Your search keyword '"Brian W. Dymock"' showing total 22 results

1. Intranasal administration of a stapled relaxin‐3 mimetic has anxiolytic‐ and antidepressant‐like activity in rats

Author

Rajamani Lakshminarayanan, Norrapat Shih, Gavin S. Dawe, Subhi Marwari, Anders Poulsen, Brian W. Dymock, R. Manjunatha Kini, and Charles W. Johannes

Subjects

Male, Models, Molecular, 0301 basic medicine, Agonist, medicine.drug_class, Peptidomimetic, Anxiety, Pharmacology, Anxiolytic, Receptors, G-Protein-Coupled, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, Orexigenic, medicine, Animals, Humans, Receptor, Administration, Intranasal, Cells, Cultured, Dose-Response Relationship, Drug, Depression, business.industry, Research Papers, Antidepressive Agents, Rats, Neuropsychopharmacology, HEK293 Cells, 030104 developmental biology, Anti-Anxiety Agents, Female, Nasal administration, business, Relaxin-3, 030217 neurology & neurosurgery, Research Paper, medicine.drug

Abstract

Background and purpose Depression and anxiety are common causes of disability, and innovative tools and potential pharmacological targets are actively sought for prevention and treatment. Therapeutic strategies targeting the relaxin-3 peptide or its primary endogenous receptor, RXFP3, for the treatment of major depression and anxiety disorders have been limited by a lack of compounds with drug-like properties. We proposed that a hydrocarbon-stapled mimetic of relaxin-3, when administered intranasally, might be uniquely applicable to the treatment of these disorders. Experimental approach We designed a series of hydrocarbon-stapled relaxin-3 mimetics and identified the most potent compound using in vitro receptor binding and activation assays. Further, we assessed the effect of intranasal delivery of relaxin-3 and the lead stapled mimetic in rat models of anxiety and depression. Key results We developed an i,i+7 stapled relaxin-3 mimetic that manifested a stabilized α-helical structure, proteolytic resistance, and confirmed agonist activity in receptor binding and activation in vitro assays. The stapled peptide agonist enhanced food intake after intracerebral infusion in rats, confirming in vivo activity. We showed that intranasal delivery of the lead i,i+7 stapled peptide or relaxin-3 had orexigenic effects in rats, indicating a potential clinically translatable route of delivery. Further, intranasal administration of the lead i,i+7 stapled peptide exerted anxiolytic and antidepressant-like activity in anxiety- and depression-related behaviour paradigms. Conclusions and implications Our preclinical findings demonstrate that targeting the relaxin-3/RXFP3 receptor system via intranasal delivery of an i,i+7 stapled relaxin-3 mimetic may represent an effective treatment approach for depression, anxiety, and related neuropsychiatric disorders.

Published

2019

2. Design and synthesis of potent dual inhibitors of JAK2 and HDAC based on fusing the pharmacophores of XL019 and vorinostat

Author

Yu-yi Chu-Farseeva, Anders Poulsen, Jeffrey J.Y. Yen, Brian W. Dymock, Nurulhuda Mustafa, Wee Joo Chng, and Eng Chong Tan

Subjects

0301 basic medicine, Proline, Antineoplastic Agents, Apoptosis, Hydroxamic Acids, HeLa, Structure-Activity Relationship, 03 medical and health sciences, 0302 clinical medicine, Neoplasms, Drug Discovery, medicine, Humans, Protein Kinase Inhibitors, Vorinostat, Pharmacology, chemistry.chemical_classification, biology, Chemistry, Organic Chemistry, General Medicine, Janus Kinase 2, HDAC6, biology.organism_classification, Histone Deacetylase Inhibitors, Molecular Docking Simulation, Pyrimidines, 030104 developmental biology, Enzyme, Cell culture, Drug Design, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Pharmacophore, HeLa Cells, medicine.drug

Abstract

Specifically blocking more than one oncogenic pathway simultaneously in a cancer cell with a combination of different drugs is the mainstay of the majority of cancer treatments. Being able to do this via two targeted pathways without inducing side effects through a general mechanism, such as chemotherapy, could bring benefit to patients. In this work we describe a new dual inhibitor of the JAK-STAT and HDAC pathways through designing and developing two types of molecule based on the JAK2 selective inhibitor XL019 and the pan-HDAC inhibitor, vorinostat. Both series of compounds had examples with low nanomolar JAK2 and HDAC1/6 inhibition. In some cases good HDAC1 selectivity was achieved while retaining HDAC6 activity. The observed potency is explained through molecular docking studies of all three enzymes. One example, 69c had 16–25 fold selectivity against the three other JAK-family proteins JAK1, JAK3 and TYK2. A number of compounds had sub-micromolar potencies against a panel of 4 solid tumor cell lines and 4 hematological cell lines with the most potent compound, 45h, having a cellular IC50 of 70 nM against the multiple myeloma cell line KMS-12-BM. Evidence of both JAK and HDAC pathway inhibition is presented in Hela cells showing that both pathways are modulated. Evidence of apoptosis with two compounds in 4 sold tumor cell lines is also presented.

Published

2018

3. Merging of ruxolitinib and vorinostat leads to highly potent inhibitors of JAK2 and histone deacetylase 6 (HDAC6)

Author

Anders Poulsen, Sten Ohlson, Brian W. Dymock, Lianbin Yao, and Pondy Murugappan Ramanujulu

Subjects

0301 basic medicine, Ruxolitinib, Clinical Biochemistry, Pharmaceutical Science, Pharmacology, Histone Deacetylase 6, Biochemistry, Inhibitory Concentration 50, Structure-Activity Relationship, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Nitriles, Drug Discovery, medicine, Humans, Potency, Protein Kinase Inhibitors, Molecular Biology, IC50, Vorinostat, Cell Proliferation, Chemistry, Organic Chemistry, Janus Kinase 2, HDAC6, HDAC1, Histone Deacetylase Inhibitors, Pyrimidines, 030104 developmental biology, Drug Design, 030220 oncology & carcinogenesis, Pyrazoles, Molecular Medicine, Histone deacetylase, Pharmacophore, medicine.drug

Abstract

Inhibition of more than one pathway in a cancer cell with a single molecule could result in better therapies with less complex dosing regimens. In this work multi-component ligands have been prepared by joining together key pharmacophores of two different enzyme inhibitors in a way which increases potency against the individual pathways. Selective JAK1/2 inhibitor, ruxolitinib (3), and pan-HDAC inhibitor vorinostat (4) were linked together by a single nitrogen atom to create a new series of compounds with very potent JAK2 and HDAC6 inhibition with selectivity against HDAC1. A preferred compound, 13b, had unprecedented sub-nanomolar JAK2 potency with an IC50 of 41 pM and a sub-nanomolar IC50 against HDAC6 of 200 pM. Binding models show a good fit into both JAK2 and HDAC6.

Published

2018

4. Design and synthesis of triple inhibitors of janus kinase (JAK), histone deacetylase (HDAC) and Heat Shock Protein 90 (HSP90)

Author

Sten Ohlson, Brian W. Dymock, and Lianbin Yao

Subjects

0301 basic medicine, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, Heat shock protein, Nitriles, Drug Discovery, medicine, HSP90 Heat-Shock Proteins, Protein Kinase Inhibitors, Molecular Biology, Vorinostat, Janus kinase 2, biology, Chemistry, Organic Chemistry, Janus Kinase 2, Amides, Cell biology, Histone Deacetylase Inhibitors, Pyrimidines, 030104 developmental biology, Biological target, Drug Design, 030220 oncology & carcinogenesis, biology.protein, Pyrazoles, Molecular Medicine, Histone deacetylase, Pharmacophore, Signal transduction, Janus kinase, medicine.drug

Abstract

Inhibition of multiple signaling pathways in a cancer cell with a single molecule could result in better therapies that are simpler to administer. Efficacy may be achieved with reduced potency against individual targets if there is synergy through multiple pathway inhibition. To achieve this, it is necessary to be able to build multi-component ligands by joining together key pharmacophores in a way which maintains sufficient activity against the individual pathways. In this work, designed triple inhibiting ligands are explored aiming to block three completely different target types: a kinase (JAK2), an epigenetic target (HDAC) and a chaperone (HSP90). Although these enzymes have totally different functions they are related through inter-dependent pathways in the developing cancer cell. Synthesis of several complex multi-inhibiting ligands are presented along with initial enzyme inhibition data against 3 biological target classes of interest. A lead compound, 47, was discovered which had low micromolar activity for all 3 targets. Further development of these complex trispecific designed multiple ligands could result in a 'transient drug', an alternative combination therapy for treating cancer mediated via a single molecule.

Published

2018

5. Dual blockade of the lipid kinase PIP4Ks and mitotic pathways leads to cancer-selective lethality

Author

Radoslaw M. Sobota, Pei-Ju Liao, Frank McCormick, Mayumi Kitagawa, Noriaki Minami, Nayana Prabhu, Brian W. Dymock, Sang Hyun Lee, Oltea Sampetrean, Go Ka Diam, David M. Epstein, Kyunghee Lee, Dai Lingyun, Jasmine Wong, Pär Nordlund, Sujoy Ghosh, Hideyuki Saya, Andreas Larsson, See Cheng Shang, and School of Biological Sciences

Subjects

0301 basic medicine, MAPK/ERK pathway, Indoles, Nude, General Physics and Astronomy, Mice, 0302 clinical medicine, Neoplasms, 2.1 Biological and endogenous factors, Aetiology, lcsh:Science, Mitotic catastrophe, Inbred BALB C, Cancer, Mice, Inbred BALB C, Tumor, Multidisciplinary, Kinase, Chemistry, Intracellular Signaling Peptides and Proteins, Cell biology, Phosphotransferases (Alcohol Group Acceptor), 030220 oncology & carcinogenesis, Female, Signal Transduction, Cell Survival, Science, Cancer-selective Lethality, Mice, Nude, Mitosis, Article, General Biochemistry, Genetics and Molecular Biology, Cell Line, 03 medical and health sciences, Downregulation and upregulation, Cell Line, Tumor, Dual Inhibitory, Animals, Humans, Protein Kinase Inhibitors, Protein kinase B, PI3K/AKT/mTOR pathway, Cell Proliferation, Acrylonitrile, Phosphotransferases, Membrane Proteins, General Chemistry, Isoquinolines, Xenograft Model Antitumor Assays, 030104 developmental biology, Cancer cell, ras Proteins, lcsh:Q

Abstract

Achieving robust cancer-specific lethality is the ultimate clinical goal. Here, we identify a compound with dual-inhibitory properties, named a131, that selectively kills cancer cells, while protecting normal cells. Through an unbiased CETSA screen, we identify the PIP4K lipid kinases as the target of a131. Ablation of the PIP4Ks generates a phenocopy of the pharmacological effects of PIP4K inhibition by a131. Notably, PIP4Ks inhibition by a131 causes reversible growth arrest in normal cells by transcriptionally upregulating PIK3IP1, a suppressor of the PI3K/Akt/mTOR pathway. Strikingly, Ras activation overrides a131-induced PIK3IP1 upregulation and activates the PI3K/Akt/mTOR pathway. Consequently, Ras-transformed cells override a131-induced growth arrest and enter mitosis where a131’s ability to de-cluster supernumerary centrosomes in cancer cells eliminates Ras-activated cells through mitotic catastrophe. Our discovery of drugs with a dual-inhibitory mechanism provides a unique pharmacological strategy against cancer and evidence of cross-activation between the Ras/Raf/MEK/ERK and PI3K/AKT/mTOR pathways via a Ras˧PIK3IP1˧PI3K signaling network., The Ras/Raf/MEK/ERK and PI3K/Akt/mTOR signaling pathways are essential for cancer cell survival. Here, the authors describes a molecule a131 with dual-inhibitory properties, which targets PI5P4K and mitosis, and it is involved in Ras/Raf/MEK/ERK and PI3K/Akt/mTOR crosstalk, thereby causing reversible growth arrest in normal cells and cell death of tumor cells.

Published

2017

6. Design and Synthesis of Ligand Efficient Dual Inhibitors of Janus Kinase (JAK) and Histone Deacetylase (HDAC) Based on Ruxolitinib and Vorinostat

Author

Prachi Singh, Lianbin Yao, Pondy Murugappan Ramanujulu, Anders Poulsen, Jeannie X. T. Lee, Wee Joo Chng, Minh-Dao Duong-Thi, Nurulhuda Mustafa, Jeffrey J.Y. Yen, Brian W. Dymock, Eng Chong Tan, and Sten Ohlson

Subjects

Models, Molecular, 0301 basic medicine, Ruxolitinib, Pharmacology, Hydroxamic Acids, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Nitriles, Drug Discovery, medicine, Animals, Humans, Protein Kinase Inhibitors, Vorinostat, Mice, Inbred BALB C, Chemistry, Kinase, HDAC11, Spectrum Analysis, Janus Kinase 1, Janus Kinase 2, Ligand (biochemistry), Histone Deacetylase Inhibitors, Pyrimidines, 030104 developmental biology, Cell culture, 030220 oncology & carcinogenesis, Pyrazoles, Molecular Medicine, Histone deacetylase, Janus kinase, Chromatography, Liquid, medicine.drug

Abstract

Concomitant inhibition of multiple oncogenic pathways is a desirable goal in cancer therapy. To achieve such an outcome with a single molecule would simplify treatment regimes. Herein the core features of ruxolitinib (1), a marketed JAK1/2 inhibitor, have been merged with the HDAC inhibitor vorinostat (2), leading to new molecules that are bispecific targeted JAK/HDAC inhibitors. A preferred pyrazole substituted pyrrolopyrimidine, 24, inhibits JAK1 and HDACs 1, 2, 3, 6, and 10 with IC50 values of less than 20 nM, is

Published

2017

7. Recently discovered EZH2 and EHMT2 (G9a) inhibitors

Author

Uttara Soumyanarayanan and Brian W. Dymock

Subjects

0301 basic medicine, Pharmacology, Methyltransferase, Molecular Structure, Tazemetostat, Pyridones, SET domain, EZH2, Antineoplastic Agents, Methyltransferases, macromolecular substances, Biology, Bioinformatics, EHMT2, 03 medical and health sciences, 030104 developmental biology, Neoplasms, Drug Discovery, Animals, Humans, Molecular Medicine, Enzyme Inhibitors

Abstract

Methyltransferase enzymes are promising epigenetic oncotargets. Recent efforts toward the development of inhibitors of two methyltransferases, EZH2 and G9a, as potential anticancer therapies are reviewed with a focus on the structure–activity relationships of compounds published from 2012. Benzamide-substituted 2-pyridones are still by far the most popular selective EZH2 inhibitor class but alternative classes are now being reported. There are now three EZH2 inhibitors in clinical development with the first responses in lymphoma patients with tazemetostat. Potent inhibitors of G9a are also published but no examples have yet reached the clinic. Dual blockage of EZH2–G9a is exemplified by one series of compounds. We conclude this review by presenting the three clinical stage compounds with the first clinical response data.

Published

2016

8. Antioxidants inhibit neuronal toxicity in Parkinson's disease‐linked LRRK2

Author

Brian W. Dymock, Dario C. Angeles, Patrick Ho, Zhi Dong Zhou, Eng-King Tan, and Kah-Leong Lim

Subjects

0301 basic medicine, Piceatannol, Antioxidant, Parkinson's disease, Kinase, business.industry, General Neuroscience, medicine.medical_treatment, Dopaminergic, Pharmacology, medicine.disease, Bioinformatics, Brief Communication, LRRK2, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, chemistry, medicine, Neurology (clinical), Kinase activity, business, 030217 neurology & neurosurgery, Thymoquinone

Abstract

Mutations in leucine‐rich repeat kinase‐2 are the most common cause of familial Parkinson's disease. The prevalent G2019S mutation increase oxidative, kinase and toxic activity and inhibit endogenous peroxidases. We initially screened a library of 84 antioxidants and identified seven phenolic compounds that inhibited kinase activity on leucine‐rich repeat kinase‐2 substrates. The representative antioxidants (piceatannol, thymoquinone, and esculetin) with strong kinase inhibitor activity, reduced loss in dopaminergic neurons, oxidative dysfunction, and locomotor defects in G2019S‐expressing neuronal and Drosophila models compared to weak inhibitors. We provide proof of principle that natural antioxidants with dual antioxidant and kinase inhibitor properties could be useful for leucine‐rich repeat kinase‐2‐linked Parkinson's disease.

Published

2016

9. Discovery of the cancer cell selective dual acting anti-cancer agent (Z)-2-(1H-indol-3-yl)-3-(isoquinolin-5-yl)acrylonitrile (A131)

Author

Pei-Ju Liao, Sang Hyun Lee, Mayumi Kitagawa, Kyunghee Lee, Brian W. Dymock, Cheng Shang See, and Jasmine Wong

Subjects

0301 basic medicine, Male, Programmed cell death, Colorectal cancer, medicine.medical_treatment, Phenotypic screening, Mice, Nude, Mitosis, Antineoplastic Agents, 01 natural sciences, Targeted therapy, HeLa, 03 medical and health sciences, Mice, Cell Line, Tumor, Neoplasms, Drug Discovery, medicine, Animals, Humans, Cell Proliferation, Pharmacology, Mice, Inbred BALB C, biology, Acrylonitrile, 010405 organic chemistry, Chemistry, Organic Chemistry, Cancer, General Medicine, medicine.disease, biology.organism_classification, Isoquinolines, 0104 chemical sciences, Rats, 030104 developmental biology, Drug Resistance, Neoplasm, Cancer cell, Colonic Neoplasms, Cancer research, Drug Screening Assays, Antitumor

Abstract

Selective targeting of cancer cells over normal cells is a key objective of targeted therapy. However few approaches achieve true mechanistic selectivity resulting in debilitating side effects and dose limitation. In this work we describe the discovery of A131 (4a), a new agent with an unprecedented dual mechanism of action targeting both mitosis and autophagy. Compound 4a was first identified in a phenotypic screen in which HeLa cells treated with 4a manifested mitotic arrest along with formation of multiple vesicles. Further investigations showed that 4a causes an increase in mitotic marker pH3 and autophagy marker LC3. Importantly 4a induces cell death in cancer cells while sparing normal cells which regrow after 4a is removed. Dual activities against pH3 and LC3 markers are required for cancer cell selectivity. An extensive SAR investigation confirmed 4a as the optimal dual inhibitor with potency against a panel of 30 cancer cell lines (average antiproliferative GI50 1.5 μM). In a mouse model of paclitaxel-resistant colon cancer, 4a showed 74% tumor growth inhibition when administered at a dose of 20 mg/kg IP twice a day.

Published

2018

10. Intracellular Hyper-Acidification Potentiated by Hydrogen Sulfide Mediates Invasive and Therapy Resistant Cancer Cell Death

Author

Zheng-Wei Lee, Xin-Yi Teo, Zhi J. Song, Dawn S. Nin, Wisna Novera, Bok A. Choo, Brian W. Dymock, Philip K. Moore, Ruby Y.-J. Huang, and Lih-Wen Deng

Subjects

0301 basic medicine, Pharmacology, lactate, Programmed cell death, therapy resistance, biology, Intracellular pH, lcsh:RM1-950, hydrogen sulfide, invasive cancer, intracellular acidification, 03 medical and health sciences, lcsh:Therapeutics. Pharmacology, 030104 developmental biology, Cancer cell, Monocarboxylate transporter 4, biology.protein, Glycolysis, Pharmacology (medical), Cytotoxicity, Intracellular, Homeostasis, Original Research

Abstract

Slow and continuous release of H2S by GYY4137 has previously been demonstrated to kill cancer cells by increasing glycolysis and impairing anion exchanger and sodium/proton exchanger activity. This action is specific for cancer cells. The resulting lactate overproduction and defective pH homeostasis bring about intracellular acidification-induced cancer cell death. The present study investigated the potency of H2S released by GYY4137 against invasive and radio- as well as chemo-resistant cancers, known to be glycolytically active. We characterized and utilized cancer cell line pairs of various organ origins, based on their aggressive behaviors, and assessed their response to GYY4137. We compared glycolytic activity, via lactate production, and intracellular pH of each cancer cell line pair after exposure to H2S. Invasive and therapy resistant cancers, collectively termed aggressive cancers, are receptive to H2S-mediated cytotoxicity, albeit at a higher concentration of GYY4137 donor. While lactate production was enhanced, intracellular pH of aggressive cancers was only modestly decreased. Inherently, the magnitude of intracellular pH decrease is a key determinant for cancer cell sensitivity to H2S. We demonstrated the utility of coupling GYY4137 with either simvastatin, known to inhibit monocarboxylate transporter 4 (MCT4), or metformin, to further boost glycolysis, in bringing about cell death for aggressive cancers. Simvastatin inhibiting lactate extrusion thence contained excess lactate induced by GYY4137 within intracellular compartment. In contrast, the combined exposure to both GYY4137 and metformin overwhelms cancer cells with lactate over-production exceeding its expulsion rate. Together, GYY4137 and simvastatin or metformin synergize to induce intracellular hyper-acidification-mediated cancer cell death.

Published

2017

11. SAHA and cisplatin sensitize gastric cancer cells to doxorubicin by induction of DNA damage, apoptosis and perturbation of AMPK-mTOR signalling

Author

Edmund J.D. Lee, Han-Ming Shen, Jian Yun Loh, Paul Edward Hutchinson, Hwei Ling Tan, Ee Sin Chen, Brian W. Dymock, Kim Kiat Lim, Kwi Shan Seah, Thi Thuy Trang Nguyen, and Yun Chau Long

Subjects

0301 basic medicine, medicine.drug_class, DNA damage, Cell Survival, Caspase 3, Antineoplastic Agents, Apoptosis, Biology, AMP-Activated Protein Kinases, 03 medical and health sciences, 0302 clinical medicine, Stomach Neoplasms, Cell Line, Tumor, medicine, Humans, Doxorubicin, PI3K/AKT/mTOR pathway, Cisplatin, Vorinostat, TOR Serine-Threonine Kinases, Histone deacetylase inhibitor, AMPK, Cell Biology, Histone Deacetylase Inhibitors, 030104 developmental biology, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, medicine.drug, DNA Damage, Signal Transduction

Abstract

Chemotherapy remains the most prescribed anti-cancer therapy, despite patients suffering severe side effects and frequently developing chemoresistance. These complications can be partially overcome by combining different chemotherapeutic agents that target multiple biological pathways. However, selecting efficacious drug combinations remains challenging. We previously used fission yeast Schizosaccharomycespombe as a surrogate model to predict drug combinations, and showed that suberoylanilide hydroxamic acid (SAHA) and cisplatin can sensitise gastric adenocarcinoma cells toward the cytotoxic effects of doxorubicin. Yet, how this combination undermines cell viability is unknown. Here, we show that SAHA and doxorubicin markedly enhance the cleavage of two apoptosis markers, caspase 3 and poly-ADP ribose polymerase (PARP-1), and increase the phosphorylation of γH2AX, a marker of DNA damage. Further, we found a prominent reduction in Ser485 phosphorylation of AMP-dependent protein kinase (AMPK), and reductions in its target mTOR and downstream ribosomal protein S6 phosphorylation. We show that SAHA contributes most of the effect, as confirmed using another histone deacetylase inhibitor, trichostatin A. Overall, our results show that the combination of SAHA and doxorubicin can induce apoptosis in gastric adenocarcinoma in a synthetically lethal manner, and that fission yeast offers an efficient tool for identifying potent drug combinations against human cancer cells.

Published

2017

12. Towards Selective Mycobacterial ClpP1P2 Inhibitors with Reduced Activity against the Human Proteasome

Author

Wilfried Moreira, Sridhar Santhanakrishnan, Anders Poulsen, Thomas Dick, Brian W. Dymock, Grace J. Y. Ngan, Kanda Sangthongpitag, and Choon Bing Low

Subjects

0301 basic medicine, Models, Molecular, Proteases, medicine.medical_treatment, Mycobacterium smegmatis, Microbial Sensitivity Tests, Pharmacology, Mycobacterium tuberculosis, Bortezomib, 03 medical and health sciences, chemistry.chemical_compound, Mice, Bacterial Proteins, medicine, Potency, Animals, Pharmacology (medical), Experimental Therapeutics, dipeptidyl boronic acid, Tuberculosis, Pulmonary, antimycobacterial, Protease, biology, Serine Endopeptidases, Endopeptidase Clp, biology.organism_classification, Anti-Bacterial Agents, 030104 developmental biology, Infectious Diseases, chemistry, Proteasome, Drug Design, Toxicity, caseinolytic protease, Lead compound, Proteasome Inhibitors, medicine.drug

Abstract

Mycobacterium tuberculosis is responsible for the greatest number of deaths worldwide due to a bacterial agent. We recently identified bortezomib (Velcade; compound 1) as a promising antituberculosis (anti-TB) compound. We showed that compound 1 inhibits the mycobacterial caseinolytic proteases P1 and P2 (ClpP1P2) and exhibits bactericidal activity, and we established compound 1 and ClpP1P2 as an attractive lead/target couple. However, compound 1 is a human-proteasome inhibitor currently approved for cancer therapy and, as such, exhibits significant toxicity. Selective inhibition of the bacterial protease over the human proteasome is desirable in order to maintain antibacterial activity while reducing toxicity. We made use of structural data in order to design a series of dipeptidyl-boronate derivatives of compound 1. We tested these derivatives for whole-cell ClpP1P2 and human-proteasome inhibition as well as bacterial-growth inhibition and identified compounds that were up to 100-fold-less active against the human proteasome but that retained ClpP1P2 and mycobacterial-growth inhibition as well as bactericidal potency. The lead compound, compound 58, had low micromolar ClpP1P2 and anti- M. tuberculosis activity, good aqueous solubility, no cytochrome P450 liabilities, moderate plasma protein binding, and low toxicity in two human liver cell lines, and despite high clearance in microsomes, this compound was only moderately cleared when administered intravenously or orally to mice. Higher-dose oral pharmacokinetics indicated good dose linearity. Furthermore, compound 58 was inhibitory to only 11% of a panel of 62 proteases. Our work suggests that selectivity over the human proteasome can be achieved with a drug-like template while retaining potency against ClpP1P2 and, crucially, anti- M. tuberculosis activity.

Published

2017

13. Bortezomib Warhead-Switch Confers Dual Activity against Mycobacterial Caseinolytic Protease and Proteasome and Selectivity against Human Proteasome

Author

Sridhar Santhanakrishnan, Thomas Dick, Brian W. Dymock, and Wilfried Moreira

Subjects

0301 basic medicine, Microbiology (medical), medicine.medical_treatment, lcsh:QR1-502, Biology, Microbiology, lcsh:Microbiology, ClpP1P2, Bortezomib, 03 medical and health sciences, chemistry.chemical_compound, medicine, Cytotoxicity, Original Research, chemistry.chemical_classification, Protease, Dipeptide, selective inhibitors, 030104 developmental biology, Enzyme, TB, chemistry, Proteasome, Biochemistry, Proteasome inhibitor, Boronic acid, medicine.drug

Abstract

Mycobacteria harbor two main degradative proteolytic machineries, the caseinolytic protease ClpP1P2 and a proteasome. We recently showed that Bortezomib inhibits ClpP1P2 and exhibits whole cell activity against Mycobacterium tuberculosis. Bortezomib, a dipeptide with a boronic acid warhead, is a human proteasome inhibitor approved for cancer therapy. The boronic acid warhead of the compound has been shown to drive potency against both the human proteasome and ClpP1P2 protease. Selectivity for the bacterial ClpP1P2 protease over the human proteasome is lacking but needs to be achieved to move this new anti-tuberculosis lead forward. In this study we explored whether an alternative warhead could influence Bortezomib's selectivity. We synthesized an analog containing a chloromethyl ketone instead of the boronic acid warhead and determined potencies against the bacterial and human enzymes. Surprisingly, the analog retained activity against mycobacterial ClpP1P2 and was active against the mycobacterial proteasome, but was devoid of activity against the human proteasome. Interrogation of a set of chloromethyl ketone peptides identified three additional compounds similarly inhibiting both ClpP1P2 and the proteasome in the bacteria while leaving the human proteasome untouched. Finally, we showed that these compounds display bactericidal activity against M. tuberculosis with cytotoxicity ranging from acceptable to undetectable. These results suggest that selectivity over the human proteasome is achievable. Selectivity, together with dual-targeting of mycobacterial ClpP1P2 and proteasome makes this new scaffold an attractive starting point for optimization.

Published

2017

14. Design and Synthesis of Janus Kinase 2 (JAK2) and Histone Deacetlyase (HDAC) Bispecific Inhibitors Based on Pacritinib and Evidence of Dual Pathway Inhibition in Hematological Cell Lines

Author

Eugene Guorong Yang, Jeffrey J.Y. Yen, Eng Chong Tan, Anders Poulsen, Pondy Murugappan Ramanujulu, Wee Joo Chng, Nurulhuda Mustafa, and Brian W. Dymock

Subjects

0301 basic medicine, Bridged-Ring Compounds, Models, Molecular, Antineoplastic Agents, Apoptosis, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Drug Discovery, medicine, Humans, Vorinostat, Protein Kinase Inhibitors, Cell Proliferation, Janus kinase 2, biology, Chemistry, Kinase, HDAC6, Janus Kinase 2, Histone Deacetylase Inhibitors, 030104 developmental biology, Pacritinib, Pyrimidines, Biochemistry, Cell culture, 030220 oncology & carcinogenesis, Hematologic Neoplasms, biology.protein, Cancer research, Molecular Medicine, Pharmacophore, FLT3 Inhibitor, medicine.drug, Signal Transduction

Abstract

Blockage of more than one oncoprotein or pathway is now a standard approach in modern cancer therapy. Multiple inhibition is typically achieved with two or more drugs. Herein, we describe a pharmacophore merging strategy combining the JAK2/FLT3 inhibitor pacritnib with the pan-HDAC inhibitor, vorinostat, to create bispecific single molecules with both JAK and HDAC targeted inhibition. A preferred ether hydroxamate, 51, inhibits JAK2 and HDAC6 with low nanomolar potency, is100 nM potent against HDACs 2 and 10, submicromolar potent against HDACs 1, 8, and 11, and50-fold selective for JAK2 in a panel of 97 kinases. Broad cellular antiproliferative potency is supported by demonstration of JAK-STAT and HDAC pathway blockade in several hematological cell lines, inhibition of colony formation in HEL cells, and analysis of apoptosis. This study provides new tool compounds for further exploration of dual JAK-HDAC pathway inhibiton achieved with a single molecule.

Published

2016

15. Discovery of medium ring thiophosphorus based heterocycles as antiproliferative agents

Author

Kaye Peh, Lih-Wen Deng, Brian W. Dymock, Donavan Neo, Philip K. Moore, Wisna Novera, Pondy Murugappan Ramanujulu, and Wei Feng

Subjects

0301 basic medicine, Stereochemistry, Hydrogen sulfide, Clinical Biochemistry, Pharmaceutical Science, chemistry.chemical_element, Ring (chemistry), 01 natural sciences, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, Heterocyclic Compounds, Cell Line, Tumor, Drug Discovery, Molecule, Potency, Humans, Hydrogen Sulfide, Molecular Biology, Cell Proliferation, Aqueous solution, 010405 organic chemistry, Organic Chemistry, Phosphorus, Sulfur, 0104 chemical sciences, 030104 developmental biology, chemistry, Cell culture, Molecular Medicine, Organic synthesis, Female

Abstract

Hydrogen sulfide (H 2 S) has been investigated for its potential in therapy. Recently, we reported novel H 2 S donor molecules based on a thiophosphorus core, which slowly release H 2 S and have improved anti-proliferative activity in cancer cell lines compared to the most widely studied H 2 S donor GYY4137 ( 1 ). Herein, we have prepared new thiophosphorus organic H 2 S donors with different ring sizes and evaluated them in two solid tumor cell lines and one normal cell line. A seven membered ring compound, 17 , was found to be the most potent with sub-micromolar IC 50s in breast (0.76 μM) and ovarian (0.76 μM) cancer cell lines. No significant H 2 S release was detected in aqueous solution for this compound. However, confocal imaging showed that H 2 S was released from 17 inside cells at a similar level to the widely studied H 2 S donor GYY4137, which was shown to release 10 μM H 2 S after 12 h at a concentration of 400 μM. Comparison of 17 with its non-sulfur oxygen analogue, 26 , provided evidence that the sulfur atom is important for its potency. However, the significant potency observed for 26 (5.94–11.0 μM) indicates that the high potency of 17 is not entirely due to release of H 2 S. Additional mechanism(s) appear to be responsible for the observed activity, hence more detailed studies are required to better understand the role of H 2 S in cancer with potent thiophosphorus agents.

Published

2016

16. Overcoming chloroquine resistance in malaria: Design, synthesis and structure-activity relationships of novel chemoreversal agents

Author

François Nosten, Aicha Boudhar, Chiew Yee Loh, Kevin S. W. Tan, Xiao Wei Ng, Brian W. Dymock, Wan Ni Chia, and Zhi Ming Tan

Subjects

0301 basic medicine, Models, Molecular, Plasmodium falciparum, Drug Resistance, Molecular Conformation, Drug resistance, Chemistry Techniques, Synthetic, Pharmacology, 01 natural sciences, Cell Line, 03 medical and health sciences, Antimalarials, Inhibitory Concentration 50, Mice, Structure-Activity Relationship, Chloroquine, Drug Discovery, medicine, Structure–activity relationship, Animals, Artemisinin, Chloroquine resistance, biology, Dose-Response Relationship, Drug, Chemistry, Organic Chemistry, Biological Transport, General Medicine, medicine.disease, biology.organism_classification, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, 030104 developmental biology, Infectious disease (medical specialty), Drug Design, Malaria, medicine.drug

Abstract

Malaria remains a significant infectious disease with even artemisinin-based therapies now facing resistance in the field. Development of new therapies is urgently needed, either by finding new compounds with unique modes of action, or by reversing resistance towards known drugs with 'chemosensitizers' or 'chemoreversal' agents (CRA). Concerning the latter, we have focused on the resistance mechanisms developed against chloroquine (CQ). We have synthesized a series of compounds related to previously identified CRAs, and found promising novel compounds. These compounds show encouraging results in a coumarin labeled chloroquine uptake assay, exhibiting a dose response in resensitising parasites to the antimalarial effects of chloroquine. Selected compounds show consistent potency across a panel of chloroquine and artemisinin sensitive and resistant parasites, and a wide therapeutic window. This data supports further study of CRAs in the treatment of malaria and, ultimately, their use in chloroquine-based combination therapies.

Published

2016

17. A novel slow-releasing hydrogen sulfide donor, FW1256, exerts anti-inflammatory effects in mouse macrophages and in vivo

Author

Brian W. Dymock, Kaye Peh, Wei Feng, Philip K. Moore, Meng Teng Peh, and Caleb Huang

Subjects

0301 basic medicine, Male, Programmed cell death, medicine.drug_class, Interleukin-1beta, Anti-Inflammatory Agents, Nitric Oxide Synthase Type II, Inflammation, Pharmacology, Nitric Oxide, Anti-inflammatory, Dinoprostone, Cell Line, 03 medical and health sciences, Mice, In vivo, medicine, Cytotoxic T cell, Animals, Secretion, Hydrogen Sulfide, Cell Death, Chemistry, Interleukin-6, Tumor Necrosis Factor-alpha, Macrophages, NF-kappa B, Mice, Inbred C57BL, Cytosol, 030104 developmental biology, RAW 264.7 Cells, Biochemistry, Cyclooxygenase 2, lipids (amino acids, peptides, and proteins), Tumor necrosis factor alpha, medicine.symptom, Signal Transduction

Abstract

Exogenous hydrogen sulfide (H2S) is known to exert anti-inflammatory effects both in macrophages and in animal models. In this study, we first showed that NaHS caused a concentration dependent reduction in TNFα and IL-6 secretion in LPS-stimulated RAW264.7 macrophages in the absence of cell death. Thereafter, we screened a series of novel slow H2S donors for similar activity. One such compound, FW1256, concentration dependently decreased TNFα, IL-6, PGE2 and NO generation in LPS-stimulated RAW264.7 macrophages and BMDMs. FW1256 also significantly reduced IL-1β, COX-2 and iNOS mRNA and protein in LPS-stimulated RAW264.7 macrophages. Mechanistically, FW1256 decreased NFκB activation as evidenced by reduced cytosolic phospho-IκBα levels and reduced nuclear p65 levels in LPS-stimulated RAW264.7 macrophages treated with FW1256. Using a H2S fluorescent probe in FW1256-treated RAW264.7 macrophages, H2S release from FW1256 was apparent over a period of 24h in these cells. Moreover, the effect of FW1256 on TNFα and IL-6 by FW1256 in LPS-stimulated RAW264.7 macrophages was reversed by treatment with the H2S scavenger, vitamin B12a. FW1256 had no cytotoxic effect on LPS-stimulated RAW264.7 macrophages or BMDMs. In vivo, FW1256 administration also reduced IL-1β, TNFα, nitrate/nitrite and PGE2 levels in LPS-treated mice. We show here a novel slow H2S-releasing compound that exerts anti-inflammatory effects in macrophages and in vivo. FW1256 may be a useful tool to study the biological effects of exogenous H2S and could also have future therapeutic value in inflammatory conditions.

Published

2016

18. A Small Molecule Targeting the Transmembrane Domain of Death Receptor p75NTR Induces Melanoma Cell Death and Reduces Tumor Growth

Author

Zhi Lin, Bo Young Ahn, Brian W. Dymock, Ngoc Ha Dang, Donna L. Senger, Bryan W. Berger, Carlos F. Ibáñez, Eddy T. H. Goh, Vanessa Lopes-Rodrigues, and Shuhailah Salim

Subjects

0301 basic medicine, Pharmacology, Programmed cell death, Melanoma, Clinical Biochemistry, Biology, medicine.disease, Biochemistry, Small molecule, Cell biology, 03 medical and health sciences, Transmembrane domain, 030104 developmental biology, Membrane protein, Cell surface receptor, Drug Discovery, medicine, biology.protein, Molecular Medicine, sense organs, Receptor, Molecular Biology, Neurotrophin

Abstract

Small molecules offer powerful ways to alter protein function. However, most proteins in the human proteome lack small-molecule probes, including the large class of non-catalytic transmembrane receptors, such as death receptors. We hypothesized that small molecules targeting the interfaces between transmembrane domains (TMDs) in receptor complexes may induce conformational changes that alter receptor function. Applying this concept in a screening assay, we identified a compound targeting the TMD of death receptor p75NTR that induced profound conformational changes and receptor activity. The compound triggered apoptotic cell death dependent on p75NTR and JNK activity in neurons and melanoma cells, and inhibited tumor growth in a melanoma mouse model. Due to their small size and crucial role in receptor activation, TMDs represent attractive targets for small-molecule manipulation of receptor function.

Published

2018

19. Predicting chemotherapeutic drug combinations through gene network profiling

Author

Louxin Zhang, Kwi Shan Seah, Audrey Yuen, Seok Hwee Koo, Thi Thuy Trang Nguyen, Brian W. Dymock, Edmund J.D. Lee, Eugene Guorong Yang, Shermaine Yu Wen Pang, Kim Kiat Lim, Jie Yin Yee, Wee Han Ang, Ee Sin Chen, and Jacqueline Chua

Subjects

0301 basic medicine, medicine.drug_class, Gene regulatory network, Antineoplastic Agents, Drug resistance, Synthetic lethality, Computational biology, Biology, Pharmacology, Article, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Gene Expression Regulation, Fungal, Schizosaccharomyces, medicine, Humans, Doxorubicin, Gene Regulatory Networks, Cell Proliferation, Multidisciplinary, Gene Expression Profiling, Histone deacetylase inhibitor, biology.organism_classification, Drug Resistance, Multiple, Gene expression profiling, Drug Combinations, 030104 developmental biology, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Schizosaccharomyces pombe, Mutation, Drug Screening Assays, Antitumor, medicine.drug

Abstract

Contemporary chemotherapeutic treatments incorporate the use of several agents in combination. However, selecting the most appropriate drugs for such therapy is not necessarily an easy or straightforward task. Here, we describe a targeted approach that can facilitate the reliable selection of chemotherapeutic drug combinations through the interrogation of drug-resistance gene networks. Our method employed single-cell eukaryote fission yeast (Schizosaccharomyces pombe) as a model of proliferating cells to delineate a drug resistance gene network using a synthetic lethality workflow. Using the results of a previous unbiased screen, we assessed the genetic overlap of doxorubicin with six other drugs harboring varied mechanisms of action. Using this fission yeast model, drug-specific ontological sub-classifications were identified through the computation of relative hypersensitivities. We found that human gastric adenocarcinoma cells can be sensitized to doxorubicin by concomitant treatment with cisplatin, an intra-DNA strand crosslinking agent and suberoylanilide hydroxamic acid, a histone deacetylase inhibitor. Our findings point to the utility of fission yeast as a model and the differential targeting of a conserved gene interaction network when screening for successful chemotherapeutic drug combinations for human cells.

Published

2016

20. Overcoming Chloroquine Resistance in Malaria: Design, Synthesis, and Structure-Activity Relationships of Novel Hybrid Compounds

Author

Xiao Wei Ng, Brian W. Dymock, Aicha Boudhar, Zhi Ming Tan, Chiew Yee Loh, François Nosten, Kevin S. W. Tan, and Wan Ni Chia

Subjects

0301 basic medicine, Membrane permeability, Plasmodium falciparum, Pharmacology, 03 medical and health sciences, Antimalarials, Structure-Activity Relationship, 0302 clinical medicine, Chloroquine, parasitic diseases, medicine, Potency, Structure–activity relationship, Pharmacology (medical), Experimental Therapeutics, Artemisinin, biology, Chemistry, medicine.disease, biology.organism_classification, In vitro, Artemisinins, 030104 developmental biology, Infectious Diseases, 030220 oncology & carcinogenesis, Malaria, medicine.drug

Abstract

Resistance to antimalarial therapies, including artemisinin, has emerged as a significant challenge. Reversal of acquired resistance can be achieved using agents that resensitize resistant parasites to a previously efficacious therapy. Building on our initial work describing novel chemoreversal agents (CRAs) that resensitize resistant parasites to chloroquine (CQ), we herein report new hybrid single agents as an innovative strategy in the battle against resistant malaria. Synthetically linking a CRA scaffold to chloroquine produces hybrid compounds with restored potency toward a range of resistant malaria parasites. A preferred compound, compound 35, showed broad activity and good potency against seven strains resistant to chloroquine and artemisinin. Assessment of aqueous solubility, membrane permeability, and in vitro toxicity in a hepatocyte line and a cardiomyocyte line indicates that compound 35 has a good therapeutic window and favorable drug-like properties. This study provides initial support for CQ-CRA hybrid compounds as a potential treatment for resistant malaria.

Published

2015

21. The rise of epigenetic drug discovery

Author

Brian W. Dymock

Subjects

0301 basic medicine, Pharmacology, Genetics, biology, Drug discovery, Methylation, 03 medical and health sciences, 030104 developmental biology, Histone, Acetylation, Drug Discovery, biology.protein, Molecular Medicine, Epigenetics, Epigenomics

Published

2016

22. Hydrocarbon stapled B chain analogues of relaxin-3 retain biological activity

Author

Charles W. Johannes, Subhi Marwari, Rajamani Lakshminarayanan, Deron R. Herr, Anders Poulsen, Gavin S. Dawe, Tharindunee Jayakody, Francis Chee Kuan Tan, and Brian W. Dymock

Subjects

0301 basic medicine, MAP Kinase Signaling System, Physiology, Proteolysis, INSL7, Peptide, Biochemistry, Receptors, G-Protein-Coupled, 03 medical and health sciences, Structure-Activity Relationship, Cellular and Molecular Neuroscience, 0302 clinical medicine, Endocrinology, cAMP, medicine, Cyclic AMP, Structure–activity relationship, Humans, Stapled peptide, Receptor, G protein-coupled receptor, chemistry.chemical_classification, RXFP3, medicine.diagnostic_test, ERK1/2, Chemistry, Colforsin, Relaxin, Biological activity, Hydrocarbons, 030104 developmental biology, HEK293 Cells, Relaxin-3, Peptides, 030217 neurology & neurosurgery, Relaxin/insulin-like family peptide receptor 2, hormones, hormone substitutes, and hormone antagonists, Protein Binding

Abstract

Relaxin-3 or insulin-like peptide 7 (INSL7) is the most recently discovered relaxin/insulin-like family peptide. Mature relaxin-3 consists of an A chain and a B chain held by disulphide bonds. According to structure activity relationship studies, the relaxin-3 B chain is more important in binding and activating the receptor. RXFP3 (also known as Relaxin-3 receptor 1, GPCR 135, somatostatin- and angiotensin- like peptide receptor or SALPR) was identified as the cognate receptor for relaxin-3 by expression profiles and binding studies. Recent studies imply roles of this system in mediating stress and anxiety, feeding, metabolism and cognition. Stapling of peptides is a technique used to develop peptide drugs for otherwise undruggable targets. The main advantages of stapling include, increased activity due to reduced proteolysis, increased affinity to receptors and increased cell permeability. Stable agonists and antagonists of RXFP3 are crucial for understanding the physiological significance of this system. So far, agonists and antagonists of RXFP3 are peptides. In this study, for the first time, we have introduced stapling of the relaxin-3 B chain at 14th and 18th positions (14s18) and 18th and 22nd position (18s22). These stapled peptides showed greater helicity than the unstapled relaxin-3 B chain in circular dichroism analysis. Both stapled peptides bound RXFP3 and activated RXFP3 as observed in an inhibition of forskolin-induced cAMP assay and a ERK1/2 activation assay, although with different potencies. Therefore, we conclude that stapling of the relaxin3 B chain does not compromise its ability to activate RXFP3 and is a promising method for developing stable peptide agonists and antagonists of RXFP3 to aid relaxin-3/RXFP3 research.