Your search keyword '"Wanchi Fung"' showing total 6 results

1. Structure-guided discovery of a novel, potent, and orally bioavailable 3,5-dimethylisoxazole aryl-benzimidazole BET bromodomain inhibitor

Author

Wanchi Fung, Kobayashi Tetsuya, Anita Niedziela-Majka, Bob Jiang, Kim Jordan, Saritha Kusam, David G. Breckenridge, Hai Yang, Britton Kenneth Corkey, Kristyna Elbel, Chin Tay, Elaine Kan, Sammy Metobo, David Sperandio, Du Jinfa, Richard M. Neve, Sophia L. Shevick, Eric B. Lansdon, Kerim Babaoglu, Gregory Chin, Heather Webb, Debi Jin, Annapurna Sapre, Vangelis Aktoudianakis, Latesh Lad, Jamie Bates, Xiaowu Chen, Jeff Zablocki, Gene Eisenberg, Nate Larson, Richard L. Mackman, Martinez Ruben, Magdeleine Hung, Zachary Newby, and Mish Michael R

Subjects

Benzimidazole, BRD4, Cell Survival, Clinical Biochemistry, Administration, Oral, Biological Availability, Pharmaceutical Science, Biochemistry, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Protein Domains, Cell Line, Tumor, Drug Discovery, Animals, Humans, Potency, Tumor growth, Epigenetics, Molecular Biology, Cell Proliferation, Dose-Response Relationship, Drug, Molecular Structure, Aryl, Organic Chemistry, Isoxazoles, Neoplasms, Experimental, Bioavailability, Bromodomain, chemistry, Molecular Medicine, Benzimidazoles, Multiple Myeloma, Transcription Factors

Abstract

The bromodomain and extra-terminal (BET) family of proteins, consisting of the bromodomains containing protein 2 (BRD2), BRD3, BRD4, and the testis-specific BRDT, are key epigenetic regulators of gene transcription and has emerged as an attractive target for anticancer therapy. Herein, we describe the discovery of a novel potent BET bromodomain inhibitor, using a systematic structure-based approach focused on improving potency, metabolic stability, and permeability. The optimized dimethylisoxazole aryl-benzimidazole inhibitor exhibited high potency towards BRD4 and related BET proteins in biochemical and cell-based assays and inhibited tumor growth in two proof-of-concept preclinical animal models.

Published

2019

2. Fully human anti-CD39 antibody potently inhibits ATPase activity in cancer cells via uncompetitive allosteric mechanism

Author

Clifford Wong, John Corbin, Karolina Losenkova, Maria Kovalenko, Alana G. Lerner, Tracy dela Cruz, Vanessa B. Soros, Gennady G. Yegutkin, Bradley N. Spatola, Wanchi Fung, Courtney Beers, and Megan Welch

Subjects

Immunology, Allosteric regulation, enzyme inhibitor, Antibody Affinity, Antineoplastic Agents, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Report, enzyme kinetics, Cell Line, Tumor, medicine, Extracellular, Immunology and Allergy, cancer, Humans, enzyme mechanism, Enzyme Inhibitors, 030304 developmental biology, Adenosine Triphosphatases, 0303 health sciences, Tumor microenvironment, CD39, biology, Apyrase, Antibodies, Monoclonal, Adenosine, allosteric regulation, Cell biology, ATP, chemistry, Enzyme inhibitor, monoclonal antibody, 030220 oncology & carcinogenesis, Cancer cell, Nucleoside triphosphate, biology.protein, cancer therapy, sense organs, Binding Sites, Antibody, Antibody, medicine.drug

Abstract

The extracellular ATP/adenosine axis in the tumor microenvironment (TME) has emerged as an important immune-regulatory pathway. Nucleoside triphosphate diphosphohydrolase-1 (NTPDase1), otherwise known as CD39, is highly expressed in the TME, both on infiltrating immune cells and tumor cells across a broad set of cancer indications. CD39 processes pro-inflammatory extracellular ATP to ADP and AMP, which is then processed by Ecto-5ʹ-nucleotidase/CD73 to immunosuppressive adenosine. Directly inhibiting the enzymatic function of CD39 via an antibody has the potential to unleash an immune-mediated anti-tumor response via two mechanisms: 1) increasing the availability of immunostimulatory extracellular ATP released by damaged and/or dying cells, and 2) reducing the generation and accumulation of suppressive adenosine within the TME. Tizona Therapeutics has engineered a novel first-in-class fully human anti-CD39 antibody, TTX-030, that directly inhibits CD39 ATPase enzymatic function with sub-nanomolar potency. Further characterization of the mechanism of inhibition by TTX-030 using CD39+ human melanoma cell line SK-MEL-28 revealed an uncompetitive allosteric mechanism (α

Published

2020

3. Insights Into Spinal Dorsal Horn Circuit Function and Dysfunction Using Optical Approaches

Author

Erika K. Harding, Samuel Wanchi Fung, and Robert P. Bonin

Subjects

somatosensation, 0301 basic medicine, Spinal Cord Dorsal Horn, Sensory processing, Cognitive Neuroscience, medicine.medical_treatment, Central nervous system, Sensation, Neuroscience (miscellaneous), Review, Optogenetics, Inhibitory postsynaptic potential, Somatosensory system, lcsh:RC321-571, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Calcium imaging, Interneurons, medicine, Animals, Humans, pain, optogenetics, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, dorsal horn, Proprioception, business.industry, spinal cord, Somatosensory Cortex, Spinal cord, Sensory Systems, calcium imaging, in vivo, 030104 developmental biology, medicine.anatomical_structure, Nerve Net, business, Neuroscience, 030217 neurology & neurosurgery

Abstract

Somatosensation encompasses a variety of essential modalities including touch, pressure, proprioception, temperature, pain, and itch. These peripheral sensations are crucial for all types of behaviors, ranging from social interaction to danger avoidance. Somatosensory information is transmitted from primary afferent fibers in the periphery into the central nervous system via the dorsal horn of the spinal cord. The dorsal horn functions as an intermediary processing center for this information, comprising a complex network of excitatory and inhibitory interneurons as well as projection neurons that transmit the processed somatosensory information from the spinal cord to the brain. It is now known that there can be dysfunction within this spinal cord circuitry in pathological pain conditions and that these perturbations contribute to the development and maintenance of pathological pain. However, the complex and heterogeneous network of the spinal dorsal horn has hampered efforts to further elucidate its role in somatosensory processing. Emerging optical techniques promise to illuminate the underlying organization and function of the dorsal horn and provide insights into the role of spinal cord sensory processing in shaping the behavioral response to somatosensory input that we ultimately observe. This review article will focus on recent advances in optogenetics and fluorescence imaging techniques in the spinal cord, encompassing findings from both in vivo and in vitro preparations. We will also discuss the current limitations and difficulties of employing these techniques to interrogate the spinal cord and current practices and approaches to overcome these challenges.

Published

2020

4. Lipid-Sensing High-Throughput ApoA-I Assays

Author

Jeffrey W. Chisholm, Nikos Pagratis, Leanna Lagpacan, Karen Schwartz, Wanchi Fung, Katherine M. Brendza, Debi Jin, Xiaohong Liu, Anita Niedziela-Majka, Latesh Lad, Roman Sakowicz, and Magdeleine Hung

Subjects

lipid analysis, Apolipoprotein B, Biochemistry, Analytical Chemistry, chemistry.chemical_compound, apolipoprotein A1, high density lipoprotein cholesterol, Fluorescence Resonance Energy Transfer, polycyclic compounds, biotinylation, Cells, Cultured, biology, terbium, ABC transporter A1, risk assessment, Lipids, Cholesterol, radioactivity, Biotinylation, Molecular Medicine, lipids (amino acids, peptides, and proteins), Lipoproteins, HDL, ATP Binding Cassette Transporter 1, Biotechnology, Phospholipid, Biotin, foam cell, lipid, cholesterol transport, phospholipid transfer, Humans, artery wall, Fluorescent Dyes, Apolipoprotein A-I, human cell, Macrophages, nutritional and metabolic diseases, Atherosclerosis, Lipid Metabolism, High-Throughput Screening Assays, Förster resonance energy transfer, chemistry, ABCA1, cholesterol metabolism, biology.protein, amino terminal sequence, ATP-Binding Cassette Transporters, Streptavidin, protein determination, Adenosine triphosphate, high throughput screening, Lipoprotein

Abstract

Apolipoprotein A-I (ApoA-I), a primary protein component of high-density lipoprotein (HDL), plays an important role in cholesterol metabolism mediating the formation of HDL and the efflux of cellular cholesterol from macrophage foam cells in arterial walls. Lipidation of ApoA-I is mediated by adenosine triphosphate (ATP) binding cassette A1 (ABCA1). Insufficient ABCA1 activity may lead to increased risk of atherosclerosis due to reduced HDL formation and cholesterol efflux. The standard radioactive assay for measuring cholesterol transport to ApoA-I has low throughput and poor dynamic range, and it fails to measure phospholipid transfer. We describe the development of two sensitive, nonradioactive high-throughput assays that report on the lipidation of ApoA-I: a homogeneous assay based on time-resolved fluorescence resonance energy transfer (TR-FRET) and a discontinuous assay that uses the label-free Epic platform. The TR-FRET assay employs HiLyte Fluor 647-labeled ApoA-I with N-terminal biotin bound to streptavidin-terbium. When fluorescent ApoA-I was incorporated into HDL, TR-FRET decreased proportionally to the increase in the ratio of lipids to ApoA-I, demonstrating that the assay was sensitive to the amount of lipid bound to ApoA-I. In the Epic assay, biotinylated ApoA-I was captured on a streptavidin-coated biosensor. Measured resonant wavelength shift was proportional to the amount of lipids associated with ApoA-I, indicating that the assay senses ApoA-I lipidation. © 2012 Society for Laboratory Automation and Screening.

Published

2012

5. Mutations in adenosine deaminase-like (ADAL) protein confer resistance to the antiproliferative agents N6-cyclopropyl-PMEDAP and GS-9219

Author

Christian R, Frey, Graciela, Andrei, Ivan, Votruba, Carina, Cannizzaro, Bin, Han, Wanchi, Fung, Magdeleine, Hung, Xiaohong, Liu, Romas, Geleziunas, Pierre, Fiten, Ghislain, Opdenakker, Robert, Snoeck, and Tomas, Cihlar

Subjects

Alanine, Sequence Homology, Amino Acid, Protein Conformation, Adenine, Blotting, Western, Molecular Sequence Data, Uterine Cervical Neoplasms, Antineoplastic Agents, Nucleoside Deaminases, Drug Resistance, Neoplasm, Purines, Mutation, Tumor Cells, Cultured, Humans, Female, Prodrugs, Amino Acid Sequence

Abstract

GS 9219 is a double prodrug of antiproliferative nucleotide analog 9-(2-Phosphonylmethoxyethyl)guanine (PMEG), with potent in vivo efficacy against various hematological malignancies. This study investigates the role of adenosine deaminase-like (ADAL) protein in the intracellular activation of GS-9219.A cell line resistant to 9-(2-Phosphonylmethoxyethyl)-N(6)-cyclopropyl-2,6-diaminopurine (cPrPMEDAP), an intermediate metabolite of GS-9219, was generated and characterized.The resistant cell line was cross-resistant to cPrPMEDAP and GS-9219, due to a defect in the deamination of cPrPMEDAP to PMEG. Mutations in the ADAL gene (H286R and S180N) were identified in the resistant cells that adversely-affected its enzymatic activity. Introduction of the wild-type ADAL gene re-sensitized resistant cells to both cPrPMEDAP and GS-9219.The ADAL protein plays an essential role in the intracellular activation of GS-9219 by catalyzing the deamination of cPrPMEDAP metabolite to PMEG. Mutations affecting the activity of ADAL confer resistance to both GS-9219 and its metabolite cPrPMEDAP.

Published

2013

6. The HCV non-nucleoside inhibitor Tegobuvir utilizes a novel mechanism of action to inhibit NS5B polymerase function

Author

Maisoun Sulfab, Weidong Zhong, Vivian Randall W, Steven S. Bondy, Wanchi Fung, Hengli Tang, Uli Schmitz, Christy M. Hebner, Johan Neyts, Michelle Nash, Trenkle James D, Magdeleine Hung, Xiaohong Liu, John O. Link, Roman Sakowicz, Yang Tian, Katherine M. Brendza, Kyla Bjornson, James G. Taylor, and Bin Han

Subjects

Gastroenterology and hepatology, viruses, Hepacivirus, Viral Nonstructural Proteins, Biochemistry, Mass Spectrometry, law.invention, chemistry.chemical_compound, law, Drug Discovery, Polymerase, chemistry.chemical_classification, Multidisciplinary, biology, Reverse Transcriptase Polymerase Chain Reaction, virus diseases, Transfection, Antivirals, Hepatitis C, Enzymes, Pyridazines, Infectious hepatitis, Recombinant DNA, Medicine, medicine.symptom, Research Article, Drugs and Devices, Drug Research and Development, Immunoprecipitation, Science, Blotting, Western, Antiviral Agents, Microbiology, Cell Line, Virology, medicine, Humans, Biology, NS5B, Liver diseases, DNA Primers, Enzyme Kinetics, Base Sequence, biochemical phenomena, metabolism, and nutrition, Molecular biology, Viral Replication, digestive system diseases, Enzyme, Mechanism of action, chemistry, Purines, biology.protein, Heterologous expression

Abstract

Tegobuvir (TGV) is a novel non-nucleoside inhibitor (NNI) of HCV RNA replication with demonstrated antiviral activity in patients with genotype 1 chronic HCV infection. The mechanism of action of TGV has not been clearly defined despite the identification of resistance mutations mapping to the NS5B polymerase region. TGV does not inhibit NS5B enzymatic activity in biochemical assays in vitro, suggesting a more complex antiviral mechanism with cellular components. Here, we demonstrate that TGV exerts anti-HCV activity utilizing a unique chemical activation and subsequent direct interaction with the NS5B protein. Treatment of HCV subgenomic replicon cells with TGV results in a modified form of NS5B with a distinctly altered mobility on a SDS-PAGE gel. Further analysis reveals that the aberrantly migrating NS5B species contains the inhibitor molecule. Formation of this complex does not require the presence of any other HCV proteins. The intensity of the aberrantly migrating NS5B species is strongly dependent on cellular glutathione levels as well as CYP 1A activity. Furthermore analysis of NS5B protein purified from a heterologous expression system treated with TGV by mass spectrometry suggests that TGV undergoes a CYP- mediated intracellular activation step and the resulting metabolite, after forming a glutathione conjugate, directly and specifically interacts with NS5B. Taken together, these data demonstrate that upon metabolic activation TGV is a specific, covalent inhibitor of the HCV NS5B polymerase and is mechanistically distinct from other classes of the non-nucleoside inhibitors (NNI) of the viral polymerase.

Published

2012