Your search keyword '"Virus Release drug effects"' showing total 144 results

51. MG-132 reduces virus release in Bovine herpesvirus-1 infection.

Author

Fiorito F, Iovane V, Cantiello A, Marullo A, De Martino L, and Iovane G

Subjects

Animals, Apoptosis, Autophagy, Cattle, Cell Line, NF-kappa B metabolism, Herpesvirus 1, Bovine physiology, Leupeptins pharmacology, Proteasome Inhibitors pharmacology, Virus Release drug effects

Abstract

Bovine herpesvirus 1 (BoHV-1) can provoke conjunctivitis, abortions and shipping fever. BoHV-1 infection can also cause immunosuppression and increased susceptibility to secondary bacterial infections, leading to pneumonia and occasionally to death. Herein, we investigated the influence of MG-132, a proteasome inhibitor, on BoHV-1 infection in bovine kidney (MDBK) cells. Infection of MDBK cells with BoHV-1 induces apoptotic cell death that enhances virus release. Whereas, MG-132 inhibited virus-induced apoptosis and stimulated autophagy. Protein expression of viral infected cell protein 0 (bICP0), which is constitutively expressed during infection and is able to stimulate Nuclear factor kappa B (NF-κB), was completely inhibited by MG-132. These results were accompanied by a significant delay in the NF-κB activation. Interestingly, the efficient virus release provoked by BoHV-1-induced apoptosis was significantly reduced by MG-132. Overall, this study suggests that MG-132, through the activation of autophagy, may limit BoHV-1 replication during productive infection, by providing an antiviral defense mechanism.

Published

2017

52. Sorafenib Impedes Rift Valley Fever Virus Egress by Inhibiting Valosin-Containing Protein Function in the Cellular Secretory Pathway.

Author

Brahms A, Mudhasani R, Pinkham C, Kota K, Nasar F, Zamani R, Bavari S, and Kehn-Hall K

Subjects

Adenosine Triphosphatases genetics, Animals, Carcinoma, Hepatocellular drug therapy, Carcinoma, Hepatocellular metabolism, Carcinoma, Hepatocellular virology, Cell Cycle Proteins genetics, Chlorocebus aethiops, Humans, Liver Neoplasms drug therapy, Liver Neoplasms metabolism, Liver Neoplasms virology, Niacinamide pharmacology, Rift Valley Fever metabolism, Rift Valley Fever virology, Rift Valley fever virus drug effects, Sorafenib, Tumor Cells, Cultured, Valosin Containing Protein, Vero Cells, Virion drug effects, Virus Replication drug effects, Adenosine Triphosphatases metabolism, Cell Cycle Proteins metabolism, Niacinamide analogs & derivatives, Phenylurea Compounds pharmacology, Rift Valley Fever drug therapy, Rift Valley fever virus physiology, Secretory Pathway drug effects, Virus Release drug effects

Abstract

There is an urgent need for therapeutic development to combat infections caused by Rift Valley fever virus (RVFV), which causes devastating disease in both humans and animals. In an effort to repurpose drugs for RVFV treatment, our previous studies screened a library of FDA-approved drugs. The most promising candidate identified was the hepatocellular and renal cell carcinoma drug sorafenib. Mechanism-of-action studies indicated that sorafenib targeted a late stage in virus infection and caused a buildup of virions within cells. In addition, small interfering RNA (siRNA) knockdown studies suggested that nonclassical targets of sorafenib are important for the propagation of RVFV. Here we extend our previous findings to identify the mechanism by which sorafenib inhibits the release of RVFV virions from the cell. Confocal microscopy imaging revealed that glycoprotein Gn colocalizes and accumulates within the endoplasmic reticulum (ER) and the transport of Gn from the Golgi complex to the host cell membrane is reduced. Transmission electron microscopy demonstrated that sorafenib caused virions to be present inside large vacuoles inside the cells. p97/valosin-containing protein (VCP), which is involved in membrane remodeling in the secretory pathway and a known target of sorafenib, was found to be important for RVFV egress. Knockdown of VCP resulted in decreased RVFV replication, reduced Gn Golgi complex localization, and increased Gn ER accumulation. The intracellular accumulation of RVFV virions was also observed in cells transfected with siRNA targeting VCP. Collectively, these data indicate that sorafenib causes a disruption in viral egress by targeting VCP and the secretory pathway, resulting in a buildup of virions within dilated ER vesicles. IMPORTANCE In humans, symptoms of RVFV infection mainly include a self-limiting febrile illness. However, in some cases, infected individuals can also experience hemorrhagic fever, neurological disorders, liver failure, and blindness, which could collectively be lethal. The ability of RVFV to expand geographically outside sub-Saharan Africa is of concern, particularly to the Americas, where native mosquito species are capable of virus transmission. Currently, there are no FDA-approved therapeutics to treat RVFV infection, and thus, there is an urgent need to understand the mechanisms by which the virus hijacks the host cell machinery to replicate. The significance of our research is in identifying the cellular target of sorafenib that inhibits RVFV propagation, so that this information can be used as a tool for the further development of therapeutics used to treat RVFV infection., (Copyright © 2017 American Society for Microbiology.)

Published

2017

53. A clue to unprecedented strategy to HIV eradication: "Lock-in and apoptosis".

Author

Tateishi H, Monde K, Anraku K, Koga R, Hayashi Y, Ciftci HI, DeMirci H, Higashi T, Motoyama K, Arima H, Otsuka M, and Fujita M

Subjects

Anti-HIV Agents chemistry, Cell Membrane virology, Cell Survival drug effects, Cytoplasm virology, Disease Eradication, HIV Infections prevention & control, HIV-1 drug effects, HIV-1 metabolism, HeLa Cells, Humans, Inositol Phosphates chemical synthesis, Inositol Phosphates chemistry, Jurkat Cells, Molecular Structure, Small Molecule Libraries chemical synthesis, Small Molecule Libraries chemistry, Stereoisomerism, Virus Activation, Virus Latency drug effects, Virus Release drug effects, Anti-HIV Agents chemical synthesis, Anti-HIV Agents pharmacology, HIV-1 physiology, Inositol Phosphates pharmacology, Protein Precursors antagonists & inhibitors, Small Molecule Libraries pharmacology

Abstract

Despite the development of antiretroviral therapy against HIV, eradication of the virus from the body, as a means to a cure, remains in progress. A "kick and kill" strategy proposes "kick" of the latent HIV to an active HIV to eventually be "killed". Latency-reverting agents that can perform the "kick" function are under development and have shown promise. Management of the infected cells not to produce virions after the "kick" step is important to this strategy. Here we show that a newly synthesized compound, L-HIPPO, captures the HIV-1 protein Pr55 Gag and intercepts its function to translocate the virus from the cytoplasm to the plasma membrane leading to virion budding. The infecting virus thus "locked-in" subsequently induces apoptosis of the host cells. This "lock-in and apoptosis" approach performed by our novel compound in HIV-infected cells provides a means to bridge the gap between the "kick" and "kill" steps of this eradication strategy. By building upon previous progress in latency reverting agents, our compound appears to provide a promising step toward the goal of HIV eradication from the body.

Published

2017

54. Antiviral effects of Retro-2 cycl and Retro-2.1 against Enterovirus 71 in vitro and in vivo.

Author

Dai W, Wu Y, Bi J, Lu X, Hou A, Zhou Y, Sun B, Kong W, Barbier J, Cintrat JC, Gao F, Gillet D, Su W, and Jiang C

Subjects

Animals, Antiviral Agents toxicity, Benzamides toxicity, Cell Line, Cell Survival drug effects, Disease Models, Animal, Enterovirus A, Human physiology, Humans, Inhibitory Concentration 50, Mice, Inbred BALB C, Microbial Sensitivity Tests, Survival Analysis, Thiophenes toxicity, Antiviral Agents administration & dosage, Antiviral Agents pharmacology, Benzamides administration & dosage, Benzamides pharmacology, Enterovirus A, Human drug effects, Hand, Foot and Mouth Disease drug therapy, Thiophenes administration & dosage, Thiophenes pharmacology, Virus Release drug effects

Abstract

Enterovirus 71 (EV71) is one of the causative pathogens of hand, foot and mouth disease (HFMD), especially the form associated with fatal neurological disorders. Sustained outbreaks of EV71 infections remain a serious health threat worldwide. However, no antiviral agent against EV71 for clinical therapy has been approved. Retro-2 cycl and Retro-2.1 are inhibitors of several pathogens specifically targeting the intracellular vesicle transport, which also participates in the EV71 lifecycle processes including progeny virus release. Here, we reported that Retro-2 cycl and Retro-2.1, respectively, could inhibit EV71 infection with 50% effective concentrations of 12.56 μM and 0.05 μM in a cytopathic effect inhibition assay and showed relatively low cytotoxicity with 50% cytotoxicity concentrations of more than 500 μM and 267.80 μM. Preliminary mechanism studies revealed that Retro-2 cycl and Retro-2.1 did not inhibit EV71 protein synthesis or RNA replication but could block progeny EV71 release specifically. Furthermore, administration of Retro-2 cycl at the dose of 10 mg/kg significantly protected 90% of newborn mice from lethal EV71 challenge. Consequently, our results for the first time identified Retro-2 cycl and Retro-2.1 as effective inhibitors of EV71 as well as lead compounds, which would contribute to anti-EV71 drug development. We also identified progeny virus release and the intracellular vesicle transport as antiviral targets for EV71., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

55. Inhibition of highly pathogenic avian influenza (HPAI) virus by a peptide derived from vFLIP through its direct destabilization of viruses.

Author

Moon HJ, Nikapitiya C, Lee HC, Park ME, Kim JH, Kim TH, Yoon JE, Cho WK, Ma JY, Kim CJ, Jung JU, and Lee JS

Subjects

Animals, Antiviral Agents isolation & purification, Disease Models, Animal, Dogs, Influenza A virus physiology, Lung virology, Madin Darby Canine Kidney Cells, Mice, Inbred BALB C, Oligopeptides isolation & purification, Orthomyxoviridae Infections pathology, Orthomyxoviridae Infections prevention & control, Respiratory Syncytial Viruses drug effects, Respiratory Syncytial Viruses physiology, Survival Analysis, Treatment Outcome, Vesiculovirus drug effects, Vesiculovirus physiology, Viral Load, Virus Internalization drug effects, Virus Release drug effects, Antiviral Agents metabolism, Influenza A virus drug effects, Oligopeptides metabolism, Viral Proteins metabolism, Virus Replication drug effects

Abstract

The antiviral activities of synthesized Kα2-helix peptide, which was derived from the viral FLICE-like inhibitor protein (vFLIP) of Kaposi's sarcoma-associated herpesvirus (KSHV), against influenza A virus (IAV) were investigated in vitro and in vivo, and mechanisms of action were suggested. In addition to the robust autophagy activity of the Kα2-helix peptide, the present study showed that treatment with the Kα2 peptide fused with the TAT peptide significantly inhibited IAV replication and transmission. Moreover, TAT-Kα2 peptide protected the mice, that were challenged with lethal doses of highly pathogenic influenza A H5N1 or H1N1 viruses. Mechanistically, we found that TAT-Kα2 peptide destabilized the viral membranes, depending on their lipid composition of the viral envelop. In addition to IAV, the Kα2 peptide inhibited infections with enveloped viruses, such as Vesicular Stomatitis Virus (VSV) and Respiratory Syncytial Virus (RSV), without cytotoxicity. These results suggest that TAT-Kα2 peptide is a potential antiviral agent for controlling emerging or re-emerging enveloped viruses, particularly diverse subtypes of IAVs.

Published

2017

56. Suramin inhibits Zika virus replication by interfering with virus attachment and release of infectious particles.

Author

Albulescu IC, Kovacikova K, Tas A, Snijder EJ, and van Hemert MJ

Subjects

Animals, Chlorocebus aethiops, Cytopathogenic Effect, Viral drug effects, DNA Replication drug effects, Flavivirus drug effects, Glycosylation drug effects, Mycophenolic Acid administration & dosage, Mycophenolic Acid antagonists & inhibitors, RNA, Viral analysis, RNA, Viral biosynthesis, RNA, Viral drug effects, Suramin administration & dosage, Time Factors, Vero Cells, Virus Internalization drug effects, Zika Virus growth & development, Zika Virus physiology, Zika Virus Infection drug therapy, Zika Virus Infection virology, Suramin antagonists & inhibitors, Virion drug effects, Virus Attachment drug effects, Virus Release drug effects, Virus Replication drug effects, Zika Virus drug effects

Abstract

Zika virus (ZIKV) is a mosquito-borne flavivirus that mostly causes asymptomatic infections or mild disease characterized by low-grade fever, rash, conjunctivitis, and malaise. However, the recent massive ZIKV epidemics in the Americas have also linked ZIKV infection to fetal malformations like microcephaly and Guillain-Barré syndrome in adults, and have uncovered previously unrecognized routes of vertical and sexual transmission. Here we describe inhibition of ZIKV replication by suramin, originally an anti-parasitic drug, which was more recently shown to inhibit multiple viruses. In cell culture-based assays, using reduction of cytopathic effect as read-out, suramin had an EC 50 of ∼40 μM and a selectivity index of 48. In single replication cycle experiments, suramin treatment also caused a strong dose-dependent decrease in intracellular ZIKV RNA levels and a >3-log reduction in infectious progeny titers. Time-of-addition experiments revealed that suramin inhibits a very early step of the replication cycle as well as the release of infectious progeny. Only during the first 2 h of infection suramin treatment strongly reduced the fraction of cells that became infected with ZIKV, suggesting the drug affects virus binding/entry. Binding experiments at 4 °C using 35 S-labeled ZIKV demonstrated that suramin interferes with attachment to host cells. When suramin treatment was initiated post-entry, viral RNA synthesis was unaffected, while both the release of genomes and the infectivity of ZIKV were reduced. This suggests the compound also affects virion biogenesis, possibly by interfering with glycosylation and the maturation of ZIKV during its traffic through the secretory pathway. The inhibitory effect of suramin on ZIKV attachment and virion biogenesis and its broad-spectrum activity warrant further evaluation of this compound as a potential therapeutic., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

57. Discovery of Novel Small-Molecule Inhibitors of LIM Domain Kinase for Inhibiting HIV-1.

Author

Yi F, Guo J, Dabbagh D, Spear M, He S, Kehn-Hall K, Fontenot J, Yin Y, Bibian M, Park CM, Zheng K, Park HJ, Soloveva V, Gharaibeh D, Retterer C, Zamani R, Pitt ML, Naughton J, Jiang Y, Shang H, Hakami RM, Ling B, Young JAT, Bavari S, Xu X, Feng Y, and Wu Y

Subjects

Antiviral Agents chemical synthesis, Antiviral Agents isolation & purification, Cells, Cultured, Ebolavirus drug effects, Encephalitis Virus, Venezuelan Equine drug effects, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors isolation & purification, HIV-1 physiology, Herpesvirus 1, Human drug effects, Humans, Microbial Sensitivity Tests, Molecular Docking Simulation, Rift Valley fever virus drug effects, Antiviral Agents pharmacology, Enzyme Inhibitors pharmacology, HIV-1 drug effects, Lim Kinases antagonists & inhibitors, Virus Release drug effects, Virus Replication drug effects

Abstract

A dynamic actin cytoskeleton is necessary for viral entry, intracellular migration, and virion release. For HIV-1 infection, during entry, the virus triggers early actin activity by hijacking chemokine coreceptor signaling, which activates a host dependency factor, cofilin, and its kinase, the LIM domain kinase (LIMK). Although knockdown of human LIM domain kinase 1 (LIMK1) with short hairpin RNA (shRNA) inhibits HIV infection, no specific small-molecule inhibitor of LIMK has been available. Here, we describe the design and discovery of novel classes of small-molecule inhibitors of LIMK for inhibiting HIV infection. We identified R10015 as a lead compound that blocks LIMK activity by binding to the ATP-binding pocket. R10015 specifically blocks viral DNA synthesis, nuclear migration, and virion release. In addition, R10015 inhibits multiple viruses, including Zaire ebolavirus (EBOV), Rift Valley fever virus (RVFV), Venezuelan equine encephalitis virus (VEEV), and herpes simplex virus 1 (HSV-1), suggesting that LIMK inhibitors could be developed as a new class of broad-spectrum antiviral drugs. IMPORTANCE The actin cytoskeleton is a structure that gives the cell shape and the ability to migrate. Viruses frequently rely on actin dynamics for entry and intracellular migration. In cells, actin dynamics are regulated by kinases, such as the LIM domain kinase (LIMK), which regulates actin activity through phosphorylation of cofilin, an actin-depolymerizing factor. Recent studies have found that LIMK/cofilin are targeted by viruses such as HIV-1 for propelling viral intracellular migration. Although inhibiting LIMK1 expression blocks HIV-1 infection, no highly specific LIMK inhibitor is available. This study describes the design, medicinal synthesis, and discovery of small-molecule LIMK inhibitors for blocking HIV-1 and several other viruses and emphasizes the feasibility of developing LIMK inhibitors as broad-spectrum antiviral drugs., (Copyright © 2017 Yi et al.)

Published

2017

58. An Immortalized Human Dorsal Root Ganglion Cell Line Provides a Novel Context To Study Herpes Simplex Virus 1 Latency and Reactivation.

Author

Thellman NM, Botting C, Madaj Z, and Triezenberg SJ

Subjects

Acyclovir pharmacology, Antiviral Agents pharmacology, Cell Culture Techniques, Cell Line, Doxycycline pharmacology, Ganglia, Spinal drug effects, Gene Expression Regulation, Viral, Herpes Simplex virology, Humans, Membrane Glycoproteins genetics, Nerve Growth Factor pharmacology, Peripherins genetics, Protein-Tyrosine Kinases genetics, Proto-Oncogene Proteins c-ret genetics, Receptor, trkA genetics, Receptor, trkB, Receptor, trkC genetics, Sensory Receptor Cells physiology, Virus Release drug effects, Virus Replication drug effects, Ganglia, Spinal virology, Herpesvirus 1, Human physiology, Sensory Receptor Cells virology, Virus Activation, Virus Latency

Abstract

A defining characteristic of alphaherpesviruses is the establishment of lifelong latency in host sensory ganglia with occasional reactivation causing recurrent lytic infections. As an alternative to rodent models, we explored the use of an immortalized cell line derived from human dorsal root ganglia. HD10.6 cells proliferate by virtue of a transduced tetracycline-regulated v- myc oncogene. In the presence of doxycycline, HD10.6 cells mature to exhibit neuronal morphology and express sensory neuron-associated markers such as neurotrophin receptors TrkA, TrkB, TrkC, and RET and the sensory neurofilament peripherin. Infection of mature HD10.6 neurons by herpes simplex virus 1 (HSV-1) results in a delayed but productive infection. However, infection at a low multiplicity of infection (MOI) in the presence of acyclovir results in a quiescent infection resembling latency in which viral genomes are retained in a low number of neurons, viral gene expression is minimal, and infectious virus is not released. At least some of the quiescent viral genomes retain the capacity to reactivate, resulting in viral DNA replication and release of infectious virus. Reactivation can be induced by depletion of nerve growth factor; other commonly used reactivation stimuli have no significant effect. IMPORTANCE Infections by herpes simplex viruses (HSV) cause painful cold sores or genital lesions in many people; less often, they affect the eye or even the brain. After the initial infection, the virus remains inactive or latent in nerve cells that sense the region where that infection occurred. To learn how virus maintains and reactivates from latency, studies are done in neurons taken from rodents or in whole animals to preserve the full context of infection. However, some cellular mechanisms involved in HSV infection in rodents are different from those in humans. We describe the use of a human cell line that has the properties of a sensory neuron. HSV infection in these cultured cells shows the properties expected for a latent infection, including reactivation to produce newly infectious virus. Thus, we now have a cell culture model for latency that is derived from the normal host for this virus., (Copyright © 2017 American Society for Microbiology.)

Published

2017

59. Combination antiretroviral therapy and cell-cell spread of wild-type and drug-resistant human immunodeficiency virus-1.

Author

Titanji BK, Pillay D, and Jolly C

Subjects

Cell Line, HIV Protease Inhibitors pharmacology, Humans, Reverse Transcriptase Inhibitors pharmacology, T-Lymphocytes virology, Virus Cultivation, Anti-Retroviral Agents pharmacology, Antiretroviral Therapy, Highly Active, Drug Resistance, Viral, HIV-1 drug effects, HIV-1 physiology, Virus Internalization drug effects, Virus Release drug effects

Abstract

Human immunodeficiency virus-1 (HIV-1) disseminates between T cells either by cell-free infection or by highly efficient direct cell-cell spread. The high local multiplicity that characterizes cell-cell infection causes variability in the effectiveness of antiretroviral drugs applied as single agents. Whereas protease inhibitors (PIs) are effective inhibitors of HIV-1 cell-cell and cell-free infection, some reverse transcriptase inhibitors (RTIs) show reduced potency; however, antiretrovirals are not administered as single agents and are used clinically as combination antiretroviral therapy (cART). Here we explored the efficacy of PI- and RTI-based cART against cell-cell spread of wild-type and drug-resistant HIV-1 strains. Using a quantitative assay to measure cell-cell spread of HIV-1 between T cells, we evaluated the efficacy of different clinically relevant drug combinations. We show that combining PIs and RTIs improves the potency of inhibition of HIV-1 and effectively blocks both cell-free and cell-cell spread. Combining drugs that alone are poor inhibitors of cell-cell spread markedly improves HIV-1 inhibition, demonstrating that clinically relevant combinations of ART can inhibit this mode of HIV-1 spread. Furthermore, comparison of wild-type and drug-resistant viruses reveals that PI- and RTI-resistant viruses have a replicative advantage over wild-type virus when spreading by cell-cell means in the presence of cART, suggesting that in the context of inadequate drug combinations or drug resistance, cell-cell spread could potentially allow for ongoing viral replication.

Published

2017

60. A Novel Inhibitor IDPP Interferes with Entry and Egress of HCV by Targeting Glycoprotein E1 in a Genotype-Specific Manner.

Author

Lee M, Yang J, Jo E, Lee JY, Kim HY, Bartenschlager R, Shin EC, Bae YS, and Windisch MP

Subjects

Amino Acid Substitution, Antiviral Agents chemical synthesis, Carbamates, Drug Combinations, Drug Discovery, Drug Resistance, Viral drug effects, Drug Resistance, Viral genetics, Drug Synergism, Gene Expression, Hepacivirus genetics, Hepacivirus metabolism, Hepatocytes virology, High-Throughput Screening Assays, Host-Pathogen Interactions, Humans, Imidazoles pharmacology, Interferon-alpha pharmacology, Oligopeptides pharmacology, Primary Cell Culture, Pyridines chemical synthesis, Pyrimidines chemical synthesis, Pyrrolidines, Sofosbuvir pharmacology, Valine analogs & derivatives, Viral Envelope Proteins genetics, Viral Envelope Proteins metabolism, Virion drug effects, Virion genetics, Virion metabolism, Antiviral Agents pharmacology, Hepacivirus drug effects, Pyridines pharmacology, Pyrimidines pharmacology, Viral Envelope Proteins antagonists & inhibitors, Virus Internalization drug effects, Virus Release drug effects

Abstract

Despite recent advances in curing chronic hepatitis C (CHC), the high economic burden to therapy, viral drug resistance, difficult to treat hepatitis C virus (HCV) genotypes and patient groups are still of concern. To address this unmet medical needs, we devised strategies to identify novel viral interventions through target-free high-throughput screening of small molecules utilizing a phenotypic-based HCV infection assay. Thereby, a very potent (EC 50 46 ± 26 pM) iminodipyridinopyrimidine (IDPP) drug candidate was selected, and confirmed in primary human hepatocytes (EC 50 0.5 nM). IDPP mainly targets a post-attachment step of HCV without affecting endosomal acidification, prevents the secretion of infectious particles and viral cell-to-cell spread. The putative molecular target of IDPP is glycoprotein E1, as revealed by selection for viral drug resistance (Gly-257-Arg). IDPP was synergistic in combination with FDA-approved HCV drugs and inhibited pre-existing resistant HCV strains induced by today's therapies. Interestingly, IDPP exclusively inhibited HCV genotype 2. However, we identified the genotype-specificity determining region in E1 and generated HCV genotype 1 susceptible to IDPP by changing one amino acid in E1 (Gln-257-Gly). Together, our results indicate an opportunity to provide an alternative treatment option for CHC and will shed light on the poorly understood function of HCV glycoprotein E1.

Published

2017

61. Viral dependence on cellular ion channels - an emerging anti-viral target?

Author

Hover S, Foster B, Barr JN, and Mankouri J

Subjects

Heart Rate, Humans, Neurons virology, Respiratory Tract Diseases virology, Viral Proteins metabolism, Virus Release drug effects, Antiviral Agents pharmacology, Host-Pathogen Interactions drug effects, Ion Channels metabolism, Virion metabolism, Virus Internalization drug effects

Abstract

The broad range of cellular functions governed by ion channels represents an attractive target for viral manipulation. Indeed, modulation of host cell ion channel activity by viral proteins is being increasingly identified as an important virus-host interaction. Recent examples have demonstrated that virion entry, virus egress and the maintenance of a cellular environment conducive to virus persistence are, in part, dependent on virus manipulation of ion channel activity. Most excitingly, evidence has emerged that targeting ion channels pharmacologically can impede virus life cycles. Here, we discuss current examples of virus-ion channel interactions and the potential of targeting ion channel function as a new, pharmacologically safe and broad-ranging anti-viral therapeutic strategy.

Published

2017

62. Cholesterol reducing agents inhibit assembly of type I parainfluenza viruses.

Author

Bajimaya S, Hayashi T, Frankl T, Bryk P, Ward B, and Takimoto T

Subjects

Cell Membrane metabolism, Cell Membrane virology, Humans, Parainfluenza Virus 1, Human genetics, Parainfluenza Virus 1, Human physiology, Paramyxoviridae Infections drug therapy, Paramyxoviridae Infections metabolism, Protein Transport, Viral Proteins genetics, Viral Proteins metabolism, Virus Release drug effects, Anticholesteremic Agents pharmacology, Cholesterol metabolism, Parainfluenza Virus 1, Human drug effects, Paramyxoviridae Infections virology, Virus Assembly drug effects

Abstract

Many enveloped RNA viruses utilize lipid rafts for the assembly of progeny virions, but the role of cholesterol, a major component of rafts, on paramyxovirus budding and virion formation is controversial. In this study, we analyzed the effects of FDA-approved cholesterol-reducing agents, gemfibrozil and lovastatin, on raft formation and assembly of human parainfluenza virus type 1 (hPIV1) and Sendai virus (SeV). Treatment of the human airway epithelial A549 cells with the agents, especially when combined, significantly decreased production of infectious hPIV1 and SeV. Mechanistic analysis indicated that depletion of cellular cholesterol reduced cell surface accumulation of envelope glycoproteins and association of viral matrix and nucleocapsids with raft membrane, which resulted in impaired virus budding and release from the cells. These results indicate that cellular cholesterol is required for assembly and formation of type 1 parainfluenza viruses and suggest that cholesterol could be an attractive target for antiviral agents against hPIV1., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2017

63. Pseudolaric acid B inhibits the secretion of hepatitis B virus.

Author

Yu J, Wang Z, Ren P, Zhong T, Wang Y, Song F, Hou J, Yu X, and Hua S

Subjects

Apoptosis drug effects, Carcinoma, Hepatocellular pathology, Carcinoma, Hepatocellular prevention & control, Carcinoma, Hepatocellular virology, Cell Cycle drug effects, Cell Line, Tumor, Cell Proliferation drug effects, Hep G2 Cells, Hepatitis B virus physiology, Humans, Liver Neoplasms pathology, Liver Neoplasms prevention & control, Liver Neoplasms virology, Virus Replication drug effects, Diterpenes pharmacology, Hepatitis B virus drug effects, Virus Release drug effects

Abstract

High hepatitis B virus (HBV) load and chronic hepatitis B infection increase the risk of developing hepatocellular carcinoma (HCC), and is also associated with recurrence of HBV-related HCC. The aim of the present study was to investigate whether pseudolaric acid B (PAB), a diterpene acid isolated from the root and trunk bark of Pseudolarix kaempferi Gordon (Pinaceae), has an inhibitory role on the HBV secretion in HBV-related HCC. By detecting HBV surface antigen (HBsAg) by ELISA it was found that PAB inhibited HBV secretion in HepG2215 compared to control group, but did not decrease the intracellular HBV level, and the results were repeated in HepG2 cell transfect with HBV gene. Therefore, our results proved that PAB had the ability to inhibit HBV secretion. Moreover, it was shown that HepG2215 cells with HBV gene accumulated more in G0/G1 phase than HepG2 cells without HBV gene through detecting cell cycle distribution by flow cytometry, which indicated that HBV replication might favor the cell cycle environment of G0/G1 phase. However, HepG2 cells entered G2/M phase earlier than HepG2215 when PAB treatment induced G2/M arrest, therefore, HBV retarded the entry of G2/M to sustain the status of G0/G1 phase, while PAB finally changed the cell cycle environment favored by HBV virus. In addition, PAB also induced HepG2215 cell apoptosis, which would be helpful to kill the cells infected by HBV and help for devouring HBV by macrophage. Therefore, PAB inhibited HBV secretion through apoptosis and cell cycle arrest. The present findings contribute to a future potential chemotherapeutic drug in the treatment of HBV-related HCC.

Published

2017

64. The Intracellular Cholesterol Transport Inhibitor U18666A Inhibits the Exosome-Dependent Release of Mature Hepatitis C Virus.

Author

Elgner F, Ren H, Medvedev R, Ploen D, Himmelsbach K, Boller K, and Hildt E

Subjects

Animals, Biological Transport drug effects, Cell Line, Tumor, Cholesterol metabolism, Exosomes ultrastructure, Exosomes virology, Gene Expression, Genes, Reporter, Hepacivirus physiology, Hepacivirus ultrastructure, Hepatocytes ultrastructure, Hepatocytes virology, Humans, Luminescent Proteins genetics, Luminescent Proteins metabolism, Multivesicular Bodies drug effects, Multivesicular Bodies ultrastructure, Multivesicular Bodies virology, Virion drug effects, Virion physiology, Virion ultrastructure, Virus Assembly physiology, Red Fluorescent Protein, Androstenes pharmacology, Anticholesteremic Agents pharmacology, Exosomes drug effects, Hepacivirus drug effects, Hepatocytes drug effects, Virus Release drug effects

Abstract

Hepatitis C virus (HCV) particles are described as lipoviroparticles which are released similarly to very-low-density lipoproteins (VLDLs). However, the release mechanism is still poorly understood; the canonical endoplasmic reticulum-Golgi intermediate compartment (ERGIC) pathway as well as endosome-dependent release has been proposed. Recently, the role of exosomes in the transmission of HCV has been reported. Only a minor fraction of the de novo-synthesized lipoviroparticles is released by the infected cell. To investigate the relevance of multivesicular bodies (MVBs) for viral morphogenesis and release, the MVB inhibitor U18666A was used. Intracellular trafficking was analyzed by confocal microscopy and electron microscopy. Moreover, an mCherry-tagged HCV variant was used. Conditions were established that enable U18666A-dependent inhibition of MVBs without affecting viral replication. Under these conditions, significant inhibition of the HCV release was observed. The assembly of viral particles is not affected. In U18666A-treated cells, intact infectious viral particles accumulate in CD63-positive exosomal structures and large dysfunctional lysosomal structures (multilamellar bodies). These retained particles possess a lower density, reflecting a misloading with lipids. Our data indicate that at least a fraction of HCV particles leaves the cell via the endosomal pathway. Endosomes facilitate the sorting of HCV particles for release or degradation., Importance: There are still a variety of open questions regarding morphogenesis and release of hepatitis C virus. The HCV-infected cell produces significant more viral particles that are released, raising the question about the fate of the nonreleased particles. Moreover, the relevance of the endosomal pathway for the release of HCV is under debate. Use of the MVB (multivesicular body) inhibitor U18666A enabled a detailed analysis of the impact of MVBs for viral morphogenesis and release. It was revealed that infectious, fully assembled HCV particles are either MVB-dependently released or intracellularly degraded by the lysosome. Our data indicate that at least a fraction of HCV particles leaves the cell via the endosomal pathway independent from the constitutive secretory pathway. Our study describes a so-far-unprecedented cross talk between two pathways regulating on the one hand the release of infectious viral particles and on the other hand the intracellular degradation of nonreleased particles., (Copyright © 2016, American Society for Microbiology. All Rights Reserved.)

Published

2016

65. An extract from Taxodium distichum targets hemagglutinin- and neuraminidase-related activities of influenza virus in vitro.

Author

Hsieh CF, Chen YL, Lin CF, Ho JY, Huang CH, Chiu CH, Hsieh PW, and Horng JT

Subjects

Animals, Cell Line, Cell Survival drug effects, Dogs, Hemagglutinins chemistry, Humans, Madin Darby Canine Kidney Cells, Microscopy, Fluorescence, Neuraminidase antagonists & inhibitors, Orthomyxoviridae enzymology, Plant Extracts chemistry, Plant Extracts toxicity, RNA, Viral chemistry, RNA, Viral metabolism, Taxodium metabolism, Viral Proteins metabolism, Virus Internalization drug effects, Virus Release drug effects, Hemagglutinins metabolism, Neuraminidase metabolism, Orthomyxoviridae metabolism, Plant Extracts metabolism, Taxodium chemistry

Abstract

Influenza virus remains an emerging virus and causes pandemics with high levels of fatality. After screening different plant extracts with potential anti-influenza activity, a water extract of Taxodium distichum stems (TDSWex) showed excellent activity against influenza viruses. The EC 50 of TDSWex was 0.051 ± 0.024 mg/mL against influenza virus A/WSN/33. TDSWex had excellent antiviral efficacy against various strains of human influenza A and B viruses, particularly oseltamivir-resistant clinical isolates and a swine-origin influenza strain. We observed that the synthesis of viral RNA and protein were inhibited in the presence of TDSWex. The results of the time-of-addition assay suggested that TDSWex inhibited viral entry and budding. In the hemagglutination inhibition assay, TDSWex inhibited the hemagglutination of red blood cells, implying that the extract targeted hemagglutin-related functions such as viral entry. In the attachment and penetration assay, TDSWex showed antiviral activity with EC 50 s of 0.045 ± 0.026 and 0.012 ± 0.003 mg/mL, respectively. In addition, TDSWex blocked neuraminidase activity. We conclude that TDSWex has bimodal activities against both hemagglutinin and neuraminidase during viral replication.

Published

2016

66. Human transbodies to VP40 inhibit cellular egress of Ebola virus-like particles.

Author

Teimoori S, Seesuay W, Jittavisutthikul S, Chaisri U, Sookrung N, Densumite J, Saelim N, Chulanetra M, Maneewatch S, and Chaicumpa W

Subjects

Carcinoma, Hepatocellular pathology, Carcinoma, Hepatocellular ultrastructure, Carcinoma, Hepatocellular virology, Cell Line, Tumor, Ebolavirus physiology, Ebolavirus ultrastructure, Host-Pathogen Interactions, Humans, Liver Neoplasms pathology, Liver Neoplasms ultrastructure, Liver Neoplasms virology, Microscopy, Electron, Scanning, Models, Molecular, Peptide Library, Protein Binding, Protein Domains, Single-Chain Antibodies chemistry, Single-Chain Antibodies immunology, Viral Matrix Proteins chemistry, Viral Matrix Proteins genetics, Virion drug effects, Virion physiology, Virion ultrastructure, Virus Release physiology, Ebolavirus drug effects, Single-Chain Antibodies pharmacology, Viral Matrix Proteins immunology, Virus Release drug effects

Abstract

A direct acting anti-Ebola agent is needed. VP40, a conserved protein across Ebolavirus (EBOV) species has several pivotal roles in the virus life cycle. Inhibition of VP40 functions would lessen the virion integrity and interfere with the viral assembly, budding, and spread. In this study, cell penetrable human scFvs (HuscFvs) that bound to EBOV VP40 were produced by phage display technology. Gene sequences coding for VP40-bound-HuscFvs were subcloned from phagemids into protein expression plasmids downstream to a gene of cell penetrating peptide, i.e., nonaarginine (R9). By electron microscopy, transbodies from three clones effectively inhibited egress of the Ebola virus-like particles from human hepatic cells transduced with pseudo-typed-Lentivirus particles carrying EBOV VP40 and GP genes. Computerized simulation indicated that the effective HuscFvs bound to multiple basic residues in the cationic patch of VP40 C-terminal domain which are important in membrane-binding for viral matrix assembly and virus budding. The transbodies bound also to VP40 N-terminal domain and L domain peptide encompassed the PTAPPEY (WW binding) motif, suggesting that they might confer VP40 function inhibition through additional mechanism(s). The generated transbodies are worthwhile tested with authentic EBOV before developing to direct acting anti-Ebola agent for preclinical and clinical trials., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016

67. Novel Acylguanidine-Based Inhibitor of HIV-1.

Author

Mwimanzi P, Tietjen I, Miller SC, Shahid A, Cobarrubias K, Kinloch NN, Baraki B, Richard J, Finzi A, Fedida D, Brumme ZL, and Brockman MA

Subjects

Antigens, CD genetics, CD4 Antigens genetics, Cell Line, GPI-Linked Proteins genetics, Humans, Mutation drug effects, Virion drug effects, Virus Release drug effects, Virus Replication drug effects, env Gene Products, Human Immunodeficiency Virus genetics, Anti-HIV Agents pharmacology, HIV Infections drug therapy, HIV-1 drug effects

Abstract

Unlabelled: The emergence of transmissible HIV-1 strains with resistance to antiretroviral drugs highlights a continual need for new therapies. Here we describe a novel acylguanidine-containing compound, 1-(2-(azepan-1-yl)nicotinoyl)guanidine (or SM111), that inhibits in vitro replication of HIV-1, including strains resistant to licensed protease, reverse transcriptase, and integrase inhibitors, without major cellular toxicity. At inhibitory concentrations, intracellular p24(Gag) production was unaffected, but virion release (measured as extracellular p24(Gag)) was reduced and virion infectivity was substantially impaired, suggesting that SM111 acts at a late stage of viral replication. SM111-mediated inhibition of HIV-1 was partially overcome by a Vpu I17R mutation alone or a Vpu W22* truncation in combination with Env N136Y. These mutations enhanced virion infectivity and Env expression on the surface of infected cells in the absence and presence of SM111 but also impaired Vpu's ability to downregulate CD4 and BST2/tetherin. Taken together, our results support acylguanidines as a class of HIV-1 inhibitors with a distinct mechanism of action compared to that of licensed antiretrovirals. Further research on SM111 and similar compounds may help to elucidate knowledge gaps related to Vpu's role in promoting viral egress and infectivity., Importance: New inhibitors of HIV-1 replication may be useful as therapeutics to counteract drug resistance and as reagents to perform more detailed studies of viral pathogenesis. SM111 is a small molecule that blocks the replication of wild-type and drug-resistant HIV-1 strains by impairing viral release and substantially reducing virion infectivity, most likely through its ability to prevent Env expression at the infected cell surface. Partial resistance to SM111 is mediated by mutations in Vpu and/or Env, suggesting that the compound affects host/viral protein interactions that are important during viral egress. Further characterization of SM111 and similar compounds may allow more detailed pharmacological studies of HIV-1 egress and provide opportunities to develop new treatments for HIV-1., (Copyright © 2016, American Society for Microbiology. All Rights Reserved.)

Published

2016

68. Control and Eradication Strategies of Hepatitis B Virus.

Author

Shih C, Chou SF, Yang CC, Huang JY, Choijilsuren G, and Jhou RS

Subjects

DNA, Circular metabolism, DNA, Viral metabolism, Hepatitis B Vaccines immunology, Hepatitis B virus growth & development, Hepatitis B virus immunology, Humans, RNA Interference, RNA, Small Interfering therapeutic use, Virus Internalization drug effects, Virus Release drug effects, Virus Replication drug effects, Antiviral Agents therapeutic use, Hepatitis B Vaccines therapeutic use, Hepatitis B virus drug effects, Hepatitis B, Chronic drug therapy, Immunotherapy methods

Abstract

Hepatitis B virus (HBV) is a major human pathogen, and chronic hepatitis can lead to cirrhosis and malignant hepatocellular carcinoma. While HBV vaccine and treatment are available, it has remained a challenge to completely eradicate the virus from patients. Current therapy using either interferon or polymerase inhibitors cannot cure HBV with a high efficacy. Lifelong therapy is needed to suppress HBV in patients who achieve no seroconversion. Here, we review recent exciting advances of new strategies, including the inhibition of viral entry, the destruction or silencing of HBV covalently closed circular DNA (cccDNA), and breaking immune tolerance. Combinations of different therapeutic strategies could improve the cure rate of viral persistence in chronic hepatitis B., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

69. Micrococcin P1, a naturally occurring macrocyclic peptide inhibiting hepatitis C virus entry in a pan-genotypic manner.

Author

Lee M, Yang J, Park S, Jo E, Kim HY, Bae YS, and Windisch MP

Subjects

Antiviral Agents chemistry, Bacteriocins chemistry, Cell Line, Cells, Cultured, Dose-Response Relationship, Drug, Drug Resistance, Viral drug effects, Drug Synergism, Hepatitis C drug therapy, Hepatitis C virology, Humans, Peptides chemistry, Virus Release drug effects, Virus Replication drug effects, Antiviral Agents pharmacology, Bacteriocins pharmacology, Genotype, Hepacivirus drug effects, Hepacivirus physiology, Peptides pharmacology, Virus Internalization drug effects

Abstract

Hepatitis C virus (HCV) is considered a major public health concern worldwide. Despite recent advances in curing chronic hepatitis C, unmet medical needs still remain, especially due to the high economic burden of therapies. Accordingly, our study aimed to identify affordable novel HCV inhibitors by screening of natural product compound libraries. We identified micrococcin P1, a macrocyclic peptide antibiotic, inhibiting HCV entry in a pan-genotypic manner with an EC50 range of 0.1-0.5 μM. Micrococcin P1 interfered with HCV entry at an attachment step. Furthermore, micrococcin P1 efficiently inhibited HCV spread by blocking cell-free infection as well as cell-to-cell transmission, without affecting the secretion of infectious virions. Interestingly, the putative molecular target of micrococcin P1 is glycoprotein E2 (IIe-630-Thr), as revealed by selection for viral drug resistance. In addition, micrococcin P1 inhibited sofosbuvir-resistant HCV strains and showed synergy in combination with selected HCV drugs, suggesting an alternative treatment paradigm for patients. In conclusion, we identified micrococcin P1 as specifically inhibiting entry of all HCV genotypes and demonstrated that micrococcin P1 potentially could add value to therapies in combination with current HCV interventions., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016

70. Toll-like receptor 9 ligand D-type oligodeoxynucleotide D35 as a broad inhibitor for influenza A virus replication that is associated with suppression of neuraminidase activity.

Author

Yamada H, Nagase S, Takahashi K, Sakoda Y, Kida H, and Okamoto S

Subjects

Animals, Antiviral Agents chemical synthesis, Antiviral Agents chemistry, Antiviral Agents pharmacology, Cell Survival drug effects, Dogs, HEK293 Cells, Humans, Influenza A virus growth & development, Influenza A virus physiology, Ligands, Lung virology, Madin Darby Canine Kidney Cells, Mice, Mice, Inbred BALB C, Neuraminidase chemistry, Neuraminidase genetics, Oligodeoxyribonucleotides administration & dosage, Oligodeoxyribonucleotides chemical synthesis, Oligodeoxyribonucleotides chemistry, Oseltamivir pharmacology, Toll-Like Receptor 9 chemistry, Toll-Like Receptor 9 immunology, Virus Release drug effects, Virus Replication drug effects, Influenza A virus drug effects, Neuraminidase antagonists & inhibitors, Oligodeoxyribonucleotides pharmacology, Toll-Like Receptor 9 metabolism

Abstract

The most effective drugs available to treat influenza are neuraminidase (NA) inhibitors, which provide important additional measures for the control of influenza virus infections. However, since the emergence of NA inhibitor-resistant viruses may compromise the clinical utility of this class of anti-influenza agents, it is very important to develop new anti-influenza agents which target a different region in NA responsible for its sensitivity from that for NA inhibitors and could be used to treat NA inhibitors-resistant isolates. The oligodeoxynucleotide D35, multimerized and aggregated, suppressed replication of influenza A viruses except A/WSN/33 (WSN). The suppressive viral replication by D35 depended on G-terad and multimer formation. The range of the suppressive viral replication at the late stage, including virus assembly and release from infected cells, was much larger than that at the initial stage, viral attachment and entry. D35 suppressed NA activity of influenza A viruses. Furthermore, replacing the NA gene of A/Puerto Rico/8/34 (PR8), in which viral replication was inhibited by D35 at the late stage, with the NA gene from WSN, in which viral replication was not inhibited, eliminated the D35-dependent suppression. D35 showed an additive anti-influenza effect with oseltamivir. It was also effective in vivo. These results suggest that the influenza virus NA mainly contributes to the D35-suppressible virus release from infected cells at the late stage. In addition, because administration of D35 into the virus-infected mice suppressed viral replication and weight loss, clinical application of D35 could be considered., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016

71. Spironolactone blocks Epstein-Barr virus production by inhibiting EBV SM protein function.

Author

Verma D, Thompson J, and Swaminathan S

Subjects

Capsid Proteins antagonists & inhibitors, Capsid Proteins genetics, Capsid Proteins physiology, Cell Line, DNA Replication drug effects, Gene Deletion, Gene Expression Regulation, Viral drug effects, Gene Knockout Techniques, Genes, Viral drug effects, HEK293 Cells, Herpesvirus 4, Human genetics, Humans, Immediate-Early Proteins genetics, Immediate-Early Proteins physiology, Mineralocorticoid Receptor Antagonists pharmacology, Spironolactone analogs & derivatives, Spironolactone chemistry, Structure-Activity Relationship, Trans-Activators genetics, Trans-Activators physiology, Transcriptome drug effects, Virus Release drug effects, Virus Replication drug effects, Virus Replication genetics, Virus Replication physiology, Antiviral Agents pharmacology, Herpesvirus 4, Human drug effects, Herpesvirus 4, Human physiology, Immediate-Early Proteins antagonists & inhibitors, Spironolactone pharmacology, Trans-Activators antagonists & inhibitors

Abstract

Clinically available drugs active against Epstein-Barr virus (EBV) and other human herpesviruses are limited to those targeting viral DNA replication. To identify compounds directed against other steps in the viral life cycle, we searched for drugs active against the EBV SM protein, which is essential for infectious virus production. SM has a highly gene-specific mode of action and preferentially enhances expression of several late lytic cycle EBV genes. Here we demonstrate that spironolactone, a mineralocorticoid receptor antagonist approved for clinical use, inhibits SM function and infectious EBV production. Expression of EBV viral capsid antigen is highly SM dependent, and spironolactone inhibits viral capsid antigen synthesis and capsid formation, blocking EBV virion production at a step subsequent to viral DNA replication. In addition, spironolactone inhibits expression of other SM-dependent genes necessary for infectious virion formation. We further demonstrate that molecules structurally related to spironolactone with similar antimineralocorticoid blocking activity do not inhibit EBV production. These findings pave the way for development of antiherpesvirus drugs with new mechanisms of action directed against SM and homologous essential proteins in other herpesviruses.

Published

2016

72. Iminosugars Inhibit Dengue Virus Production via Inhibition of ER Alpha-Glucosidases--Not Glycolipid Processing Enzymes.

Author

Sayce AC, Alonzi DS, Killingbeck SS, Tyrrell BE, Hill ML, Caputo AT, Iwaki R, Kinami K, Ide D, Kiappes JL, Beatty PR, Kato A, Harris E, Dwek RA, Miller JL, and Zitzmann N

Subjects

Animals, Cells, Cultured, Dengue Virus physiology, Endoplasmic Reticulum drug effects, Enzyme Inhibitors chemistry, Humans, Imino Sugars chemistry, Indolizines chemistry, Macrophages drug effects, Macrophages virology, Models, Molecular, Molecular Structure, Virus Release drug effects, Antiviral Agents metabolism, Dengue Virus growth & development, Endoplasmic Reticulum enzymology, Enzyme Inhibitors metabolism, Imino Sugars metabolism, Indolizines metabolism, alpha-Glucosidases metabolism

Abstract

It has long been thought that iminosugar antiviral activity is a function of inhibition of endoplasmic reticulum-resident α-glucosidases, and on this basis, many iminosugars have been investigated as therapeutic agents for treatment of infection by a diverse spectrum of viruses, including dengue virus (DENV). However, iminosugars are glycomimetics possessing a nitrogen atom in place of the endocyclic oxygen atom, and the ubiquity of glycans in host metabolism suggests that multiple pathways can be targeted via iminosugar treatment. Successful treatment of patients with glycolipid processing defects using iminosugars highlights the clinical exploitation of iminosugar inhibition of enzymes other than ER α-glucosidases. Evidence correlating antiviral activity with successful inhibition of ER glucosidases together with the exclusion of alternative mechanisms of action of iminosugars in the context of DENV infection is limited. Celgosivir, a bicyclic iminosugar evaluated in phase Ib clinical trials as a therapeutic for the treatment of DENV infection, was confirmed to be antiviral in a lethal mouse model of antibody-enhanced DENV infection. In this study we provide the first evidence of the antiviral activity of celgosivir in primary human macrophages in vitro, in which it inhibits DENV secretion with an EC50 of 5 μM. We further demonstrate that monocyclic glucose-mimicking iminosugars inhibit isolated glycoprotein and glycolipid processing enzymes and that this inhibition also occurs in primary cells treated with these drugs. By comparison to bicyclic glucose-mimicking iminosugars which inhibit glycoprotein processing but do not inhibit glycolipid processing and galactose-mimicking iminosugars which do not inhibit glycoprotein processing but do inhibit glycolipid processing, we demonstrate that inhibition of endoplasmic reticulum-resident α-glucosidases, not glycolipid processing, is responsible for iminosugar antiviral activity against DENV. Our data suggest that inhibition of ER α-glucosidases prevents release of virus and is the primary antiviral mechanism of action of iminosugars against DENV.

Published

2016

73. Pentagalloylglucose Blocks the Nuclear Transport and the Process of Nucleocapsid Egress to Inhibit HSV-1 Infection.

Author

Jin F, Ma K, Chen M, Zou M, Wu Y, Li F, and Wang Y

Subjects

Animals, Humans, Active Transport, Cell Nucleus drug effects, Antiviral Agents metabolism, Herpesvirus 1, Human drug effects, Herpesvirus 1, Human physiology, Hydrolyzable Tannins metabolism, Nucleocapsid drug effects, Virus Release drug effects

Abstract

Herpes simplex virus type 1 (HSV-1), a widespread virus, causes a variety of human viral diseases worldwide. The serious threat of drug-resistance highlights the extreme urgency to develop novel antiviral drugs with different mechanisms of action. Pentagalloylglucose (PGG) is a natural polyphenolic compound with significant anti-HSV activity; however, the mechanisms underlying its antiviral activity need to be defined by further studies. In this study, we found that PGG treatment delays the nuclear transport process of HSV-1 particles by inhibiting the upregulation of dynein (a cellular major motor protein) induced by HSV-1 infection. Furthermore, PGG treatment affects the nucleocapsid egress of HSV-1 by inhibiting the expression and disrupting the cellular localization of pEGFP-UL31 and pEGFP-UL34, which are indispensable for HSV-1 nucleocapsid egress from the nucleus. However, the over-expression of pEGFP-UL31 and pEGFP-UL34 could decrease the antiviral effect of PGG. In this study, for the first time, the antiviral activity of PGG against acyclovir-resistant virus was demonstrated in vitro, and the possible mechanisms of its anti-HSV activities were identified based on the inhibition of nuclear transport and nucleocapsid egress in HSV-1. It was further confirmed that PGG could be a promising candidate for HSV therapy, especially for drug-resistant strains.

Published

2016

74. DNA-AuNP networks on cell membranes as a protective barrier to inhibit viral attachment, entry and budding.

Author

Li CM, Zheng LL, Yang XX, Wan XY, Wu WB, Zhen SJ, Li YF, Luo LF, and Huang CZ

Subjects

Antiviral Agents administration & dosage, Antiviral Agents chemistry, Bronchi cytology, Carcinoma, Squamous Cell pathology, Cell Line, Cell Line, Tumor, Cell Membrane chemistry, Cell Membrane drug effects, Cell Survival, Cytopathogenic Effect, Viral, DNA administration & dosage, DNA chemical synthesis, Epithelial Cells drug effects, Epithelial Cells virology, Gold Colloid administration & dosage, Humans, Laryngeal Neoplasms pathology, Respiratory Syncytial Viruses physiology, Viral Plaque Assay, Antiviral Agents pharmacology, Cell Membrane virology, DNA pharmacology, Gold Colloid pharmacology, Nanoconjugates administration & dosage, Nanoparticles administration & dosage, Respiratory Syncytial Viruses drug effects, Virus Attachment drug effects, Virus Internalization drug effects, Virus Release drug effects

Abstract

Viral infections have caused numerous diseases and deaths worldwide. Due to the emergence of new viruses and frequent virus variation, conventional antiviral strategies that directly target viral or cellular proteins are limited because of the specificity, drug resistance and rapid clearance from the human body. Therefore, developing safe and potent antiviral agents with activity against viral infection at multiple points in the viral life cycle remains a major challenge. In this report, we propose a new modality to inhibit viral infection by fabricating DNA conjugated gold nanoparticle (DNA-AuNP) networks on cell membranes as a protective barrier. The DNA-AuNPs networks were found, via a plaque formation assay and viral titers, to have potent antiviral ability and protect host cells from human respiratory syncytial virus (RSV). Confocal immunofluorescence image analysis showed 80 ± 3.8% of viral attachment, 91.1 ± 0.9% of viral entry and 87.9 ± 2.8% of viral budding were inhibited by the DNA-AuNP networks, which were further confirmed by real-time fluorescence imaging of the RSV infection process. The antiviral activity of the networks may be attributed to steric effects, the disruption of membrane glycoproteins and limited fusion of cell membrane bilayers, all of which play important roles in viral infection. Therefore, our results suggest that the DNA-AuNP networks have not only prophylactic effects to inhibit virus attachment and entry, but also therapeutic effects to inhibit viral budding and cell-to-cell spread. More importantly, this proof-of-principle study provides a pathway for the development of a universal, broad-spectrum antiviral therapy., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2016

75. Impact of HIV-1 infection pathways on susceptibility to antiviral drugs and on virus spread.

Author

Shimura K, Miyazato P, Oishi S, Fujii N, and Matsuoka M

Subjects

Cell Line, Humans, Anti-HIV Agents pharmacology, HIV-1 drug effects, HIV-1 physiology, Virus Internalization drug effects, Virus Release drug effects, Virus Replication drug effects

Abstract

The infection routes of HIV-1 can affect several viral properties, including dissemination, pathogenesis, and immune evasion. In this study, we evaluated the inhibitory activity of a wide variety of anti-HIV drugs, focusing on the impact that different infection pathways have on their efficacy. Compared to cell-free infection, inhibitory activities were reduced in cell-to-cell productive transmission for all drugs tested. We detected weak reporter-expressing target cells after cell-to-cell transmission in the presence of integrase strand transfer inhibitors (INSTIs). Further analysis revealed that this expression was mainly due to unintegrated circular HIV (cHIV) DNAs, consisting of 1-LTR and 2-LTR circles. When in vitro-constructed cHIV DNAs were introduced into cells, the production of infectious and intercellular transmittable virions was observed, suggesting that cHIV DNA could be a source of infectious virus. These results highlight some advantages of the cell-to-cell infection mode for viral expansion, particularly in the presence of anti-retroviral drugs., (Copyright © 2015 Elsevier Inc. All rights reserved.)

Published

2015

76. A p7 Ion Channel-derived Peptide Inhibits Hepatitis C Virus Infection in Vitro.

Author

Hong W, Lang Y, Li T, Zeng Z, Song Y, Wu Y, Li W, and Cao Z

Subjects

Antiviral Agents chemistry, HeLa Cells, Hepacivirus genetics, Hepatitis C genetics, Hepatitis C metabolism, Humans, Peptides chemistry, Antiviral Agents pharmacology, Hepacivirus metabolism, Hepatitis C drug therapy, Ion Channels chemistry, Peptides pharmacology, Viral Proteins chemistry, Virus Release drug effects

Abstract

Viral infection is an early stage of its life cycle and represents a promising target for antiviral drug development. Here we designed and characterized three peptide inhibitors of hepatitis C virus (HCV) infection based on the structural features of the membrane-associated p7 polypeptide of HCV. The three peptides exhibited low toxicity and high stability while potently inhibiting initial HCV infection and suppressed established HCV infection at non-cytotoxic concentrations in vitro. The most efficient peptide (designated H2-3), which is derived from the H2 helical region of HCV p7 ion channel, inhibited HCV infection by inactivating both intracellular and extracellular viral particles. The H2-3 peptide inactivated free HCV with an EC50 (50% effective concentration) of 82.11 nm, which is >1000-fold lower than the CC50 (50% cytotoxic concentration) of Huh7.5.1 cells. H2-3 peptide also bound to cell membrane and protected host cells from viral infection. The peptide H2-3 did not alter the normal electrophysiological profile of the p7 ion channel or block viral release from Huh7.5.1 cells. Our work highlights a new anti-viral peptide design strategy based on ion channel, giving the possibility that ion channels are potential resources to generate antiviral peptides., (© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

77. The Interferon-Inducible Protein Tetherin Inhibits Hepatitis B Virus Virion Secretion.

Author

Yan R, Zhao X, Cai D, Liu Y, Block TM, Guo JT, and Guo H

Subjects

Antigens, CD genetics, Capsid ultrastructure, Cell Line, GPI-Linked Proteins biosynthesis, GPI-Linked Proteins genetics, Gene Expression Regulation drug effects, Glycosylphosphatidylinositols, Hepatitis B virus ultrastructure, Hepatocytes metabolism, Hepatocytes ultrastructure, Hepatocytes virology, Humans, Interferon-alpha pharmacology, Antigens, CD biosynthesis, Antiviral Agents pharmacology, Capsid metabolism, Hepatitis B virus physiology, Virus Release drug effects, Virus Replication drug effects

Abstract

Unlabelled: Interferon alpha (IFN-α) is an approved medication for chronic hepatitis B therapy. Besides acting as an immunomodulator, IFN-α elicits a pleiotropic antiviral state in hepatitis B virus (HBV)-infected hepatocytes, but whether or not IFN-α impedes the late steps of the HBV life cycle, such as HBV secretion, remains elusive. Here we report that IFN-α treatment of HepAD38 cells with established HBV replication selectively reduced HBV virion release without altering intracellular viral replication or the secretion of HBV subviral particles and nonenveloped capsids. In search of the interferon-stimulated gene(s) that is responsible for the reduction of HBV virion release, we found that tetherin, a broad-spectrum antiviral transmembrane protein that inhibits the egress of a variety of enveloped viruses, was highly induced by IFN-α in HepAD38 cells and in primary human hepatocytes. We further demonstrated that the expression of full-length tetherin, but not the C-terminal glycosylphosphatidylinositol (GPI) anchor-truncated form, inhibited HBV virion egress from HepAD38 cells. In addition, GPI anchor-truncated tetherin exhibited a dominant-negative effect and was incorporated into the liberated virions. We also found colocalization of tetherin and HBV L protein at the intracellular multivesicular body, where the budding of HBV virions takes place. In line with this, electron microscopy demonstrated that HBV virions were tethered in the lumen of the cisterna membrane under tetherin expression. Finally, knockdown of tetherin or overexpression of dominant negative tetherin attenuated the IFN-α-mediated reduction of HBV virion release. Taken together, our study suggests that IFN-α inhibits HBV virion egress from hepatocytes through the induction of tetherin., Importance: Tetherin is a host restriction factor that blocks the egress of a variety of enveloped viruses through tethering the budding virions on the cell surface with its membrane anchor domains. Here we report that interferon directly and selectively inhibits the secretion of HBV virions, but not subviral particles or nonenveloped capsids, through the induction of tetherin in hepatocyte-derived cells. The antiviral function of tetherin requires the carboxyl-terminal GPI anchor, while the GPI anchor deletion mutant exhibits dominant negative activity and attaches to liberated HBV virions. Consistent with the fact that HBV is an intracellular budding virus, microscopy analyses demonstrated that the tethering of HBV virions occurs in the intracellular cisterna and that tetherin colocalizes with HBV virions on the multivesicular body, which is the HBV virion budding site. Our study not only expands the antiviral spectrum of tetherin but also sheds light on the mechanisms of interferon-elicited anti-HBV responses., (Copyright © 2015, American Society for Microbiology. All Rights Reserved.)

Published

2015

78. Anion homeostasis is important for non-lytic release of BK polyomavirus from infected cells.

Author

Evans GL, Caller LG, Foster V, and Crump CM

Subjects

4,4'-Diisothiocyanostilbene-2,2'-Disulfonic Acid pharmacology, Biological Transport, Cell Line, Humans, Vacuoles metabolism, Virus Release drug effects, Virus Replication, Voltage-Dependent Anion Channels antagonists & inhibitors, Anions metabolism, BK Virus physiology, Homeostasis

Abstract

BK polyomavirus (BKPyV) is a member of a family of potentially oncogenic viruses, whose reactivation can cause severe pathological conditions in transplant patients, leading to graft rejection. As with many non-enveloped viruses, it is assumed that virus release occurs through lysis of the host cell. We now show the first evidence for a non-lytic release pathway for BKPyV and that this pathway can be blocked by the anion channel inhibitor DIDS. Our data show a dose-dependent effect of DIDS on the release of BKPyV virions. We also observed an accumulation of viral capsids in large LAMP-1-positive acidic organelles within the cytoplasm of cells upon DIDS treatment, suggesting potential late endosome or lysosome-related compartments are involved in non-lytic BKPyV release. These data highlight a novel mechanism by which polyomaviruses can be released from infected cells in an active and non-lytic manner, and that anion homeostasis regulation is important in this pathway., (© 2015 The Authors.)

Published

2015

79. Suramin Inhibits Chikungunya Virus Entry and Transmission.

Author

Ho YJ, Wang YM, Lu JW, Wu TY, Lin LI, Kuo SC, and Lin CC

Subjects

Animals, Antiviral Agents chemistry, Antiviral Agents pharmacology, Cell Line, Models, Molecular, Molecular Conformation, Suramin chemistry, Viral Envelope Proteins chemistry, Viral Envelope Proteins metabolism, Viral Plaque Assay, Virus Release drug effects, Chikungunya Fever virology, Chikungunya virus physiology, Suramin pharmacology, Virus Internalization drug effects

Abstract

The mosquito-borne Chikungunya virus (CHIKV) is a profound global threat due to its high rate of contagion and the lack of vaccine or effective treatment. Suramin is a symmetric polyanionic naphthylurea that is widely used in the clinical treatment of parasite infections. Numerous studies have reported the broad antiviral activities of suramin; however, inhibition effects against CHIKV have not yet been demonstrated. The aim of this study was thus to investigate the antiviral effect of suramin on CHIKV infection and to elucidate the molecular mechanism underlying inhibition using plaque reduction assay, RT-qPCR, western blot analysis, and plaque assay. Microneutralization assay was used to determine the EC50 of suramin in the CHIKV-S27 strain as well as in three other clinical strains (0611aTw, 0810bTw and 0706aTw). Time-of-addition was used to reveal the anti-CHIKV mechanism of suramin. We also evaluated anti-CHIKV activity with regard to viral entry, virus release, and cell-to-cell transmission. Cytopathic effect, viral RNA, viral protein, and the virus yield of CHIKV infection were shown to diminish in the presence of suramin in a dose-dependent manner. Suramin was also shown the inhibitory activities of the three clinical isolates. Suramin inhibited the early progression of CHIKV infection, due perhaps to interference with virus fusion and binding, which subsequently prevented viral entry. Results of a molecular docking simulation indicate that suramin may embed within the cavity of the E1/E2 heterodimer to interfere with their function. Suramin was also shown to reduce viral release and cell-to-cell transmission of CHIKV. In conclusion, Suramin shows considerable potential as a novel anti-CHIKV agent targeting viral entry, extracellular transmission, and cell-to-cell transmission.

Published

2015

80. Phosphorylation of Nonmuscle myosin II-A regulatory light chain resists Sendai virus fusion with host cells.

Author

Das P, Saha S, Chandra S, Das A, Dey SK, Das MR, Sen S, Sarkar DP, and Jana SS

Subjects

Amino Acid Sequence, Animals, CHO Cells, Cell Line, Tumor, Cricetinae, Cricetulus, Heterocyclic Compounds, 4 or More Rings pharmacology, Humans, Microscopy, Atomic Force, Microscopy, Fluorescence, Mutagenesis, Myosin Light Chains genetics, Myosin Light Chains metabolism, Nonmuscle Myosin Type IIA antagonists & inhibitors, Nonmuscle Myosin Type IIA genetics, Nonmuscle Myosin Type IIB metabolism, Phosphorylation drug effects, RNA Interference, RNA, Small Interfering metabolism, Sequence Alignment, Virus Internalization drug effects, Virus Release drug effects, rho-Associated Kinases metabolism, Nonmuscle Myosin Type IIA metabolism, Sendai virus physiology

Abstract

Enveloped viruses enter host cells through membrane fusion and the cells in turn alter their shape to accommodate components of the virus. However, the role of nonmuscle myosin II of the actomyosin complex of host cells in membrane fusion is yet to be understood. Herein, we show that both (-) blebbistatin, a specific inhibitor of nonmuscle myosin II (NMII) and small interfering RNA markedly augment fusion of Sendai virus (SeV), with chinese hamster ovary cells and human hepatocarcinoma cells. Inhibition of RLC phosphorylation using inhibitors against ROCK, but not PKC and MRCK, or overexpression of phospho-dead mutant of RLC enhances membrane fusion. SeV infection increases cellular stiffness and myosin light chain phosphorylation at two hour post infection. Taken together, the present investigation strongly indicates that Rho-ROCK-NMII contractility signaling pathway may provide a physical barrier to host cells against viral fusion.

Published

2015

81. Viroporin Activity of the Foot-and-Mouth Disease Virus Non-Structural 2B Protein.

Author

Ao D, Guo HC, Sun SQ, Sun DH, Fung TS, Wei YQ, Han SC, Yao XP, Cao SZ, Liu DX, and Liu XT

Subjects

Amantadine pharmacology, Animals, Calcium metabolism, Cell Line, Cell Membrane Permeability, Cricetinae, Endoplasmic Reticulum virology, Escherichia coli virology, Foot-and-Mouth Disease Virus genetics, Humans, Protein Structure, Tertiary, Virus Release drug effects, Virus Replication physiology, Autophagy genetics, Cell Membrane metabolism, Foot-and-Mouth Disease Virus metabolism, Viral Nonstructural Proteins antagonists & inhibitors, Viral Regulatory and Accessory Proteins antagonists & inhibitors

Abstract

Viroporins are a family of low-molecular-weight hydrophobic transmembrane proteins that are encoded by various animal viruses. Viroporins form transmembrane pores in host cells via oligomerization, thereby destroying cellular homeostasis and inducing cytopathy for virus replication and virion release. Among the Picornaviridae family of viruses, the 2B protein encoded by enteroviruses is well understood, whereas the viroporin activity of the 2B protein encoded by the foot-and-mouth disease virus (FMDV) has not yet been described. An analysis of the FMDV 2B protein domains by computer-aided programs conducted in this study revealed that this protein may contain two transmembrane regions. Further biochemical, biophysical and functional studies revealed that the protein possesses a number of features typical of a viroporin when it is overexpressed in bacterial and mammalian cells as well as in FMDV-infected cells. The protein was found to be mainly localized in the endoplasmic reticulum (ER), with both the N- and C-terminal domains stretched into the cytosol. It exhibited cytotoxicity in Escherichia coli, which attenuated 2B protein expression. The release of virions from cells infected with FMDV was inhibited by amantadine, a viroporin inhibitor. The 2B protein monomers interacted with each other to form both intracellular and extracellular oligomers. The Ca(2+) concentration in the cells increased, and the integrity of the cytoplasmic membrane was disrupted in cells that expressed the 2B protein. Moreover, the 2B protein induced intense autophagy in host cells. All of the results of this study demonstrate that the FMDV 2B protein has properties that are also found in other viroporins and may be involved in the infection mechanism of FMDV.

Published

2015

82. BST2/tetherin inhibition of alphavirus exit.

Author

Ooi YS, Dubé M, and Kielian M

Subjects

GPI-Linked Proteins metabolism, HeLa Cells, Humans, Alphavirus immunology, Alphavirus physiology, Antigens, CD metabolism, Virus Release drug effects

Abstract

Alphaviruses such as chikungunya virus (CHIKV) and Semliki Forest virus (SFV) are small enveloped RNA viruses that bud from the plasma membrane. Tetherin/BST2 is an interferon-induced host membrane protein that inhibits the release of many enveloped viruses via direct tethering of budded particles to the cell surface. Alphaviruses have highly organized structures and exclude host membrane proteins from the site of budding, suggesting that their release might be insensitive to tetherin inhibition. Here, we demonstrated that exogenously-expressed tetherin efficiently inhibited the release of SFV and CHIKV particles from host cells without affecting virus entry and infection. Alphavirus release was also inhibited by the endogenous levels of tetherin in HeLa cells. While rubella virus (RuV) and dengue virus (DENV) have structural similarities to alphaviruses, tetherin inhibited the release of RuV but not DENV. We found that two recently identified tetherin isoforms differing in length at the N-terminus exhibited distinct capabilities in restricting alphavirus release. SFV exit was efficiently inhibited by the long isoform but not the short isoform of tetherin, while both isoforms inhibited vesicular stomatitis virus exit. Thus, in spite of the organized structure of the virus particle, tetherin specifically blocks alphavirus release and shows an interesting isoform requirement.

Published

2015

83. A novel minimal in vitro system for analyzing HIV-1 Gag-mediated budding.

Author

Gui D, Gupta S, Xu J, Zandi R, Gill S, Huang IC, Rao AL, and Mohideen U

Subjects

Cell Membrane drug effects, Cell Membrane metabolism, Cell Membrane virology, HIV-1 drug effects, HIV-1 metabolism, Kinetics, RNA, Viral metabolism, Urea pharmacology, HIV-1 physiology, Unilamellar Liposomes metabolism, Virus Release drug effects, gag Gene Products, Human Immunodeficiency Virus metabolism

Abstract

A biomimetic minimalist model membrane was used to study the mechanism and kinetics of cell-free in vitro HIV-1 Gag budding from a giant unilamellar vesicle (GUV). Real-time interaction of Gag, RNA, and lipid, leading to the formation of mini-vesicles, was measured using confocal microscopy. Gag forms resolution-limited punctae on the GUV lipid membrane. Introduction of the Gag and urea to a GUV solution containing RNA led to the budding of mini-vesicles on the inside surface of the GUV. The GUV diameter showed a linear decrease in time due to bud formation. Both bud formation and decrease in GUV size were proportional to Gag concentration. In the absence of RNA, addition of urea to GUVs incubated with Gag also resulted in subvesicle formation. These observations suggest the possibility that clustering of GAG proteins leads to membrane invagination even in the absence of host cell proteins. The method presented here is promising, and allows for systematic study of the dynamics of assembly of immature HIV and help classify the hierarchy of factors that impact the Gag protein initiated assembly of retroviruses such as HIV.

Published

2015

84. Phage-mediated dispersal of biofilm and distribution of bacterial virulence genes is induced by quorum sensing.

Author

Rossmann FS, Racek T, Wobser D, Puchalka J, Rabener EM, Reiger M, Hendrickx AP, Diederich AK, Jung K, Klein C, and Huebner J

Subjects

Animals, Biofilms drug effects, Caco-2 Cells, Ciprofloxacin pharmacology, Endocarditis, Bacterial pathology, Female, Humans, Mice, Mice, Inbred BALB C, Rats, Rats, Wistar, Sepsis pathology, Virus Release drug effects, Biofilms growth & development, Endocarditis, Bacterial microbiology, Enterococcus faecalis pathogenicity, Enterococcus faecalis physiology, Enterococcus faecalis virology, Prophages physiology, Quorum Sensing, Sepsis microbiology, Virulence Factors metabolism, Virus Release physiology

Abstract

The microbiome and the phage meta-genome within the human gut are influenced by antibiotic treatments. Identifying a novel mechanism, here we demonstrate that bacteria use the universal communication molecule AI-2 to induce virulence genes and transfer them via phage release. High concentrations (i.e. 100 μM) of AI-2 promote dispersal of bacteria from already established biofilms, and is associated with release of phages capable of infecting other bacteria. Enterococcus faecalis V583ΔABC harbours 7 prophages in its genome, and a mutant deficient in one of these prophages (i.e. prophage 5) showed a greatly reduced dispersal of biofilm. Infection of a probiotic E. faecalis strain without lytic prophages with prophage 5 resulted in increased biofilm formation and also in biofilm dispersal upon induction with AI-2. Infection of the probiotic E. faecalis strain with phage-containing supernatants released through AI-2 from E. faecalis V583ΔABC resulted in a strong increase in pathogenicity of this strain. The polylysogenic probiotic strain was also more virulent in a mouse sepsis model and a rat endocarditis model. Both AI-2 and ciprofloxacin lead to phage release, indicating that conditions in the gastrointestinal tract of hospitalized patients treated with antibiotics might lead to distribution of virulence genes to apathogenic enterococci and possibly also to other commensals or even to beneficial probiotic strains.

Published

2015

85. Suppression of influenza A virus replication in human lung epithelial cells by noncytotoxic concentrations bafilomycin A1.

Author

Yeganeh B, Ghavami S, Kroeker AL, Mahood TH, Stelmack GL, Klonisch T, Coombs KM, and Halayko AJ

Subjects

Animals, Autophagy, Cell Line, Tumor, Dogs, Drug Evaluation, Preclinical, Humans, Influenza A Virus, H1N1 Subtype drug effects, Madin Darby Canine Kidney Cells, Virus Attachment, Virus Release drug effects, Alveolar Epithelial Cells virology, Antiviral Agents pharmacology, Influenza A Virus, H1N1 Subtype physiology, Macrolides pharmacology, Virus Replication drug effects

Abstract

Subcellular trafficking within host cells plays a critical role in viral life cycles, including influenza A virus (IAV). Thus targeting relevant subcellular compartments holds promise for effective intervention to control the impact of influenza infection. Bafilomycin A1 (Baf-A1), when used at relative high concentrations (≥10 nM), inhibits vacuolar ATPase (V-ATPase) and reduces endosome acidification and lysosome number, thus inhibiting IAV replication but promoting host cell cytotoxicity. We tested the hypothesis that much lower doses of Baf-A1 also have anti-IAV activity, but without toxic effects. Thus we assessed the antiviral activity of Baf-A1 at different concentrations (0.1-100 nM) in human alveolar epithelial cells (A549) infected with IAV strain A/PR/8/34 virus (H1N1). Infected and mock-infected cells pre- and cotreated with Baf-A1 were harvested 0-24 h postinfection and analyzed by immunoblotting, immunofluorescence, and confocal and electron microscopy. We found that Baf-A1 had disparate concentration-dependent effects on subcellular organelles and suppressed affected IAV replication. At concentrations ≥10 nM Baf-A1 inhibited acid lysosome formation, which resulted in greatly reduced IAV replication and release. Notably, at a very low concentration of 0.1 nM that is insufficient to reduce lysosome number, Baf-A1 retained the capacity to significantly impair IAV nuclear accumulation as well as IAV replication and release. In contrast to the effects of high concentrations of Baf-A1, very low concentrations did not exhibit cytotoxic effects or induce apoptotic cell death, based on morphological and FACS analyses. In conclusion, our results reveal that low-concentration Baf-A1 is an effective inhibitor of IAV replication, without impacting host cell viability., (Copyright © 2015 the American Physiological Society.)

Published

2015

86. The effects of neuraminidase inhibitors on the release of oseltamivir-sensitive and oseltamivir-resistant influenza viruses from primary cultures of human tracheal epithelium.

Author

Yamaya M, Nadine L, Kubo H, Saito K, Saito R, and Nishimura H

Subjects

Aged, Aged, 80 and over, Cells, Cultured, Female, Humans, Influenza A Virus, H1N1 Subtype physiology, Inhibitory Concentration 50, Male, Respiratory Mucosa, Virus Release drug effects, Virus Replication drug effects, Antiviral Agents pharmacology, Drug Resistance, Viral, Epithelial Cells drug effects, Epithelial Cells virology, Influenza A Virus, H1N1 Subtype drug effects, Oseltamivir pharmacology

Abstract

Defining the effects of neuraminidase inhibitors on influenza virus infection may provide important information for the treatment of patients. The effects of neuraminidase inhibitors have been examined using various methods, including viral release from kidney cells. However, the effects of neuraminidase inhibitors on viral release from primary cultures of human tracheal epithelial cells, which retain functions of the original tissues, have not been studied. The effects of neuraminidase inhibitors on the replication of the pandemic influenza virus [A/Sendai-H/N0633/2009 (H1N1) pdm09] and the seasonal influenza virus [A/Sendai-H/216/2009 (H1N1)] that was isolated during the 2008-2009 season were examined. The virus stocks were generated by infecting tracheal cells with the pandemic or seasonal influenza virus. Four types of inhibitors (oseltamivir, zanamivir, laninamivir, and peramivir) reduced pandemic viral titers and concentrations of the cytokines interleukin-6 and tumor necrosis factor-α in supernatants and viral RNA in cells. However, oseltamivir did not reduce seasonal viral titers, cytokine concentrations and viral RNA, and the 50% inhibitory concentration (IC50 ) of oseltamivir for neuraminidase activity in the seasonal virus was 300-fold higher than that observed for the pandemic influenza virus. The seasonal influenza virus had an oseltamivir-resistant genotype. The magnitude of the IC50 values of the neuraminidase inhibitors for the seasonal influenza virus was inversely related to the magnitude of the inhibitory effects on viral release. These methods for measuring the release of virus and inflammatory cytokines from primary cultures of human tracheal epithelium may provide useful information regarding the effects of neuraminidase inhibitors on influenza viruses., (© 2014 Wiley Periodicals, Inc.)

Published

2015

87. Antiviral therapy for human rabies.

Author

Appolinario CM and Jackson AC

Subjects

Adrenal Cortex Hormones, Amides therapeutic use, Animals, Central Nervous System immunology, Central Nervous System pathology, Central Nervous System virology, Combined Modality Therapy, Contraindications, Humans, Minocycline, Molecular Targeted Therapy, Pyrazines therapeutic use, RNA, Small Interfering therapeutic use, Rabies immunology, Rabies pathology, Rabies virology, Rabies virus genetics, Rabies virus pathogenicity, Virus Assembly drug effects, Virus Release drug effects, Antiviral Agents therapeutic use, Central Nervous System drug effects, Immunologic Factors therapeutic use, Neuroprotective Agents therapeutic use, Rabies drug therapy, Rabies virus drug effects

Abstract

Human rabies is virtually always fatal despite numerous attempts at aggressive therapy. Most survivors received one or more doses of rabies vaccine prior to the onset of the disease. The Milwaukee Protocol has proved to be ineffective for rabies and should no longer be used. New approaches are needed and an improved understanding of basic mechanisms responsible for the clinical disease in rabies may prove to be useful for the development of novel therapeutic approaches. Antiviral therapy is thought to be an important component of combination therapy for the management of human rabies, and immunotherapy and neuroprotective therapy should also be strongly considered. There are many important issues for consideration regarding drug delivery to the central nervous system in rabies, which are in part related to the presence of the blood-brain barrier and also the blood-spinal cord barrier. Ribavirin and interferon-α have proved to be disappointing agents for the therapy of rabies. There is insufficient evidence to support the continued use of ketamine or amantadine for the therapy of rabies. Minocycline or corticosteroids should not be used because of concerns about aggravating the disease. A variety of new antiviral agents are under development and evaluation, including favipiravir, RNA interference (for example, small interfering [si]RNAs) and novel targeted approaches, including interference with viral capsid assembly and viral egress.

Published

2015

88. Understanding early serum hepatitis D virus and hepatitis B surface antigen kinetics during pegylated interferon-alpha therapy via mathematical modeling.

Author

Guedj J, Rotman Y, Cotler SJ, Koh C, Schmid P, Albrecht J, Haynes-Williams V, Liang TJ, Hoofnagle JH, Heller T, and Dahari H

Subjects

Adolescent, Adult, Antiviral Agents therapeutic use, Clinical Trials as Topic, Female, Hepatitis B, Chronic complications, Hepatitis B, Chronic drug therapy, Hepatitis D, Chronic complications, Hepatitis D, Chronic drug therapy, Humans, Interferon-alpha therapeutic use, Male, Middle Aged, Polyethylene Glycols therapeutic use, Recombinant Proteins pharmacology, Recombinant Proteins therapeutic use, Treatment Outcome, Virus Release drug effects, Virus Replication drug effects, Young Adult, Antiviral Agents pharmacology, Hepatitis B Surface Antigens blood, Hepatitis Delta Virus drug effects, Interferon-alpha pharmacology, Models, Biological, Polyethylene Glycols pharmacology, RNA, Viral blood

Abstract

Unlabelled: There is little information on the early kinetics of hepatitis delta virus (HDV) and hepatitis B surface antigen (HBsAg) during interferon-α therapy. Here a mathematical model was developed and fitted to frequent HDV and HBsAg kinetic data from 10 patients during the first 28 weeks of pegylated-interferon-α2a (peg-IFN) therapy. Three patients achieved a complete virological response (CVR), defined as undetectable HDV 6 months after treatment stopped with loss of HBsAg and anti-HBsAg seroconversion. After initiation of therapy, a median delay of 9 days (interquartile range [IQR]: 5-15) was observed with no significant changes in HDV level. Thereafter, HDV declined in a biphasic manner, where a rapid first phase lasting for 25 days (IQR: 23-58) was followed by a slower or plateau second phase. The model predicts that the main effect of peg-IFN is to reduce HDV production/release with a median effectiveness of 96% (IQR: 93-99.8). Median serum HDV half-life (t1/2 ) was estimated as 2.9 days (IQR: 1.5-5.3) corresponding to a pretreatment production and clearance of about 10(10) (IQR: 10(9.7) -10(10.7) ) virions/day. None of the patients with flat second phase in HDV achieved CVR. HBsAg kinetics of decline paralleled the second phase of HDV decline consistent with HBsAg-productive-infected cells being the main source of production of HDV, with a median t1/2 of 135 days (IQR: 20-460). The interferon lambda-3 polymorphism (rs12979860) was not associated with kinetic parameters., Conclusion: Modeling results provide insights into HDV-host dynamics, the relationship between serum HBsAg levels and HBsAg-infected cells, IFN's mode of action, and its effectiveness. The observation that a flat second phase in HDV and HBsAg kinetics was associated with failure to achieve CVR provides the basis to develop early stopping rules during peg-IFN treatment in HDV-infected patients., (© 2014 by the American Association for the Study of Liver Diseases. This article has been contributed to by U.S. Government employees and their work is in the public domain in the USA.)

Published

2014

89. Characterization of a broadly neutralizing monoclonal antibody that targets the fusion domain of group 2 influenza A virus hemagglutinin.

Author

Tan GS, Lee PS, Hoffman RM, Mazel-Sanchez B, Krammer F, Leon PE, Ward AB, Wilson IA, and Palese P

Subjects

Animals, Antibodies, Monoclonal therapeutic use, Antibodies, Neutralizing therapeutic use, Antibodies, Viral therapeutic use, Cell Line, Disease Models, Animal, Epitopes immunology, Female, Hemagglutinin Glycoproteins, Influenza Virus therapeutic use, Humans, Immunization, Passive, Mice, Inbred BALB C, Microscopy, Electron, Transmission, Orthomyxoviridae Infections prevention & control, Orthomyxoviridae Infections therapy, Treatment Outcome, Virus Internalization drug effects, Virus Release drug effects, Antibodies, Monoclonal immunology, Antibodies, Neutralizing immunology, Antibodies, Viral immunology, Hemagglutinin Glycoproteins, Influenza Virus immunology

Abstract

Unlabelled: Due to continuous changes to its antigenic regions, influenza viruses can evade immune detection and cause a significant amount of morbidity and mortality around the world. Influenza vaccinations can protect against disease but must be annually reformulated to match the current circulating strains. In the development of a broad-spectrum influenza vaccine, the elucidation of conserved epitopes is paramount. To this end, we designed an immunization strategy in mice to boost the humoral response against conserved regions of the hemagglutinin (HA) glycoprotein. Of note, generation and identification of broadly neutralizing antibodies that target group 2 HAs are rare and thus far have yielded only a few monoclonal antibodies (MAbs). Here, we demonstrate that mouse MAb 9H10 has broad and potent in vitro neutralizing activity against H3 and H10 group 2 influenza A subtypes. In the mouse model, MAb 9H10 protects mice against two divergent mouse-adapted H3N2 strains, in both pre- and postexposure administration regimens. In vitro and cell-free assays suggest that MAb 9H10 inhibits viral replication by blocking HA-dependent fusion of the viral and endosomal membranes early in the replication cycle and by disrupting viral particle egress in the late stage of infection. Interestingly, electron microscopy reconstructions of MAb 9H10 bound to the HA reveal that it binds a similar binding footprint to MAbs CR8020 and CR8043., Importance: The influenza hemagglutinin is the major antigenic target of the humoral immune response. However, due to continuous antigenic changes that occur on the surface of this glycoprotein, influenza viruses can escape the immune system and cause significant disease to the host. Toward the development of broad-spectrum therapeutics and vaccines against influenza virus, elucidation of conserved regions of influenza viruses is crucial. Thus, defining these types of epitopes through the generation and characterization of broadly neutralizing monoclonal antibodies (MAbs) can greatly assist others in highlighting conserved regions of hemagglutinin. Here, we demonstrate that MAb 9H10 that targets the hemagglutinin stalk has broadly neutralizing activity against group 2 influenza A viruses in vitro and in vivo., (Copyright © 2014, American Society for Microbiology. All Rights Reserved.)

Published

2014

90. Antiviral activity of baicalin against influenza A (H1N1/H3N2) virus in cell culture and in mice and its inhibition of neuraminidase.

Author

Ding Y, Dou J, Teng Z, Yu J, Wang T, Lu N, Wang H, and Zhou C

Subjects

Administration, Intravenous, Animals, Antiviral Agents isolation & purification, Antiviral Agents therapeutic use, Cell Culture Techniques, Disease Models, Animal, Dogs, Enzyme Inhibitors isolation & purification, Enzyme Inhibitors pharmacology, Enzyme Inhibitors therapeutic use, Flavonoids isolation & purification, Flavonoids therapeutic use, Influenza A Virus, H1N1 Subtype enzymology, Influenza A Virus, H1N1 Subtype physiology, Influenza A Virus, H3N2 Subtype enzymology, Influenza A Virus, H3N2 Subtype physiology, Inhibitory Concentration 50, Lung pathology, Lung virology, Madin Darby Canine Kidney Cells, Mice, Microbial Sensitivity Tests, Orthomyxoviridae Infections drug therapy, Scutellaria chemistry, Survival Analysis, Treatment Outcome, Virus Release drug effects, Antiviral Agents pharmacology, Flavonoids pharmacology, Influenza A Virus, H1N1 Subtype drug effects, Influenza A Virus, H3N2 Subtype drug effects, Neuraminidase antagonists & inhibitors, Viral Proteins antagonists & inhibitors

Abstract

Scutellaria baicalensis Georgi, a Chinese herbal decoction, has been used for the treatment of the common cold, fever and influenza virus infections. In previous studies, we found that oral administration of baicalein resulted in the inhibition of influenza A virus replication in vivo, which was linked to baicalin in serum. However, the effective dose and underlying mechanisms of the efficacy of baicalin against influenza A virus have not been fully elucidated. In this study, the antiviral effects of baicalin in influenza-virus-infected MDCK cells and mice were examined. The neuraminidase inhibition assay was performed to investigate the mechanism of action of baicalin. In vitro results showed that baicalin exhibited a half-maximal effective concentration (EC50) of 43.3 μg/ml against the influenza A/FM1/1/47 (H1N1) virus and 104.9 μg/ml against the influenza A/Beijing/32/92 (H3N2) virus. When added to MDCK cell cultures after inoculation with influenza virus, baicalin demonstrated obvious antiviral activity that increased in a dose-dependent manner, indicating that baicalin affected virus budding. Baicalin had clear inhibitory effects against neuraminidases, with half-maximal inhibitory concentration (IC50) of 52.3 μg/ml against the influenza A/FM1/1/47 (H1N1) virus and 85.8 μg/ml against the influenza A/Beijing/32/92 (H3N2) virus. In vivo studies showed that an intravenous injection of baicalin effectively reduced the death rate, prolonged the mean day to death (MDD) and improved the lung parameters of mice infected with influenza A virus. These results demonstrate that baicalin acts as a neuraminidase inhibitor, with clear inhibitory activities that are effective against different strains of influenza A virus in both cell culture and a mouse model, and that baicalin has potential utility in the management of influenza virus infections.

Published

2014

91. Cecropin P1 inhibits porcine reproductive and respiratory syndrome virus by blocking attachment.

Author

Guo C, Huang Y, Cong P, Liu X, Chen Y, and He Z

Subjects

Animals, Cell Line, Epithelial Cells immunology, Epithelial Cells virology, Macrophages, Alveolar immunology, Macrophages, Alveolar virology, Swine, Virus Release drug effects, Peptides metabolism, Porcine respiratory and reproductive syndrome virus immunology, Porcine respiratory and reproductive syndrome virus physiology, Virus Attachment drug effects

Abstract

Background: Porcine reproductive and respiratory syndrome virus (PRRSV) is a continuous threat to the pig industry, causing high economic losses worldwide. Current vaccines have specific limitations in terms of their safety and efficacy, so the development of novel antiviral drugs is urgently required. The aim of this study was to evaluate the inhibitory effects and underlying molecular mechanisms of the antimicrobial peptide cecropin P1 (CP1) against PRRSV infection in vitro., Results: CP1 not only displayed extracellular virucidal activity against PRRSV, but also exerted a potent inhibitory effect when added either before, simultaneously with, or after viral inoculation. The inhibitory effect of CP1 occurred during viral attachment, but not at viral entry into Marc-145 cells. CP1 also inhibited viral particle release and attenuated virus-induced apoptosis during the late phase of infection. CP1 exerted similar inhibitory effects against PRRSV infection in porcine alveolar macrophages, the cells targeted by the virus in vivo during its infection of pigs. The expression of interleukin 6 was elevated by CP1 in porcine alveolar macrophages, which might contribute to its inhibition of PRRSV infection., Conclusions: Collectively, our findings provide a new direction for the development of potential therapeutic drugs against PRRSV infection.

Published

2014

92. Genistein inhibits the replication of avian leucosis virus subgroup J in DF-1 cells.

Author

Qian K, Gao AJ, Zhu MY, Shao HX, Jin WJ, Ye JQ, and Qin AJ

Subjects

Animals, Cell Line, Chickens, Microbial Sensitivity Tests, Transcription, Genetic drug effects, Antiviral Agents pharmacology, Avian Leukosis Virus drug effects, Avian Leukosis Virus physiology, Genistein pharmacology, Virus Release drug effects, Virus Replication drug effects

Abstract

To investigate the antiviral effects of genistein on the replication of avian leukosis virus subgroup J (ALV-J) in DF-1 cells, the cells were treated with genistein at different time points and the antiviral effects were examined by using a variety of assays. We determined that genistein strongly inhibited viral gene expression and decreased the viral protein level in the cell supernatant and the cytoplasm without alerting virus receptor expression and viral attachment. We also observed that genistein was not found to interfere with virus entry, but significantly inhibited both viral gene transcriptions at 24h post infection and virus release, which indicate that genistein exerts its inhibitory effects on the late phase of ALV-J replicative cycle. These results demonstrate that genistein effectively block ALV-J replication by inhibiting virus transcription and release in DF-1 cells, which may be useful for therapeutic drug design., (Copyright © 2014 Elsevier B.V. All rights reserved.)

Published

2014

93. Characterization of the mode of action of a potent dengue virus capsid inhibitor.

Author

Scaturro P, Trist IM, Paul D, Kumar A, Acosta EG, Byrd CM, Jordan R, Brancale A, and Bartenschlager R

Subjects

Amino Acid Sequence, Animals, Antiviral Agents chemistry, Capsid chemistry, Capsid Proteins chemistry, Cell Line, Tumor, Chlorocebus aethiops, Cricetinae, Crystallography, X-Ray, Dengue Virus chemistry, Dengue Virus physiology, HEK293 Cells, Hepatocytes drug effects, Hepatocytes virology, Heterocyclic Compounds, 3-Ring chemistry, Humans, Molecular Docking Simulation, Molecular Sequence Data, Sequence Alignment, Thiadiazoles chemistry, Vero Cells, Virion chemistry, Virion drug effects, Virus Internalization drug effects, Virus Release drug effects, Antiviral Agents pharmacology, Capsid drug effects, Capsid Proteins antagonists & inhibitors, Dengue Virus drug effects, Heterocyclic Compounds, 3-Ring pharmacology, Thiadiazoles pharmacology, Virus Assembly drug effects

Abstract

Unlabelled: Dengue viruses (DV) represent a significant global health burden, with up to 400 million infections every year and around 500,000 infected individuals developing life-threatening disease. In spite of attempts to develop vaccine candidates and antiviral drugs, there is a lack of approved therapeutics for the treatment of DV infection. We have previously reported the identification of ST-148, a small-molecule inhibitor exhibiting broad and potent antiviral activity against DV in vitro and in vivo (C. M. Byrd et al., Antimicrob. Agents Chemother. 57:15-25, 2013, doi:10 .1128/AAC.01429-12). In the present study, we investigated the mode of action of this promising compound by using a combination of biochemical, virological, and imaging-based techniques. We confirmed that ST-148 targets the capsid protein and obtained evidence of bimodal antiviral activity affecting both assembly/release and entry of infectious DV particles. Importantly, by using a robust bioluminescence resonance energy transfer-based assay, we observed an ST-148-dependent increase of capsid self-interaction. These results were corroborated by molecular modeling studies that also revealed a plausible model for compound binding to capsid protein and inhibition by a distinct resistance mutation. These results suggest that ST-148-enhanced capsid protein self-interaction perturbs assembly and disassembly of DV nucleocapsids, probably by inducing structural rigidity. Thus, as previously reported for other enveloped viruses, stabilization of capsid protein structure is an attractive therapeutic concept that also is applicable to flaviviruses., Importance: Dengue viruses are arthropod-borne viruses representing a significant global health burden. They infect up to 400 million people and are endemic to subtropical and tropical areas of the world. Currently, there are neither vaccines nor approved therapeutics for the prophylaxis or treatment of DV infections, respectively. This study reports the characterization of the mode of action of ST-148, a small-molecule capsid inhibitor with potent antiviral activity against all DV serotypes. Our results demonstrate that ST-148 stabilizes capsid protein self-interaction, thereby likely perturbing assembly and disassembly of viral nucleocapsids by inducing structural rigidity. This, in turn, might interfere with the release of viral RNA from incoming nucleocapsids (uncoating) as well as assembly of progeny virus particles. As previously reported for other enveloped viruses, we propose the capsid as a novel tractable target for flavivirus inhibitors., (Copyright © 2014, American Society for Microbiology. All Rights Reserved.)

Published

2014

94. Comparison of effects of inhibitors of viral and cellular protein kinases on human cytomegalovirus disruption of nuclear lamina and nuclear egress.

Author

Sharma M and Coen DM

Subjects

Capsid metabolism, Cell Line, Cell Nucleus drug effects, Cytomegalovirus drug effects, Cytomegalovirus genetics, Cytomegalovirus physiology, Cytomegalovirus Infections virology, Humans, Nuclear Lamina drug effects, Phosphotransferases (Alcohol Group Acceptor) genetics, Phosphotransferases (Alcohol Group Acceptor) metabolism, Protein Kinase C metabolism, Virus Assembly drug effects, Cell Nucleus virology, Cytomegalovirus enzymology, Cytomegalovirus Infections enzymology, Nuclear Lamina virology, Phosphotransferases (Alcohol Group Acceptor) antagonists & inhibitors, Protein Kinase C antagonists & inhibitors, Protein Kinase Inhibitors pharmacology, Virus Release drug effects

Abstract

Human cytomegalovirus (HCMV) kinase UL97 is required for efficient nuclear lamina disruption during nuclear egress. However, cellular protein kinase C (PKC) has been implicated in this process in other systems. Comparing the effects of UL97 and cellular kinase inhibitors on HCMV nuclear egress confirms a role for UL97 in lamina disruption and nuclear egress. A pan-PKC inhibitor did not affect lamina disruption but did reduce the number of cytoplasmic capsids more than the number of nuclear capsids., (Copyright © 2014, American Society for Microbiology. All Rights Reserved.)

Published

2014

95. Monoclonal antibody targeting chikungunya virus envelope 1 protein inhibits virus release.

Author

Masrinoul P, Puiprom O, Tanaka A, Kuwahara M, Chaichana P, Ikuta K, Ramasoota P, and Okabayashi T

Subjects

Animals, Antibodies, Monoclonal immunology, Antibodies, Viral immunology, Chikungunya Fever virology, Chikungunya virus immunology, Chikungunya virus physiology, Female, Humans, Mice, Mice, Inbred BALB C, Virus Internalization drug effects, Antibodies, Monoclonal pharmacology, Antibodies, Viral pharmacology, Chikungunya Fever drug therapy, Chikungunya virus drug effects, Viral Envelope Proteins immunology, Virus Release drug effects

Abstract

Chikungunya virus (CHIKV) causes an acute clinical illness characterized by sudden high fever, intense joint pain, and skin rash. Recent outbreaks of chikungunya disease in Africa and Asia are a major public health concern; however, there is currently no effective licensed vaccine or specific treatment. This study reported the development of a mouse monoclonal antibody (MAb), CK47, which recognizes domain III within the viral envelope 1 protein and inhibited the viral release process, thereby preventing the production of progeny virus. The MAb had no effect on virus entry and replication processes. Thus, CK47 may be a useful tool for studying the mechanisms underlying CHIKV release and may show potential as a therapeutic agent., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2014

96. Essential role of calcium in the infection process of broad-spectrum methicillin-resistant Staphylococcus aureus bacteriophage.

Author

Chhibber S, Kaur T, and Kaur S

Subjects

Bacteriophages pathogenicity, Staphylococcal Infections therapy, Calcium pharmacology, Methicillin-Resistant Staphylococcus aureus virology, Virus Attachment drug effects, Virus Internalization drug effects, Virus Release drug effects

Abstract

Phage therapy presents an alternative therapeutic option in treating infections caused by methicillin-resistant Staphylococcus aureus (MRSA) strains not responding to antibiotic therapy. However, it is essential to study the role of external factors that may influence the yield and potency of phage preparations intended for use in various in vitro and in vivo studies. The present study focuses on the effects of calcium in the entire infection process of a broad-spectrum lytic bacteriophage: MR-10. The presence of calcium increased the adsorption rate of the phage and also participated in the process of penetration of the phage genome into the host cytoplasm. A final concentration of 5 mM of calcium ions supplemented in soft agar during the phage titration process significantly increased the phage titer. Hence, incorporation of such divalent cations during the isolation of lytic phages active against MRSA strains and during the preparation of high-titer active phage preparations would definitely increase the isolation frequency and the final phage yield. This will contribute towards more effective phage preparations for use in treatments against MRSA infections., (© 2014 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2014

97. Small-molecule probes targeting the viral PPxY-host Nedd4 interface block egress of a broad range of RNA viruses.

Author

Han Z, Lu J, Liu Y, Davis B, Lee MS, Olson MA, Ruthel G, Freedman BD, Schnell MJ, Wrobel JE, Reitz AB, and Harty RN

Subjects

Blotting, Western, Endosomal Sorting Complexes Required for Transport antagonists & inhibitors, Genetic Complementation Test, Humans, Nedd4 Ubiquitin Protein Ligases, RNA Virus Infections virology, RNA Viruses drug effects, RNA, Viral genetics, Structure-Activity Relationship, Ubiquitin-Protein Ligases antagonists & inhibitors, Viral Matrix Proteins antagonists & inhibitors, Virion drug effects, Virion physiology, Endosomal Sorting Complexes Required for Transport metabolism, Pharmaceutical Preparations metabolism, Protein Binding drug effects, RNA Virus Infections drug therapy, RNA Viruses physiology, Small Molecule Libraries, Ubiquitin-Protein Ligases metabolism, Viral Matrix Proteins metabolism, Virus Release drug effects

Abstract

Unlabelled: Budding of filoviruses, arenaviruses, and rhabdoviruses is facilitated by subversion of host proteins, such as Nedd4 E3 ubiquitin ligase, by viral PPxY late (L) budding domains expressed within the matrix proteins of these RNA viruses. As L domains are important for budding and are highly conserved in a wide array of RNA viruses, they represent potential broad-spectrum targets for the development of antiviral drugs. To identify potential competitive blockers, we used the known Nedd4 WW domain-PPxY interaction interface as the basis of an in silico screen. Using PPxY-dependent budding of Marburg (MARV) VP40 virus-like particles (VLPs) as our model system, we identified small-molecule hit 1 that inhibited Nedd4-PPxY interaction and PPxY-dependent budding. This lead candidate was subsequently improved with additional structure-activity relationship (SAR) analog testing which enhanced antibudding activity into the nanomolar range. Current lead compounds 4 and 5 exhibit on-target effects by specifically blocking the MARV VP40 PPxY-host Nedd4 interaction and subsequent PPxY-dependent egress of MARV VP40 VLPs. In addition, lead compounds 4 and 5 exhibited antibudding activity against Ebola and Lassa fever VLPs, as well as vesicular stomatitis and rabies viruses (VSV and RABV, respectively). These data provide target validation and suggest that inhibition of the PPxY-Nedd4 interaction can serve as the basis for the development of a novel class of broad-spectrum, host-oriented antivirals targeting viruses that depend on a functional PPxY L domain for efficient egress., Importance: There is an urgent and unmet need for the development of safe and effective therapeutics against biodefense and high-priority pathogens, including filoviruses (Ebola and Marburg) and arenaviruses (e.g., Lassa and Junin) which cause severe hemorrhagic fever syndromes with high mortality rates. We along with others have established that efficient budding of filoviruses, arenaviruses, and other viruses is critically dependent on the subversion of host proteins. As disruption of virus budding would prevent virus dissemination, identification of small-molecule compounds that block these critical viral-host interactions should effectively block disease progression and transmission. Our findings provide validation for targeting these virus-host interactions as we have identified lead inhibitors with broad-spectrum antiviral activity. In addition, such inhibitors might prove useful for newly emerging RNA viruses for which no therapeutics would be available., (Copyright © 2014, American Society for Microbiology. All Rights Reserved.)

Published

2014

98. Turmeric curcumin inhibits entry of all hepatitis C virus genotypes into human liver cells.

Author

Anggakusuma, Colpitts CC, Schang LM, Rachmawati H, Frentzen A, Pfaender S, Behrendt P, Brown RJ, Bankwitz D, Steinmann J, Ott M, Meuleman P, Rice CM, Ploss A, Pietschmann T, and Steinmann E

Subjects

Animals, Antiviral Agents therapeutic use, Cell Line, Cell Line, Tumor, Curcumin therapeutic use, Hepacivirus physiology, Hepatitis C virology, Humans, Mice, Virus Assembly drug effects, Virus Release drug effects, Virus Replication drug effects, Antiviral Agents pharmacology, Curcumin pharmacology, Hepacivirus drug effects, Hepatitis C prevention & control, Hepatocytes virology, Virus Internalization drug effects

Abstract

Objective: Hepatitis C virus (HCV) infection causes severe liver disease and affects more than 160 million individuals worldwide. People undergoing liver organ transplantation face universal re-infection of the graft. Therefore, affordable antiviral strategies targeting the early stages of infection are urgently needed to prevent the recurrence of HCV infection. The aim of the study was to determine the potency of turmeric curcumin as an HCV entry inhibitor., Design: The antiviral activity of curcumin and its derivatives was evaluated using HCV pseudo-particles (HCVpp) and cell-culture-derived HCV (HCVcc) in hepatoma cell lines and primary human hepatocytes. The mechanism of action was dissected using R18-labelled virions and a membrane fluidity assay., Results: Curcumin treatment had no effect on HCV RNA replication or viral assembly/release. However, co-incubation of HCV with curcumin potently inhibited entry of all major HCV genotypes. Similar antiviral activities were also exerted by other curcumin derivatives but not by tetrahydrocurcumin, suggesting the importance of α,β-unsaturated ketone groups for the antiviral activity. Expression levels of known HCV receptors were unaltered, while pretreating the virus with the compound reduced viral infectivity without viral lysis. Membrane fluidity experiments indicated that curcumin affected the fluidity of the HCV envelope resulting in impairment of viral binding and fusion. Curcumin has also been found to inhibit cell-to-cell transmission and to be effective in combination with other antiviral agents., Conclusions: Turmeric curcumin inhibits HCV entry independently of the genotype and in primary human hepatocytes by affecting membrane fluidity thereby impairing virus binding and fusion.

Published

2014

99. Heat shock protein 90 positively regulates Chikungunya virus replication by stabilizing viral non-structural protein nsP2 during infection.

Author

Das I, Basantray I, Mamidi P, Nayak TK, B M P, Chattopadhyay S, and Chattopadhyay S

Subjects

Animals, Antiviral Agents pharmacology, Benzoquinones pharmacology, Chlorocebus aethiops, HSP90 Heat-Shock Proteins antagonists & inhibitors, Lactams, Macrocyclic pharmacology, Protein Biosynthesis drug effects, Protein Biosynthesis genetics, Protein Stability, Vero Cells, Viral Nonstructural Proteins genetics, Virus Release drug effects, Chikungunya virus physiology, HSP90 Heat-Shock Proteins metabolism, Viral Nonstructural Proteins metabolism, Virus Replication drug effects

Abstract

Background: The high morbidity and socio-economic loss associated with the recent massive global outbreak of Chikungunya virus (CHIKV) emphasize the need to understand the biology of the virus for developing effective antiviral therapies., Methods and Findings: In this study, an attempt was made to understand the molecular mechanism involved in Heat shock protein 90 (Hsp90) mediated regulation of CHIKV infection in mammalian cells using CHIKV prototype strain (S 27) and Indian outbreak strain of 2006 (DRDE-06). Our results showed that Hsp90 is required at a very early stage of viral replication and Hsp90 inhibitor Geldanamycin (GA) can abrogate new virus particle formation more effectively in the case of S 27 than that of DRDE-06. Further analysis revealed that CHIKV nsP2 protein level is specifically reduced by GA treatment as well as HSP90-siRNA transfection; however, viral RNA remains unaltered. Immunoprecipitation analysis showed that nsP2 interacts with Hsp90 during infection; however this interaction is reduced in the presence of GA. In addition, our analysis on Hsp90 associated PI3K/Akt/mTOR signaling pathway demonstrated that CHIKV infection stabilizes Raf1 and activates Hsp90 client protein Akt, which in turn phosphorylates mTOR. Subsequently, this phosphorylation leads to the activation of two important downstream effectors, S6K and 4EBP1, which may facilitate translation of viral as well as cellular mRNAs. Hence, the data suggests that CHIKV infection is regulated by Hsp90 associated Akt phosphorylation and DRDE-06 is more efficient than S 27 in enhancing the activation of host signaling molecules for its efficient replication and virus production., Conclusion: Hsp90 positively regulates Chikungunya virus replication by stabilizing CHIKV-nsP2 through its interaction during infection. The study highlights the possible molecular mechanism of GA mediated inhibition of CHIKV replication and differential effect of this drug on S 27 and DRDE-06, which will be informative for developing effective anti-CHIKV therapies in future.

Published

2014

100. Genistein as antiviral drug against HIV ion channel.

Author

Sauter D, Schwarz S, Wang K, Zhang R, Sun B, and Schwarz W

Subjects

Animals, Antiviral Agents chemistry, Female, Flavanones chemistry, Flavonoids chemistry, Gene Expression, Genistein chemistry, Human Immunodeficiency Virus Proteins antagonists & inhibitors, Humans, Ion Channels drug effects, Patch-Clamp Techniques, RNA, Complementary genetics, Transgenes, Viral Regulatory and Accessory Proteins antagonists & inhibitors, Virus Release drug effects, Xenopus laevis, Antiviral Agents pharmacology, Flavanones pharmacology, Flavonoids pharmacology, Genistein pharmacology, HIV Infections drug therapy, HIV-1 drug effects

Abstract

Various drugs found in Chinese herbs are well known for their antiviral potency. We have tested several flavonoids with respect to their potency to block the viral protein U of the human immunodeficiency type 1 virus, which is believed to form a cation-permeable ion channel in the infected cell. We used Xenopus oocytes with heterologously expressed viral protein U as model system to test the efficacy of the drugs in voltage-clamp experiments. This method had been demonstrated in the past as a useful tool to screen drugs for their potency in inhibition of ion channel activity. The viral protein U-mediated current could be inhibited by Ba(2+) with a K1/2 value of 1.6 mM. Therefore, we determined viral protein U-mediated current as current component blocked by 10 mM Ba(2+). We screened several flavonoids with respect to their effects on this current. The flavonols quercetin and kaempferol, and the flavanols (-)epigallochatechin and (-)epichatechin were ineffective. The flavanone naringenin showed at 20 µM slight (about 10%) inhibition. The most potent drug was the isoflavon genistein which exhibited at 20 µM significant inhibition of about 40% with a K1/2 value of 81 ± 4 µM. We suggest that viral ion channels, in general, may be a good target for development of antiviral agents, and that, in particular, isoflavons may be candidates for development of drugs targeting viral protein U., (Georg Thieme Verlag KG Stuttgart · New York.)

Published

2014