Your search keyword '"suramin"' showing total 1,316 results

1. Chronic nicotine, but not suramin or resveratrol, partially remediates the mania-like profile of dopamine transporter knockdown mice

Author

Kwiatkowski, Molly A, Roberts, Benjamin Z, van Enkhuizen, Jordy, Ji, Baohu, Zhou, Xianjin, and Young, Jared W

Subjects

Biological Psychology, Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Psychology, Brain Disorders, Neurosciences, Mental Health, Serious Mental Illness, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Mental health, Good Health and Well Being, Animals, Disease Models, Animal, Dopamine Plasma Membrane Transport Proteins, Exploratory Behavior, Female, Humans, Male, Mania, Mice, Mice, Inbred C57BL, Nicotine, Resveratrol, Suramin, Bipolar Disorder, Dopamine transporter, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry, Biological psychology

Abstract

Bipolar disorder (BD) is a severe mental illness affecting 2% of the global population. Current pharmacotherapies provide incomplete symptom remediation, highlighting the need for novel therapeutics. BD is characterized by fluctuations between mania and depression, likely driven by shifts between hyperdopaminergia and hypercholinergia, respectively. Hyperdopaminergia may result from insufficient activity of the dopamine transporter (DAT), the primary mediator of synaptic dopamine clearance. The DAT knockdown (DAT KD) mouse recreates this mechanism and exhibits a highly reproducible hyperexploratory profile in the cross-species translatable Behavioral Pattern Monitor (BPM) that is: (a) consistent with that observed in BD mania patients; and (b) partially normalized by chronic lithium and valproate treatment. The DAT KD/BPM model of mania therefore exhibits high levels of face-, construct-, and predictive-validity for the pre-clinical assessment of putative anti-mania drugs. Three different drug regimens - chronic nicotine (nicotinic acetylcholine receptor (nAChR) agonist; 40 mg/kg/d, 26 d), subchronic suramin (anti-purinergic; 20 mg/kg, 1 × /wk, 4 wks), and subchronic resveratrol (striatal DAT upregulator; 20 mg/kg/d, 4 d) - were administered to separate cohorts of male and female DAT KD- and wildtype (WT) littermate mice, and exploration was assessed in the BPM. Throughout, DAT KD mice exhibited robust hyperexploratory profiles relative to WTs. Nicotine partially normalized this behavior. Resveratrol modestly upregulated DAT expression but did not normalize DAT KD behavior. These results support the mania-like profile of DAT KD mice, which may be partially remediated by nAChR agonists via restoration of disrupted catecholaminergic/cholinergic equilibrium. Delineating the precise mechanism of action of nicotine could identify more selective therapeutic targets.

Published

2021

2. Structure of the Ebola virus polymerase complex

Author

Bin Yuan, Qi Peng, Jinlong Cheng, Min Wang, Jin Zhong, Jianxun Qi, George F. Gao, and Yi Shi

Subjects

Protein Subunits, Multidisciplinary, Catalytic Domain, Cryoelectron Microscopy, Humans, RNA, Viral, Viral Regulatory and Accessory Proteins, DNA-Directed RNA Polymerases, Suramin, Hemorrhagic Fever, Ebola, Ebolavirus, Virus Replication, Antiviral Agents

Abstract

Filoviruses, including Ebola virus, pose an increasing threat to the public health. Although two therapeutic monoclonal antibodies have been approved to treat the Ebola virus disease

Published

2022

3. Initiation and modulation of Tau protein phase separation by the drug suramin

Author

Prabhu Rajaiah Prince, Janine Hochmair, Hévila Brognaro, Susanna Gevorgyan, Maximilian Franck, Robin Schubert, Kristina Lorenzen, Selin Yazici, Eckhard Mandelkow, Susanne Wegmann, and Christian Betzel

Subjects

Multidisciplinary, Heparin, metabolism [RNA], Humans, RNA, tau Proteins, pharmacology [Suramin], Suramin, ddc:600, metabolism [tau Proteins], metabolism [Alzheimer Disease]

Abstract

Scientific reports 13(1), 3963 (2023). doi:10.1038/s41598-023-29846-9, Tau is an intrinsically disordered neuronal protein in the central nervous system. Aggregated Tau is the main component of neurofibrillary tangles observed in Alzheimer’s disease. In vitro, Tau aggregation can be triggered by polyanionic co-factors, like RNA or heparin. At different concentration ratios, the same polyanions can induce Tau condensates via liquid–liquid phase separation (LLPS), which over time develop pathological aggregation seeding potential. Data obtained by time resolved Dynamic Light Scattering experiments (trDLS), light and electron microscopy show that intermolecular electrostatic interactions between Tau and the negatively charged drug suramin induce Tau condensation and compete with the interactions driving and stabilizing the formation of Tau:heparin and Tau:RNA coacervates, thus, reducing their potential to induce cellular Tau aggregation. Tau:suramin condensates do not seed Tau aggregation in a HEK cell model for Tau aggregation, even after extended incubation. These observations indicate that electrostatically driven Tau condensation can occur without pathological aggregation when initiated by small anionic molecules. Our results provide a novel avenue for therapeutic intervention of aberrant Tau phase separation, utilizing small anionic compounds., Published by Macmillan Publishers Limited, part of Springer Nature, [London]

Published

2023

4. Targeted Redesign of Suramin Analogs for Novel Antimicrobial Lead Development

Author

Debayan Dey, Suryanarayanarao Ramakumar, and Graeme L. Conn

Subjects

Drug, Antiparasitic, medicine.drug_class, General Chemical Engineering, media_common.quotation_subject, Suramin, Computational biology, Library and Information Sciences, Antiviral Agents, DNA-binding protein, chemistry.chemical_compound, RNA polymerase, polycyclic compounds, medicine, Humans, Structure–activity relationship, Repurposing, media_common, Virtual screening, SARS-CoV-2, Chemistry, COVID-19, General Chemistry, Anti-Bacterial Agents, Computer Science Applications, Nucleic acid, RNA, Viral, medicine.drug

Abstract

The emergence of new viral infections and drug resistant bacteria urgently necessitates expedient therapeutic development. Repurposing and redesign of existing drugs against different targets is one potential way in which to accelerate this process. Suramin was initially developed as a successful anti-parasitic drug but has also shown promising antiviral and antibacterial activities. However, due to its high conformational flexibility and negative charge, suramin is considered quite promiscuous towards positively charged sites within nucleic acid binding proteins. Although some suramin analogs have been developed against specific targets, only limited structure activity relationship (SAR) studies were performed, and virtual screening has yet to be used to identify more specific inhibitor(s) based on its scaffold. Using available structures, we investigated suramin’s target diversity, confirming that suramin preferentially binds to protein pockets which are both positively charged and enriched in aromatic or leucine residues. Further, suramin’s high conformational flexibility allows adaptation to structurally diverse binding surfaces. From this platform, we developed a framework for structure- and docking-guided elaboration of suramin analog scaffolds using virtual screening of suramin and heparin analogs against a panel of diverse therapeutically relevant viral and bacterial protein targets. Use of this new framework to design potentially specific suramin analogs is exemplified using the SARS-CoV-2 RNA-dependent RNA polymerase (RdRp) and nucleocapsid protein, identifying leads that might inhibit a wide range of coronaviruses. The approach presented here establishes a computational framework for designing suramin analogs against different bacterial and viral targets and repurposing existing drugs for more specific inhibitory activity.For Table of Contents Use OnlyTable of Contents Graphic

Published

2021

5. Effects of Stromal Cell Conditioned Medium and Antipurinergic Treatment on Macrophage Phenotype

Author

Ahmad S. Arabiyat, Daniel J. Yeisley, Viviana R. Güiza-Argüello, Fatir Qureshi, Robert A. Culibrk, Juergen Hahn, and Mariah S. Hahn

Subjects

Adenosine Triphosphate, Culture Media, Conditioned, Macrophages, Biomedical Engineering, Medicine (miscellaneous), Humans, Cytokines, Bioengineering, Mesenchymal Stem Cells, Suramin

Abstract

The immunomodulatory capacity of the human mesenchymal stromal cell (MSC) secretome has been a critical driver for the development of cell-free MSC products, such as conditioned medium (CM), for regenerative medicine applications. This is particularly true as cell-free MSC products present several advantages over direct autologous or allogeneic MSC delivery with respect to safety, manufacturability, and defined potency. Recently, significant effort has been placed into creating novel MSC CM formulations with an immunomodulatory capacity tailored for specific regenerative contexts. For instance, the immunoregulatory nature of MSC CM has previously been tuned through a number of cytokine-priming strategies. Herein, we propose an alternate method to tailor the immunomodulatory "phenotype" of cytokine-primed MSC CM through coupling with the pharmacological agent, suramin. Suramin interferes with the signaling of purines including extracellular adenosine triphosphate (ATP), which plays a critical role in the activation of the innate immune system after injury. Toward this end, human THP-1-derived macrophages were activated to a proinflammatory phenotype and treated with (1) unprimed/native MSC CM, (2) interferon-γ/tumor necrosis factor α-primed MSC CM (primed CM), (3) suramin alone, or (4) primed MSC CM and suramin (primed CM/suramin). Markers of key macrophage functions-cytokine secretion, autophagy, oxidative stress modulation, and activation/migration-were assessed. Consistent with previous literature, primed CM elevated macrophage secretion of several proinflammatory and pleiotropic cytokines relative to native CM; whereas addition of suramin imparted consistent shifts in terms of TNFα (↓), interleukin-10 (↓), and hepatocyte growth factor (↑) irrespective of CM. In addition, both primed CM and suramin, individually and combined, increased reactive oxygen species production relative to native CM, and addition of suramin to primed CM shifted levels of CX3CL1, a factor involved in ATP-associated macrophage regulation. Varimax rotation assessment of the secreted cytokine profiles confirmed that primed CM/suramin resulted in a THP-1 phenotypic shift away from the lipopolysaccharide-activated proinflammatory state that was distinct from that of primed CM or native CM alone. This altered primed CM/suramin-associated phenotype may prove beneficial for healing in certain regenerative contexts. These results may inform future work coupling antipurinergic treatments with MSC-derived therapies in regenerative medicine applications.

Published

2022

6. Profiles of urine and blood metabolomics in autism spectrum disorders

Author

Orawan Louthrenoo, Nipon Chattipakorn, Intawat Nookaew, Chanisa Thonusin, Narueporn Likhitweerawong, Nonglak Boonchooduang, and Siriporn C. Chattipakorn

Subjects

medicine.medical_specialty, Neurology, genetic structures, Autism Spectrum Disorder, Suramin, Urine, Bioinformatics, behavioral disciplines and activities, Biochemistry, Article, Cellular and Molecular Neuroscience, Metabolomics, Isothiocyanates, mental disorders, medicine, Metabolome, Animals, Humans, business.industry, Targeted interventions, medicine.disease, Autism spectrum disorder, Sulfoxides, Potential biomarkers, Autism, Neurology (clinical), business, Biomarkers, Metabolic Networks and Pathways

Abstract

Early diagnosis and treatment for autism spectrum disorder (ASD) pose challenges. The current diagnostic approach for ASD is mainly clinical assessment of patient behaviors. Biomarkers-based identification of ASD would be useful for pediatricians. Currently, there is no specific treatment for ASD, and evidence for the efficacy of alternative treatments remains inconclusive. The prevalence of ASD is increasing, and it is becoming more urgent to find the pathogenesis of such disorder. Metabolomic studies have been used to deeply investigate the alteration of metabolic pathways, including those associated with ASD. Metabolomics is a promising tool for identifying potential biomarkers and possible pathogenesis of ASD. This review comprehensively summarizes and discusses the abnormal metabolic pathways in ASD children, as indicated by evidence from metabolomic studies in urine and blood. In addition, the targeted interventions that could correct the metabolomic profiles relating to the improvement of autistic behaviors in affected animals and humans have been included. The results revealed that the possible underlying pathophysiology of ASD were alterations of amino acids, reactive oxidative stress, neurotransmitters, and microbiota-gut-brain axis. The potential common pathways shared by animal and human studies related to the improvement of ASD symptoms after pharmacological interventions were mammalian-microbial co-metabolite, purine metabolism, and fatty acid oxidation. The content of this review may contribute to novel biomarkers for the early diagnosis of ASD and possible therapeutic paradigms.

Published

2021

7. Small-Molecule Inhibitors of the Coronavirus Spike: ACE2 Protein–Protein Interaction as Blockers of Viral Attachment and Entry for SARS-CoV-2

Author

Oscar Alcazar, Peter Buchwald, Sung Ting Chuang, Jose Manuel Condor Capcha, Lina A. Shehadeh, Damir Bojadzic, and Jinshui Chen

Subjects

0301 basic medicine, protein−protein interaction, Suramin, 030106 microbiology, coronavirus, Virus Attachment, ACE2, Pharmacology, spike protein, medicine.disease_cause, Article, Protein–protein interaction, 03 medical and health sciences, chemistry.chemical_compound, Chloroquine, medicine, Humans, Protein Interaction Domains and Motifs, Pandemics, IC50, Coronavirus, biology, SARS-CoV-2, COVID-19, antiviral, Small molecule, Congo red, 030104 developmental biology, Infectious Diseases, chemistry, Spike Glycoprotein, Coronavirus, biology.protein, Angiotensin-Converting Enzyme 2, Antibody, medicine.drug

Abstract

Inhibitors of the protein–protein interaction (PPI) between the SARS-CoV-2 spike protein and human ACE2 (hACE2), which acts as a ligand–receptor pair that initiates the viral attachment and cellular entry of this coronavirus causing the ongoing COVID-19 pandemic, are of considerable interest as potential antiviral agents. While blockade of such PPIs with small molecules is more challenging than that with antibodies, small-molecule inhibitors (SMIs) might offer alternatives that are less strain- and mutation-sensitive, suitable for oral or inhaled administration, and more controllable/less immunogenic. Here, we report the identification of SMIs of this PPI by screening our compound library focused around the chemical space of organic dyes. Among promising candidates identified, several dyes (Congo red, direct violet 1, Evans blue) and novel druglike compounds (DRI-C23041, DRI-C91005) inhibited the interaction of hACE2 with the spike proteins of SARS-CoV-2 as well as SARS-CoV with low micromolar activity in our cell-free ELISA-type assays (IC50’s of 0.2–3.0 μM), whereas control compounds, such as sunset yellow FCF, chloroquine, and suramin, showed no activity. Protein thermal shift assays indicated that the SMIs of interest identified here bind SARS-CoV-2-S and not hACE2. While dyes seemed to be promiscuous inhibitors, DRI-C23041 showed some selectivity and inhibited the entry of two different SARS-CoV-2-S expressing pseudoviruses into hACE2-expressing cells in a concentration-dependent manner with low micromolar IC50’s (6–7 μM). This provides proof-of-principle evidence for the feasibility of small-molecule inhibition of PPIs critical for SARS-CoV-2 attachment/entry and serves as a first guide in the search for SMI-based alternative antiviral therapies for the prevention and treatment of diseases caused by coronaviruses in general and COVID-19 in particular.

Published

2021

8. Physiological and proteomic profiles of Trypanosoma brucei rhodesiense parasite isolated from suramin responsive and non-responsive HAT patients in Busoga, Uganda

Author

James M. Njunge, Martin K. Rono, Bartholomew N. Ondigo, Catherine N. Mutuku, Erick O. Awuoche, Kariuki Ndung’u, Paul O. Mireji, Vincent O. Adung'a, Modesta O. Akoth, Rosemary Bateta, and Clarence M. Mang’era

Subjects

Male, Proteomics, Trypanosoma brucei rhodesiense, 0301 basic medicine, Regular article, Suramin, Trypanosoma brucei brucei, 030231 tropical medicine, Drug resistance, Infectious and parasitic diseases, RC109-216, Biology, Microbiology, Mice, 03 medical and health sciences, 0302 clinical medicine, In vivo, parasitic diseases, medicine, polycyclic compounds, Animals, Humans, Parasite hosting, Parasites, Uganda, Pharmacology (medical), African trypanosomiasis, Pharmacology, chemistry.chemical_classification, medicine.disease, Phenotype, Drug sensitive, Trypanosoma brucei rhodesience, Trypanosomiasis, African, 030104 developmental biology, Infectious Diseases, Enzyme, chemistry, Parasitology, medicine.drug

Abstract

Human African Trypanosomiasis (HAT) is a disease of major economic importance in Sub-Saharan Africa. The HAT is caused by Trypanosoma brucei rhodesiense (Tbr) parasite in eastern and southern Africa, with suramin as drug of choice for treatment of early stage of the disease. Suramin treatment failures has been observed among HAT patients in Tbr foci in Uganda. In this study, we assessed Tbr parasite strains isolated from HAT patients responsive (Tbr EATRO-232) and non-responsive (Tbr EATRO-734) to suramin treatment in Busoga, Uganda for 1) putative role of suramin resistance in the treatment failure 2) correlation of suramin resistance with Tbr pathogenicity and 3) proteomic pathways underpinning the potential suramin resistance phenotype in vivo. We first assessed suramin response in each isolate by infecting male Swiss white mice followed by treatment using a series of suramin doses. We then assessed relative pathogenicity of the two Tbr isolates by assessing changes pathogenicity indices (prepatent period, survival and mortality). We finally isolated proteins from mice infected by the isolates, and assessed their proteomic profiles using mass spectrometry. We established putative resistance to 2.5 mg/kg suramin in the parasite Tbr EATRO-734. We established that Tbr EATRO-734 proliferated slower and has significantly enriched pathways associated with detoxification and metabolism of energy and drugs relative to Tbr EATRO-232. The Tbr EATRO-734 also has more abundantly expressed mitochondrion proteins and enzymes than Tbr EATRO-232. The suramin treatment failure may be linked to the relatively higher resistance to suramin in Tbr EATRO-734 than Tbr EATRO-232, among other host and parasite specific factors. However, the Tbr EATRO-734 appears to be less pathogenic than Tbr EATRO-232, as evidenced by its lower rate of parasitaemia. The Tbr EATRO-734 putatively surmount suramin challenges through induction of energy metabolism pathways. These cellular and molecular processes may be involved in suramin resistance in Tbr., Graphical abstract Image 1, Highlights • Tbr EATRO-734 and Tbr EATRO-232 are resistant and susceptible to suramin respectively. • Tbr EATRO-734 highly expressed mitochondrion proteins/enzymes than Tbr EATRO-232. • Tbr EATRO-734 surmounts suramin challenges by induction of energy metabolism. • VSG proteins that may confer suramin resistance were identified in Tbr EATRO-734. • Proteins involved in trypanosome sensitive to suramin were induced in Tbr EATRO-232.

Published

2021

9. Chronic nicotine, but not suramin or resveratrol, partially remediates the mania-like profile of dopamine transporter knockdown mice

Author

Xianjin Zhou, Jared W. Young, Baohu Ji, Jordy van Enkhuizen, Benjamin Z Roberts, and Molly A. Kwiatkowski

Subjects

Male, Agonist, Nicotine, medicine.drug_class, Suramin, Pharmacology, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, Dopamine, mental disorders, Animals, Humans, Medicine, Pharmacology (medical), Biological Psychiatry, Dopamine transporter, Dopamine Plasma Membrane Transport Proteins, biology, business.industry, 030227 psychiatry, Mice, Inbred C57BL, Disease Models, Animal, Mania, Psychiatry and Mental health, Nicotinic acetylcholine receptor, nervous system, Neurology, Mechanism of action, Resveratrol, Exploratory Behavior, biology.protein, Cholinergic, Female, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery, medicine.drug

Abstract

Bipolar disorder (BD) is a severe mental illness affecting 2% of the global population. Current pharmacotherapies provide incomplete symptom remediation, highlighting the need for novel therapeutics. BD is characterized by fluctuations between mania and depression, likely driven by shifts between hyperdopaminergia and hypercholinergia, respectively. Hyperdopaminergia may result from insufficient activity of the dopamine transporter (DAT), the primary mediator of synaptic dopamine clearance. The DAT knockdown (DAT KD) mouse recreates this mechanism and exhibits a highly reproducible hyperexploratory profile in the cross-species translatable Behavioral Pattern Monitor (BPM) that is: (a) consistent with that observed in BD mania patients; and (b) partially normalized by chronic lithium and valproate treatment. The DAT KD/BPM model of mania therefore exhibits high levels of face-, construct-, and predictive-validity for the pre-clinical assessment of putative anti-mania drugs. Three different drug regimens – chronic nicotine (nicotinic acetylcholine receptor (nAChR) agonist; 40 mg/kg/d, 26 d), subchronic suramin (anti-purinergic; 20 mg/kg, 1 × /wk, 4 wks), and subchronic resveratrol (striatal DAT upregulator; 20 mg/kg/d, 4 d) – were administered to separate cohorts of male and female DAT KD- and wildtype (WT) littermate mice, and exploration was assessed in the BPM. Throughout, DAT KD mice exhibited robust hyperexploratory profiles relative to WTs. Nicotine partially normalized this behavior. Resveratrol modestly upregulated DAT expression but did not normalize DAT KD behavior. These results support the mania-like profile of DAT KD mice, which may be partially remediated by nAChR agonists via restoration of disrupted catecholaminergic/cholinergic equilibrium. Delineating the precise mechanism of action of nicotine could identify more selective therapeutic targets.

Published

2021

10. Effect and underlying mechanisms of airborne particulate matter 2.5 (PM2.5) on cultured human corneal epithelial cells

Author

Kenji Kashiwagi and Yoko Iizuka

Subjects

0301 basic medicine, China, Cell Survival, Corneal diseases, Suramin, lcsh:Medicine, 010501 environmental sciences, Granulocyte, 01 natural sciences, complex mixtures, Article, Cell Line, Proinflammatory cytokine, Cornea, Pathogenesis, 03 medical and health sciences, Autophagy, medicine, Humans, Macrophage, lcsh:Science, 0105 earth and related environmental sciences, Air Pollutants, Multidisciplinary, Interleukin-6, Tumor Necrosis Factor-alpha, Chemistry, Interleukin-8, lcsh:R, Granulocyte-Macrophage Colony-Stimulating Factor, Epithelial Cells, In vitro, eye diseases, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Cell culture, Environmental chemistry, Interleukin-2, Particulate Matter, lcsh:Q, sense organs, medicine.drug

Abstract

Health problems caused by airborne particulate matter with a diameter less than 2.5 (PM2.5), especially in the respiratory system, have become a worldwide problem, but the influence and mechanisms of PM2.5 on the ocular surface have not been sufficiently elucidated. We investigated in vitro the onset and pathogenesis of corneal damage induced by PM2.5. Two types of PM2.5 samples originating from Beijing (designated #28) and the Gobi Desert (designated #30) were added to the culture medium of immortalized cultured human corneal epithelial cells (HCECs) to examine the effects on survival rates, autophagy, and proinflammatory cytokine production. Both types of PM2.5 significantly reduced the HCEC survival rate in a concentration-dependent manner by triggering autophagy. In particular, compared with #30, #28 induced much more severe damage in HCECs. Physical contact between PM2.5 and HCECs was not a primary contributor to PM2.5-induced HCEC damage. Among the 38 proinflammatory cytokines examined in this study, significant increases in the granulocyte macrophage colony-stimulating factor (GM-CSF) and interleukin-6 levels and a significant reduction in the interleukin-8 level were detected in culture medium of PM2.5-exposed HCECs. Simultaneous addition of a GM-CSF inhibitor, suramin, alleviated the HCEC impairment induced by PM2.5. In conclusion, PM2.5 induces HCEC death by triggering autophagy. Some cytokines that are released from HCECs, including GM-CSF, may be involved in HCEC damage caused by PM2.5 exposure.

Published

2020

11. Identification of HMGA2 inhibitors by AlphaScreen-based ultra-high-throughput screening assays

Author

Stefan Vasile, Fenfei Leng, Sabrina Battista, Juliano Freitas, Jeremy W. Chambers, Alyssa Garabedian, Federica D'Alessio, Miriam Romano, Prem P. Chapagain, Linjia Su, Francisco Fernandez-Lima, Alfredo Fusco, Layton H. Smith, Nadezda Bryan, Fabiana Falanga, and Lidia Kos

Subjects

Antiparasitic, medicine.drug_class, Carcinogenesis, Suramin, Amino Acid Motifs, Biophysics, lcsh:Medicine, Biochemistry, Article, HMGA2, High-Throughput Screening Assays, parasitic diseases, medicine, Humans, HMGA1a Protein, lcsh:Science, Cancer, Multidisciplinary, Adipogenesis, Binding Sites, biology, Base Sequence, Chemistry, Drug discovery, HMGA2 Protein, Biological techniques, lcsh:R, Suramin binding, DNA, HMGA1, Chemical biology, DNA-Binding Proteins, High-mobility group, biology.protein, lcsh:Q, medicine.drug, Biotechnology

Abstract

The mammalian high mobility group protein AT-hook 2 (HMGA2) is a multi-functional DNA-binding protein that plays important roles in tumorigenesis and adipogenesis. Previous results showed that HMGA2 is a potential therapeutic target of anticancer and anti-obesity drugs by inhibiting its DNA-binding activities. Here we report the development of a miniaturized, automated AlphaScreen ultra-high-throughput screening assay to identify inhibitors targeting HMGA2-DNA interactions. After screening the LOPAC1280 compound library, we identified several compounds that strongly inhibit HMGA2-DNA interactions including suramin, a century-old, negatively charged antiparasitic drug. Our results show that the inhibition is likely through suramin binding to the “AT-hook” DNA-binding motifs and therefore preventing HMGA2 from binding to the minor groove of AT-rich DNA sequences. Since HMGA1 proteins also carry multiple “AT-hook” DNA-binding motifs, suramin is expected to inhibit HMGA1-DNA interactions as well. Biochemical and biophysical studies show that charge-charge interactions and hydrogen bonding between the suramin sulfonated groups and Arg/Lys residues play critical roles in the binding of suramin to the “AT-hook” DNA-binding motifs. Furthermore, our results suggest that HMGA2 may be one of suramin’s cellular targets.

Published

2020

12. Highly Potent and Selective Ectonucleoside Triphosphate Diphosphohydrolase (ENTPDase1, 2, 3 and 8) Inhibitors Having 2-substituted-7- trifluoromethyl-thiadiazolopyrimidones Scaffold

Author

Jean Sévigny, Sumera Zaib, Saira Afzal, Peter Langer, Behzad Jafari, Jamshed Iqbal, and Joanna Lecka

Subjects

Adenosine Triphosphatases, chemistry.chemical_classification, Molecular Structure, Chemistry, Suramin, Apyrase, Pyrimidinones, Isozyme, Isoenzymes, Molecular Docking Simulation, Structure-Activity Relationship, Enzyme, Biochemistry, Docking (molecular), Thiadiazoles, Drug Discovery, Extracellular, medicine, Humans, Nucleotide, Enzyme Inhibitors, Nucleoside, IC50, medicine.drug

Abstract

Background: The ecto-nucleoside triphosphate diphosphohydrolases (NTPDases) terminate nucleotide signaling via the hydrolysis of extracellular nucleoside-5'-triphosphate and nucleoside- 5'-diphosphate, to nucleoside-5'-monophosphate and composed of eight Ca2+/Mg2+ dependent ectonucleotidases (NTPDase1-8). Extracellular nucleotides are involved in a variety of physiological mechanisms. However, they are rapidly inactivated by ectonucleotidases that are involved in the sequential removal of phosphate group from nucleotides with the release of inorganic phosphate and their respective nucleoside. Ectonucleoside triphosphate diphosphohydrolases (NTPDases) represent the key enzymes responsible for nucleotides hydrolysis and their overexpression has been related to certain pathological conditions. Therefore, the inhibitors of NTPDases are of particular importance in order to investigate their potential to treat various diseases e.g., cancer, ischemia and other disorders of the cardiovascular and immune system. Methods: Keeping in view the importance of NTPDase inhibitors, a series of thiadiazolopyrimidones were evaluated for their potential inhibitory activity towards NTPDases by the malachite green assay. Results: The results suggested that some of the compounds were found as non-selective inhibitors of isozyme of NTPDases, however, most of the compounds act as potent and selective inhibitors. In case of substituted amino derivatives (4c-m), the compounds 4m (IC50 = 1.13 ± 0.09 μM) and 4g (IC50 = 1.72 ± 0.08 μM) were found to be the most potent inhibitors of h-NTPDase1 and 2, respectively. Whereas, compound 4d showed the best inhibitory potential for both h-NTPDase3 (IC50 = 1.25 ± 0.06 μM) and h-NTPDase8 (0.21 ± 0.02 μM). Among 5a-t derivatives, compounds 5e (IC50 = 2.52 ± 0.15 μM), 5p (IC50 = 3.17 ± 0.05 μM), 5n (IC50 = 1.22 ± 0.06 μM) and 5b (IC50 = 0.35 ± 0.001 μM) were found to be the most potent inhibitors of h-NTPDase1, 2, 3 and 8, respectively. Interestingly, the inhibitory concentration values of above-mentioned inhibitors were several folds greater than suramin, a reference control. In order to determine the binding interactions, molecular docking studies of the most potent inhibitors were conducted into the homology models of NTPDases and the putative binding analysis further confirmed that selective and potent compounds bind deep inside the active pocket of the respective enzymes. Conclusions: The docking analysis proposed that the inhibitory activity correlates with the hydrogen bonds inside the binding pocket. Thus, these derivatives are of interest and may further be investigated for their importance in medicinal chemistry.

Published

2020

13. Silent Mating–Type Information Regulation 2 Homolog 1 Attenuates the Neurotoxicity Associated with Alzheimer Disease via a Mechanism Which May Involve Regulation of Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-α

Author

Jie Xiang, Yang-Ting Dong, Ling Shan, Kun Cao, and Zhi-Zhong Guan

Subjects

Male, 0301 basic medicine, Suramin, Peroxisome proliferator-activated receptor, Mitochondrion, Neuroprotection, Pathology and Forensic Medicine, Mice, 03 medical and health sciences, 0302 clinical medicine, Sirtuin 1, Alzheimer Disease, Coactivator, medicine, Animals, Humans, Receptor, Aged, Aged, 80 and over, chemistry.chemical_classification, Neurotoxicity, Brain, medicine.disease, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, Rats, Cell biology, 030104 developmental biology, chemistry, Apoptosis, Female, 030217 neurology & neurosurgery, medicine.drug

Abstract

To investigate the neuroprotective role of silent mating-type information regulation 2 homolog 1 (SIRT1) in Alzheimer disease (AD), brain tissues from patients with AD and APP/PS1 mice as well as primary rat neurons exposed to oligomers of amyloid-β peptide were examined. The animals were treated with resveratrol (RSV) or suramin for 2 months. Cell cultures were treated with RSV, suramin, and the peroxisome proliferator-activated receptor gamma coactivator 1-α (PGC-1α) stimulator ZLN005. Cells were transiently transfected with PGC-1α silencing RNA. The level of SIRT1 in brain tissues from patients with AD and APP/PS1 mice, including nuclear and mitochondrial proteins, as well as in primary neurons exposed to oligomers of amyloid-β peptide, was decreased. Overexpression of APP/PS1 impaired learning and memory of mice; produced more senile plaques, disrupted membranes, and resulted in broken or absent cristae of mitochondria in the brain; decreased levels of A disintegrin and metallopeptidase domain 10, beta-secretase 2, 8-oxoguanine DNA glycosylase-1, PGC-1α, and NAD+; and increased levels of beta-secretase 1 and apoptosis. Interestingly, these changes were attenuated significantly by RSV treatment but enhanced by suramin administration. By activating PGC-1α but inhibiting SIRT1, apoptotic cell death was significantly decreased; however, by activating SIRT1 but inhibiting PGC-1α with small interfering PGC-1α, these levels remained unchanged. These findings indicate that SIRT1 may protect against AD-associated neurotoxicity, which might involve PGC-1α regulation.

Published

2020

14. Suramin and NF449 are IP5K inhibitors that disrupt inositol hexakisphosphate–mediated regulation of cullin–RING ligase and sensitize cancer cells to MLN4924/pevonedistat

Author

Sining He, Xiaozhe Zhang, Xiuyan Yang, Jian Zhang, Jing Wu, Yang Su, Xiaoli Yang, Feng Rao, and Shaodong Shi

Subjects

0301 basic medicine, Phytic Acid, Suramin, Cyclopentanes, Protein degradation, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, Neoplasms, medicine, Humans, Inositol, Enzyme Inhibitors, COP9 signalosome, Inositol phosphate, Molecular Biology, chemistry.chemical_classification, DNA ligase, 030102 biochemistry & molecular biology, biology, Benzenesulfonates, Cell Biology, Cullin Proteins, HCT116 Cells, Neoplasm Proteins, Cell biology, Ubiquitin ligase, Phosphotransferases (Alcohol Group Acceptor), HEK293 Cells, Pyrimidines, 030104 developmental biology, chemistry, Enzymology, biology.protein, Neddylation, medicine.drug

Abstract

Inositol hexakisphosphate (IP(6)) is an abundant metabolite synthesized from inositol 1,3,4,5,6-pentakisphosphate (IP(5)) by the single IP(5) 2-kinase (IP5K). Genetic and biochemical studies have shown that IP(6) usually functions as a structural cofactor in protein(s) mediating mRNA export, DNA repair, necroptosis, 3D genome organization, HIV infection, and cullin–RING ligase (CRL) deneddylation. However, it remains unknown whether pharmacological perturbation of cellular IP(6) levels affects any of these processes. Here, we performed screening for small molecules that regulate human IP5K activity, revealing that the antiparasitic drug and polysulfonic compound suramin efficiently inhibits IP5K in vitro and in vivo. The results from docking experiments and biochemical validations suggested that the suramin targets IP5K in a distinct bidentate manner by concurrently binding to the ATP- and IP(5)-binding pockets, thereby inhibiting both IP(5) phosphorylation and ATP hydrolysis. NF449, a suramin analog with additional sulfonate moieties, more potently inhibited IP5K. Both suramin and NF449 disrupted IP(6)-dependent sequestration of CRL by the deneddylase COP9 signalosome, thereby affecting CRL activity cycle and component dynamics in an IP5K-dependent manner. Finally, nontoxic doses of suramin, NF449, or NF110 exacerbate the loss of cell viability elicited by the neddylation inhibitor and clinical trial drug MLN4924/pevonedistat, suggesting synergistic ef-fects. Suramin and its analogs provide structural templates for designing potent and specific IP5K inhibitors, which could be used in combination therapy along with MLN4924/pevonedistat. IP5K is a potential mechanistic target of suramin, accounting for suramin's therapeutic effects.

Published

2020

15. The neuroprotective effects of SIRT1 in mice carrying the APP/PS1 double-transgenic mutation and in SH-SY5Y cells over-expressing human APP670/671 may involve elevated levels of α7 nicotinic acetylcholine receptors

Author

Zhi-Zhong Guan, Yang-Ting Dong, Yi Li, Xiao-Lan Qi, Hui Song, Jie Xiang, Yi Xu, Wen-Feng Yu, and Kun Cao

Subjects

MAPK/ERK pathway, Aging, SH-SY5Y, alpha7 Nicotinic Acetylcholine Receptor, MAP Kinase Signaling System, Suramin, Spatial Learning, Hippocampus, Morris water navigation task, Gene Expression, Mice, Transgenic, Biology, Pharmacology, Neuroprotection, chemistry.chemical_compound, Amyloid beta-Protein Precursor, Mice, SIRT1, Sirtuin 1, Memory, Cell Line, Tumor, medicine, APP/PS1 mice, Animals, Humans, Methyllycaconitine, Neurons, Cell Biology, MAPK, α7 nAChR, medicine.anatomical_structure, chemistry, Cerebral cortex, Mutation, RNA Interference, Alzheimer’s disease, Biomarkers, medicine.drug, Research Paper

Abstract

Background: Both the silent information regulator-1 (SIRT1) and α7 nicotinic acetylcholine receptors (α7 nAChR) play important roles in the pathogenesis of Alzheimer's disease (AD), but interactions between these two remain largely unknown. Our present aim was to determine whether the neuroprotective effect of SIRT1, due to inhibition of aggregation of the β-amyloid peptide (Aβ), involves activation of α7 nAChR. Methods: In present study, four-month-old mice carrying the APP/PS1 mutation were administered resveratrol (RSV, a stimulator of SIRT1) or suramin (an inhibitor) once daily for two months, following which their spatial learning and memory were assessed using the Morris water maze test. Deposits of Aβ in vivo were detected by near-infrared imaging (NIRI) and confocal laser scanning. SH-SY5Y cells over-expressing human APP670/671 (SH-SY5Y/APPSWE cells) were treated with RSV, suramin, U0126 (an inhibitor of the MAPK/ERK1/2 pathway) or methyllycaconitine (MLA, an inhibitor of α7 nAChR), as well as transiently transfected with SIRT1 silencing RNA. Levels of proteins and mRNA were determined by Western blotting and qRT-PCR, respectively. Findings: The results show that the learning and memory of mice carrying the APP/PS1 mutation had declined by 6 months of age and the levels of SIRT1 and α7 nAChR in their hippocampus and cortex were lowered. Activation of SIRT1 improved their spatial learning and memory and reduced the production and aggregation of Aβ in the hippocampus and cerebral cortex; whereas inhibition of SIRT1 had the opposite effects. In addition, activation of SIRT1 increased the levels of both α7 nAChR and αAPP in the brains these animals. Finally, activation of SIRT1 elevated the levels of phosphor-ERK1/2, while inhibition of ERK1/2 counteracted the increase in α7 nAChR caused by RSV. Interpretation: These findings indicate that neuroprotection by SIRT1 may involve increasing levels of α7 nAChR through activation of the MAPK/ERK1/2 signaling pathway. Funding Statement: This work was financed by grants from the Natural Science Foundation of China (U1812403), and the Foundation of Guizhou Province of China (2014-06, 2014-6008, 2016-4001). Declaration of Interests: The authors declare that they have no competing interests. Ethical Approval Statement: All animal experimental procedures were performed in accordance with the guidelines of the Animal Ethical and Experimental Committee of Guizhou Medical University.

Published

2020

16. P2R Inhibitors Prevent Antibody-Mediated Complement Activation in an Animal Model of Neuromyelitis Optica: P2R Inhibitors Prevent Autoantibody Injury

Author

Sudhakar Reddy Kalluri, Rajneesh Srivastava, Selin Kenet, Goutam K. Tanti, Klaus Dornmair, Jeffrey L. Bennett, Thomas Misgeld, Bernhard Hemmer, Matthias T. Wyss, and Marina Herwerth

Subjects

Suramin, Purinergic receptor blockers, Mice, pharmacology [Immunoglobulin G], Animals, Humans, Pharmacology (medical), ddc:610, Two-photon imaging, drug therapy [Neuromyelitis Optica], Complement Activation, Autoantibodies, Pharmacology, Aquaporin 4, metabolism [Antigens, Surface], metabolism [Astrocytes], pharmacology [Antigens, Surface], Neuromyelitis optica, Disease Models, Animal, Immunoglobulin G, Astrocytes, Antigens, Surface, metabolism [Autoantibodies], Neurology (clinical), Aquaporin-4

Abstract

Purinergic 2 receptors (P2Rs) contribute to disease-related immune cell signaling and are upregulated in various pathological settings, including neuroinflammation. P2R inhibitors have been used to treat inflammatory diseases and can protect against complement-mediated cell injury. However, the mechanisms behind these anti-inflammatory properties of P2R inhibitors are not well understood, and their potential in CNS autoimmunity is underexplored. Here, we tested the effects of P2R inhibitors on glial toxicity in a mouse model of neuromyelitis optica spectrum disorder (NMOSD). NMOSD is a destructive CNS autoimmune disorder, in which autoantibodies against astrocytic surface antigen Aquaporin 4 (AQP4) mediate complement-dependent loss of astrocytes. Using two-photon microscopy in vivo, we found that various classes of P2R inhibitors prevented AQP4-IgG/complement-dependent astrocyte death. In vitro, these drugs inhibited the binding of AQP4-IgG or MOG-IgG to their antigen in a dose-dependent manner. Size-exclusion chromatography and circular dichroism spectroscopy revealed a partial unfolding of antibodies in the presence of various P2R inhibitors, suggesting a shared interference with IgG antibodies leading to their conformational change. Our study demonstrates that P2R inhibitors can disrupt complement activation by direct interaction with IgG. This mechanism is likely to influence the role of P2R inhibitors in autoimmune disease models and their therapeutic impact in human disease., Neurotherapeutics, 19 (5), ISSN:1878-7479, ISSN:1933-7213

Published

2022

17. Activation of retinal glial (Müller) cells by extracellular ATP induces pronounced increases in extracellular H+ flux

Author

Michael Gongwer, Robert Paul Malchow, Boriana K. Tchernookova, Matthew A. Kreitzer, Jason Jacoby, David Swygart, Lexi Shepherd, Ryan Kaufman, Marin Young, Hannah Caringal, and Chad Heer

Subjects

0301 basic medicine, Photoreceptors, P2Y receptor, Caudata, Sensory Receptors, lcsh:Medicine, Social Sciences, 4,4'-Diisothiocyanostilbene-2,2'-Disulfonic Acid, Ambystoma, Biochemistry, chemistry.chemical_compound, 0302 clinical medicine, Adenosine Triphosphate, Cell Signaling, Animal Cells, Medicine and Health Sciences, Psychology, Skates, Fish, lcsh:Science, Uncategorized, Neurons, Multidisciplinary, Physics, Lampreys, Eukaryota, Neurochemistry, Neurotransmitters, Hydrogen-Ion Concentration, Adenosine Diphosphate, Chemistry, Pyridoxal Phosphate, Receptors, Purinergic P2Y, Physical Sciences, Vertebrates, Engineering and Technology, Sensory Perception, Signal transduction, Anatomy, Cellular Types, Glutamate, Protons, Intracellular, Signal Transduction, Research Article, Thapsigargin, Ocular Anatomy, Ependymoglial Cells, Suramin, In Vitro Techniques, Retina, Amphibians, 03 medical and health sciences, Ocular System, Extracellular, Animals, Humans, PPADS, Calcium Signaling, Salamanders, Electrodes, Ion transporter, Nuclear Physics, Nucleons, Ion Transport, lcsh:R, Chemical Compounds, Organisms, Bicarbonate transport, Biology and Life Sciences, Afferent Neurons, Extracellular Fluid, Cell Biology, Macaca mulatta, Rats, Ictaluridae, Macaca fascicularis, Bicarbonates, 030104 developmental biology, chemistry, Cellular Neuroscience, Biophysics, lcsh:Q, sense organs, Electronics, Microelectrodes, 030217 neurology & neurosurgery, Neuroscience

Abstract

Small alterations in extracellular acidity are potentially important modulators of neuronal signaling within the vertebrate retina. Here we report a novel extracellular acidification mechanism mediated by glial cells in the retina. Using self-referencing H+-selective microelectrodes to measure extracellular H+ fluxes, we show that activation of retinal Müller (glial) cells of the tiger salamander by micromolar concentrations of extracellular ATP induces a pronounced extracellular H+ flux independent of bicarbonate transport. ADP, UTP and the non-hydrolyzable analog ATPγs at micromolar concentrations were also potent stimulators of extracellular H+ fluxes, but adenosine was not. The extracellular H+ fluxes induced by ATP were mimicked by the P2Y1 agonist MRS 2365 and were significantly reduced by the P2 receptor blockers suramin and PPADS, suggesting activation of P2Y receptors. Bath-applied ATP induced an intracellular rise in calcium in Müller cells; both the calcium rise and the extracellular H+ fluxes were significantly attenuated when calcium re-loading into the endoplasmic reticulum was inhibited by thapsigargin and when the PLC-IP3 signaling pathway was disrupted with 2-APB and U73122. The anion transport inhibitor DIDS also markedly reduced the ATP-induced increase in H+ flux while SITS had no effect. ATP-induced H+ fluxes were also observed from Müller cells isolated from human, rat, monkey, skate and lamprey retinae, suggesting a highly evolutionarily conserved mechanism of potential general importance. Extracellular ATP also induced significant increases in extracellular H+ flux at the level of both the outer and inner plexiform layers in retinal slices of tiger salamander which was significantly reduced by suramin and PPADS. We suggest that the novel H+ flux mediated by ATP-activation of Müller cells and of other glia as well may be a key mechanism modulating neuronal signaling in the vertebrate retina and throughout the brain.

Published

2022

18. Electrostatic Tuning of Anion Attraction from the Cytoplasm to the Pore of the CFTR Chloride Channel

Author

Paul Linsdell, Yassine El Hiani, Elizabeth A. Cowley, and Alexander Negoda

Subjects

Anions, 0301 basic medicine, Cytoplasm, Patch-Clamp Techniques, Static Electricity, Biophysics, Cystic Fibrosis Transmembrane Conductance Regulator, Suramin, Biochemistry, Cell Line, Ion, 03 medical and health sciences, Coordination Complexes, Cricetinae, Animals, Humans, Patch clamp, Platinum, 030102 biochemistry & molecular biology, biology, Chemistry, Charge density, Conductance, Cell Biology, General Medicine, Cystic fibrosis transmembrane conductance regulator, Electrophysiology, 030104 developmental biology, Mutagenesis, Site-Directed, biology.protein, Chloride channel

Abstract

Anions enter from the cytoplasm into the channel pore of the cystic fibrosis transmembrane conductance regulator (CFTR) Cl- channel not via a central pathway but via a single lateral portal or fenestration. High Cl- conductance is dependent on electrostatic attraction of cytoplasmic Cl- ions by four positively charged amino acid side-chains located within this portal. Here we use a mutagenic approach to investigate the functional effects of transplanting or supplementing these positive charges at nearby portal-lining sites. Using patch clamp recording, we find that the functionally important positive charges at K190 and R303 can be transplanted to four nearby sites (N186, L197, W356, and A367) with little loss of Cl- conductance. Introduction of additional positive charge at these sites had almost no effect on Cl- conductance, but did increase the sensitivity to channel block by intracellular suramin and Pt(NO2)42- anions. We suggest that it is the number of positive charges within the portal, rather than their exact location, that is the most important factor influencing Cl- conductance. The portal appears well optimized in terms of charge distribution to maximize Cl- conductance.

Published

2019

19. Multiprong control of glioblastoma multiforme invasiveness: blockade of pro-inflammatory signaling, anti-angiogenesis, and homeostasis restoration

Author

Ludmila Belayev, Madigan M. Reid, Valerie A Cruz Flores, Nicolas G. Bazan, William Lewis, and Juan E Gallo

Subjects

Vascular Endothelial Growth Factor A, Cancer Research, Bevacizumab, Angiogenesis, Lipid mediators, Inflammation, Angiogenesis Inhibitors, Glial tumor, Suramin, chemistry.chemical_compound, Glioma, medicine, Tumor Microenvironment, Homeostasis, Humans, Tumor microenvironment, Neovascularization, Pathologic, business.industry, Brain Neoplasms, medicine.disease, Angiogenesis inhibitor, Vascular endothelial growth factor, chemistry, Oncology, Platelet-activating factor, Cancer research, Commentary, medicine.symptom, business, Glioblastoma, medicine.drug

Abstract

Glioblastoma multiforme (GBM) is the most invasive type of glial tumor with poor overall survival, despite advances in surgical resection, chemotherapy, and radiation. One of the main challenges in treating GBM is related to the tumor’s location, complex and heterogeneous biology, and high invasiveness. To meet the demand for oxygen and nutrients, growing tumors induce new blood vessels growth. Antibodies directed against vascular endothelial growth factor (VEGF), which promotes angiogenesis, have been developed to limit tumor growth. Bevacizumab (Avastin), an anti-VEGF monoclonal antibody, is the first approved angiogenesis inhibitor with therapeutic promise. However, it has limited efficacy, likely due to adaptive mutations in GBM, leading to overall survival compared to the standard of care in GBM patients. Molecular connections between angiogenesis, inflammation, oxidative stress pathways, and the development of gliomas have been recognized. Improvement in treatment outcomes for patients with GBM requires a multifaceted approach due to the converging dysregulation of signaling pathways. While most GBM clinical trials focus on “anti-angiogenic” modalities, stimulating inflammation resolution is a novel host-centric therapeutic avenue. The selective therapeutic possibilities for targeting the tumor microenvironment, specifically angiogenic and inflammatory pathways expand. So, a combination of agents aiming to interfere with several mechanisms might be beneficial to improve outcomes. Our approach might also be combined with other therapies to enhance sustained effectiveness. Here, we discuss Suramab (anti-angiogenic), LAU-0901 (a platelet-activating factor receptor antagonist), Elovanoid (ELV; a novel lipid mediator), and their combination as potential alternatives to contain GBM growth and invasiveness.

Published

2021

20. Purinergic signaling is essential for full Psickle activation by hypoxia and by normoxic acid pH in mature human sickle red cells and in vitro-differentiated cultured human sickle reticulocytes

Author

David H, Vandorpe, Alicia, Rivera, Markus, Ganter, Selasi, Dankwa, Jay G, Wohlgemuth, Jeffrey S, Dlott, L Michael, Snyder, Carlo, Brugnara, Manoj, Duraisingh, and Seth L, Alper

Subjects

Adenosine Triphosphate, Erythrocytes, Reticulocytes, Probenecid, Cations, Apyrase, Humans, Anemia, Sickle Cell, Suramin, Hydrogen-Ion Concentration, Hypoxia, Cells, Cultured

Abstract

Paracrine ATP release by erythrocytes has been shown to regulate endothelial cell function via purinergic signaling, and this erythoid-endothelial signaling network is pathologically dysregulated in sickle cell disease. We tested the role of extracellular ATP-mediated purinergic signaling in the activation of Psickle, the mechanosensitive Ca

Published

2021

21. The anti-parasitic drug suramin potently inhibits formation of seminal amyloid fibrils and their interaction with HIV-1

Author

Suiyi Tan, Shuwen Liu, Zhipeng Chen, Yan Lan, Zhaofeng Li, Tao Qi, Wenjuan Li, Yurong Qiu, Zichao Yang, Jinqing Li, Cheng Hongyan, Lin Li, and Tingting Zhang

Subjects

Adult, Male, 0301 basic medicine, Amyloid, Sexual transmission, Anti-HIV Agents, Antiparasitic, medicine.drug_class, Suramin, HIV Infections, Peptide, Pharmacology, Microbiology, Biochemistry, 03 medical and health sciences, Semen, Microbicide, medicine, Animals, Humans, Molecular Biology, chemistry.chemical_classification, 030102 biochemistry & molecular biology, Chemistry, Cell Biology, Healthy Volunteers, Peptide Fragments, 030104 developmental biology, Anti-Retroviral Agents, Mechanism of action, Transcytosis, HIV-1, Rabbits, medicine.symptom, Peptides, medicine.drug

Abstract

Seminal amyloid fibrils are made up of naturally occurring peptide fragments and are key targets for the development of combination microbicides or antiviral drugs. Previously, we reported that the polysulfonic compound ADS-J1 is a potential candidate microbicide that not only inhibits HIV-1 entry, but also seminal fibrils. However, the carcinogenic azo moieties in ADS-J1 preclude its clinical application. Here, we screened several ADS-J1–like analogs and found that the antiparasitic drug suramin most potently inhibited seminal amyloid fibrils. Using various biochemical methods, including Congo red staining, CD analysis, transmission EM, viral infection assays, surface plasmon resonance imaging, and molecular dynamics simulations, we investigated suramin's inhibitory effects and its putative mechanism of action. We found that by forming a multivalent interaction, suramin binds to proteolytic peptides and mature fibrils, thereby inhibiting seminal fibril formation and blocking fibril-mediated enhancement of viral infection. Of note, suramin exhibited potent anti-HIV activities, and combining suramin with several antiretroviral drugs produced synergistic effects against HIV-1 in semen. Suramin also displayed a good safety profile for vaginal application. Moreover, suramin inhibited the semen-derived enhancer of viral infection (SEVI)/semen-mediated enhancement of HIV-1 transcytosis through genital epithelial cells and the subsequent infection of target cells. Collectively, suramin has great potential for further development as a combination microbicide to reduce the spread of the AIDS pandemic by targeting both viral and host factors involved in HIV-1 sexual transmission.

Published

2019

22. Manipulating Active Structure and Function of Cationic Antimicrobial Peptide CM15 with the Polysulfonated Drug Suramin: A Step Closer to in Vivo Complexity

Author

Judit Henczkó, Ferenc Zsila, Tünde Juhász, Tamás Beke-Somfai, Kata Horváti, Szilvia Bősze, Mayra Quemé-Peña, Zoltán Varga, Csaba Németh, Bernadett Pályi, Judith Mihály, and Imola Cs. Szigyártó

Subjects

folding, Suramin, Lipid Bilayers, Antimicrobial peptides, Peptide, 010402 general chemistry, 01 natural sciences, Biochemistry, Protein Structure, Secondary, antimicrobial peptides, Anti-Infective Agents, In vivo, Escherichia coli, medicine, Membrane activity, Humans, Lipid bilayer, Molecular Biology, Protein secondary structure, Cells, Cultured, chemistry.chemical_classification, suramin, Full Paper, 010405 organic chemistry, Chemistry, Circular Dichroism, Organic Chemistry, Full Papers, Antimicrobial, 0104 chemical sciences, IR spectroscopy, Biophysics, Molecular Medicine, Antimicrobial Cationic Peptides, medicine.drug

Abstract

Antimicrobial peptides (AMPs) kill bacteria by targeting their membranes through various mechanisms involving peptide assembly, often coupled with disorder‐to‐order structural transition. However, for several AMPs, similar conformational changes in cases in which small organic compounds of both endogenous and exogenous origin have induced folded peptide conformations have recently been reported. Thus, the function of AMPs and of natural host defence peptides can be significantly affected by the local complex molecular environment in vivo; nonetheless, this area is hardly explored. To address the relevance of such interactions with regard to structure and function, we have tested the effects of the therapeutic drug suramin on the membrane activity and antibacterial efficiency of CM15, a potent hybrid AMP. The results provided insight into a dynamic system in which peptide interaction with lipid bilayers is interfered with by the competitive binding of CM15 to suramin, resulting in an equilibrium dependent on peptide‐to‐drug ratio and vesicle surface charge. In vitro bacterial tests showed that when CM15⋅suramin complex formation dominates over membrane binding, antimicrobial activity is abolished. On the basis of this case study, it is proposed that small‐molecule secondary structure regulators can modify AMP function and that this should be considered and could potentially be exploited in future development of AMP‐based antimicrobial agents.

Published

2019

23. HSP60/10 chaperonin systems are inhibited by a variety of approved drugs, natural products, and known bioactive molecules

Author

Sanofar Abdeen, Nilshad Salim, Jared Sivinski, Mckayla Stevens, Siddhi Chitre, Eli Chapman, Anne-Marie Ray, Quyen Q. Hoang, Steven M. Johnson, Alex Washburn, and Yangshin Park

Subjects

Protein Folding, medicine.drug_class, Clinical Biochemistry, Antibiotics, Pharmaceutical Science, Suramin, macromolecular substances, Trypanosoma brucei, medicine.disease_cause, Rafoxanide, Salicylanilides, 01 natural sciences, Biochemistry, Article, Chaperonin, Inhibitory Concentration 50, Heat shock protein, Drug Discovery, Chaperonin 10, Escherichia coli, medicine, Humans, Molecular Biology, Biological Products, biology, 010405 organic chemistry, Chemistry, Organic Chemistry, Chaperonin 60, biology.organism_classification, GroEL, 0104 chemical sciences, enzymes and coenzymes (carbohydrates), 010404 medicinal & biomolecular chemistry, biological sciences, bacteria, Molecular Medicine, HSP60, Bacteria

Abstract

All living organisms contain a unique class of molecular chaperones called 60 kDa heat shock proteins (HSP60 – also known as GroEL in bacteria). While some organisms contain more than one HSP60 or GroEL isoform, at least one isoform has always proven to be essential. Because of this, we have been investigating targeting HSP60 and GroEL chaperonin systems as an antibiotic strategy. Our initial studies focused on applying this antibiotic strategy for treating African sleeping sickness (caused by Trypanosoma brucei parasites) and drug-resistant bacterial infections (in particular Methicillin-resistant Staphylococcus aureus – MRSA). Intriguingly, during our studies we found that three known antibiotics – suramin, closantel, and rafoxanide – were potent inhibitors of bacterial GroEL and human HSP60 chaperonin systems. These findings prompted us to explore what other approved drugs, natural products, and known bioactive molecules might also inhibit HSP60 and GroEL chaperonin systems. Initial high-throughput screening of 3680 approved drugs, natural products, and known bioactives identified 161 hit inhibitors of the Escherichia coli GroEL chaperonin system (4.3% hit rate). From a purchased subset of 60 hits, 29 compounds (48%) re-confirmed as selective GroEL inhibitors in our assays, all of which were nearly equipotent against human HSP60. These findings illuminate the notion that targeting chaperonin systems might be a more common occurrence than we previously appreciated. Future studies are needed to determine if the in vivo modes of action of these approved drugs, natural products, and known bioactive molecules are related to GroEL and HSP60 inhibition.

Published

2019

24. Suramin, screened from an approved drug library, inhibits HuR functions and attenuates malignant phenotype of oral cancer cells

Author

Kanchu Tei, Katsumi Maenaka, Kazuhiro Matsushita, Masahiro Sakaitani, Tetsuya Kitamura, Satoko Otsuguro, Takao Nomura, and Wataru Kakuguchi

Subjects

0301 basic medicine, Cancer Research, Cell Survival, Suramin, Cell, Antineoplastic Agents, drug repositioning, ELAV-Like Protein 1, Small Molecule Libraries, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, Cell Line, Tumor, medicine, Humans, Radiology, Nuclear Medicine and imaging, Cyclin B1, Original Research, Cancer Biology, AU-rich element, Gene knockdown, Wound Healing, suramin, Chemistry, screening, AU-rich elements, Tongue Neoplasms, 030104 developmental biology, medicine.anatomical_structure, Oncology, Cell culture, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, HuR, AU‐rich elements, Cyclin A2, medicine.drug

Abstract

AU‐rich elements (ARE) exist in the 3′‐untranslated regions of the mRNA transcribed from cell growth‐related genes such as proto‐oncogenes, cyclin‐related genes, and growth factors. HuR binds and stabilizes ARE‐mRNA. HuR is expressed abundantly in cancer cells and related malignant phenotypes. HuR knockdown attenuates the malignant phenotype of oral cancer cells. In this study, we screened 1570 compounds in the approved drug library by differential scanning fluorimetry (DSF) to discover a HuR‐targeted compound. Firstly, 55 compounds were selected by DSF. Then, 8 compounds that showed a shift in the melting temperature value in a concentration‐dependent manner were selected by DSF. Of them, suramin, an anti‐trypanosomal drug, binds to HuR, exhibiting fast‐on and fast‐off kinetic behavior on surface plasmon resonance (SPR). We confirmed that suramin significantly decreased mRNA and protein expression of cyclin A2 and cyclin B1. The cyclin A2 and cyclin B1 mRNAs were destabilized by suramin. Furthermore, the motile and invasive activities of a tongue carcinoma cell line treated with suramin were markedly lower than those of control cells. The above findings suggest that suramin binds to HuR and inhibits its function. We also showed that the anticancer effects of suramin were caused by the inhibition of HuR function, indicating its potential as a novel therapeutic agent in the treatment of oral cancer. Our results suggest that suramin, via its different mechanism, may effectively suppress progressive oral cancer that cannot be controlled using other anticancer agents.

Published

2018

25. Surface plasmon resonance approach to study drug interactions with SARS-CoV-2 RNA-dependent RNA polymerase highlights treatment potential of suramin

Author

Matej Butala, Martina Mravinec, and Gregor Bajc

Subjects

Sofosbuvir, Suramin, viruses, Short Communication, RNA-dependent RNA polymerase, Biology, Favipiravir, Antiviral Agents, chemistry.chemical_compound, Virology, RNA polymerase, Surface plasmon resonance, medicine, Humans, Drug Interactions, suramin, SARS-CoV-2, RNA, COVID-19, površinska plazmonska resonanca, udc:577.2, covid-19, Viral replication, chemistry, RNA, Viral, surface plasmon resonance, medicine.drug

Abstract

The SARS-CoV-2 RNA-dependent RNA polymerase (RdRp) is essential for virus replication, therefore it is a promising drug target. Here we present a surface plasmon resonance approach to study the interaction of RdRp with drugs in real time. We monitored the effect of favipiravir, ribavirin, sofosbuvir triphosphate PSI-7409 and suramin on RdRp binding to RNA immobilized on the chip. Suramin precluded interaction of RdRp with RNA and even displaced RdRp from RNA.

Published

2021

26. Autocrine regulation of wound healing by ATP release and P2Y

Author

T B-D, McEwan, R A, Sophocleous, P, Cuthbertson, K J, Mansfield, M L, Sanderson-Smith, and R, Sluyter

Subjects

Receptors, Purinergic P2Y2, Autocrine Communication, Wound Healing, Adenosine Triphosphate, HEK293 Cells, Purinergic P2Y Receptor Antagonists, Humans, Suramin

Abstract

Application of exogenous nucleotides can modulate wound healing via the activation of purinergic receptors. However, evidence for the release of endogenous nucleotides and the subsequent activation of purinergic receptors in this process has not been well defined. Therefore, the current study aimed to investigate wound-mediated nucleotide release and autocrine purinergic signalling during HaCaT keratinocyte wound closure following scratch injury.An in vitro scratch wound apparatus was employed to study wound healing over 24-h in the presence of modulators of ATP release, P2 receptors and pathways downstream of P2 receptor activation.Adenosine 5'-triphosphate (ATP) was released from scratched cells. The ectonucleotidase apyrase and pharmacological inhibition of the nucleotide release hemichannel, pannexin-1, decreased wound closure over time. The non-selective P2Y receptor antagonist suramin and the selective P2YThese data describe a novel autocrine signalling mechanism in which wound-mediated release of endogenous ATP in response to mechanical scratching of HaCaT cells activates P2Y

Published

2021

27. The role of SIRT5 and p53 proteins in the sensitivity of colon cancer cells to chemotherapeutic agent 5-Fluorouracil

Author

Asli Koc and Ozlem Ekremoglu

Subjects

SIRT5, Antimetabolites, Antineoplastic, Genotype, Colorectal cancer, Cell Survival, Suramin, medicine.medical_treatment, Resveratrol, chemistry.chemical_compound, Western blot, Cell Line, Tumor, Genetics, medicine, Biomarkers, Tumor, Humans, Sirtuins, MTT assay, Molecular Biology, Chemotherapy, medicine.diagnostic_test, Dose-Response Relationship, Drug, Chemistry, General Medicine, medicine.disease, HCT116 Cells, Apoptosis, Drug Resistance, Neoplasm, Gene Knockdown Techniques, Colonic Neoplasms, Cancer research, Fluorouracil, Tumor Suppressor Protein p53, medicine.drug

Abstract

In the treatment of colorectal cancer, it is important to develop drug combinations that will increase the effectiveness of chemotherapy and to determine the molecular targets of the drugs. Therefore, combined therapies that can increase the sensitivity of 5-Fluorouracil (5-FU) and the molecular pathways involved in this process are important in the treatment of the disease. Here we examined the SIRT5 (Resveratrol and Suramin) and p53 (Nutlin3a) modulators alone or in combination with 5-FU on the proliferation of colon cancer cells and effect of 5-FU on the SIRT5 and FOXO3a protein expressions whether p53 dependent or independent manner. METHODS AND RESULTS: According to our MTT assay results, Resveratrol (RSV), Nutlin3a and Suramin was found to be more effective in HCT-116 p53+/+ cells and these differences were evaluated together with the effect of 5-FU on the SIRT5, FOXO3a and Bim protein expressions in HCT-116 p53 +/+ and HCT-116 p53 -/- cells. SIRT5 is known to deacetylate FOXO3a which plays roles in the induction of apoptosis via Bim protein. Our western blot experiment results showed that while Suramin decreased SIRT5 and RSV decreased FOXO3a protein expressions significantly in HCT-116 p53 -/- cells, 5-FU decreased significantly SIRT5 and FOXO3a protein expressions in a p53 independent manner.In this study, the effect of 5-FU on SIRT5 and FOXO 3a proteins was determined for the first time in HCT-116 p53 +/+ and HCT-116 p53 -/- cells. These results may help the discovery of new markers in colon cancer treatment.

Published

2021

28. Characterization of drug-induced human mitochondrial ADP/ATP carrier inhibition

Author

Edmund R.S. Kunji, Tom J J Schirris, Stephany Jaiquel Baron, and Martin S. King

Subjects

0301 basic medicine, Drug, Chebulinic acid, Arylamine N-Acetyltransferase, Suramin, media_common.quotation_subject, Cell Respiration, Medicine (miscellaneous), 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Adenosine Triphosphate, Cell Line, Tumor, mitochondrial transport proteins, medicine, Humans, adenine nucleotide translocase, Binding site, Pharmacology, Toxicology and Pharmaceutics (miscellaneous), Mitochondrial transport, media_common, Binding Sites, Chemistry, transport inhibition kinetics, Biological Transport, Mitochondria, Adenosine Diphosphate, Isoenzymes, Cytosol, Kinetics, 030104 developmental biology, Renal disorders Radboud Institute for Molecular Life Sciences [Radboudumc 11], Biochemistry, Pharmaceutical Preparations, ATP–ADP translocase, Mitochondrial ADP, ATP Translocases, thermostability shift, 030217 neurology & neurosurgery, Function (biology), drug-induced mitochondrial dysfunction, medicine.drug, HeLa Cells, Research Paper

Abstract

An increasing number of commonly prescribed drugs are known to interfere with mitochondrial function, causing cellular toxicity, but the underlying mechanisms are largely unknown. Although often not considered, mitochondrial transport proteins form a significant class of potential mitochondrial off-targets. So far, most drug interactions have been reported for the mitochondrial ADP/ATP carrier (AAC), which exchanges cytosolic ADP for mitochondrial ATP. Here, we show inhibition of cellular respiratory capacity by only a subset of the 18 published AAC inhibitors, which questions whether all compound do indeed inhibit such a central metabolic process. This could be explained by the lack of a simple, direct model system to evaluate and compare drug-induced AAC inhibition. Methods: For its development, we have expressed and purified human AAC1 (hAAC1) and applied two approaches. In the first, thermostability shift assays were carried out to investigate the binding of these compounds to human AAC1. In the second, the effect of these compounds on transport was assessed in proteoliposomes with reconstituted human AAC1, enabling characterization of their inhibition kinetics. Results: Of the proposed inhibitors, chebulinic acid, CD-437 and suramin are the most potent with IC50-values in the low micromolar range, whereas another six are effective at a concentration of 100 μM. Remarkably, half of all previously published AAC inhibitors do not show significant inhibition in our assays, indicating that they are false positives. Finally, we show that inhibitor strength correlates with a negatively charged surface area of the inhibitor, matching the positively charged surface of the substrate binding site. Conclusion: Consequently, we have provided a straightforward model system to investigate AAC inhibition and have gained new insights into the chemical compound features important for inhibition. Better evaluation methods of drug-induced inhibition of mitochondrial transport proteins will contribute to the development of drugs with an enhanced safety profile.

Published

2021

29. The Repurposed Drugs Suramin and Quinacrine Cooperatively Inhibit SARS-CoV-2 3CLpro In Vitro

Author

Eberle, Raphael J., Olivier, Danilo S., Amaral, Marcos S., Gering, Ian, Willbold, Dieter, Arni, Raghuvir K., Coronado, Monika A., Forschungszentrum Jülich, Heinrich-Heine-Universität Düsseldorf, Federal University of Tocantins, Federal University of Mato Grosso do Sul, Forchungszentrum Jülich, and Universidade Estadual Paulista (Unesp)

Subjects

COVID-19 Vaccines, quinacrine, Suramin, Molecular Dynamics Simulation, Viral Nonstructural Proteins, Microbiology, Antiviral Agents, Article, ddc:050, Humans, Protease Inhibitors, Pandemics, Coronavirus 3C Proteases, suramin, SARS-CoV-2, Repurposing approved drugs, Drug Repositioning, COVID-19, 3CLpro, QR1-502, COVID-19 Drug Treatment, Molecular Docking Simulation, Cysteine Endopeptidases, repurposing approved drugs, Quinacrine, main protease, Main protease

Abstract

Since the first report of a new pneumonia disease in December 2019 (Wuhan, China) the WHO reported more than 148 million confirmed cases and 3.1 million losses globally up to now. The causative agent of COVID-19 (SARS-CoV-2) has spread worldwide, resulting in a pandemic of unprecedented magnitude. To date, several clinically safe and efficient vaccines (e.g., Pfizer-BioNTech, Moderna, Johnson &amp, Johnson, and AstraZeneca COVID-19 vaccines) as well as drugs for emergency use have been approved. However, increasing numbers of SARS-Cov-2 variants make it imminent to identify an alternative way to treat SARS-CoV-2 infections. A well-known strategy to identify molecules with inhibitory potential against SARS-CoV-2 proteins is repurposing clinically developed drugs, e.g., antiparasitic drugs. The results described in this study demonstrated the inhibitory potential of quinacrine and suramin against SARS-CoV-2 main protease (3CLpro). Quinacrine and suramin molecules presented a competitive and noncompetitive inhibition mode, respectively, with IC50 values in the low micromolar range. Surface plasmon resonance (SPR) experiments demonstrated that quinacrine and suramin alone possessed a moderate or weak affinity with SARS-CoV-2 3CLpro but suramin binding increased quinacrine interaction by around a factor of eight. Using docking and molecular dynamics simulations, we identified a possible binding mode and the amino acids involved in these interactions. Our results suggested that suramin, in combination with quinacrine, showed promising synergistic efficacy to inhibit SARS-CoV-2 3CLpro. We suppose that the identification of effective, synergistic drug combinations could lead to the design of better treatments for the COVID-19 disease and repurposable drug candidates offer fast therapeutic breakthroughs, mainly in a pandemic moment.

Published

2021

30. Suramin, penciclovir, and anidulafungin exhibit potential in the treatment of COVID-19 via binding to nsp12 of SARS-CoV-2

Author

Suman Kundu, H. K. Das, Manisha Saini, Varnita Anand, Sanjay Kumar Dey, A. Sai Rajesh, Chetna Dhembla, and Shruti Bhatt

Subjects

Combination therapy, medicine.drug_class, Suramin, Antibiotics, Pharmacology, Anidulafungin, Antiviral Agents, Structural Biology, medicine, Humans, Molecular Biology, chemistry.chemical_classification, biology, SARS-CoV-2, Chemistry, COVID-19, Active site, General Medicine, Molecular Docking Simulation, Drug repositioning, Enzyme, Penciclovir, biology.protein, medicine.drug

Abstract

COVID-19, for which no confirmed therapeutic agents are available, has claimed over 48,14,000 lives globally. A feasible and quicker method to resolve this problem may be ���drug repositioning���. We investigated selected FDA and WHO-EML approved drugs based on their previously promising potential as antivirals, antibacterials or antifungals. These drugs were docked onto the nsp12 protein, which reigns the RNA-dependent RNA polymerase activity of SARS-CoV-2, a key therapeutic target for coronaviruses. Docked complexes were reevaluated using MM-GBSA analysis and the top three inhibitor-protein complexes were subjected to 100 ns long molecular dynamics simulation followed by another round of MM-GBSA analysis. The RMSF plots, binding energies and the mode of physicochemical interaction of the active site of the protein with the drugs were evaluated. Suramin, Penciclovir, and Anidulafungin were found to bind to nsp12 with similar binding energies as that of Remdesivir, which has been used as a therapy for COVID-19. In addition, recent experimental evidences indicate that these drugs exhibit antiviral efficacy against SARS-CoV-2. Such evidence, along with the significant and varied physical interactions of these drugs with the key viral enzyme outlined in this investigation, indicates that they might have a prospective therapeutic potential in the treatment of COVID-19 as monotherapy or combination therapy with Remdesivir. Communicated by Ramaswamy H. Sarma

Published

2021

31. Exogenous ATP modulates PGE

Author

Shamima, Akter, Rakesh Kumar, Sharma, Shilpa, Sharma, Saumya, Rastogi, Bernd L, Fiebich, and Ravi Shankar, Akundi

Subjects

Inflammation, Lipopolysaccharides, Male, Neurons, Cell Death, Macrophages, Suramin, Macrophage Activation, Cyclin-Dependent Kinase 9, p38 Mitogen-Activated Protein Kinases, Dinoprostone, Monocytes, Mice, Inbred C57BL, Mice, Adenosine Triphosphate, RAW 264.7 Cells, Cyclooxygenase 2, Receptors, Purinergic P2X, Culture Media, Conditioned, Animals, Humans, RNA, Messenger, Phosphorylation

Abstract

An important mediator of inflammation is prostaglandin E

Published

2020

32. Structural Basis of Inhibition of the Pioneer Transcription Factor NF-Y by Suramin

Author

Andrea Bernardini, Carlo Camilloni, Andrea Saponaro, Marco Nardini, Michela Lapi, Valentina Nardone, Diletta Dolfini, Sebastiano Pasqualato, Nerina Gnesutta, Cristina Airoldi, Antonio Chaves-Sanjuan, Roberto Mantovani, Nardone, V, Chaves-Sanjuan, A, Lapi, M, Airoldi, C, Saponaro, A, Pasqualato, S, Dolfini, D, Camilloni, C, Bernardini, A, Gnesutta, N, Mantovani, R, and Nardini, M

Subjects

histone fold, Magnetic Resonance Spectroscopy, Suramin, CAAT box, Molecular Dynamics Simulation, CCAAT box, Biophysical Phenomena, Article, Structure-Activity Relationship, medicine, Humans, Amino Acid Sequence, Transcription factor, lcsh:QH301-705.5, transcription factor, suramin, Chemistry, Rational design, Isothermal titration calorimetry, Promoter, General Medicine, DNA, inhibition, Cell biology, lcsh:Biology (General), CCAAT-Binding Factor, Docking (molecular), Histone fold, Protein Multimerization, NF-Y, medicine.drug, Transcription Factors

Abstract

NF-Y is a transcription factor (TF) comprising three subunits (NF-YA, NF-YB, NF-YC) that binds with high specificity to the CCAAT sequence, a widespread regulatory element in gene promoters of prosurvival, cell-cycle-promoting, and metabolic genes. Tumor cells undergo &ldquo, metabolic rewiring&rdquo, through overexpression of genes involved in such pathways, many of which are under NF-Y control. In addition, NF-YA appears to be overexpressed in many tumor types. Thus, limiting NF-Y activity may represent a desirable anti-cancer strategy, which is an ongoing field of research. With virtual-screening docking simulations on a library of pharmacologically active compounds, we identified suramin as a potential NF-Y inhibitor. We focused on suramin given its high water-solubility that is an important factor for in vitro testing, since NF-Y is sensitive to DMSO. By electrophoretic mobility shift assays (EMSA), isothermal titration calorimetry (ITC), STD NMR, X-ray crystallography, and molecular dynamics (MD) simulations, we showed that suramin binds to the histone fold domains (HFDs) of NF-Y, preventing DNA-binding. Our analyses, provide atomic-level detail on the interaction between suramin and NF-Y and reveal a region of the protein, nearby the suramin-binding site and poorly conserved in other HFD-containing TFs, that may represent a promising starting point for rational design of more specific and potent inhibitors with potential therapeutic applications.

Published

2020

33. Purinergic Receptors Crosstalk with CCR5 to Amplify Ca

Author

Mizuho, Horioka, Emilie, Ceraudo, Emily, Lorenzen, Thomas P, Sakmar, and Thomas, Huber

Subjects

Purinergic Antagonists, Receptors, CCR5, Receptors, Purinergic, Receptor Cross-Talk, Suramin, Receptors, G-Protein-Coupled, Adenosine Triphosphate, HEK293 Cells, G protein bias, Purinergic Agonists, GPCR signaling, Humans, Calcium Signaling, Chemokines, Purinergic receptors, Chemokine CCL5, CCR5, Crosstalk, Original Research

Abstract

Many G protein-coupled receptors (GPCRs) signal through more than one subtype of heterotrimeric G proteins. For example, the C–C chemokine receptor type 5 (CCR5), which serves as a co-receptor to facilitate cellular entry of human immunodeficiency virus 1 (HIV-1), normally signals through the heterotrimeric G protein, Gi. However, CCR5 also exhibits G protein signaling bias and certain chemokine analogs can cause a switch to Gq pathways to induce Ca2+ signaling. We want to understand how much of the Ca2+ signaling from Gi-coupled receptors is due to G protein promiscuity and how much is due to transactivation and crosstalk with other receptors. We propose a possible mechanism underlying the apparent switching between different G protein signaling pathways. We show that chemokine-mediated Ca2+ flux in HEK293T cells expressing CCR5 can be primed and enhanced by ATP pretreatment. In addition, agonist-dependent lysosomal exocytosis results in the release of ATP to the extracellular milieu, which amplifies cellular signaling networks. ATP is quickly degraded via ADP and AMP to adenosine. ATP, ADP and adenosine activate different cell surface purinergic receptors. Endogenous Gq-coupled purinergic P2Y receptors amplify Ca2+ signaling and allow for Gi- and Gq-coupled receptor signaling pathways to converge. Associated secretory release of GPCR ligands, such as chemokines, opioids, and monoamines, should also lead to concomitant release of ATP with a synergistic effect on Ca2+ signaling. Our results suggest that crosstalk between ATP-activated purinergic receptors and other Gi-coupled GPCRs is an important cooperative mechanism to amplify the intracellular Ca2+ signaling response. Electronic supplementary material The online version of this article (10.1007/s10571-020-01002-1) contains supplementary material, which is available to authorized users.

Published

2020

34. Structure-based drug repositioning explains ibrutinib as VEGFR2 inhibitor

Author

Daniele Parisi, Jörg-Christian Heinrich, V. Joachim Haupt, Melissa F. Adasme, Michael Schroeder, Kristien Van Belle, Thierry Louat, Gary Jennings, Yves Moreau, Jean Herman, Ben Sprangers, and Sebastian Salentin

Subjects

B Cells, Kinase Inhibitors, Biochemistry, chemistry.chemical_compound, White Blood Cells, Database and Informatics Methods, Protein Structure Databases, Jurkat Cells, RNA interference, Piperidines, Animal Cells, Medicine and Health Sciences, Macromolecular Structure Analysis, Agammaglobulinaemia Tyrosine Kinase, Medicine, Drug Interactions, Enzyme Inhibitors, media_common, B-Lymphocytes, biology, Kinase, T Cells, Enzymes, Nucleic acids, Drug repositioning, Genetic interference, Ibrutinib, Epigenetics, Cellular Types, Tyrosine kinase, Research Article, Signal Transduction, Drug, Protein Structure, Science, media_common.quotation_subject, Immune Cells, Immunology, Suramin, Research and Analysis Methods, Gene product, Therapeutic index, Genetics, Bruton's tyrosine kinase, Humans, Antibody-Producing Cells, Molecular Biology, Pharmacology, Drug Screening, Blood Cells, business.industry, Adenine, Drug Repositioning, Biology and Life Sciences, Proteins, Cell Biology, Vascular Endothelial Growth Factor Receptor-2, Biological Databases, Pyrimidines, chemistry, biology.protein, Cancer research, Enzymology, RNA, Pyrazoles, Gene expression, business, Protein Kinases

Abstract

Many drugs are promiscuous and bind to multiple targets. On the one hand, these targets may be linked to unwanted side effects, but on the other, they may achieve a combined desired effect (polypharmacology) or represent multiple diseases (drug repositioning). With the growth of 3D structures of drug-target complexes, it is today possible to study drug promiscuity at the structural level and to screen vast amounts of drug-target interactions to predict side effects, polypharmacological potential, and repositioning opportunities. Here, we pursue such an approach to identify drugs inactivating B-cells, whose dysregulation can function as a driver of autoimmune diseases. Screening over 500 kinases, we identified 22 candidate targets, whose knock out impeded the activation of B-cells. Among these 22 is the gene KDR, whose gene product VEGFR2 is a prominent cancer target with anti-VEGFR2 drugs on the market for over a decade. The main result of this paper is that structure-based drug repositioning for the identified kinase targets identified the cancer drug ibrutinib as micromolar VEGFR2 inhibitor with a very high therapeutic index in B-cell inactivation. These findings prove that ibrutinib is not only acting on the Bruton's tyrosine kinase BTK, against which it was designed. Instead, it may be a polypharmacological drug, which additionally targets angiogenesis via inhibition of VEGFR2. Therefore ibrutinib carries potential to treat other VEGFR2 associated disease. Structure-based drug repositioning explains ibrutinib's anti VEGFR2 action through the conservation of a specific pattern of interactions of the drug with BTK and VEGFR2. Overall, structure-based drug repositioning was able to predict these findings at a fraction of the time and cost of a conventional screen. ispartof: PLOS ONE vol:15 issue:5 ispartof: location:United States status: published

Published

2020

35. 100 Years of Suramin

Author

Natalie Wiedemar, Dennis A. Hauser, and Pascal Mäser

Subjects

Trypanosoma brucei rhodesiense, Suramin, Pharmacology, Trypanosoma brucei, 03 medical and health sciences, 0302 clinical medicine, Molecular level, parasitic diseases, medicine, polycyclic compounds, Animals, Humans, Pharmacology (medical), heterocyclic compounds, Polypharmacology, 030304 developmental biology, 0303 health sciences, biology, business.industry, organic chemicals, biology.organism_classification, Trypanocidal Agents, 3. Good health, Infectious Diseases, Trypanosomiasis, African, 030220 oncology & carcinogenesis, Minireview, business, medicine.drug

Abstract

Suramin is 100 years old and is still being used to treat the first stage of acute human sleeping sickness, caused by; Trypanosoma brucei; rhodesiense; Suramin is a multifunctional molecule with a wide array of potential applications, from parasitic and viral diseases to cancer, snakebite, and autism. Suramin is also an enigmatic molecule: What are its targets? How does it get into cells in the first place? Here, we provide an overview of the many different candidate targets of suramin and discuss its modes of action and routes of cellular uptake. We reason that, once the polypharmacology of suramin is understood at the molecular level, new, more specific, and less toxic molecules can be identified for the numerous potential applications of suramin.

Published

2020

36. Suramin Inhibits Chikungunya Virus Replication by Interacting with Virions and Blocking the Early Steps of Infection

Author

Andrea Brancale, Irina C. Albulescu, Martijn J. van Hemert, Tabitha E. Hoornweg, Kristina Kovacikova, Eric J. Snijder, Leonie White-Scholten, Ali Tas, Jolanda M. Smit, Salvatore Ferla, and Microbes in Health and Disease (MHD)

Subjects

0301 basic medicine, Models, Molecular, E2 envelope protein, fusion, viruses, CHIKV, lcsh:QR1-502, EPITOPE, medicine.disease_cause, Virus Replication, lcsh:Microbiology, E2, Viral Envelope Proteins, BINDING, Chlorocebus aethiops, polycyclic compounds, alphavirus, Chikungunya, Mutation, biology, drug repurposing, Chemistry, virus diseases, antiviral, Infectious Diseases, ENTRY, Chikungunya virus, medicine.drug, STRAIN, Suramin, 030106 microbiology, Virus Attachment, Alphavirus, Antiviral Agents, Virus, Article, 03 medical and health sciences, Virology, parasitic diseases, medicine, Animals, Humans, Vero Cells, attachment, RELEASE, suramin, Binding Sites, Virion, Suramin binding, Virus Internalization, biology.organism_classification, Reverse genetics, 030104 developmental biology, Viral replication, Chikungunya Fever

Abstract

Chikungunya virus (CHIKV) is a mosquito-transmitted alphavirus that can cause a debilitating disease that is primarily characterized by persistent joint pain. CHIKV has been emerging globally, while neither a vaccine nor antiviral medication is available. The anti-parasitic drug suramin was previously shown to inhibit CHIKV replication. In this study we aimed to obtain more detailed insight into its mechanism of action. We found that suramin interacts with virions and can inhibit virus binding to cells. It also appeared to inhibit post-attachment steps of the infection process, likely by preventing conformational changes of the envelope glycoproteins required for fusion and the progression of infection. Suramin-resistant CHIKV strains were selected and genotyping and reverse genetics experiments indicated that mutations in E2 were responsible for resistance. The substitutions N5R and H18Q were reverse engineered in the E2 glycoprotein in order to understand their role in resistance. The binding of suramin-resistant viruses with these two E2 mutations was inhibited by suramin like that of wild-type virus, but they appeared to be able to overcome the post-attachment inhibitory effect of suramin. Conversely, a virus with a G82R mutation in E2 (implicated in attenuation of vaccine strain 181/25), which renders it dependent on the interaction with heparan sulfate for entry, was more sensitive to suramin than wild-type virus. Using molecular modelling studies, we predicted the potential suramin binding sites on the mature spikes of the chikungunya virion. We conclude that suramin interferes with CHIKV entry by interacting with the E2 envelope protein, which inhibits attachment and also interferes with conformational changes required for fusion.

Published

2020

37. Trypanocidal activity of tetradentated pyridine-based manganese complexes is not linked to inactivation of superoxide dismutase

Author

Dietmar Steverding, Karolina Kolosevska, and Manuel Sánchez-Moreno

Subjects

0301 basic medicine, Eflornithine, Trypanosoma brucei brucei, Immunology, HL-60 Cells, Microbial Sensitivity Tests, Suramin, Pyrogallol, Trypanosoma brucei, Ornithine Decarboxylase, Antioxidants, Ornithine decarboxylase, Superoxide dismutase, 03 medical and health sciences, chemistry.chemical_compound, medicine, Humans, Drug Interactions, Trypanosoma cruzi, chemistry.chemical_classification, biology, Superoxide Dismutase, General Medicine, Ornithine Decarboxylase Inhibitors, biology.organism_classification, Trypanocidal Agents, Trypanosomiasis, African, 030104 developmental biology, Infectious Diseases, Enzyme, Manganese Compounds, Ornithine Decarboxylase Inhibitor, chemistry, Biochemistry, biology.protein, Parasitology, Growth inhibition, medicine.drug

Abstract

Two tetradentated pyridine-based manganese complexes (Cpd2 and Cpd3) were previously reported to inhibit efficiently the growth of Trypanosoma cruzi in vitro and in vivo. Cpd3 was also shown to be a potent inhibitor of trypanosomal iron superoxide dismutase (Fe-SOD) and its trypanocidal activity linked to the inhibition of this enzyme. Here we investigated the anti-trypanosomal activity of the two compounds against bloodstream forms of Trypanosoma brucei. Both compounds displayed potent trypanocidal activity against T. brucei bloodstream forms with minimum inhibitory concentrations (MICs) and 50% growth inhibition (GI50) values of 1 μM and 0.2–0.3 μM, respectively. Cpd2 and Cpd3 also showed cytotoxicity against HL-60 cells but based on GI50 values the human cells were 14 and 87 times less sensitive indicating moderate selectivity. In contrast to previous observation, Cpd3 did not inhibit Fe-SOD within trypanosomes and Cpd2 inhibited the enzyme only by 34%. As Fe-SOD together with ornithine decarboxylase play vital roles in the antioxidant defence in bloodstream forms of T. brucei, inhibition of both enzymes should be synergistically. Therefore, the interaction of Cpd2 and Cpd3 with the ornithine decarboxylase inhibitor eflornithine was determined. Both compounds were found in combination with eflornithine to produce only an additive effect. Thus, the observed lack of synergy between Cpd2/Cpd3 and eflornithine can be regarded as further indication that both compounds are not very strong inhibitors of trypanosomal Fe-SOD. Nevertheless, tetradentated pyridine-based manganese complexes are interesting compounds with promising anti-trypanosomal activity.

Published

2018

38. Trypanosoma brucei rhodesiense infection in a Chinese traveler returning from the Serengeti National Park in Tanzania

Author

Zhu-Yun Chen, Yao-Ying Lin, Han-Guo Xie, Mu-Xin Chen, Qin Liu, Xiao-Ling Chen, Jia-Xu Chen, Xiao-Nong Zhou, Hua Zheng, Yi Zhang, and Qing Liu

Subjects

0301 basic medicine, Adult, Trypanosoma brucei rhodesiense, medicine.medical_specialty, China, Parks, Recreational, 030231 tropical medicine, Case Report, Imported infection, Suramin, Polymerase Chain Reaction, Tanzania, lcsh:Infectious and parasitic diseases, 03 medical and health sciences, 0302 clinical medicine, Communicable Diseases, Imported, parasitic diseases, medicine, Humans, African trypanosomiasis, lcsh:RC109-216, Socioeconomics, Pentamidine, Travel, biology, National park, Public health, lcsh:Public aspects of medicine, Human African trypanosomiasis, Public Health, Environmental and Occupational Health, lcsh:RA1-1270, General Medicine, 030108 mycology & parasitology, biology.organism_classification, medicine.disease, Treatment, Infectious Diseases, Geography, Treatment Outcome, Trypanosomiasis, African, Tropical medicine, Female, Trypanosomiasis, medicine.drug

Abstract

Background Human African trypanosomiasis (HAT) is one of the most complex parasitic diseases known to humankind. It usually occurs in endemic areas in Africa, but is occasionally detected in returning travelers and migrants in non-endemic countries. Case presentation In August 2017, a case of HAT was diagnosed in China in a traveler returning from the Masai Mara area in Kenya and the Serengeti area in Tanzania. The traveler visited Africa from 23 July to 5 August, 2017. Upon return to China, she developed a fever (on 8 August), and Trypanosoma brucei rhodesiense infection was confirmed by laboratory tests (on 14 August) including observation of parasites in blood films and by polymerase chain reaction. She was treated with pentamidine followed by suramin, and recovered 1 month later. Conclusions This is the first imported rhodesiense HAT case reported in China. This case alerts clinical and public health workers to be aware of HAT in travelers, and expatriates and migrants who have visited at-risk areas in Africa. Electronic supplementary material The online version of this article (10.1186/s40249-018-0432-5) contains supplementary material, which is available to authorized users.

Published

2018

39. Quantitative contributions of processes by which polyanion drugs reduce intracellular bioavailability and transfection efficiency of cationic siRNA lipoplex

Author

Bertrand Z. Yeung, M. Guillaume Wientjes, Pharavee Jaiprasart, Sukyung Woo, Ze Lu, Minjian Cui, Jessie L.-S. Au, and Chien Ming Hsieh

Subjects

0301 basic medicine, Small interfering RNA, Survivin, Suramin, Biological Availability, Pharmaceutical Science, Transfection, Endocytosis, Article, 03 medical and health sciences, 0302 clinical medicine, RNA interference, medicine, Humans, Gene silencing, Cationic liposome, Gene Silencing, RNA, Small Interfering, Gene knockdown, Heparin, Chemistry, 030104 developmental biology, 030220 oncology & carcinogenesis, Liposomes, Biophysics, HT29 Cells, medicine.drug

Abstract

RNA Interference (RNAi) is a potentially useful tool to correct the detrimental effects of faulty genes; several RNAi are undergoing clinical evaluation in various diseases. The present study identified the relative contributions of three mechanisms by which polyanion drugs reduced the gene silencing activity of Lipoplex, a complex of small interfering RNA (siRNA) and cationic liposomes. The study used a siRNA against the chemoresistance gene survivin and two model polyanion drugs (suramin, heparin). Products of Lipoplex destabilization were separated, identified, and/or quantified using ultrafiltration, gel electrophoresis, and RT-qPCR (quantitative reverse transcription polymerase chain reaction). Cell binding and endocytosis of fluorescence-labeled Lipoplex and the amount of siRNA at its site of action RISC (RNA-induced silencing complex) were evaluated using endocytosis markers, confocal microscopy, quantitative image analysis, immunoprecipitation, and RT-qPCR. The results show suramin and heparin exerted multiple concentration-dependent effects. First, these agents altered several Lipoplex properties (i.e., reduced particle size, changed surface charge, modified composition of protein biocorona). Second, both caused Lipoplex destabilization to release double- and single-strand siRNA and/or smaller siRNA-lipid complexes with reduced siRNA cargo. Third, both prevented the cell surface binding and internalization of Lipoplex, diminished the siRNA concentration in RISC, and retarded the mRNA knockdown. Suramin and heparin yielded qualitatively and quantitatively different results. Analysis of the experimental results of suramin using quantitative pharmacology (QP) modeling indicated the major cause of gene silencing activity loss depended on drug concentration, changing from inhibition of endocytosis at lower concentration (accounting for 60% loss at ~ 9 μM) to inhibition of cell surface binding and loss of siRNA cargo at higher concentrations (accounting for 64% and 27%, respectively, at 70 μM). In summary, the present study demonstrates the complex and dynamic interactions between polyanions and Lipoplex, and the use of QP modeling to delineate the contributions of three mechanisms to the eventual loss of gene silencing activity.

Published

2018

40. UDP-sugars activate P2Y14 receptors to mediate vasoconstriction of the porcine coronary artery

Author

Natalia Dovlatova, Vera Ralevic, William R. Dunn, Zainab Abbas, Stan Heptinstall, M. Liaque Latif, and Susan C. Fox

Subjects

0301 basic medicine, Male, DABCO, 1,4-diazabicyclo[2.2.2]octane, P2Y14 receptor, RCF, relative centrifugal force, Physiology, Swine, ERK, extracellular signal-regulated kinases, TBST, Tris-buffered saline and Tween 20, Pharmacology, chemistry.chemical_compound, Isothiocyanates, Vasoconstrictor Agents, Sugar nucleotides, SDS, sodium dodecyl sulphate, Receptor, Forskolin, Thiourea, UDP sugars, L-NAME, Nω-nitro-L-arginine methyl ester, Receptor antagonist, Coronary Vessels, OCT, optimal temperature cutting compound, PPTN, 4-((piperidin-4-yl)-phenyl)-7-(4-(trifluoromethyl)-phenyl)-2-naphthoic acid, SNP, sodium nitroprusside, Molecular Medicine, Female, FITC, fluorescein isothiocyanate, Signal transduction, medicine.drug, Signal Transduction, Agonist, Adult, Uridine Diphosphate Glucose, NTPDase1, nucleotide triphosphate diphosphohydrolase-1, medicine.drug_class, Suramin, P2 receptor, P2Y6 receptor, Coronary artery, Article, 03 medical and health sciences, PBS, phosphate buffered saline, medicine, Animals, Humans, PPADS, PAGE, polyacrylamide gel electrophoresis, MRS2690, diphosphoric acid 1-α-d-glucopyranosyl ester 2-[(4′-methylthio)uridin-5″-yl] ester disodium salt, NO, nitric oxide, Receptors, Purinergic P2, Colforsin, MRS2690, Uridine Diphosphate Sugars, 030104 developmental biology, UDP-glucose, chemistry, MAPK, mitogen-activated protein kinases, Vasoconstriction, BSA, bovine serum albumin, MRS2578, N,N"-1,4-butanediylbis[N'-(3-isothiocyanatophenyl)thiourea, VASP, vasodilator-stimulated phosphoprotein, KCl, potassium chloride, DAPI, 4′,6-diamidino-2-phenylindole

Abstract

Aims UDP-sugars can act as extracellular signalling molecules, but relatively little is known about their cardiovascular actions. The P2Y14 receptor is a Gi/o-coupled receptor which is activated by UDP-glucose and related sugar nucleotides. In this study we sought to investigate whether P2Y14 receptors are functionally expressed in the porcine coronary artery using a selective P2Y14 receptor agonist, MRS2690, and a novel selective P2Y14 receptor antagonist, PPTN (4,7-disubstituted naphthoic acid derivative). Methods and results Isometric tension recordings were used to evaluate the effects of UDP-sugars in porcine isolated coronary artery segments. The effects of the P2 receptor antagonists suramin and PPADS, the P2Y14 receptor antagonist PPTN, and the P2Y6 receptor antagonist MRS2578, were investigated. Measurement of vasodilator-stimulated phosphoprotein (VASP) phosphorylation using flow cytometry was used to assess changes in cAMP levels. UDP-glucose, UDP-glucuronic acid UDP-N-acetylglucosamine (P2Y14 receptor agonists), elicited concentration-dependent contractions in the porcine coronary artery. MRS2690 was a more potent vasoconstrictor than the UDP-sugars. Concentration dependent contractile responses to MRS2690 and UDP-sugars were enhanced in the presence of forskolin (activator of cAMP), where the level of basal tone was maintained by addition of U46619, a thromboxane A2 mimetic. Contractile responses to MRS2690 were blocked by PPTN, but not by MRS2578. Contractile responses to UDP-glucose were also attenuated by PPTN and suramin, but not by MRS2578. Forskolin-induced VASP-phosphorylation was reduced in porcine coronary arteries exposed to UDP-glucose and MRS2690, consistent with P2Y14 receptor coupling to Gi/o proteins and inhibition of adenylyl cyclase activity. Conclusions Our data support a role of UDP-sugars as extracellular signalling molecules and show for the first time that they mediate contraction of porcine coronary arteries via P2Y14 receptors.

Published

2018

41. Identification and evaluation of the inhibitory effect of Prunella vulgaris extract on SARS-coronavirus 2 virus entry

Author

Xiaojian Yao, Darwyn Kobasa, Titus Abiola Olukitibi, Zhujun Ao, Mable Chan, Maggie Jing Ouyang, and Mona Mahmoudi

Subjects

RNA viruses, 0301 basic medicine, Pulmonology, Coronaviruses, Physiology, Molecular biology, Cell Lines, viruses, Prunella vulgaris, Biochemistry, Medical Conditions, Immune Physiology, Chlorocebus aethiops, Prunella, Enzyme-Linked Immunoassays, Neutralizing antibody, Pathology and laboratory medicine, Immune System Proteins, Multidisciplinary, biology, Medical microbiology, Infectious Diseases, Viruses, Spike Glycoprotein, Coronavirus, Medicine, Drug Therapy, Combination, Biological Cultures, Angiotensin-Converting Enzyme 2, SARS CoV 2, Pathogens, Research Article, Protein Binding, medicine.drug, Viral Entry, SARS coronavirus, Science, Suramin, Immunology, 030106 microbiology, DNA construction, Research and Analysis Methods, Microbiology, Antibodies, Virus, Cell Line, Respiratory Disorders, 03 medical and health sciences, Viral entry, Virology, medicine, Animals, Humans, Immunoassays, Vero Cells, Medicine and health sciences, Biology and life sciences, Plant Extracts, SARS-CoV-2, Organisms, Viral pathogens, Wild type, Proteins, COVID-19, Virus Internalization, biology.organism_classification, Antibodies, Neutralizing, Microbial pathogens, COVID-19 Drug Treatment, Molecular biology techniques, 030104 developmental biology, Cell culture, Respiratory Infections, Plasmid Construction, Mutation, Immunologic Techniques, biology.protein, Vero cell, Viral Transmission and Infection

Abstract

Until now, antiviral therapeutic agents are still urgently required for treatment or prevention of SARS-coronavirus 2 (SCoV-2) virus infection. In this study, we established a sensitive SCoV-2 Spike glycoprotein (SP), including an SP mutant D614G, pseudotyped HIV-1-based vector system and tested their ability to infect ACE2-expressing cells. Based on this system, we have demonstrated that an aqueous extract from the Natural herb Prunella vulgaris (NhPV) displayed potent inhibitory effects on SCoV-2 SP (including SPG614 mutant) pseudotyped virus (SCoV-2-SP-PVs) mediated infections. Moreover, we have compared NhPV with another compound, Suramin, for their anti-SARS-CoV-2 activities and the mode of their actions, and found that both NhPV and Suramin are able to directly interrupt SCoV-2–SP binding to its receptor ACE2 and block the viral entry step. Importantly, the inhibitory effects of NhPV and Suramin were confirmed by the wild type SARS-CoV-2 (hCoV-19/Canada/ON-VIDO-01/2020) virus infection in Vero cells. Furthermore, our results also demonstrated that the combination of NhPV/Suramin with an anti-SARS-CoV-2 neutralizing antibody mediated a more potent blocking effect against SCoV2-SP-PVs. Overall, by using SARS-CoV-2 SP-pseudotyped HIV-1-based entry system, we provide strong evidence that NhPV and Suramin have anti-SARS-CoV-2 activity and may be developed as a novel antiviral approach against SARS-CoV-2 infection.

Published

2021

42. Synthesis and evaluation of N-(4-(substituted)-3-(trifluoromethyl) phenyl) isobutyramides and their N-ethyl analogous as anticancer, anti-angiogenic & antioxidant agents: In vitro and in silico analysis

Author

Sonali S. Kamble, Sanjay S. Sawant, Shrikant V. Hese, Parshuram M. Pisal, Kamini T Bagul, Rajesh N. Gacche, Rohan J. Meshram, Rahul V. Pinjari, Vinod T. Kamble, and Ajay S. Sawant

Subjects

0301 basic medicine, Antioxidant, Cell Survival, DPPH, Suramin, medicine.medical_treatment, Angiogenesis Inhibitors, Antineoplastic Agents, Pharmacology, Biochemistry, Antioxidants, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Picrates, Structural Biology, Cell Line, Tumor, medicine, Humans, Cell Proliferation, Trifluoromethyl, Hydroxyl Radical, Chemistry, Biphenyl Compounds, Organic Chemistry, AutoDock, Ascorbic acid, Amides, In vitro, Molecular Docking Simulation, Computational Mathematics, 030104 developmental biology, Cell culture, 030220 oncology & carcinogenesis, Cytokines, medicine.drug

Abstract

N-(4-(substituted)-3-(trifluoromethyl) phenyl) isobutyramides and their N-ethyl analogues (flutamides) are versatile scaffolds with a wide spectrum of biological activities. A series of new N-(4-(substituted)-3-(trifluoromethyl) phenyl) isobutyramides (8a-t) and their N-ethyl analogous (9a-t) were synthesized and characterized. The inhibitory potential of the synthesized compounds on the viability of three human cancer cell lines HEP3BPN 11 (liver), MDA-MB 453 (breast), and HL 60 (leukemia) were assessed. Among all the compounds 8 L, 8q, 9n and 9p showed higher inhibitory activity on the viability of HL 60 than the standard methotrexate. These lead molecules were then tested for their potential to inhibit the activity of proangiogenic cytokines. The compound 9n showed significantly better inhibition against two cytokines viz. TNFα and Leptin as compared to the standard suramin, while 9p has activity comparable to suramin against IGF1, VEGF, FGFb, and Leptin. The 8q is found to be strong antiangiogenic agent against IGF1, VEGF and TGFβ; while 8 L has showed activity against TNFα, VEGF, and Leptin inhibition. Furthermore antioxidant potential of 8a–t and 9a-t compounds was screened using DPPH, OH and SOR radical scavenging activities. The OH radical scavenging activity of 8c and DPPH activities of 9n as well as 9o are significant as compared to respective standards ascorbic acid and α-tocopherol. The 8c, 9p and 9 h have also exhibited potential antioxidant activity. Additionally, we present in silico molecular docking data to provide the structural rationale of observed TNFα inhibition against newly synthesized compounds. Overall, the synthesized flutamide derivatives have not only anticancer activity, but also possess dual inhibitory effect (anti-angiogenesis and antioxidant) and hence can act as a promising avenue to develop further anticancer agents.

Published

2021

43. Emodin Inhibits ATP-Induced Proliferation and Migration by Suppressing P2Y Receptors in Human Lung Adenocarcinoma Cells

Author

Xia Wang, Long Li, Danian Zhu, Nana Song, Ruijuan Guan, and Linlin Shen

Subjects

0301 basic medicine, P2Y receptor, Epithelial-Mesenchymal Transition, Lung Neoplasms, Emodin, Physiology, Adenocarcinoma of Lung, Suramin, Adenocarcinoma, NF-κB, lcsh:Physiology, lcsh:Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Adenosine Triphosphate, Cell Movement, Cell Line, Tumor, Claudin-1, Extracellular, Humans, lcsh:QD415-436, Receptor, Cell Proliferation, bcl-2-Associated X Protein, A549 cell, lcsh:QP1-981, Chemistry, Cell growth, NF-kappa B, Cell migration, Cadherins, G1 Phase Cell Cycle Checkpoints, Cell biology, ATP, 030104 developmental biology, Microscopy, Fluorescence, Proto-Oncogene Proteins c-bcl-2, A549cells, A549 Cells, 030220 oncology & carcinogenesis, Receptors, Purinergic P2Y, Purinergic P2Y Receptor Antagonists, Calcium, Intracellular, Signal Transduction

Abstract

Background/Aims: Extracellular ATP performs multiple important functions via activation of P2 receptors on the cell surface. P2Y receptors play critical roles in ATP evoked response in human lung adenocarcinoma cells (A549 cells). Emodin is an anthraquinone derivative originally isolated from Chinese rhubarb, possesses anticancer properties. In this study we examined the inhibiting effects of emodin on proliferation, migration and epithelial-mesenchymal transition (EMT) by suppressing P2Y receptors-dependent Ca2+ increase and nuclear factor-κB (NF-KB) signaling in A549 cells. Methods: A549 cells were pretreated with emodin before stimulation with ATP for the indicated time. Then, intracellular Ca2+ concentration ([Ca2+]i) was measured by Fluo-8/AM staining. Cell proliferation and cell cycle progression were tested by CCK8 assay and flow cytometry In addition, wound healing and western blot were performed to determine cell migration and related protein levels (Bcl-2, Bax, claudin-1, NF-κB). Results: Emodin blunted ATP/UTP-induced increase of [Ca2+]i and cell proliferation concentration-dependently Meanwhile, it decreased ATP-induced cells accumulation in the S phase. Furthermore, emodin altered protein abundance of Bcl-2, Bax and claudin-1 and attenuated EMT caused by ATP. Such ATP-induced cellular reactions were also inhibited by a nonselective P2Y receptors antagonist, suramin, in a similar way to emodin. Besides, emodin could inhibit activation of NF-κB, thus suppressed ATP-induced proliferation, migration and EMT. Conclusion: Our results demonstrated that emodin inhibits ATP-induced proliferation, migration, EMT by suppressing P2Y receptors-mediated [Ca2+]i increase and NF-κB signaling in A549 cells.

Published

2017

44. Suramin Inhibits Osteoarthritic Cartilage Degradation by Increasing Extracellular Levels of Chondroprotective Tissue Inhibitor of Metalloproteinases 3

Author

Chanalaris, Anastasios, Doherty, Christine, Marsden, Brian D, Bambridge, Gabriel, Wren, Stephen P, Nagase, Hideaki, and Troeberg, Linda

Subjects

Tissue Inhibitor of Metalloproteinase-3, Dose-Response Relationship, Drug, Swine, Articles, Suramin, chemistry, Cartilage, Chondrocytes, HEK293 Cells, Organ Culture Techniques, Cell Line, Tumor, Osteoarthritis, Animals, Humans, Extracellular Space, Protein Binding

Abstract

Osteoarthritis is a common degenerative joint disease for which no disease-modifying drugs are currently available. Attempts to treat the disease with small molecule inhibitors of the metalloproteinases that degrade the cartilage matrix have been hampered by a lack of specificity. We aimed to inhibit cartilage degradation by augmenting levels of the endogenous metalloproteinase inhibitor, tissue inhibitor of metalloproteinases (TIMP)-3, through blocking its interaction with the endocytic scavenger receptor, low-density lipoprotein receptor-related protein 1 (LRP1). We discovered that suramin (C51H40N6O23S6) bound to TIMP-3 with a KD value of 1.9 ± 0.2 nM and inhibited its endocytosis via LRP1, thus increasing extracellular levels of TIMP-3 and inhibiting cartilage degradation by the TIMP-3 target enzyme, adamalysin-like metalloproteinase with thrombospondin motifs 5. NF279 (8,8'-[carbonylbis(imino-4,1-phenylenecarbonylimino-4,1-phenylenecarbonylimino)]bis-1,3,5-naphthalenetrisulfonic acid hexasodium salt), a structural analog of suramin, has an increased affinity for TIMP-3 and increased ability to inhibit TIMP-3 endocytosis and protect cartilage. Suramin is thus a promising scaffold for the development of novel therapeutics to increase TIMP-3 levels and inhibit cartilage degradation in osteoarthritis.

Published

2017

45. Impact of FDA-Approved Drugs on the Prostaglandin Transporter OATP2A1/SLCO2A1

Author

Shunsuke Kamo, Ikumi Tamai, Yoshinobu Nakamura, Tomoka Gose, Rika Aotani, and Takeo Nakanishi

Subjects

0301 basic medicine, Losartan Potassium, Drug, Suramin, media_common.quotation_subject, Organic Anion Transporters, Pharmaceutical Science, Antineoplastic Agents, Pharmacology, 030226 pharmacology & pharmacy, Pranlukast, Cell Line, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine, Anthranilic acid, Humans, IC50, SLCO2A1, media_common, PROSTAGLANDIN TRANSPORTER, biology, Anti-Inflammatory Agents, Non-Steroidal, Biological Transport, Fluoresceins, HEK293 Cells, 030104 developmental biology, chemistry, Prostaglandins, biology.protein, medicine.drug

Abstract

To understand interaction of drugs with the prostaglandin transporter OATP2A1/SLCO2A1 that regulates disposition of prostaglandins, we explored the impact of 636 drugs in an FDA-approved drug library on 6-carboxyfluorescein (6-CF) uptake by OATP2A1-expressing HEK293 cells (HEK/2A1). Fifty-one and 10 drugs were found to inhibit and enhance 6-CF uptake by more than 50%, respectively. Effect of the 51 drugs on 6-CF uptake was positively correlated with that on PGE2 uptake (r = 0.64, p < 0.001). Among those, 5 drugs not structurally related to prostaglandins, suramin, pranlukast, zafirlukast, olmesartan medoxomil, and losartan potassium, exhibited more than 90% PGE2 uptake inhibition. Inhibitory affinity of suramin to OATP2A1 was the highest (IC50,2A1 of 0.17 μM), and its IC50 values to MRP4-mediated PGE2 transport (IC50,MRP4) and PGE2 synthesis in human U-937 cells treated with phorbol 12-myristate 13-acetate (IC50,Syn) were 73.6 and 336.7 times higher than IC50,2A1, respectively. Moreover, structure-activity relationship study in 29 nonsteroidal anti-inflammatory drugs contained in the library displayed inhibitory activities of anthranilic acid derivatives, but enhancing effects of propionic acid derivatives. These results demonstrate that suramin is a potent selective inhibitor of OATP2A1, providing a comprehensive information about drugs in clinical use that interact with OATP2A1.

Published

2017

46. Synergistic effects of combination treatment using EGCG and suramin against the chikungunya virus

Author

Yu-Ming Wang, Jeng-Wei Lu, Yi-Jung Ho, Chun-Yu Liang, Chang-Chi Lin, Ming-Kuan Hu, Po-Shiuan Hsieh, Zhiyuan Gong, and Shih-Ming Huang

Subjects

0301 basic medicine, viruses, Suramin, 030106 microbiology, Biophysics, Biology, medicine.disease_cause, Antiviral Agents, complex mixtures, Biochemistry, Arbovirus, Catechin, Virus, Microbiology, 03 medical and health sciences, Combined treatment, Viral entry, medicine, Humans, heterocyclic compounds, Viral rna, Chikungunya, Molecular Biology, Cytopathic effect, Dose-Response Relationship, Drug, food and beverages, virus diseases, Drug Synergism, Cell Biology, medicine.disease, Virology, Drug Combinations, Treatment Outcome, 030104 developmental biology, Chikungunya Fever, Chikungunya virus, medicine.drug

Abstract

Chikungunya is a severe disease that results from infection with the chikungunya virus (CHIKV), an arbovirus. Thus, we (1) explored a new approach to combining previously researched drugs that have shown the potential to inhibit CHIKV infection; and (2) demonstrated the antiviral effects of (-)-Epigallocatechin-3-gallate (EGCG) and the underlying mechanisms. Specifically, we used U2OS cells infected with CHIVK to assess the synergistic antiviral activities of EGCG and suramin. EGCG presented the ability to inhibit the viral RNA, progeny yield, and cytopathic effect (CPE) of CHIKV and also demonstrated the ability to protect against virus entry, replication, and release. Moreover, the results confirmed that EGCG and suramin can have synergistic effects against CHIKV strain S27 infection and two other clinical isolates of CHIKV. Our findings suggest that treatment with a combination of EGCG and suramin could provide a basis for the development of novel stretages against CHIKV infection.

Published

2017

47. A small-molecule screen identifies the antitrypanosomal agent suramin and analogues NF023 and NF449 as inhibitors of STAT5a/b

Author

Angela Berg and Thorsten Berg

Subjects

0301 basic medicine, animal structures, Suramin, High-throughput screening, Clinical Biochemistry, Pharmaceutical Science, Pharmacology, SH2 domain, Biochemistry, Protein–protein interaction, Small Molecule Libraries, Structure-Activity Relationship, 03 medical and health sciences, 0302 clinical medicine, Drug Discovery, STAT5 Transcription Factor, medicine, Humans, Molecular Biology, Transcription factor, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Tumor Suppressor Proteins, Benzenesulfonates, Organic Chemistry, food and beverages, Small molecule, In vitro, High-Throughput Screening Assays, 030104 developmental biology, 030220 oncology & carcinogenesis, STAT protein, Molecular Medicine, medicine.drug

Abstract

The transcription factor STAT5a is a potential target for tumor therapy. We present a fluorescence polarization-based, high-throughput screen of chemical libraries containing natural products and known bioactive molecules, for the identification of small-molecule inhibitors of the STAT5a SH2 domain. This screen identified suramin, a drug used to treat African trypanosomiasis, and its analogues NF023 and NF449 as inhibitors of the SH2 domains of STAT5a/b. Our data extend the known in vitro targets of suramin and analogues to include members of the STAT protein family.

Published

2017

48. Viability of SH-SY5Y cells is associated with purinergic P2 receptor expression alterations

Author

Uğur Akcan, Murat Giriş, Vuslat Yilmaz, Arda Örçen, Erdem Tüzün, and Gaye Erten

Subjects

Male, 0301 basic medicine, P2Y receptor, SH-SY5Y, Cell Survival, Immunoblotting, Suramin, Biology, P2 receptor, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, P2Y12, Cell Line, Tumor, Purinergic P2 Receptor Antagonists, Animals, Humans, Protein Isoforms, PPADS, Viability assay, Receptor, General Environmental Science, Receptors, Purinergic P2, Reverse Transcriptase Polymerase Chain Reaction, Purinergic receptor, Age Factors, Brain, Flow Cytometry, Molecular biology, Gene Expression Regulation, Neoplastic, Mice, Inbred C57BL, 030104 developmental biology, Neurology, chemistry, Pyridoxal Phosphate, 030217 neurology & neurosurgery

Abstract

To investigate the role of metabotrophic purinergic P2Y receptors in neuroblastoma cell survival, expression of P2 receptors by normal mouse (C57BL/6) brain and human neuroblastoma SH-SY5Y cells was investigated by Western blot and real time PCR studies. Viability of SH-SY5Y cells treated with purinergic receptor antagonists suramin and pyridoxal-phosphate-6-azophenyl-2',4'-disulfonate (PPADS) was evaluated by MTT assay and flow cytometry. In the brain samples of C57BL/6 mice, expressions of P2Y4 and P2X7 were significantly reduced, whereas that of P2Y1 was significantly elevated in an age-dependent manner. SH-SY5Y cell viability was significantly reduced and necrotic cell rates were mildly increased by 400 μM suramin and 100 μM PPADS treatment. Antagonist treatment downregulated P2Y1, P2Y2 and P2Y4 and upregulated P2Y6, P2Y12 and P2X7 mRNA levels in SH-SY5Y cells on the 24th hour. These alterations were abolished for all P2 receptors except P2Y1 in the 48th hour. P2Y receptors are expressed by both normal mouse brain and human neuroblastoma cells. Purinergic receptor antagonism interferes with neuroblastoma viability through elevation of necrotic cell death and modulation of P2 receptor expression. P2Y receptors might thus be useful targets for future anti-tumor treatment trials.

Published

2017

49. Evaluation of the Performance of an Ophthalmic Thermosensitive Hydrogel Containing Combination of Suramin and Bevacizumab

Author

Daniel Alberto Allemandi, Emiliano López, Santiago Daniel Palma, Daniela Alejandra Quinteros, Belkys A. Maletto, Juan E Gallo, and Juan Lucio Silva Couto

Subjects

Controlled Release, Farmacología y Farmacia, medicine.medical_specialty, CIENCIAS MÉDICAS Y DE LA SALUD, Thermosensitive Hydrogels, Bevacizumab, Suramin, Suramab, Administration, Ophthalmic, Angiogenesis Inhibitors, Aqueous dispersion, Poloxamer, Pharmacology, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, In vivo, Drug Discovery, medicine, Sprague dawley rats, Animals, Humans, Corneal Neovascularization, Neovascularization, Chemistry, Temperature, Hydrogels, Controlled release, Rats, Surgery, Medicina Básica, Drug Combinations, Suramine, Antiangiogenic effect, 030221 ophthalmology & optometry, 030217 neurology & neurosurgery, medicine.drug

Abstract

Suramab (SUM) is a new pharmaceutical combination made up of suramine (SUR) and bevacizumab (BVM), which showed a high synergistic effect when administered jointly. As the pharmaceutical vehicle, poloxamer aqueous dispersions were used since this system is able to maintain their fluidity at low temperatures (35�C). In the present study we aimed at evaluating the effect of Poloxamer to prolong the effect of SUM. These formulations were characterized using rheological, biopharmaceutical (drug release) and morphological (SEM) technique. Corneal NV was induced in Sprague Dawley rats Corneal. At 15 days of follow up animals were sacrificed and perfused with black drawing ink. Digital photographs were taken and the area of neovascularisation (ANV) was calculated using the image programmed. The rheological behavior was influenced by the addition of drugs, resulting in a decrease in the gelation temperature (Tsol/gel). Both drugs were released from poloxamer gels by means of an anomalous mechanism. However, BVM was released faster than SUR, with their combination (SUM) to appearing to reduce delivery, probably due to interactions between the drugs or with the polymeric matrix. The in vivo studies showed that SUM-poloxamer gel was able to increase the corneal antiangiogenic effect compared to the SUM solution and BVM alone at 15 days of follow-up. Furthermore no injurious effects were observed in the histological tissue examination after drug administration. The presence of Poloxamer, known to modulate control release of biological agents, seems to have a favorable effect on SUM subconjunctival administered. Fil: Quinteros, Daniela Alejandra. Consejo Nacional de Investigaciones Científicas y Técnicas. Centro Científico Tecnológico Conicet - Córdoba. Unidad de Investigación y Desarrollo en Tecnología Farmacéutica. Universidad Nacional de Córdoba. Facultad de Ciencias Químicas. Unidad de Investigación y Desarrollo en Tecnología Farmacéutica; Argentina Fil: Lopez, Emiliano Sebastian. Universidad Austral. Facultad de Ciencias Biomédicas; Argentina. Consejo Nacional de Investigaciones Científicas y Técnicas; Argentina Fil: Silva Couto, Juan Lucio. Universidad Austral. Facultad de Ciencias Biomédicas; Argentina Fil: Maletto, Belkys Angélica. Consejo Nacional de Investigaciones Científicas y Técnicas. Centro Científico Tecnológico Córdoba. Centro de Investigaciones en Bioquímica Clínica e Inmunología; Argentina Fil: Allemandi, Daniel Alberto. Consejo Nacional de Investigaciones Científicas y Técnicas. Centro Científico Tecnológico Conicet - Córdoba. Unidad de Investigación y Desarrollo en Tecnología Farmacéutica. Universidad Nacional de Córdoba. Facultad de Ciencias Químicas. Unidad de Investigación y Desarrollo en Tecnología Farmacéutica; Argentina Fil: Palma, Santiago Daniel. Consejo Nacional de Investigaciones Científicas y Técnicas. Centro Científico Tecnológico Conicet - Córdoba. Unidad de Investigación y Desarrollo en Tecnología Farmacéutica. Universidad Nacional de Córdoba. Facultad de Ciencias Químicas. Unidad de Investigación y Desarrollo en Tecnología Farmacéutica; Argentina Fil: Gallo, Juan Eduardo Maria. Universidad Austral. Facultad de Ciencias Biomédicas; Argentina. Consejo Nacional de Investigaciones Científicas y Técnicas; Argentina

Published

2017

50. A fluorescence-based high-throughput assay to identify inhibitors of tyrosylprotein sulfotransferase activity

Author

Yan Wang, Wenbo Zhou, Jiashu Xie, and Robert J. Geraghty

Subjects

0301 basic medicine, Sulfotransferase, Biophysics, Peptide, Suramin, Biochemistry, Fluorescence, Substrate Specificity, Inhibitory Concentration 50, 03 medical and health sciences, chemistry.chemical_compound, Tandem Mass Spectrometry, Combinatorial Chemistry Techniques, Humans, Tyrosine, Sulfuryl, Cell adhesion, Receptor, Molecular Biology, chemistry.chemical_classification, Dose-Response Relationship, Drug, 030102 biochemistry & molecular biology, Cell Biology, Small molecule, Isoenzymes, Molecular Docking Simulation, Kinetics, 030104 developmental biology, Enzyme, chemistry, Sulfotransferases, Peptides, Baculoviridae, Chromatography, Liquid

Abstract

Tyrosylprotein sulfotransferases (TPSTs) are Golgi-resident enzymes that catalyze the transfer of a sulfuryl group to the side chain hydroxyl of tyrosine residues. Sulfotyrosine residues are involved in protein-protein interactions in the extracellular space. These interactions are important for chemokines to bind cognate receptor, for cell adhesion and trafficking, and for pathogen entry into cells. To better understand the role of TPSTs in cellular processes and disease states, we are interested in identifying small molecules to modulate TPST activity in experimental systems. Towards that end, we developed a fluorescent peptide assay for TPST2 activity. Here, we demonstrate that this assay can be used to screen the 1280 compound LOPAC library in a 384-well format and in a high-throughput manner. We identified 19 primary hits for a hit rate of 1.5%. Three of the primary hits were verified by dose-response assay and confirmed as inhibitors by a secondary mass spectrometry assay for TPST activity. One hit, suramin, possessed inhibitory properties consistent with a competitive inhibitor of substrate binding and molecular docking revealed a good fit into the TPST2 substrate-binding pocket. This assay can be used to screen larger libraries to identify small molecules that inhibit TPST sulfotransferase activity.

Published

2017