Your search keyword '"Chen, Ct"' showing total 25 results

1. DBPR116, a Prodrug of BPRMU191, in Combination with Naltrexone as a Safer Opioid Analgesic Than Morphine via Peripheral Administration.

Author

Lin SY, Chang YC, Tien YW, Kuo YH, Chang HF, Ou LC, Chen YP, Chang KH, Hsu YT, Huang YC, Yang CM, Law PY, Xi JH, Tao PL, Loh HH, Yeh TK, Zhuang H, Hsieh HP, Shih C, Chen CT, Yeh SH, and Ueng SH

Subjects

Animals, Male, Mice, Pain drug therapy, Cancer Pain drug therapy, Morphinans pharmacology, Morphinans therapeutic use, Morphinans chemistry, Morphinans pharmacokinetics, Blood-Brain Barrier metabolism, Prodrugs pharmacology, Prodrugs chemistry, Naltrexone analogs & derivatives, Naltrexone pharmacology, Naltrexone pharmacokinetics, Naltrexone administration & dosage, Naltrexone therapeutic use, Analgesics, Opioid pharmacology, Analgesics, Opioid adverse effects, Analgesics, Opioid administration & dosage, Morphine adverse effects, Morphine administration & dosage, Morphine pharmacology

Abstract

The development of opioid analgesics with reduced adverse effects is an unmet need. In a previous study, we discovered a unique combination of BPRMU191 and morphinan antagonists that produced potent antinociception with reduced adverse effects after central administration (intrathecal or intracerebroventricular). BPRMU191/naltrexone exhibits notable in vitro and in vivo pharmacological properties. However, the poor blood-brain barrier penetrative ability of BPRMU191 restricts its clinical application. In this study, we utilized a prodrug strategy to deliver sufficient brain concentrations of BPRMU191 and selected compound 2 (DBPR116) with the best physicochemical and pharmacological properties among other in vivo active prodrugs. The in vivo pharmacological studies of compound 2 /naltrexone, including thermally stimulated pain, cancer pain, constipation, sedation, psychological dependence, heart rate, and respiratory frequency measurements, demonstrated that it was a safer opioid analgesic than morphine in pain control.

Published

2024

2. Development of Furanopyrimidine-Based Orally Active Third-Generation EGFR Inhibitors for the Treatment of Non-Small Cell Lung Cancer.

Author

Li MC, Coumar MS, Lin SY, Lin YS, Huang GL, Chen CH, Lien TW, Wu YW, Chen YT, Chen CP, Huang YC, Yeh KC, Yang CM, Kalita B, Pan SL, Hsu TA, Yeh TK, Chen CT, and Hsieh HP

Subjects

Animals, Humans, Mice, Cell Line, Tumor, Cell Proliferation, Drug Resistance, Neoplasm, Mutation, Administration, Oral, Antineoplastic Agents administration & dosage, Antineoplastic Agents pharmacology, Carcinoma, Non-Small-Cell Lung drug therapy, ErbB Receptors antagonists & inhibitors, ErbB Receptors genetics, Lung Neoplasms drug therapy, Protein Kinase Inhibitors administration & dosage, Protein Kinase Inhibitors pharmacology, Pyrimidines administration & dosage, Pyrimidines pharmacology

Abstract

The development of orally bioavailable, furanopyrimidine-based double-mutant (L858R/T790M) EGFR inhibitors is described. First, selectivity for mutant EGFR was accomplished by replacing the ( S )-2-phenylglycinol moiety of 12 with either an ethanol or an alkyl substituent. Then, the cellular potency and physicochemical properties were optimized through insights from molecular modeling studies by implanting various solubilizing groups in phenyl rings A and B. Optimized lead 52 shows 8-fold selective inhibition of H1975 (EGFR L858R/T790M overexpressing) cancer cells over A431 (EGFR WT overexpressing) cancer cells; western blot analysis further confirmed EGFR mutant-selective target modulation inside the cancer cells by 52 . Notably, 52 displayed in vivo antitumor effects in two different mouse xenograft models (BaF3 transfected with mutant EGFR and H1975 tumors) with TGI = 74.9 and 97.5% after oral administration ( F = 27%), respectively. With an extraordinary kinome selectivity ( S (10) score of 0.017), 52 undergoes detailed preclinical development.

Published

2023

3. Targeting the Phosphatidylserine-Immune Checkpoint with a Small-Molecule Maytansinoid Conjugate.

Author

Lo CF, Chiu TY, Liu YT, Pan PY, Liu KL, Hsu CY, Fang MY, Huang YC, Yeh TK, Hsu TA, Chen CT, Huang LR, and Tsou LK

Subjects

Humans, Ligands, RNA, Messenger, Sorafenib pharmacology, Sorafenib therapeutic use, Tumor Microenvironment, Phosphatidylserines, Triple Negative Breast Neoplasms

Abstract

Ligand-targeting drug delivery systems have made significant strides for disease treatments with numerous clinical approvals in this era of precision medicine. Herein, we report a class of small molecule-based immune checkpoint-targeting maytansinoid conjugates. From the ligand targeting ability, pharmacokinetics profiling, in vivo anti-pancreatic cancer, triple-negative breast cancer, and sorafenib-resistant liver cancer efficacies with quantitative mRNA analysis of treated-tumor tissues, we demonstrated that conjugate 40a not only induced lasting regression of tumor growth, but it also rejuvenated the once immunosuppressive tumor microenvironment to an "inflamed hot tumor" with significant elevation of gene expressions that were not accessible in the vehicle-treated tumor. In turn, the immune checkpoint-targeting small molecule drug conjugate from this work represents a new pharmacodelivery strategy that can be expanded with combination therapy with existing immune-oncology treatment options.

Published

2022

4. Discovery of Potential Neuroprotective Agents against Paclitaxel-Induced Peripheral Neuropathy.

Author

Chen YF, Wu CH, Chen LH, Lee HW, Lee JC, Yeh TK, Chang JY, Chou MC, Wu HL, Lai YP, Song JS, Yeh KC, Chen CT, Lee CJ, Shia KS, and Shen MR

Subjects

Animals, Ganglia, Spinal, Mice, Paclitaxel toxicity, Antineoplastic Agents pharmacology, Antineoplastic Agents, Phytogenic toxicity, Neuroprotective Agents pharmacology, Neuroprotective Agents therapeutic use, Peripheral Nervous System Diseases chemically induced, Peripheral Nervous System Diseases drug therapy, Peripheral Nervous System Diseases prevention & control

Abstract

Chemotherapy-induced neurotoxicity is a common adverse effect of cancer treatment. No medication has been shown to be effective in the prevention or treatment of chemotherapy-induced neurotoxicity. Using minoxidil as an initial template for structural modifications in conjunction with an in vitro neurite outgrowth assay, an image-based high-content screening platform, and mouse behavior models, an effective neuroprotective agent CN016 was discovered. Our results showed that CN016 could inhibit paclitaxel-induced inflammatory responses and infiltration of immune cells into sensory neurons significantly. Thus, the suppression of proinflammatory factors elucidates, in part, the mechanism of action of CN016 on alleviating paclitaxel-induced peripheral neuropathy. Based on excellent efficacy in improving behavioral functions, high safety profiles (MTD > 500 mg/kg), and a large therapeutic window (MTD/MED > 50) in mice, CN016 might have great potential to become a peripherally neuroprotective agent to prevent neurotoxicity caused by chemotherapeutics as typified by paclitaxel.

Published

2022

5. Discovery of BPR1R024, an Orally Active and Selective CSF1R Inhibitor that Exhibits Antitumor and Immunomodulatory Activity in a Murine Colon Tumor Model.

Author

Lee KH, Yen WC, Lin WH, Wang PC, Lai YL, Su YC, Chang CY, Wu CS, Huang YC, Yang CM, Chou LH, Yeh TK, Chen CT, Shih C, and Hsieh HP

Subjects

Administration, Oral, Animals, Antineoplastic Agents administration & dosage, Antineoplastic Agents chemistry, Cell Line, Tumor, Colonic Neoplasms pathology, Immunomodulating Agents administration & dosage, Immunomodulating Agents chemistry, Male, Mice, Mice, Inbred C57BL, Neoplasms, Experimental, Protein Kinase Inhibitors administration & dosage, Protein Kinase Inhibitors chemistry, Rats, Sprague-Dawley, Structure-Activity Relationship, Rats, Antineoplastic Agents pharmacology, Colonic Neoplasms drug therapy, Drug Discovery, Immunomodulating Agents pharmacology, Protein Kinase Inhibitors pharmacology, Receptor, Macrophage Colony-Stimulating Factor antagonists & inhibitors

Abstract

Colony-stimulating factor-1 receptor (CSF1R) is implicated in tumor-associated macrophage (TAM) repolarization and has emerged as a promising target for cancer immunotherapy. Herein, we describe the discovery of orally active and selective CSF1R inhibitors by property-driven optimization of BPR1K871 ( 9 ), our clinical multitargeting kinase inhibitor. Molecular docking revealed an additional nonclassical hydrogen-bonding (NCHB) interaction between the unique 7-aminoquinazoline scaffold and the CSF1R hinge region, contributing to CSF1R potency enhancement. Structural studies of CSF1R and Aurora kinase B (AURB) demonstrated the differences in their back pockets, which inspired the use of a chain extension strategy to diminish the AURA/B activities. A lead compound BPR1R024 ( 12 ) exhibited potent CSF1R activity (IC 50 = 0.53 nM) and specifically inhibited protumor M2-like macrophage survival with a minimal effect on antitumor M1-like macrophage growth. In vivo , oral administration of 12 mesylate delayed the MC38 murine colon tumor growth and reversed the immunosuppressive tumor microenvironment with the increased M1/M2 ratio.

Published

2021

6. Discovery and Synthesis of a Pyrimidine-Based Aurora Kinase Inhibitor to Reduce Levels of MYC Oncoproteins.

Author

Chi YH, Yeh TK, Ke YY, Lin WH, Tsai CH, Wang WP, Chen YT, Su YC, Wang PC, Chen YF, Wu ZW, Yeh JY, Hung MC, Wu MH, Wang JY, Chen CP, Song JS, Shih C, Chen CT, and Chang CP

Subjects

Animals, Aurora Kinase A metabolism, Aurora Kinase B antagonists & inhibitors, Aurora Kinase B metabolism, Binding Sites, Cell Proliferation drug effects, Down-Regulation drug effects, Drug Evaluation, Preclinical, Humans, Lung Neoplasms drug therapy, Male, Mice, Mice, Inbred ICR, Molecular Docking Simulation, Protein Kinase Inhibitors metabolism, Protein Kinase Inhibitors pharmacology, Protein Kinase Inhibitors therapeutic use, Pyrimidines metabolism, Pyrimidines pharmacology, Pyrimidines therapeutic use, Small Cell Lung Carcinoma drug therapy, Structure-Activity Relationship, Xenograft Model Antitumor Assays, Aurora Kinase A antagonists & inhibitors, Drug Design, Protein Kinase Inhibitors chemical synthesis, Proto-Oncogene Proteins c-myc metabolism, Pyrimidines chemistry

Abstract

The A-type Aurora kinase is upregulated in many human cancers, and it stabilizes MYC-family oncoproteins, which have long been considered an undruggable target. Here, we describe the design and synthesis of a series of pyrimidine-based derivatives able to inhibit Aurora A kinase activity and reduce levels of cMYC and MYCN. Through structure-based drug design of a small molecule that induces the DFG-out conformation of Aurora A kinase, lead compound 13 was identified, which potently (IC 50 < 200 nM) inhibited the proliferation of high-MYC expressing small-cell lung cancer (SCLC) cell lines. Pharmacokinetic optimization of 13 by prodrug strategies resulted in orally bioavailable 25 , which demonstrated an 8-fold higher oral AUC ( F = 62.3%). Pharmacodynamic studies of 25 showed it to effectively reduce cMYC protein levels, leading to >80% tumor regression of NCI-H446 SCLC xenograft tumors in mice. These results support the potential of 25 for the treatment of MYC -amplified cancers including SCLC.

Published

2021

7. Identification of a Multitargeted Tyrosine Kinase Inhibitor for the Treatment of Gastrointestinal Stromal Tumors and Acute Myeloid Leukemia.

Author

Lin WH, Wu SY, Yeh TK, Chen CT, Song JS, Shiao HY, Kuo CC, Hsu T, Lu CT, Wang PC, Wu TS, Peng YH, Lin HY, Chen CP, Weng YL, Kung FC, Wu MH, Su YC, Huang KW, Chou LH, Hsueh CC, Yen KJ, Kuo PC, Huang CL, Chen LT, Shih C, Tsai HJ, and Jiaang WT

Subjects

Animals, Antineoplastic Agents chemistry, Apoptosis, Cell Proliferation, Female, Gastrointestinal Neoplasms drug therapy, Gastrointestinal Neoplasms enzymology, Gastrointestinal Neoplasms genetics, Gastrointestinal Neoplasms pathology, Gastrointestinal Stromal Tumors enzymology, Gastrointestinal Stromal Tumors genetics, Gastrointestinal Stromal Tumors pathology, Humans, Leukemia, Myeloid, Acute enzymology, Leukemia, Myeloid, Acute genetics, Leukemia, Myeloid, Acute pathology, Male, Mice, Mice, Inbred ICR, Mice, Inbred NOD, Mice, Nude, Mice, SCID, Phosphorylation, Protein Kinase Inhibitors chemistry, Proto-Oncogene Proteins c-kit genetics, Pyrimidines chemistry, Rats, Sprague-Dawley, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, fms-Like Tyrosine Kinase 3 genetics, Antineoplastic Agents pharmacology, Gastrointestinal Stromal Tumors drug therapy, Leukemia, Myeloid, Acute drug therapy, Mutation, Protein Kinase Inhibitors pharmacology, Proto-Oncogene Proteins c-kit antagonists & inhibitors, Pyrimidines pharmacology, fms-Like Tyrosine Kinase 3 antagonists & inhibitors

Abstract

Gastrointestinal stromal tumors (GISTs) are prototypes of stem cell factor receptor (c-KIT)-driven cancer. Two receptor tyrosine kinases, c-KIT and fms-tyrosine kinase (FLT3), are frequently mutated in acute myeloid leukemia (AML) patients, and these mutations are associated with poor prognosis. In this study, we discovered a multitargeted tyrosine kinase inhibitor, compound 15a , with potent inhibition against single or double mutations of c-KIT developed in GISTs. Moreover, crystal structure analysis revealed the unique binding mode of 15a with c-KIT and may elucidate its high potency in inhibiting c-KIT kinase activity. Compound 15a inhibited cell proliferation and induced apoptosis by targeting c-KIT in c-KIT-mutant GIST cell lines. The antitumor effects of 15a were also demonstrated in GIST430 and GIST patient-derived xenograft models. Further studies demonstrated that 15a inhibited the proliferation of c-KIT- and FLT3-driven AML cells in vitro and in vivo. The results of this study suggest that 15a may be a potential anticancer drug for the treatment of GISTs and AML.

Published

2019

8. Discovery of a Furanopyrimidine-Based Epidermal Growth Factor Receptor Inhibitor (DBPR112) as a Clinical Candidate for the Treatment of Non-Small Cell Lung Cancer.

Author

Lin SY, Chang Hsu Y, Peng YH, Ke YY, Lin WH, Sun HY, Shiao HY, Kuo FM, Chen PY, Lien TW, Chen CH, Chu CY, Wang SY, Yeh KC, Chen CP, Hsu TA, Wu SY, Yeh TK, Chen CT, and Hsieh HP

Subjects

Animals, Antineoplastic Agents chemistry, Antineoplastic Agents metabolism, Binding Sites, Cell Line, Tumor, Crystallography, X-Ray, Drug Design, Drug Resistance, Neoplasm genetics, ErbB Receptors antagonists & inhibitors, ErbB Receptors chemistry, ErbB Receptors genetics, ErbB Receptors metabolism, Exons, Humans, Male, Mice, Inbred ICR, Mice, Nude, Mutation, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors metabolism, Pyrimidines chemistry, Rats, Receptor, ErbB-2, Structure-Activity Relationship, Xenograft Model Antitumor Assays, Antineoplastic Agents pharmacology, Carcinoma, Non-Small-Cell Lung drug therapy, Lung Neoplasms drug therapy, Protein Kinase Inhibitors pharmacology

Abstract

Epidermal growth factor receptor (EGFR)-targeted therapy in non-small cell lung cancer represents a breakthrough in the field of precision medicine. Previously, we have identified a lead compound, furanopyrimidine 2 , which contains a ( S )-2-phenylglycinol structure as a key fragment to inhibit EGFR. However, compound 2 showed high clearance and poor oral bioavailability in its pharmacokinetics studies. In this work, we optimized compound 2 by scaffold hopping and exploiting the potent inhibitory activity of various warhead groups to obtain a clinical candidate, 78 (DBPR112), which not only displayed a potent inhibitory activity against EGFR L858R/T790M double mutations but also exhibited tenfold potency better than the third-generation inhibitor, osimertinib, against EGFR and HER2 exon 20 insertion mutations. Overall, pharmacokinetic improvement through lead-to-candidate optimization yielded fourfold oral AUC better that afatinib along with F = 41.5%, an encouraging safety profile, and significant antitumor efficacy in in vivo xenograft models. DBPR112 is currently undergoing phase 1 clinical trial in Taiwan.

Published

2019

9. Linker Optimization and Therapeutic Evaluation of Phosphatidylserine-Targeting Zinc Dipicolylamine-based Drug Conjugates.

Author

Liu YW, Chen YY, Hsu CY, Chiu TY, Liu KL, Lo CF, Fang MY, Huang YC, Yeh TK, Pak KY, Gray BD, Hsu TA, Huang KH, Shih C, Shia KS, Chen CT, and Tsou LK

Subjects

Animals, Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Apoptosis drug effects, Cell Line, Tumor, Coordination Complexes chemical synthesis, Coordination Complexes chemistry, Drug Design, Humans, Indolizines chemical synthesis, Indolizines chemistry, Male, Mice, Inbred ICR, Mice, Nude, Molecular Structure, Picolines chemical synthesis, Picolines chemistry, Structure-Activity Relationship, Topoisomerase I Inhibitors chemical synthesis, Topoisomerase I Inhibitors chemistry, Topoisomerase I Inhibitors therapeutic use, Xenograft Model Antitumor Assays, Zinc chemistry, Antineoplastic Agents therapeutic use, Coordination Complexes therapeutic use, Indolizines therapeutic use, Neoplasms drug therapy, Phosphatidylserines metabolism, Picolines therapeutic use

Abstract

We report that compound 13 , a novel phosphatidylserine-targeting zinc(II) dipicolylamine drug conjugate, readily triggers a positive feedback therapeutic loop through the in situ generation of phosphatidylserine in the tumor microenvironment. Linker modifications, pharmacokinetics profiling, in vivo antitumor studies, and micro-Western array of treated-tumor tissues were employed to show that this class of conjugates induced regeneration of apoptotic signals, which facilitated subsequent recruitment of the circulating conjugates through the zinc(II) dipicolylamine-phosphatidylserine association and resulted in compounding antitumor efficacy. Compared to the marketed compound 17 , compound 13 not only induced regressions in colorectal and pancreatic tumor models, it also exhibited at least 5-fold enhancement in antitumor efficacy with only 40% of the drug employed during treatment, culminating in a >12.5-fold increase in therapeutic potential. Our study discloses a chemically distinct apoptosis-targeting theranostic, with built-in complementary functional moieties between the targeting module and the drug mechanism to expand the arsenal of antitumor therapy.

Published

2019

10. Discovery of Conformational Control Inhibitors Switching off the Activated c-KIT and Targeting a Broad Range of Clinically Relevant c-KIT Mutants.

Author

Wu TS, Lin WH, Tsai HJ, Hsueh CC, Hsu T, Wang PC, Lin HY, Peng YH, Lu CT, Lee LC, Tu CH, Kung FC, Shiao HY, Yeh TK, Song JS, Chang JY, Su YC, Chen LT, Chen CT, Jiaang WT, and Wu SY

Subjects

Animals, Binding Sites, Cell Line, Tumor, Cell Proliferation drug effects, Crystallography, X-Ray, Drug Evaluation, Preclinical, Gastrointestinal Stromal Tumors drug therapy, Gastrointestinal Stromal Tumors pathology, Humans, Imatinib Mesylate chemistry, Imatinib Mesylate metabolism, Mice, Mice, Inbred ICR, Molecular Docking Simulation, Protein Kinase Inhibitors metabolism, Protein Kinase Inhibitors pharmacology, Protein Kinase Inhibitors therapeutic use, Protein Structure, Tertiary, Proto-Oncogene Proteins c-kit genetics, Proto-Oncogene Proteins c-kit metabolism, Pyrimidines chemistry, Structure-Activity Relationship, Urea analogs & derivatives, Urea metabolism, Urea pharmacology, Urea therapeutic use, Xenograft Model Antitumor Assays, Protein Kinase Inhibitors chemistry, Proto-Oncogene Proteins c-kit antagonists & inhibitors

Abstract

Drug resistance due to acquired mutations that constitutively activate c-KIT is a significant challenge in the treatment of patients with gastrointestinal stromal tumors (GISTs). Herein, we identified 1-(5-ethyl-isoxazol-3-yl)-3-(4-{2-[6-(4-ethylpiperazin-1-yl)pyrimidin-4-ylamino]-thiazol-5-yl}phenyl)urea (10a) as a potent inhibitor against unactivated and activated c-KIT. The binding of 10a induced rearrangements of the DFG motif, αC-helix, juxtamembrane domain, and the activation loop to switch the activated c-KIT back to its structurally inactive state. To the best of our knowledge, it is the first structural evidence demonstrating how a compound can inhibit the activated c-KIT by switching back to its inactive state through a sequence of conformational changes. Moreover, 10a can effectively inhibit various c-KIT mutants and the proliferation of several GIST cell lines. The distinct binding features and superior inhibitory potency of 10a, together with its excellent efficacy in the xenograft model, establish 10a as worthy of further clinical evaluation in the advanced GISTs.

Published

2019

11. Development of Stem-Cell-Mobilizing Agents Targeting CXCR4 Receptor for Peripheral Blood Stem Cell Transplantation and Beyond.

Author

Wu CH, Song JS, Kuan HH, Wu SH, Chou MC, Jan JJ, Tsou LK, Ke YY, Chen CT, Yeh KC, Wang SY, Yeh TK, Tseng CT, Huang CL, Wu MH, Kuo PC, Lee CJ, and Shia KS

Subjects

Animals, Benzylamines, Cyclams, HEK293 Cells, Heterocyclic Compounds metabolism, Heterocyclic Compounds pharmacology, Humans, Inhibitory Concentration 50, Male, Mice, Molecular Docking Simulation, Protein Conformation, Receptors, CXCR4 chemistry, Peripheral Blood Stem Cell Transplantation, Receptors, CXCR4 metabolism, Stem Cells drug effects, Stem Cells metabolism

Abstract

The function of the CXCR4/CXCL12 axis accounts for many disease indications, including tissue/nerve regeneration, cancer metastasis, and inflammation. Blocking CXCR4 signaling with its antagonists may lead to moving out CXCR4 + cell types from bone marrow to peripheral circulation. We have discovered a novel series of pyrimidine-based CXCR4 antagonists, a representative (i.e., 16) of which was tolerated at a higher dose and showed better HSC-mobilizing ability at the maximal response dose relative to the approved drug 1 (AMD3100), and thus considered a potential drug candidate for PBSCT indication. Docking compound 16 into the X-ray crystal structure of CXCR4 receptor revealed that it adopted a spider-like conformation striding over both major and minor subpockets. This putative binding mode provides a new insight into CXCR4 receptor-ligand interactions for further structural modifications.

Published

2018

12. Design, Synthesis, and Evaluation of Thiazolidine-2,4-dione Derivatives as a Novel Class of Glutaminase Inhibitors.

Author

Yeh TK, Kuo CC, Lee YZ, Ke YY, Chu KF, Hsu HY, Chang HY, Liu YW, Song JS, Yang CW, Lin LM, Sun M, Wu SH, Kuo PC, Shih C, Chen CT, Tsou LK, and Lee SJ

Subjects

Animals, Antineoplastic Agents blood, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Antineoplastic Agents therapeutic use, Cell Line, Tumor, Cell Proliferation drug effects, Drug Design, Enzyme Inhibitors blood, Enzyme Inhibitors therapeutic use, Glutaminase metabolism, Humans, Male, Mice, Mice, Inbred BALB C, Mice, Nude, Models, Molecular, Pancreas drug effects, Pancreas metabolism, Pancreas pathology, Pancreatic Neoplasms drug therapy, Pancreatic Neoplasms metabolism, Pancreatic Neoplasms pathology, Rats, Rats, Sprague-Dawley, Thiazolidinediones blood, Thiazolidinediones therapeutic use, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Glutaminase antagonists & inhibitors, Thiazolidinediones chemistry, Thiazolidinediones pharmacology

Abstract

Humans have two glutaminase genes, GLS (GLS1) and GLS2, each of which has two alternative transcripts: the kidney isoform (KGA) and glutaminase C (GAC) for GLS, and the liver isoform (LGA) and glutaminase B (GAB) for GLS2. Initial hit compound (Z)-5-((1-(4-bromophenyl)-2,5-dimethyl-1H-pyrrol-3-yl)methylene)thiazolidine-2,4-dione (2), a thiazolidine-2,4-dione, was obtained from a high throughput screening of 40 000 compounds against KGA. Subsequently, a series of thiazolidine-2,4-dione derivatives was synthesized. Most of these were found to inhibit KGA and GAC with comparable activities, were less potent inhibitors of GAB, and were moderately selective for GLS1 over GLS2. The relationships between chemical structure, activity, and selectivity were investigated. The lead compounds obtained were found to (1) offer in vitro cellular activities for inhibiting cell growth, clonogenicity, and cellular glutamate production, (2) exhibit high concentrations of exposure in plasma by a pharmacokinetic study, and (3) reduce the tumor size of xenografted human pancreatic AsPC-1 carcinoma cells in mice.

Published

2017

13. Stem cell mobilizers targeting chemokine receptor CXCR4: renoprotective application in acute kidney injury.

Author

Wu CH, Song JS, Chang KH, Jan JJ, Chen CT, Chou MC, Yeh KC, Wong YC, Tseng CT, Wu SH, Yeh CF, Huang CY, Wang MH, Sadani AA, Chang CP, Cheng CY, Tsou LK, and Shia KS

Subjects

Animals, Flow Cytometry, Hematopoietic Stem Cells metabolism, Humans, Male, Mice, Mice, Inbred C57BL, Rats, Signal Transduction, Acute Kidney Injury prevention & control, Chemotaxis drug effects, Hematopoietic Stem Cell Mobilization, Hematopoietic Stem Cells cytology, Quinazolines chemistry, Quinazolines pharmacology, Receptors, CXCR4 antagonists & inhibitors, Reperfusion Injury prevention & control, Triazoles chemistry, Triazoles pharmacology

Abstract

We have discovered a novel series of quinazoline-based CXCR4 antagonists. Of these, compound 19 mobilized CXCR4(+) cell types, including hematopoietic stem cells and endothelial progenitor cells, more efficiently than the marketed 1 (AMD3100) with subcutaneous administration at the same dose (6 mg/kg) in mice. This series of compounds thus provides a set of valuable tools to study diseases mediated by the CXCR4/SDF-1 axis, including myocardial infarction, ischemic stroke, and cancer metastasis. More importantly, treatment with compound 19 significantly lowered levels of blood urea nitrogen and serum creatinine in rats with renal ischemia-reperfusion injury, providing evidence for its therapeutic potential in preventing ischemic acute kidney injury. CXCR4 antagonists such as 19 might also be useful to increase circulating levels of adult stem cells, thereby exerting beneficial effects on damaged and/or inflamed tissues in diseases that currently are not treated by standard approaches.

Published

2015

14. Optimization of ligand and lipophilic efficiency to identify an in vivo active furano-pyrimidine Aurora kinase inhibitor.

Author

Shiao HY, Coumar MS, Chang CW, Ke YY, Chi YH, Chu CY, Sun HY, Chen CH, Lin WH, Fung KS, Kuo PC, Huang CT, Chang KY, Lu CT, Hsu JT, Chen CT, Jiaang WT, Chao YS, and Hsieh HP

Subjects

Animals, Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Aurora Kinase A chemistry, Aurora Kinase A metabolism, Body Weight drug effects, Cell Proliferation drug effects, Crystallography, X-Ray, Drug Design, Furans chemistry, HCT116 Cells, Heterocyclic Compounds, 2-Ring chemical synthesis, Heterocyclic Compounds, 2-Ring chemistry, Heterocyclic Compounds, 2-Ring pharmacology, Humans, Ligands, Lipids chemistry, Male, Mice, Mice, Nude, Models, Chemical, Models, Molecular, Molecular Structure, Neoplasms drug therapy, Neoplasms metabolism, Neoplasms pathology, Phenylurea Compounds chemical synthesis, Phenylurea Compounds chemistry, Phenylurea Compounds pharmacology, Protein Binding, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors chemistry, Protein Structure, Tertiary, Pyrimidines chemical synthesis, Pyrimidines chemistry, Xenograft Model Antitumor Assays, Antineoplastic Agents pharmacology, Aurora Kinase A antagonists & inhibitors, Protein Kinase Inhibitors pharmacology, Pyrimidines pharmacology

Abstract

Ligand efficiency (LE) and lipophilic efficiency (LipE) are two important indicators of "drug-likeness", which are dependent on the molecule's activity and physicochemical properties. We recently reported a furano-pyrimidine Aurora kinase inhibitor 4 (LE = 0.25; LipE = 1.75), with potent activity in vitro; however, 4 was inactive in vivo. On the basis of insights obtained from the X-ray co-crystal structure of the lead 4, various solubilizing functional groups were introduced to optimize both the activity and physicochemical properties. Emphasis was placed on identifying potential leads with improved activity as well as better LE and LipE by exercising tight control over the molecular weight and lipophilicity of the molecules. Rational optimization has led to the identification of Aurora kinase inhibitor 27 (IBPR001; LE = 0.26; LipE = 4.78), with improved in vitro potency and physicochemical properties, resulting in an in vivo active (HCT-116 colon cancer xenograft mouse model) anticancer agent.

Published

2013

15. Discovery of novel N-β-D-xylosylindole derivatives as sodium-dependent glucose cotransporter 2 (SGLT2) inhibitors for the management of hyperglycemia in diabetes.

Author

Yao CH, Song JS, Chen CT, Yeh TK, Hung MS, Chang CC, Liu YW, Yuan MC, Hsieh CJ, Huang CY, Wang MH, Chiu CH, Hsieh TC, Wu SH, Hsiao WC, Chu KF, Tsai CH, Chao YS, and Lee JC

Subjects

Animals, CHO Cells, Cricetinae, Cricetulus, Diabetes Mellitus, Experimental blood, Diabetes Mellitus, Experimental urine, Diabetes Mellitus, Type 2 blood, Diabetes Mellitus, Type 2 urine, Glucose metabolism, Glucosides pharmacokinetics, Glucosides pharmacology, Humans, Hypoglycemic Agents pharmacokinetics, Hypoglycemic Agents pharmacology, Indoles pharmacokinetics, Indoles pharmacology, Male, Mice, Mice, Inbred ICR, Rats, Rats, Sprague-Dawley, Structure-Activity Relationship, Xylose chemical synthesis, Xylose pharmacokinetics, Xylose pharmacology, Diabetes Mellitus, Experimental drug therapy, Diabetes Mellitus, Type 2 drug therapy, Glucosides chemical synthesis, Hyperglycemia drug therapy, Hypoglycemic Agents chemical synthesis, Indoles chemical synthesis, Sodium-Glucose Transporter 2 Inhibitors, Xylose analogs & derivatives

Abstract

A novel series of N-linked β-D-xylosides were synthesized and evaluated for inhibitory activity against sodium-dependent glucose cotransporter 2 (SGLT2) in a cell-based assay. Of these, the 4-chloro-3-(4-cyclopropylbenzyl)-1-(β-D-xylopyranosyl)-1H-indole 19m was found to be the most potent inhibitor, with an EC(50) value similar to that of the natural SGLT2 inhibitor phlorizin. Further studies in Sprague-Dawley (SD) rats indicated that 19m significantly increased urine glucose excretion in a dose-dependent manner with oral administration. The antihyperglycemic effect of 19m was also observed in streptozotocin (STZ) induced diabetic SD rats. These results described here are a good starting point for further investigations into N-glycoside SGLT2 inhibitors.

Published

2011

16. Discovery of non-glycoside sodium-dependent glucose co-transporter 2 (SGLT2) inhibitors by ligand-based virtual screening.

Author

Wu JS, Peng YH, Wu JM, Hsieh CJ, Wu SH, Coumar MS, Song JS, Lee JC, Tsai CH, Chen CT, Liu YW, Chao YS, and Wu SY

Subjects

Animals, Benzimidazoles chemistry, Benzimidazoles pharmacology, CHO Cells, Cluster Analysis, Computer Simulation, Cricetinae, Cricetulus, Databases, Factual, Drug Design, Glycosides chemistry, Sodium-Glucose Transporter 2 chemistry, Ligands, Models, Molecular, Quantitative Structure-Activity Relationship, Sodium-Glucose Transporter 2 Inhibitors

Abstract

A ligand-based virtual screening strategy (a combination of pharmacophore model generation, shape-based scoring, and structure clustering analysis) was developed to discover novel SGLT2 inhibitors. The best pharmacophore model, generated from eight glycoside inhibitors, was utilized to virtually screen three chemical databases that led to the identification of three non-glycoside SGLT2 inhibitors. This is the first report of the generation of a pharmacophore model from glycosides that has then been used to discover novel non-glycosides hits.

Published

2010

17. Design and synthesis of tetrahydropyridothieno[2,3-d]pyrimidine scaffold based epidermal growth factor receptor (EGFR) kinase inhibitors: the role of side chain chirality and Michael acceptor group for maximal potency.

Author

Wu CH, Coumar MS, Chu CY, Lin WH, Chen YR, Chen CT, Shiao HY, Rafi S, Wang SY, Hsu H, Chen CH, Chang CY, Chang TY, Lien TW, Fang MY, Yeh KC, Chen CP, Yeh TK, Hsieh SH, Hsu JT, Liao CC, Chao YS, and Hsieh HP

Subjects

Animals, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, Drug Design, Drug Resistance, Neoplasm, Drug Screening Assays, Antitumor, ErbB Receptors genetics, Gefitinib, Heterocyclic Compounds, 3-Ring chemistry, Heterocyclic Compounds, 3-Ring pharmacology, Humans, Male, Mice, Mice, Nude, Mutation, Neoplasm Transplantation, Pyrimidines chemistry, Pyrimidines pharmacology, Quinazolines pharmacology, Rats, Rats, Sprague-Dawley, Stereoisomerism, Structure-Activity Relationship, Transplantation, Heterologous, Antineoplastic Agents chemical synthesis, ErbB Receptors antagonists & inhibitors, Heterocyclic Compounds, 3-Ring chemical synthesis, Pyrimidines chemical synthesis

Abstract

HTS hit 7 was modified through hybrid design strategy to introduce a chiral side chain followed by introduction of Michael acceptor group to obtain potent EGFR kinase inhibitors 11 and 19. Both 11 and 19 showed over 3 orders of magnitude enhanced HCC827 antiproliferative activity compared to HTS hit 7 and also inhibited gefitinib-resistant double mutant (DM, T790M/L858R) EGFR kinase at nanomolar concentration. Moreover, treatment with 19 shrinked tumor in nude mice xenograft model.

Published

2010

18. Synthesis and biological activities of 2-amino-1-arylidenamino imidazoles as orally active anticancer agents.

Author

Li WT, Hwang DR, Song JS, Chen CP, Chuu JJ, Hu CB, Lin HL, Huang CL, Huang CY, Tseng HY, Lin CC, Chen TW, Lin CH, Wang HS, Shen CC, Chang CM, Chao YS, and Chen CT

Subjects

Administration, Oral, Animals, Antineoplastic Agents administration & dosage, Cell Line, Tumor, Cell Proliferation drug effects, Cell Survival drug effects, DNA Fragmentation drug effects, Dose-Response Relationship, Drug, Female, Humans, Imidazoles chemistry, Inhibitory Concentration 50, Leukemia P388 drug therapy, Leukemia P388 pathology, Mice, Mice, Inbred DBA, Mice, Nude, Microtubules drug effects, Microtubules metabolism, Models, Chemical, Molecular Structure, Neoplasms pathology, Structure-Activity Relationship, Tubulin metabolism, Xenograft Model Antitumor Assays, Antineoplastic Agents pharmacology, Imidazoles chemical synthesis, Imidazoles pharmacology, Neoplasms drug therapy

Abstract

2-Amino-1-arylidenaminoimidazoles, a novel class of orally (po) active microtubule-destabilizing anticancer agents, were synthesized. The compounds were designed from a hit compound identified in a drug discovery platform by using cancer cell-based high throughput screening assay. Selective synthesized compounds exerted cell cytotoxicity against human cancer cells. The underlying mechanisms for the anticancer activity were demonstrated as interacting with the tubulins and inhibiting microtubule assembly, leading to proliferation inhibition and apoptosis induction in the human tumor cells. Furthermore, two compounds showed in vivo anticancer activities in both po and intravenously (iv) administered routes and prolonged the life spans of murine leukemic P388 cells-inoculated mice. These new po active antimitotic anticancer agents are to be further examined in preclinical studies and developed for clinical uses.

Published

2010

19. Synthesis and preclinical evaluations of 2-(2-fluorophenyl)-6,7-methylenedioxyquinolin-4-one monosodium phosphate (CHM-1-P-Na) as a potent antitumor agent.

Author

Chou LC, Chen CT, Lee JC, Way TD, Huang CH, Huang SM, Teng CM, Yamori T, Wu TS, Sun CM, Chien DS, Qian K, Morris-Natschke SL, Lee KH, Huang LJ, and Kuo SC

Subjects

Animals, Antineoplastic Agents pharmacokinetics, Antineoplastic Agents pharmacology, Apoptosis, Cell Cycle Proteins, Cell Line, Tumor, Cyclin B1 biosynthesis, Drug Screening Assays, Antitumor, Female, Humans, Lethal Dose 50, Male, Mice, Mice, Nude, Mitosis, Neoplasm Transplantation, Organophosphates pharmacokinetics, Organophosphates pharmacology, Prodrugs pharmacokinetics, Prodrugs pharmacology, Protein Serine-Threonine Kinases metabolism, Quinolines pharmacokinetics, Quinolines pharmacology, Radioligand Assay, Transplantation, Heterologous, Antineoplastic Agents chemical synthesis, Organophosphates chemical synthesis, Prodrugs chemical synthesis, Quinolines chemical synthesis

Abstract

CHM-1 [2-(2-fluorophenyl)-6,7-methylenedioxyquinolin-4-one] (1) has a unique antitumor mechanism of action. However, because 1 has relatively low hydrophilicity, it was evaluated only via ip administration, which is not clinically acceptable. In this study, we synthesized the monosodium phosphate salt (CHM-1-P-Na, 4) of 1 as a hydrophilic prodrug. Compound 4 was rapidly converted into 1 following iv and po administration and also possessed excellent antitumor activity in a SKOV-3 xenograft nude mice model. Compound 4 also had clear-cut pharmacological effects on enzymes related with tumor cells. Neither 4 nor 1 significantly affected normal biological function in a safety pharmacology profiling study. Compound 1 caused apoptotic effects in breast carcinoma cells via accumulation of cyclin B1, and importantly, the endogenous levels of the mitotic spindle checkpoint proteins BubR1 directly correlated with cellular response to microtubule disruption. With excellent antitumor activity profiles, 4 is highly promising for development as an anticancer clinical trials candidate.

Published

2010

20. Synthesis and evaluation of 3-aroylindoles as anticancer agents: metabolite approach.

Author

Wu YS, Coumar MS, Chang JY, Sun HY, Kuo FM, Kuo CC, Chen YJ, Chang CY, Hsiao CL, Liou JP, Chen CP, Yao HT, Chiang YK, Tan UK, Chen CT, Chu CY, Wu SY, Yeh TK, Lin CY, and Hsieh HP

Subjects

Animals, Antineoplastic Agents pharmacokinetics, Antineoplastic Agents pharmacology, Cell Line, Tumor, Colchicine metabolism, Drug Design, Humans, Indoles metabolism, Indoles pharmacokinetics, Indoles pharmacology, Mice, Rats, Structure-Activity Relationship, Tubulin Modulators chemical synthesis, Tubulin Modulators pharmacology, Antineoplastic Agents chemical synthesis, Indoles chemical synthesis

Abstract

BPR0L075 (2) is a potential anticancer drug candidate designed from Combretastatin A-4 (1) based on the bioisosterism principle. Metabolites of 2, proposed from in vitro human microsome studies, were synthesized, leading to the identification of metabolite-derived analogue 10 with 40-350 pM potency against various cancer cell lines. Insights gained from the major inactive metabolite of 2 led to the development of 29, with better pharmacokinetics and improved potency in the tumor xenograft model than 2.

Published

2009

21. Generation of ligand-based pharmacophore model and virtual screening for identification of novel tubulin inhibitors with potent anticancer activity.

Author

Chiang YK, Kuo CC, Wu YS, Chen CT, Coumar MS, Wu JS, Hsieh HP, Chang CY, Jseng HY, Wu MH, Leou JS, Song JS, Chang JY, Lyu PC, Chao YS, and Wu SY

Subjects

Antineoplastic Agents chemistry, Artificial Intelligence, Binding Sites, Cell Cycle drug effects, Cell Proliferation drug effects, Colchicine metabolism, Costs and Cost Analysis, Databases, Factual, Drug Evaluation, Preclinical, Humans, Indoles chemistry, Indoles pharmacology, KB Cells, Ligands, Models, Molecular, Protein Multimerization drug effects, Protein Structure, Quaternary, Reproducibility of Results, Tubulin chemistry, Tubulin Modulators chemistry, Antineoplastic Agents pharmacology, Tubulin metabolism, Tubulin Modulators pharmacology

Abstract

A pharmacophore model, Hypo1, was built on the basis of 21 training-set indole compounds with varying levels of antiproliferative activity. Hypo1 possessed important chemical features required for the inhibitors and demonstrated good predictive ability for biological activity, with high correlation coefficients of 0.96 and 0.89 for the training-set and test-set compounds, respectively. Further utilization of the Hypo1 pharmacophore model to screen chemical database in silico led to the identification of four compounds with antiproliferative activity. Among these four compounds, 43 showed potent antiproliferative activity against various cancer cell lines with the strongest inhibition on the proliferation of KB cells (IC(50) = 187 nM). Further biological characterization revealed that 43 effectively inhibited tubulin polymerization and significantly induced cell cycle arrest in G(2)-M phase. In addition, 43 also showed the in vivo-like anticancer effects. To our knowledge, 43 is the most potent antiproliferative compound with antitubulin activity discovered by computer-aided drug design. The chemical novelty of 43 and its anticancer activities make this compound worthy of further lead optimization.

Published

2009

22. Structure-based drug design of a novel family of PPARgamma partial agonists: virtual screening, X-ray crystallography, and in vitro/in vivo biological activities.

Author

Lu IL, Huang CF, Peng YH, Lin YT, Hsieh HP, Chen CT, Lien TW, Lee HJ, Mahindroo N, Prakash E, Yueh A, Chen HY, Goparaju CM, Chen X, Liao CC, Chao YS, Hsu JT, and Wu SY

Subjects

Adipocytes cytology, Adipocytes drug effects, Animals, Binding Sites, Cell Differentiation drug effects, Cell Line, Crystallography, X-Ray, Humans, Ligands, Male, Mice, Models, Molecular, PPAR gamma chemistry, PPAR gamma genetics, Protein Structure, Tertiary, Transcription, Genetic genetics, Drug Design, PPAR gamma agonists, PPAR gamma metabolism

Abstract

Peroxisome proliferator-activated receptor gamma (PPARgamma) is well-known as the receptor of thiazolidinedione antidiabetic drugs. In this paper, we present a successful example of employing structure-based virtual screening, a method that combines shape-based database search with a docking study and analogue search, to discover a novel family of PPARgamma agonists based upon pyrazol-5-ylbenzenesulfonamide. Two analogues in the family show high affinity for, and specificity to, PPARgamma and act as partial agonists. They also demonstrate glucose-lowering efficacy in vivo. A structural biology study reveals that they both adopt a distinct binding mode and have no H-bonding interactions with PPARgamma. The absence of H-bonding interaction with the protein provides an explanation why both function as partial agonists since most full agonists form conserved H-bonds with the activation function helix (AF-2 helix) which, in turn, enhances the recruitment of coactivators. Moreover, the structural biology and computer docking studies reveal the specificity of the compounds for PPARgamma could be due to the restricted access to the binding pocket of other PPAR subtypes, i.e., PPARalpha and PPARdelta, and steric hindrance upon the ligand binding.

Published

2006

23. 2-[3-[2-[(2S)-2-Cyano-1-pyrrolidinyl]-2-oxoethylamino]-3-methyl-1-oxobutyl]- 1,2,3,4-tetrahydroisoquinoline: a potent, selective, and orally bioavailable dipeptide-derived inhibitor of dipeptidyl peptidase IV.

Author

Tsu H, Chen X, Chen CT, Lee SJ, Chang CN, Kao KH, Coumar MS, Yeh YT, Chien CH, Wang HS, Lin KT, Chang YY, Wu SH, Chen YS, Lu IL, Wu SY, Tsai TY, Chen WC, Hsieh HP, Chao YS, and Jiaang WT

Subjects

Administration, Oral, Animals, Blood Glucose drug effects, Dipeptidases antagonists & inhibitors, Dipeptidyl Peptidase 4 blood, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases antagonists & inhibitors, Drug Evaluation, Preclinical, Drug Tolerance, Enzyme Inhibitors chemical synthesis, Glucose administration & dosage, Glucose antagonists & inhibitors, Humans, In Vitro Techniques, Isoquinolines chemical synthesis, Male, Mice, Mice, Inbred BALB C, Molecular Conformation, Pyrrolidinones chemical synthesis, Rats, Rats, Wistar, Structure-Activity Relationship, Time Factors, Dipeptidyl Peptidase 4 drug effects, Enzyme Inhibitors pharmacology, Isoquinolines pharmacology, Pyrrolidinones pharmacology

Abstract

Dipeptidyl peptidase IV (DPP-IV) inhibitors are expected to become a new type of antidiabetic drugs. Most known DPP-IV inhibitors often resemble the dipeptide cleavage products, with a proline mimic at the P1 site. As off-target inhibitions of DPP8 and/or DPP9 have shown profound toxicities in the in vivo studies, it is important to develop selective DPP-IV inhibitors for clinical usage. To achieve this, a new class of 2-[3-[[2-[(2S)-2-cyano-1-pyrrolidinyl]-2-oxoethyl]amino]-1-oxopropyl]-based DPP-IV inhibitors was synthesized. SAR studies resulted in a number of DPP-IV inhibitors, having IC(50) values of <50 nM with excellent selectivity over both DPP8 (IC(50) > 100 microM) and DPP-II (IC(50) > 30 microM). Compound 21a suppressed the blood glucose elevation after an oral glucose challenge in Wistar rats and also inhibited plasma DPP-IV activity for up to 4 h in BALB/c mice. The results show that compound 21a possesses in vitro and in vivo activities comparable to those of NVP-LAF237 (4), which is in clinical development.

Published

2006

24. Novel indole-based peroxisome proliferator-activated receptor agonists: design, SAR, structural biology, and biological activities.

Author

Mahindroo N, Huang CF, Peng YH, Wang CC, Liao CC, Lien TW, Chittimalla SK, Huang WJ, Chai CH, Prakash E, Chen CP, Hsu TA, Peng CH, Lu IL, Lee LH, Chang YW, Chen WC, Chou YC, Chen CT, Goparaju CM, Chen YS, Lan SJ, Yu MC, Chen X, Chao YS, Wu SY, and Hsieh HP

Subjects

1-Methyl-3-isobutylxanthine pharmacology, 3T3-L1 Cells, Adipocytes cytology, Adipocytes drug effects, Adipocytes metabolism, Animals, Cell Differentiation drug effects, Crystallization, Crystallography, Deoxyglucose metabolism, Dexamethasone pharmacology, Drug Design, Humans, Indoles pharmacokinetics, Indoles pharmacology, Insulin pharmacology, Isoxazoles chemical synthesis, Isoxazoles pharmacokinetics, Isoxazoles pharmacology, Male, Mice, Mice, Inbred BALB C, Peroxisome Proliferator-Activated Receptors pharmacology, Structure-Activity Relationship, Indoles chemical synthesis, Peroxisome Proliferator-Activated Receptors agonists

Abstract

The synthesis and structure-activity relationship studies of novel indole derivatives as peroxisome proliferator-activated receptor (PPAR) agonists are reported. Indole, a drug-like scaffold, was studied as a core skeleton for the acidic head part of PPAR agonists. The structural features (acidic head, substitution on indole, and linker) were optimized first, by keeping benzisoxazole as the tail part, based on binding and functional activity at PPARgamma protein. The variations in the tail part, by introducing various heteroaromatic ring systems, were then studied. In vitro evaluation led to identification of a novel series of indole compounds with a benzisoxazole tail as potent PPAR agonists with the lead compound 14 (BPR1H036) displaying an excellent pharmacokinetic profile in BALB/c mice and an efficacious glucose lowering activity in KKA(y) mice. Structural biology studies of 14 showed that the indole ring contributes strong hydrophobic interactions with PPARgamma and could be an important moiety for the binding to the protein.

Published

2005

25. Synthesis and biological evaluation of N-heterocyclic indolyl glyoxylamides as orally active anticancer agents.

Author

Li WT, Hwang DR, Chen CP, Shen CW, Huang CL, Chen TW, Lin CH, Chang YL, Chang YY, Lo YK, Tseng HY, Lin CC, Song JS, Chen HC, Chen SJ, Wu SH, and Chen CT

Subjects

Administration, Oral, Animals, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Apoptosis, Cell Division drug effects, Drug Resistance, Multiple, Drug Resistance, Neoplasm, Drug Screening Assays, Antitumor, Female, Glyoxylates chemistry, Glyoxylates pharmacology, Humans, Indoles chemistry, Indoles pharmacology, Leukemia P388 mortality, Mice, Mice, Inbred DBA, Neoplasm Transplantation, Structure-Activity Relationship, Thiazoles chemistry, Thiazoles pharmacology, Tumor Cells, Cultured, Antineoplastic Agents chemical synthesis, Glyoxylates chemical synthesis, Indoles chemical synthesis, Thiazoles chemical synthesis

Abstract

A series of N-heterocyclic indolyl glyoxylamides were synthesized and evaluated for in vitro and in vivo anticancer activities. They exhibited a broad spectrum of anticancer activity not only in murine leukemic cancer cells but also in human gastric, breast, and uterus cancer cells as well as their multidrug resistant sublines with a wide range of IC(50) values. They also induced apoptosis and caused DNA fragmentation in human gastric cancer cells. Among the compounds studied, 7 showed the most potent activity of growth inhibition (IC(50) = 17-1711 nM) in several human cancer cells. Given orally, compounds 7 and 13 dose-dependently prolonged the survival of animals inoculated with P388 leukemic cancer cells. N-Heterocyclic indolyl glyoxylamides may be useful as orally active chemotherapeutic agents against cancer and refractory cancerous diseases of multidrug resistance phenotype.

Published

2003