG-19-B037

Published

2019

11. Effects of a Novel Selective Androgen Receptor Modulator on Dexamethasone-Induced and Hypogonadism-Induced Muscle Atrophy

Author

Amanda Jones, Dong Jin Hwang, James T. Dalton, Ramesh Narayanan, and Duane D. Miller

Subjects

Male, Testosterone propionate, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, Muscle Fibers, Skeletal, Drug Evaluation, Preclinical, Biology, Aminophenols, Biochemistry, Dexamethasone, Substrate Specificity, Rats, Sprague-Dawley, Mice, chemistry.chemical_compound, Hormone Antagonists, Endocrinology, Atrophy, Internal medicine, Acetamides, Androgen Receptor Antagonists, medicine, Animals, Anilides, Drug Interactions, Myopathy, Protein kinase B, Cells, Cultured, Dose-Response Relationship, Drug, Hypogonadism, Biochemistry (medical), Skeletal muscle, Hypertrophy, medicine.disease, Muscle atrophy, Rats, Muscular Atrophy, Levator ani, medicine.anatomical_structure, Selective androgen receptor modulator, chemistry, medicine.symptom, Biomarkers

Abstract

Glucocorticoids are the most widely used antiinflammatory drugs in the world. However, prolonged use of glucocorticoids results in undesirable side effects such as muscle wasting, osteoporosis, and diabetes. Skeletal muscle wasting, which currently has no approved therapy, is a debilitating condition resulting from either reduced muscle protein synthesis or increased degradation. The imbalance in protein synthesis could occur from increased expression and function of muscle-specific ubiquitin ligases, muscle atrophy F-box (MAFbx)/atrogin-1 and muscle ring finger 1 (MuRF1), or decreased function of the IGF-I and phosphatidylinositol-3 kinase/Akt kinase pathways. We examined the effects of a nonsteroidal tissue selective androgen receptor modulator (SARM) and testosterone on glucocorticoid-induced muscle atrophy and castration-induced muscle atrophy. The SARM and testosterone propionate blocked the dexamethasone-induced dephosphorylation of Akt and other proteins involved in protein synthesis, including Forkhead box O (FoxO). Dexamethasone caused a significant up-regulation in the expression of ubiquitin ligases, but testosterone propionate and SARM administration blocked this effect by phosphorylating FoxO. Castration induced rapid myopathy of the levator ani muscle, accompanied by up-regulation of MAFbx and MuRF1 and down-regulation of IGF-I, all of which was attenuated by a SARM. The results suggest that levator ani atrophy caused by hypogonadism may be the result of loss of IGF-I stimulation, whereas that caused by glucocorticoid treatment relies almost solely on up-regulation of MAFbx and MuRF1. Our studies provide the first evidence that glucocorticoid- and hypogonadism-induced muscle atrophy are mediated by distinct but overlapping mechanisms and that SARMs may provide a more effective and selective pharmacological approach to prevent glucocorticoid-induced muscle loss than steroidal androgen therapy.

Published

2010

12. Nonsteroidal Selective Androgen Receptor Modulators Enhance Female Sexual Motivation

Author

Charles B. Duke, Duane D. Miller, Amanda Jones, Dong Jin Hwang, James T. Dalton, Yali He, and Anjaiah Siddam

Subjects

Male, medicine.disease_cause, Bioinformatics, Rats, Sprague-Dawley, Radioligand Assay, Sexual Behavior, Animal, chemistry.chemical_compound, Anilides, Testosterone, Prostate, Stereoisomerism, Hypoactive sexual desire disorder, Organ Size, Early life, Lower incidence, Behavioral Pharmacology, Receptors, Androgen, Dihydrotestosterone, Androgens, Molecular Medicine, Female, medicine.drug, Transcriptional Activation, Testosterone propionate, Agonist, medicine.medical_specialty, medicine.drug_class, Urology, Ovariectomy, Biology, Binding, Competitive, Cell Line, Structure-Activity Relationship, Sex Factors, Internal medicine, medicine, Animals, Humans, Carcinogen, Pharmacology, Nonsteroidal, business.industry, Uterus, Luteinizing Hormone, medicine.disease, Androgen, Rats, Androgen receptor, Endocrinology, chemistry, Estrogen, Lead exposure, Follicle Stimulating Hormone, business, Carcinogenesis, Orchiectomy

Abstract

Women experience a decline in estrogen and androgen levels after natural or surgically induced menopause, effects that are associated with a loss of sexual desire and bone mineral density. Studies in our laboratories have shown the beneficial effects of selective androgen receptor modulators (SARMs) in the treatment of osteoporosis and muscle wasting in animal models. A series of S-3-(phenoxy)-2-hydroxy-2-methyl-N-(4-cyano-3-trifluoromethyl-phenyl)-propionamide analogs was synthesized to evaluate the effects of B-ring substitutions on in vitro and in vivo pharmacologic activity, especially female sexual motivation. The androgen receptor (AR) relative binding affinities ranged from 0.1 to 26.5% (relative to dihydrotestosterone) and demonstrated a range of agonist activity at 100 nM. In vivo pharmacologic activity was first assessed by using male rats. Structural modifications to the B-ring significantly affected the selectivity of the SARMs, demonstrating that single-atom substitutions can dramatically and unexpectedly influence activity in androgenic (i.e., prostate) and anabolic (i.e., muscle) tissues. (S)-N-(4-cyano-3-trifluoromethyl-phenyl)-3-(3-fluoro,4-chlorophenoxy)-2-hydroxy-2-methyl-propanamide (S-23) displayed full agonist activity in androgenic and anabolic tissues; however, the remaining SARMs were more prostate-sparing, selectively maintaining the size of the levator ani muscle in castrated rats. The partner-preference paradigm was used to evaluate the effects of SARMs on female sexual motivation. With the exception of two four-halo substituted analogs, the SARMs increased sexual motivation in ovariectomized rats, with potency and efficacy comparable with testosterone propionate. These results indicate that the AR is important in regulating female libido given the nonaromatizable nature of SARMs and it could be a superior alternative to steroidal testosterone preparations in the treatment of hypoactive sexual desire disorder.

Published

2010

13. Computationally identified novel agonists for GPRC6A

Author

Jerome Baudry, Ruisong Ye, Duane D. Miller, Dong Jin Hwang, Jeremy C. Smith, Min Pi, Karan Kapoor, and L. Darryl Quarles

Subjects

Blood Glucose, Models, Molecular, 0301 basic medicine, Physiology, medicine.medical_treatment, Drug Evaluation, Preclinical, Druggability, lcsh:Medicine, Molecular Dynamics, Biochemistry, Receptors, G-Protein-Coupled, Mice, Endocrinology, Computational Chemistry, Insulin-Secreting Cells, Insulin Secretion, Medicine and Health Sciences, Biochemical Simulations, Insulin, Glucose homeostasis, lcsh:Science, Receptor, Multidisciplinary, Molecular Structure, Organic Compounds, Chemistry, Physics, Monosaccharides, Blood Sugar, Body Fluids, Type 2 Diabetes, 3. Good health, Cell biology, Blood, Physical Sciences, Anatomy, Signal Transduction, Research Article, Endocrine Disorders, Carbohydrates, Blood sugar, GPRC6A, Cell Line, Small Molecule Libraries, Structure-Activity Relationship, 03 medical and health sciences, Terphenyl Compounds, Diabetes Mellitus, medicine, Animals, Humans, Structure–activity relationship, Computer Simulation, G protein-coupled receptor, Diabetic Endocrinology, Binding Sites, Chemical Physics, Dose-Response Relationship, Drug, Endocrine Physiology, 030102 biochemistry & molecular biology, lcsh:R, Organic Chemistry, Chemical Compounds, Biology and Life Sciences, Computational Biology, Hormones, HEK293 Cells, Glucose, 030104 developmental biology, Metabolic Disorders, lcsh:Q

Abstract

New insights into G protein coupled receptor regulation of glucose metabolism by β-cells, skeletal muscle and liver hepatocytes identify GPRC6A as a potential therapeutic target for treating type 2 diabetes mellitus (T2D). Activating GPRC6A with a small molecule drug represents a potential paradigm-shifting opportunity to make significant strides in regulating glucose homeostasis by simultaneously correcting multiple metabolic derangements that underlie T2D, including abnormalities in β-cell proliferation and insulin secretion and peripheral insulin resistance. Using a computational, structure-based high-throughput screening approach, we identified novel tri-phenyl compounds predicted to bind to the venus fly trap (VFT) and 7-transmembrane (7-TM) domains of GPRC6A. Experimental testing found that these compounds dose-dependently stimulated GPRC6A signaling in a heterologous cell expression system. Additional chemical modifications and functional analysis identified one tri-phenyl lead compound, DJ-V-159 that demonstrated the greatest potency in stimulating insulin secretion in β-cells and lowering serum glucose in wild-type mice. Collectively, these studies show that GPRC6A is a "druggable" target for developing chemical probes to treat T2DM.

Published

2018

14. Estrogen receptor β selective nonsteroidal estrogens: seeking clinical indications

Author

Ramesh Narayanan, Yali He, Christopher C. Coss, Michael L. Mohler, Kejiang Hu, Zhongzhi Wu, Duane D. Miller, Seoung-Soo Hong, James T. Dalton, and Dong Jin Hwang

Subjects

Pharmacology, Agonist, Nonsteroidal, Chemistry, medicine.drug_class, Patent literature, Estrogen receptor, Estrogens, General Medicine, Ligands, Patents as Topic, chemistry.chemical_compound, Drug Delivery Systems, Drug Discovery, medicine, Animals, Estrogen Receptor beta, Humans, Pharmacophore, Estrogen replacement therapy, hormones, hormone substitutes, and hormone antagonists, Estrogen receptor beta

Abstract

Nonsteroidal estrogens have been known since the 1930s. However, the relatively recent (1996) discovery of estrogen receptor subtype beta (ERbeta) suggested a possible paradigm shift away from SERM-like selectivity. Selective ERbeta agonism would potentially allow expansion of estrogenic targeting into new indications (discussed herein) currently precluded by the thrombogenic and hyperproliferative effects of nonselective estrogens.ERbeta agonist design has been very successful. Pharmacophores for ERbeta selective nonsteroidal estrogens are generally diphenolic compounds that achieve an inter-phenolic distance and geometry similar to 17beta-estradiol with few restraints on the nature of the element linking the phenols (or phenol mimetics). The tremendously chemodiverse ERbeta agonist patent literature is reviewed, segregating the agonists into structurally similar compounds based on their interphenolic linking elements.A comprehensive understanding of the chemotype landscape of this field and an assessment of its maturation.Subtype selective ERbeta agonist therapy seems very promising. However, more clinical testing is needed to firmly establish its therapeutic potential. At this point, ERbeta is a promising target in search of an indication.

Published

2010

15. Nonsteroidal Selective Androgen Receptor Modulators (SARMs): Dissociating the Anabolic and Androgenic Activities of the Androgen Receptor for Therapeutic Benefit

Author

Michael L. Mohler, Christopher C. Coss, Miller Duane D, James T. Dalton, Dong Jin Hwang, Casey E. Bohl, Amanda Jones, Yali He, and Ramesh Narayanan

Subjects

Models, Molecular, medicine.medical_specialty, medicine.drug_class, Quinolones, Pharmacology, Structure-Activity Relationship, Anabolic Agents, Internal medicine, Drug Discovery, Androgen Receptor Antagonists, medicine, Animals, Humans, Testosterone, Chemistry, medicine.disease, Androgen, Amides, Androgen receptor, Endocrinology, Nuclear receptor, Selective androgen receptor modulator, Receptors, Androgen, Androgen Therapy, Sarcopenia, Androgens, Molecular Medicine

Abstract

Interest in the development and therapeutic potential of nonsteroidal tissue-selective androgen receptor modulators (SARMs) has increased dramatically within the past decade. Rapidly expanding knowledge of nuclear hormone receptor structure and function and successful proof-of-principle clinical trials with SARMs have revived an almost dormant search for improved androgens. This Award Address attempts to chronicle the landmark discoveries (with emphasis on our work), organize the SARM landscape into clinically relevant bins, and provide insight into the clinical prospects for SARMs. 1.1. Origins of Androgen Use. An early (1889) and unusual experiment in androgen therapy was performed by Charles Edouard Brown-Sequard, age 72. He administered a testicular extract to himself and reported that he felt “increased vigor and capacity for work”. Despite retrospective suggestions that any effect was purely placebo, this report resulted in widespread use of testicular extracts throughout Europe and North America for several decades. Attempts to isolate the active components of testicular extract failed until 1935 when testosterone (17 hydroxy-4-andosten-3-one) was isolated from bull testes. Shortly thereafter, its synthesis was reported. In the same year, extracts of urine from males were shown to cause nitrogen retention, an indicator of anabolic metabolism. Testosterone was the first anabolic androgen to be used clinically, but its use is limited by its androgenicity and pharmacokinetic (PK) issues. 1 In the latter half of the 20th century, the chemical scaffold of testosterone was modified extensively, producing many

Published

2009

16. Preclinical Characterization of a (S)-N-(4-Cyano-3-Trifluoromethyl-Phenyl)-3-(3-Fluoro, 4-Chlorophenoxy)-2-Hydroxy-2-Methyl-Propanamide: A Selective Androgen Receptor Modulator for Hormonal Male Contraception

Author

Amanda Jones, Dong Jin Hwang, Duane D. Miller, Jiyun Chen, and James T. Dalton

Subjects

Male, Agonist, medicine.medical_specialty, medicine.drug_class, Biology, Article, Rats, Sprague-Dawley, Sexual Behavior, Animal, chemistry.chemical_compound, Endocrinology, Pregnancy, Internal medicine, medicine, Animals, Anilides, Orchiectomy, Muscle, Skeletal, Spermatogenesis, Receptor, Estradiol, Contraceptive Agents, Male, Prostate, Seminal Vesicles, Organ Size, Sperm, Rats, Selective androgen receptor modulator, chemistry, Receptors, Androgen, Androgens, Body Composition, Estradiol benzoate, Female, Hormone

Abstract

The pharmacologic effects of (S)-N-(4-cyano-3-trifluoromethyl-phenyl)-3-(3-fluoro, 4-chlorophenoxy)-2-hydroxy-2-methyl-propanamide (S-23) were characterized in male rats as an animal model of hormonal male contraception. S-23 showed high binding affinity (inhibitory constant = 1.7 ± 0.2 nm) and was identified as a full agonist in vitro. In castrated male rats, the ED50 of S-23 in the prostate and levator ani muscle was 0.43 and 0.079 mg/d, respectively. In intact male rats treated for 14 d, S-23 alone suppressed LH levels by greater than 50% at doses greater than 0.1 mg/d, with corresponding decreases in the size of the prostate but increases in the size of levator ani muscle. In intact male rats treated for up to 10 wk with S-23 and estradiol benzoate (EB; necessary to maintain sexual behavior in rats), S-23 showed biphasic effects on androgenic tissues and spermatogenesis by suppressing serum concentrations of LH and FSH. EB alone showed no effect on spermatogenesis. In the EB + S-23 (0.1 mg/d) group, four of six animals showed no sperm in the testis and zero pregnancies (none of six) in mating trials. After termination of treatment, infertility was fully reversible, with a 100% pregnancy rate observed after 100 d of recovery. S-23 increased bone mineral density and lean mass but reduced fat mass in a dose-dependent manner. This is the first study to show that a selective androgen receptor modulator combined with EB is an effective and reversible regimen for hormonal male contraception in rats. The beneficial effects of S-23 on the muscle, tissue selectivity, and favorable pharmacokinetic properties make it a strong candidate for use in oral male contraception. An aryl-propionamide selective androgen receptor modulator (S-23) is an effective and reversible agent for hormonal male contraception in rats.

Published

2008

17. Nonsteroidal Tissue‐Selective Androgen Receptor Modulators

Author

Yali He, Casey E. Bohl, James T. Dalton, Michael L. Mohler, Duane D. Miller, Dong Jin Hwang, and Ramesh Narayanan

Subjects

medicine.medical_specialty, Nonsteroidal, business.industry, Osteoporosis, Cancer cachexia, medicine.disease, Androgen receptor, chemistry.chemical_compound, Endocrinology, chemistry, Selective androgen receptor modulator, Internal medicine, Sarcopenia, medicine, business

Published

2008

18. Hydrogen utilization as a fuel: hydrogen-blending effects in flame structure and NO emission behaviour of CH4–air flame

Author

June Sung Park, Sang In Keel, Jeong Park, Jeong Soo Kim, Tae Kwon Kim, Dong-Jin Hwang, Han Chang Cho, and Dong Soon Noh

Subjects

Premixed flame, Waste management, Hydrogen, Renewable Energy, Sustainability and the Environment, Chemistry, Diffusion flame, Flame structure, Energy Engineering and Power Technology, chemistry.chemical_element, Methane, Adiabatic flame temperature, chemistry.chemical_compound, Fuel Technology, Nuclear Energy and Engineering, Chemical engineering, Fuel efficiency, Nitrogen oxide

Abstract

Hydrogen-blending effects in flame structure and NO emission behaviour are numerically studied with detailed chemistry in methane–air counterflow diffusion flames. The composition of fuel is systematically changed from pure methane to the blending fuel of methane–hydrogen through H2 molar addition up to 30%. Flame structure, which can be described representatively as a fuel consumption layer and a H2–CO consumption layer, is shown to be changed considerably in hydrogen-blending methane flames, compared to pure methane flames. The differences are displayed through maximum flame temperature, the overlap of fuel and oxygen, and the behaviours of the production rates of major species. Hydrogen-blending into hydrocarbon fuel can be a promising technology to reduce both the CO and CO2 emissions supposing that NOx emission should be reduced through some technologies in industrial burners. These drastic changes of flame structure affect NO emission behaviour considerably. The changes of thermal NO and prompt NO are also provided according to hydrogen-blending. Importantly contributing reaction steps to prompt NO are addressed in pure methane and hydrogen-blending methane flames. Copyright © 2006 John Wiley & Sons, Ltd.

Published

2007

19. Edge flame instability in low-strain-rate counterflow diffusion flames

Author

Sang In Keel, June Sung Park, Dong Soon Noh, Jeong Park, Tae Kwon Kim, Jeong Soo Kim, Dong-Jin Hwang, and Sungcho Kim

Subjects

Premixed flame, Laminar flame speed, Oscillation, Chemistry, General Chemical Engineering, Diffusion flame, General Physics and Astronomy, Energy Engineering and Power Technology, Thermodynamics, General Chemistry, Mechanics, Strain rate, Flame speed, humanities, Lewis number, fluids and secretions, Fuel Technology, Diffusion (business), reproductive and urinary physiology

Abstract

Experiments in low-strain-rate methane–air counterflow diffusion flames diluted with nitrogen have been conducted to study flame extinction behavior and edge flame oscillation in which flame length is less than the burner diameter and thus lateral conductive heat loss, in addition to radiative loss, could be high at low global strain rates. The critical mole fraction at flame extinction is examined in terms of velocity ratio and global strain rate. Onset conditions of the edge flame oscillation and the relevant modes are also provided with global strain rate and nitrogen mole fraction in the fuel stream or in terms of fuel Lewis number. It is observed that flame length is intimately relevant to lateral heat loss, and this affects flame extinction and edge flame oscillation considerably. Lateral heat loss causes flame oscillation even at fuel Lewis number less than unity. Edge flame oscillations, which result from the advancing and retreating edge flame motion of the outer flame edge of low-strain-rate flames, are categorized into three modes: a growing, a decaying, and a harmonic-oscillation mode. A flame stability map based on the flame oscillation modes is also provided for low-strain-rate flames. The important contribution of lateral heat loss even to edge flame oscillation is clarified finally.

Published

2006

20. In Vitroandin VivoStructure-Activity Relationships of Novel Androgen Receptor Ligands with Multiple Substituents in the B-Ring

Author

Jiyun Chen, James T. Dalton, Casey E. Bohl, Kiwon Chung, Scott J. Fisher, Duane D. Miller, and Dong Jin Hwang

Subjects

Male, Transcriptional Activation, Agonist, medicine.medical_specialty, Chemical Phenomena, medicine.drug_class, Stereochemistry, Ligands, Binding, Competitive, Article, Cell Line, Rats, Sprague-Dawley, Radioligand Assay, Structure-Activity Relationship, Halogens, Endocrinology, In vivo, Internal medicine, medicine, Radioligand, Animals, Structure–activity relationship, Receptor, Molecular Structure, Chemistry, Biological activity, Rats, Androgen receptor, Receptors, Androgen, Orchiectomy

Abstract

We recently reported two nonsteroidal androgen receptor (AR) ligands that demonstrate tissue-selective pharmacological activity, identifying these S-3-(phenoxy)-2-hydroxy-2-methyl-N-(4-nitro-3-trifluoromethyl-phenyl)-propionamide analogs as the first members of a new class of drugs known as selective androgen receptor modulators. The purpose of these studies was to explore additional structure-activity relationships of selective androgen receptor modulators to enhance their AR binding affinity, AR-mediated transcriptional activation, and in vivo pharmacological activity. The AR binding affinity (K(i)) of 29 novel synthetic AR ligands was determined by a radioligand competitive binding assay and ranged from 1.0-51 nM. Compounds with electron-withdrawing substituents at the para- and meta-positions of the B-ring demonstrated the highest AR binding affinity. The AR-mediated transcriptional activation was determined using a cotransfection assay in CV-1 cells. Most compounds with two substituents in the B-ring maintained or improved their functional activity in vitro. However, compounds with three halogen substituents exhibited significant regioselectivity. Fifteen compounds were selected to examine their pharmacological activity in castrated rats. In vivo pharmacological activity and selectivity were significantly changed by structural modification in the B-ring. Compounds with halogen groups at the para- and meta-positions of the B-ring displayed the highest pharmacological activity. Incorporating substituents at the ortho-position of the B-ring resulted in poor pharmacological activity. In vitro and in vivo agonist activities were partially correlated. In conclusion, novel selective androgen receptor modulators with improved in vivo pharmacological activity can be designed and synthesized based on the structure-activity relationship identified in these studies.

Published

2005

21. Nonsteroidal tissue selective androgen receptor modulators: a promising class of clinical candidates

Author

Duane D. Miller, Renukadevi Patil, Igor M. Rakov, Dong Jin Hwang, Michael L. Mohler, and Vipin A. Nair

Subjects

Pharmacology, Agonist, Nonsteroidal, medicine.drug_class, Antagonist, Endogeny, General Medicine, urologic and male genital diseases, Androgen receptor, chemistry.chemical_compound, chemistry, Nuclear receptor, Dihydrotestosterone, Drug Discovery, medicine, Testosterone, medicine.drug

Abstract

The androgen receptor (AR) is a nuclear hormone receptor that, upon binding to testosterone, dihydrotestosterone (DHT) and other endogenous androgens, supports the development, growth and maintenance of masculine features through activation of anabolic and androgenic metabolism. The AR has been demonstrated to be a productive therapeutic target. AR ligands in clinical practice include androgenic steroids, antiandrogenic steroids and antiandrogenic nonsteroidals. Of primary importance for this review are nonsteroidal selective AR modulators (SARMs) that have tissue-specific agonist and/or antagonist activities. The AR has a myriad of peripheral and central functions that can be modulated in a pleiotropic and tissue-specific fashion using the increasingly diverse collection of SARMs discussed herein. This suggests that SARMs will have a high level of clinical utility for a wide variety of health conditions. The patent literature focusing on SARMs is reviewed and reveals multiple chemical classes in various ...

Published

2005

22. The Para Substituent of S-3-(Phenoxy)-2-hydroxy-2-methyl-N-(4-nitro-3-trifluoromethyl-phenyl)-propionamides Is a Major Structural Determinant of in Vivo Disposition and Activity of Selective Androgen Receptor Modulators

Author

James T. Dalton, Di Wu, Duane D. Miller, Juhyun Kim, and Dong Jin Hwang

Subjects

Male, medicine.medical_specialty, medicine.drug_class, Pharmacology, Rats, Sprague-Dawley, Structure-Activity Relationship, chemistry.chemical_compound, In vivo, Internal medicine, medicine, Animals, Potency, Trifluoromethyl, Dose-Response Relationship, Drug, Biological activity, Androgen, Amides, In vitro, Rats, Androgen receptor, Endocrinology, chemistry, Selective androgen receptor modulator, Receptors, Androgen, Androgens, Molecular Medicine

Abstract

Selective androgen receptor modulators (SARMs) have many potential therapeutic applications, including male hypogonadism, osteoporosis, muscle-wasting diseases, sexual libido, and contraception. A series of S-3-(phenoxy)-2-hydroxy-2-methyl-N-(4-nitro-3-trifluoromethyl-phenyl)-propionamides bearing a four-halogen substituent in the B-ring that displayed in vivo activity were identified in our previous study. Interestingly, in vivo pharmacological activity was not correlated with in vitro androgen receptor (AR) binding affinity. In this study, analysis of the area under the concentration-time curve-response relationship demonstrated that the discrepancy between in vitro and in vivo pharmacological activity of these halogen-substituted SARMs was due to differences in systemic exposure rather than intrinsic pharmacological activity. Studies also suggested that two simple criteria (i.e., Ki10 nM and lower in vivo clearance) could be used to identify efficacious and potent SARMs. We tested this hypothesis using a series of four compounds incorporating either a nitro or cyano substituent at the para-position of the A- and B-aromatic rings. The S-3-(4-nitrophenoxy) and S-3-(4-cyanophenoxy) 2-hydroxy-2-methyl-N-(4-nitro-3-trifluromethylphenyl) propionamides (S-19 and S-20, respectively) and S-3-(4-nitrophenoxy) and S-3-(4-cyanophenoxy) 2-hydroxy-2-methyl-N-(4-cyano-3-trifluromethylphenyl) propionamides (S-21 and S-22, respectively) demonstrated high AR binding affinity, with Ki values ranging from 2.0 to 3.8 nM. Pharmacokinetic studies of selected compounds showed that the in vivo clearance of S-22 was the slowest followed sequentially by S-20, S-21, and S-19. The dose-response relationships for S-22 showed that S-22 exerted efficacious and selective activity in anabolic tissues at dose rates as low as 0.03 mg/day, indicative of the high potency of this compound in anabolic tissue (relative potency 4.41) and its potential for clinical use in androgen deficiency-related disorders.

Published

2005

23. Numerical study on NO formation in CH4-O2-N2 diffusion flame diluted with CO2

Author

Dong-Jin Hwang, Kyung-Hwan Lee, Jeong Park, Chang-Bo Oh, and Sang-In Keel

Subjects

Renewable Energy, Sustainability and the Environment, Chemistry, Reaction step, Flame structure, Diffusion flame, Energy Engineering and Power Technology, Thermodynamics, Branching (polymer chemistry), Adiabatic flame temperature, Dilution, Chemical effects, Fuel Technology, Nuclear Energy and Engineering, Organic chemistry, No formation

Abstract

SUMMARY Numerical study with momentum-balanced boundary conditions has been conducted to grasp chemical effects of added CO2, to either fuel- or oxidizer-side on flame structure and NO emission behaviour in CH4–O2–N2 diffusion flames. Cautious investigation is made for the comparison among the behaviours of principal chain branching and important H-removal key reactions. This describes successfully the reason why flame temperatures for fuel-side dilution are higher than those for oxidizer-side dilution. The role of the principal chain branching reaction is also recognized to be important even in the change of major flame structure caused by chemical effects. The importantly contributing reaction steps to NO production are examined. The reduced production rates of thermal NO and prompt NO due to chemical effects are much more remarkable for fuel-side dilution. It is also found that the reaction step, H+NO+M=HNO þ M plays a decisive role of the formation and destruction of prompt NO. Copyright # 2005 John Wiley & Sons, Ltd.

Published

2005

24. Numerical study on flame structure and NO formation in CH4-O2-N2 counterflow diffusion flame diluted with H2O

Author

Chang-Bo Ch, Jongwook Choi, Jeong Park, Dong-Soon Noh, Sang-In Keel, and Dong-Jin Hwang

Subjects

Renewable Energy, Sustainability and the Environment, Chemistry, Reaction step, Radical, Diffusion flame, Flame structure, Energy Engineering and Power Technology, Branching (polymer chemistry), Adiabatic flame temperature, Reaction rate, Fuel Technology, Nuclear Energy and Engineering, Chemical engineering, Thermal, Physical chemistry

Abstract

SUMMARY Numerical study on flame structure and NO emission behaviour has been conducted to grasp chemical effects of added H2O on either fuel- or oxidizer-side in CH4–O2–N2 counterflow diffusion flames. An artificial species, which has the same thermodynamic, transport, and radiation properties of added H2O, is introduced to feasibly isolate the chemical effects. Special concern is focused on the important role of remarkably produced OH radicals due to chemical effects of added H2O on flame structure and NO emission. The reason why the difference of behaviours between the principal chain branching reaction rate and flame temperature appear is attributed to the drastic change of reaction step (R120) from the production to the consumption of OH. It is also, however, seen that the most important contribution of produced OH due to chemical effects of added H2O is through reaction step (R127). The importantly contributing reaction steps to NO production are also examined. The production rates of thermal NO and prompt NO are suppressed by chemical effects of added H2O. The contribution of the reaction steps related to HNO intermediate species to the production of prompt NO is also stressed. Copyright # 2004 John Wiley & Sons, Ltd.

Published

2004

25. Comparative study of flame structures and NOx emission characteristics in fuel injection recirculation and fuel gas recirculation combustion system

Author

Sung-Hoon Shim, Jin Oh Chung, Seong-Beom Lee, Jeong Park, Sang-In Keel, and Dong-Jin Hwang

Subjects

Premixed flame, Waste management, Hydrogen, Laminar flame speed, Renewable Energy, Sustainability and the Environment, Chemistry, Diffusion flame, Flame structure, Energy Engineering and Power Technology, Thermodynamics, chemistry.chemical_element, Combustion, Adiabatic flame temperature, Fuel Technology, Nuclear Energy and Engineering, Fuel gas

Abstract

SUMMARY A numerical study with momentum-balanced boundary conditions has been conducted to grasp the chemical effects of added CO2 to fuel- and oxidizer-sides on flame structure and NO emission behaviour in H2–O2 diffusion flames with varying flame location. A reaction mechanism is proposed to show better agreements with experimental results in CO2-added hydrogen flames. Oxidizer-side dilution results in significantly higher flame temperatures and NO emission. Flame location is dramatically changed due to high diffusivity of hydrogen according to variation of the composition of fuel- and oxidizer-sides. This affects flame structure and NO emission considerably especially the chemical effects of added CO2. The present work also displays separately thermal contribution and prompt NO emission due to the chemical effects caused by thermal dissociation of added CO2 in NO emission behaviour. It is found that flame temperature and the flame location affect the contribution of thermal and prompt NO due to chemical effects considerably in NO emission behaviour. Copyright # 2004 John Wiley & Sons, Ltd.

Published

2004

26. Evaluation of chemical effects of added CO2 according flame location

Author

Sung-Beom Lee, Dong-Jin Hwang, Sang-In Keel, Kang-Tae Kim, and Jeong Park

Subjects

Reaction mechanism, Hydrogen, Renewable Energy, Sustainability and the Environment, Reaction step, Flame structure, Energy Engineering and Power Technology, chemistry.chemical_element, Branching (polymer chemistry), Dilution, Adiabatic flame temperature, chemistry.chemical_compound, Fuel Technology, Nuclear Energy and Engineering, chemistry, Carbon dioxide, Physical chemistry, Organic chemistry

Abstract

A numerical study has been conducted to clearly grasp the impact of chemical effects caused by added CO 2 and of flame location on flame structure and NO emission behaviour. Flame location affects the major source reaction of CO formation. CO 2 + H → CO + OH and the H-removal reaction, CH 4 + H → CH 3 + H 2 . It is, as a result, seen that the reduction of maximum flame temperature due to chemical effects for fuel-side dilution is mainly caused by the competition of the principal chain branching reaction with the reaction, CH 4 + H → CH 3 + H 2 . while that for fuel-side dilution is attributed to the competition of the principal chain branching reaction with the reaction, CO 2 + H → CO + OH. The importance of the NNH mechanism for NO production, where the reaction pathway is NNH -> NH → HNO, is recognized. In C-related reactions most of NO is the direct outcome of (R171) and the contribution of (R171) becomes more and more important with increasing amount of added CO 2 as much as the reaction step (R171) competes with the key reaction of thermal mechanism, (R237), for N atom. This indicates a possibility that NO emission in hydrogen flames diluted with CO 2 shows less dependent behaviour upon flame temperature.

Published

2004

27. Chemical effects of CO2 addition to oxidizer and fuel streams on flame structure in H2-O2 counterflow diffusion flames

Author

Jong-Geun Choi, Dong-Jin Hwang, Jeong Park, Sang-In Keel, Kee-Man Lee, and Sung-Hoon Shim

Subjects

Premixed flame, Waste management, Hydrogen, Renewable Energy, Sustainability and the Environment, Chemistry, Diffusion, Diffusion flame, Flame structure, Energy Engineering and Power Technology, chemistry.chemical_element, Thermodynamics, Mole fraction, Oxygen, Adiabatic flame temperature, Fuel Technology, Nuclear Energy and Engineering

Abstract

Numerical simulation of CO2 addition effects to fuel and oxidizer streams on flame structure has been conducted with detailed chemistry in H2–O2 diffusion flames of a counterflow configuration. An artificial species, which displaces added CO2 in the fuel- and oxidizer-sides and has the same thermochemical, transport, and radiation properties to that of added CO2, is introduced to extract pure chemical effects in flame structure. Chemical effects due to thermal dissociation of added CO2 causes the reduction flame temperature in addition to some thermal effects. The reason why flame temperature due to chemical effects is larger in cases of CO2 addition to oxidizer stream is well explained though a defined characteristic strain rate. The produced CO is responsible for the reaction, CO2+H=CO+OH and takes its origin from chemical effects due to thermal dissociation. It is also found that the behavior of produced CO mole fraction is closely related to added CO2 mole fraction, maximum H mole fraction and its position, and maximum flame temperature and its position. Copyright © 2003 John Wiley & Sons, Ltd.

Published

2003

28. SYNTHESIS OF CYCLOPENTENE-FUSED PYRROLOISOQUINOLINONE DERIVATIVE VIAN-ACYLIMINIUM ION CYCLIZATION

Author

Hokoon Park, Jae Yeol Lee, Soosung Kang, Jung Hoon Choi, Dong Jin Hwang, and Yong Sup Lee

Subjects

chemistry.chemical_compound, Cyclopentadiene, chemistry, Silylation, Yield (chemistry), Organic Chemistry, Epoxide, Cyclopentene, Isoquinoline, Ring (chemistry), Medicinal chemistry, Derivative (chemistry)

Abstract

In this research, a new class of pyrrolo[2,1-a]isoquinolinone derivative 7 was prepared. C-4 Hydroxylated 5-ethoxylactam 1b gave 4,5-epoxylactam 2 in high yield instead of isoquinoline derivative 3b under the N-acyliminium ion cyclization condition. The 4,5-epoxylactam 2 was converted to another N-acyliminium ion precursor 6 through base-promoted epoxide ring opening, silylation, and thermal Diels–Alder reaction with cyclopentadiene in high yield. Finally, compound 6 was cyclized in the presence of TiCl4 to provide cyclopentene-fused pyrroloisoquinoline derivative 7.

Published

2002

29. Abstract 3223: Novel tubulin inhibitor DJ101 targets the colchicine binding site and suppresses melanoma growth and metastasis

Author

Kinsie Arnst, Dong-Jin Hwang, Duane D. Miller, and Wei Li

Subjects

Cancer Research, biology, Chemistry, Melanoma, Cancer, medicine.disease, Cell morphology, Metastasis, Tubulin, Oncology, Mechanism of action, Microtubule, Cancer cell, medicine, biology.protein, Cancer research, medicine.symptom

Abstract

Interfering with microtubule dynamics is a validated approach for anticancer treatment and by selectively targeting the colchicine binding site on tubulin, microtubule destabilizing agents can evade mechanisms of drug resistance that commonly develop with other antimitotic agents such as taxanes and vinca alkaloids. We have recently reported the discovery of a potent and metabolically stable tubulin inhibitor (DJ101) that specifically targets the colchicine binding site on the beta tubulin subunit, disrupts tubulin polymerization and effectively circumvents drug efflux pumps that decrease the efficacy of existing tubulin inhibitors. To further pre-clinically evaluate DJ101 as a novel tubulin inhibitor and confirm its mechanism of action, we first visually demonstrated the ability of DJ101 to disrupt microtubule dynamics and elucidated the changes in microtubule structure and cell morphology through immunofluorescence techniques. Furthermore, we solved the crystal structure of DJ101 in complex with tubulin to determine its molecular interactions with the protein. We then demonstrated the significant in vitro potency of DJ101 against a panel of metastatic melanoma cell lines harboring major clinically relevant mutations observed in tumors and also validated its cytotoxicity against a broader array of NCI-60 cell lines. Further analysis revealed that DJ101 effectively thwarted anchorage-dependent melanoma colony formation and drastically hindered cell mobility and motility of those cancer cells. We further ascertained that DJ101 shows negligible off-target effects for major physiologically important receptors and ion channels, suggesting a good safety profile. Encouraged by the preliminary results from our in vitro assessment, we evaluated the in vivo activity of DJ101 in two different mouse models. At a dose of 30 mg/kg via i.p. injections, DJ101 nearly completely suppressed tumor growth in a human A375 melanoma xenograft model. It also appreciably inhibited metastasis potential in a murine B16F10 lung metastasis model at the same dose. In conclusion, we have described a microtubule destabilizing agent that targets the colchicine binding site on tubulin, confirmed its mechanism action, determined its potency in a vast array of cancer cell lines, particularly metastatic melanoma, demonstrated its inhibitory effect on cellular proliferation, motility and migration, and evaluated its anticancer potential in terms of tumor growth inhibition and metastasis in two in vivo models. Our findings offer a compelling rationale to further develop and advance DJ101 as a tubulin inhibitor for cancer therapy. Citation Format: Kinsie Arnst, Dong-Jin Hwang, Duane D. Miller, Wei Li. Novel tubulin inhibitor DJ101 targets the colchicine binding site and suppresses melanoma growth and metastasis [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2017; 2017 Apr 1-5; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2017;77(13 Suppl):Abstract nr 3223. doi:10.1158/1538-7445.AM2017-3223

Published

2017

30. Anthrax toxin lethal factor domain 3 is highly mobile and responsive to ligand binding

Author

Elbek K. Kurbanov, Teresa De la Mora-Rey, Kimberly M. Maize, Dong Jin Hwang, Michael A. Walters, Todd W. Geders, Rodney L. Johnson, Elizabeth A. Amin, and Barry C. Finzel

Subjects

Models, Molecular, Stereochemistry, Protein Conformation, Anthrax toxin, Bacterial Toxins, Peptide, Crystallography, X-Ray, Ligands, Anthrax, Protein structure, Structural Biology, Hydrolase, Humans, Binding site, Protein kinase A, chemistry.chemical_classification, Antigens, Bacterial, Sulfonamides, Binding Sites, biology, Chemistry, fungi, Metalloendopeptidases, General Medicine, biology.organism_classification, Ligand (biochemistry), Research Papers, Bacillus anthracis, Protein Structure, Tertiary, Drug Design, Peptides

Abstract

The secreted anthrax toxin consists of three components: the protective antigen (PA), edema factor (EF) and lethal factor (LF). LF, a zinc metalloproteinase, compromises the host immune system primarily by targeting mitogen-activated protein kinase kinases in macrophages. Peptide substrates and small-molecule inhibitors bind LF in the space between domains 3 and 4 of the hydrolase. Domain 3 is attached on a hinge to domain 2viaresidues Ile300 and Pro385, and can move through an angular arc of greater than 35° in response to the binding of different ligands. Here, multiple LF structures including five new complexes with co-crystallized inhibitors are compared and three frequently populated LF conformational states termed `bioactive', `open' and `tight' are identified. The bioactive position is observed with large substrate peptides and leaves all peptide-recognition subsites open and accessible. The tight state is seen in unliganded and small-molecule complex structures. In this state, domain 3 is clamped over certain substrate subsites, blocking access. The open position appears to be an intermediate state between these extremes and is observed owing to steric constraints imposed by specific bound ligands. The tight conformation may be the lowest-energy conformation among the reported structures, as it is the position observed with no bound ligand, while the open and bioactive conformations are likely to be ligand-induced.

Published

2014

31. HIV-1 integrase inhibitory phenylpropanoid glycosides fromClerodendron trichotomum

Author

Cha-Gyun Shin, Dong Jin Hwang, Hokoon Park, Eun-Rhan Woo, Hyoung Ja Kim, and Yong Sup Lee

Subjects

Spectrometry, Mass, Electrospray Ionization, Magnetic Resonance Spectroscopy, Phenylpropanoid glycosides, Stereochemistry, Oligonucleotides, Disaccharides, Inhibitory postsynaptic potential, Clerodendron trichotomum, Spectroscopy, Fourier Transform Infrared, Drug Discovery, Ic50 values, Humans, HIV Integrase Inhibitors, Plants, Medicinal, biology, Plant Extracts, Chemistry, Guaiacol, Organic Chemistry, Integrase, Jionoside D, HIV-1, biology.protein, Hiv 1 integrase, Molecular Medicine, Spectrophotometry, Ultraviolet, Martynoside

Abstract

Seven phenylpropanoid glycosides named acteoside (1), acteoside isomer (2), leucosceptoside A (3), plantainoside C (4), jionoside D (5), martynoside (6), and isomartynoside (7) were isolated from Clerodendron trichotomum. Compounds 1 and 2 showed potent inhibitory activities against HIV-1 integrase with IC50 values of 7.8 +/- 3.6 and 13.7 +/- 6.0 microM, respectively.

Published

2001

32. Dicaffeoyl- or digalloyl pyrrolidine and furan derivatives as HIV integrase inhibitors

Author

Yong Sup Lee, Jung Hoon Choi, Sun Nam Kim, and Dong Jin Hwang

Subjects

Pyrrolidines, Stereochemistry, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Biochemistry, Chemical synthesis, Pyrrolidine, Inhibitory Concentration 50, Structure-Activity Relationship, chemistry.chemical_compound, Caffeic Acids, Drug Discovery, Structure–activity relationship, HIV Integrase Inhibitors, Furans, Molecular Biology, chemistry.chemical_classification, biology, Organic Chemistry, Succinates, biology.organism_classification, Integrase, Enzyme, chemistry, Enzyme inhibitor, Lentivirus, HIV-1, biology.protein, Molecular Medicine, Lactone

Abstract

Human immunodeficiency virus (HIV) integrase (IN) catalyzes the integration of HIV DNA copy into the host cell DNA. Such integration is essential for the production of progeny viruses, and therefore therapeutic agents that can inhibit this process should be effective anti-HIV agents. We have previously reported the inhibitory activity of dicaffeoylglucosides against HIV IN. In the present study, we have synthesized and tested dicaffeoyl or digalloyl compounds joined through a five-membered heterocyclic ring as HIV IN inhibitors to explore the SARs of this family of compounds. The starting heterocyclic diols were prepared from L-tartaric acid, diethyl L-tartarate or D-(+)-ribonic gamma-lactone. We found that the HIV IN inhibitory activities of dicaffeoyl derivatives were comparable to that of L-chicoric acid (IC(50)=24.9 microM). On the other hand, digalloyl derivatives were more potent than L-chicoric acid with IC(50) values of 4.7--15.6 microM.

Published

2001

33. ChemInform Abstract: Synthesis of Cyclopentene-Fused Pyrroloisoquinolinone Derivative via N-Acyliminium Ion Cyclization

Author

Jung Hoon Choi, Hokoon Park, Yong Sup Lee, Dong Jin Hwang, Soosung Kang, and Jae Yeol Lee

Subjects

chemistry.chemical_compound, Cyclopentadiene, chemistry, Silylation, Yield (chemistry), Organic chemistry, Epoxide, Cyclopentene, General Medicine, Isoquinoline, Ring (chemistry), Medicinal chemistry, Derivative (chemistry)

Abstract

In this research, a new class of pyrrolo[2,1-a]isoquinolinone derivative 7 was prepared. C-4 Hydroxylated 5-ethoxylactam 1b gave 4,5-epoxylactam 2 in high yield instead of isoquinoline derivative 3b under the N-acyliminium ion cyclization condition. The 4,5-epoxylactam 2 was converted to another N-acyliminium ion precursor 6 through base-promoted epoxide ring opening, silylation, and thermal Diels–Alder reaction with cyclopentadiene in high yield. Finally, compound 6 was cyclized in the presence of TiCl4 to provide cyclopentene-fused pyrroloisoquinoline derivative 7.

Published

2010

34. ChemInform Abstract: Nonsteroidal Selective Androgen Receptor Modulators (SARMs): Dissociating the Anabolic and Androgenic Activities of the Androgen Receptor for Therapeutic Benefit

Author

Amanda Jones, Michael L. Mohler, Yali He, Ramesh Narayanan, Dong Jin Hwang, Miller Duane D, James T. Dalton, Christopher C. Coss, and Casey E. Bohl

Subjects

Nonsteroidal, Anabolism, medicine.drug_class, Chemistry, Anabolic androgen, General Medicine, Pharmacology, Androgen, Androgen receptor, chemistry.chemical_compound, Nuclear receptor, Androgen Therapy, medicine, Testosterone

Abstract

Interest in the development and therapeutic potential of nonsteroidal tissue-selective androgen receptor modulators (SARMs) has increased dramatically within the past decade. Rapidly expanding knowledge of nuclear hormone receptor structure and function and successful proof-of-principle clinical trials with SARMs have revived an almost dormant search for improved androgens. This Award Address attempts to chronicle the landmark discoveries (with emphasis on our work), organize the SARM landscape into clinically relevant bins, and provide insight into the clinical prospects for SARMs. 1.1. Origins of Androgen Use. An early (1889) and unusual experiment in androgen therapy was performed by Charles Edouard Brown-Sequard, age 72. He administered a testicular extract to himself and reported that he felt “increased vigor and capacity for work”. Despite retrospective suggestions that any effect was purely placebo, this report resulted in widespread use of testicular extracts throughout Europe and North America for several decades. Attempts to isolate the active components of testicular extract failed until 1935 when testosterone (17 hydroxy-4-andosten-3-one) was isolated from bull testes. Shortly thereafter, its synthesis was reported. In the same year, extracts of urine from males were shown to cause nitrogen retention, an indicator of anabolic metabolism. Testosterone was the first anabolic androgen to be used clinically, but its use is limited by its androgenicity and pharmacokinetic (PK) issues. 1 In the latter half of the 20th century, the chemical scaffold of testosterone was modified extensively, producing many

Published

2009

35. ChemInform Abstract: Recent and Emerging anti-Diabetes Targets

Author

Dong Jin Hwang, Duane D. Miller, Zhongzhi Wu, Yali He, and Michael L. Mohler

Subjects

medicine.medical_specialty, Blindness, Chemistry, Diabetes mellitus, medicine, Developing country, General Medicine, Disease, medicine.disease, Intensive care medicine, Obesity, Glycemic

Abstract

Diabetes is a disease that affects over 150 million people worldwide for which there are multiple oral and injectable medications. Because of trends in obesity and sedentary lifestyles, diabetes rates in both developed and developing countries are increasing at an alarming rate. Current medications are not adequately effective in maintaining long-term glycemic control in most patients, even when used in combination, leaving diabetics susceptible to developing life threatening and debilitating complications such as cardiovascular disease, blindness, kidney complications, and amputations. Consequently, there is a critical need for more potent pharmacotherapies with novel mechanisms of action. A panel of 20 emerging diabetes targets is presented, and small molecule modulators for each target will be discussed.

Published

2009

36. Effect of B-ring substitution pattern on binding mode of propionamide selective androgen receptor modulators

Author

Suni M. Mustafa, Casey E. Bohl, Charles E. Bell, Zengru Wu, Dong Jin Hwang, Duane D. Miller, Michael L. Mohler, Jiyun Chen, James T. Dalton, and Jun Yang

Subjects

Male, Cachexia, Molecular model, Stereochemistry, medicine.drug_class, Chemistry, Pharmaceutical, Clinical Biochemistry, Nitro compound, Molecular Conformation, Pharmaceutical Science, Carboxamide, Crystallography, X-Ray, Ligands, Biochemistry, Article, Prostate cancer, Drug Discovery, medicine, Molecule, Humans, Molecular Biology, chemistry.chemical_classification, Chemistry, Hydrogen bond, Muscles, Organic Chemistry, medicine.disease, Amides, Protein Structure, Tertiary, Androgen receptor, Selective androgen receptor modulator, Models, Chemical, Receptors, Androgen, Drug Design, Molecular Medicine, Osteoporosis

Abstract

Selective androgen receptor modulators (SARMs) are essentially prostate sparing androgens, which provide therapeutic potential in osteoporosis, male hormone replacement, and muscle wasting. Herein we report crystal structures of the androgen receptor (AR) ligand-binding domain (LBD) complexed to a series of potent synthetic nonsteroidal SARMs with a substituted pendant arene referred to as the B-ring. We found that hydrophilic B-ring para-substituted analogs exhibit an additional region of hydrogen bonding not seen with steroidal compounds and that multiple halogen substitutions affect the B-ring conformation and aromatic interactions with Trp741. This information elucidates interactions important for high AR binding affinity and provides new insight for structure-based drug design.

Published

2008

37. Arylisothiocyanato selective androgen receptor modulators (SARMs) for prostate cancer

Author

Huiping Xu, Duane D. Miller, Jun Yang, Michael L. Mohler, Dong Jin Hwang, Igor M. Rakov, and James T. Dalton

Subjects

Male, Spectrometry, Mass, Electrospray Ionization, Magnetic Resonance Spectroscopy, Bicalutamide, Chemical Phenomena, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Antineoplastic Agents, Ligands, Biochemistry, Article, chemistry.chemical_compound, Prostate cancer, Structure-Activity Relationship, DU145, Thioether, Isothiocyanates, Cell Line, Tumor, Drug Discovery, LNCaP, medicine, Structure–activity relationship, Animals, Humans, Molecular Biology, Cell Proliferation, Cell growth, Chemistry, Physical, Rhodamines, Organic Chemistry, Prostatic Neoplasms, Haplorhini, medicine.disease, Androgen receptor, chemistry, Receptors, Androgen, Molecular Medicine, medicine.drug

Abstract

A new series of androgen receptor targeted agents (ARTA) was prepared and tested in androgen-dependent and -independent prostate cancer cell lines. These agents were bicalutamide analogs with isothiocyanato substituted B-rings. Also, the linker sulfone of R-bicalutamide was maintained or replaced with several alternative linkages including ether, amine, N-methylamine, thioether, and methylene (in this case the product was a racemic mixture) functional groups at the X-position. To expand the structure–activity relationship (SAR) of these arylisothiocyanato AR ligands, B-ring halogenated arylisothiocyanato ligands were also prepared and tested. The arylisothiocyanato AR ligands showed strong binding affinities to AR ranging from 0.6 to 54 nM. Among them, thioether and ether linkages demonstrated high binding affinities (0.6 and 4.6 nM, respectively) and selective cell growth inhibition (approximately 3- to 6-fold) for LNCaP, an androgen-dependent prostate cancer cell line, when compared to the androgen independent prostate cell lines (DU145, PC-3, and PPC-1) and a bladder cell line (TSU-Pr1). However, the ligands were inactive (IC50>100 mM) in a normal monkey kidney cell line (CV-1) that was used as the control for non-specific toxicity.

Published

2006