Your search keyword '"entry inhibitor"' showing total 1,068 results

101. Excellent safety and effectiveness of high-dose myrcludex-B monotherapy administered for 48 weeks in HDV-related compensated cirrhosis: A case report of 3 patients.

Author

Loglio, Alessandro, Ferenci, Peter, Uceda Renteria, Sara Colonia, Tham, Christine Y.L., van Bömmel, Florian, Borghi, Marta, Holzmann, Heidemarie, Perbellini, Riccardo, Trombetta, Elena, Giovanelli, Silvia, Greco, Letizia, Porretti, Laura, Prati, Daniele, Ceriotti, Ferruccio, Lunghi, Giovanna, Bertoletti, Antonio, and Lampertico, Pietro

Subjects

*HEPATITIS D virus, *HEPATITIS B virus, *CIRRHOSIS of the liver, *LIVER function tests, *CELL surface antigens

Abstract

Short-term administration of the entry inhibitor myrcludex-B (MyrB) has been shown to be safe and effective in phase II studies in patients coinfected with hepatitis B virus (HBV) and hepatitis delta virus (HDV). However, its effectiveness and safety are unknown during long-term and high-dose treatment of patients with compensated cirrhosis in real-life settings. Herein, we describe the first 3 European patients with HDV-related compensated cirrhosis who were treated with MyrB 10 mg/day for 48 weeks as a compassionate therapy. Liver function tests, bile acids, and virological markers were monitored every 4 weeks. HBV/HDV-specific T cell quantity (up to 48 and 36 weeks) and HBV RNA levels were also assessed in 2 cases. During MyrB treatment, HDV RNA levels progressively declined from 4.4 and 5.6 logs IU/ml to undetectability in 2 cases, and from 6.8 log copies/ml to 500 copies/ml for the other patient. Alanine aminotransferase normalised after 20, 12 and 28 weeks, respectively. A significant improvement in features of portal hypertension, liver function tests and alpha-fetoprotein levels were documented in 2 cases. In the male patient with histological and clinical stigmata of autoimmune hepatitis, IgG and immunoglobulins rapidly normalised. No significant changes in HBV surface antigen levels and circulating HBV/HDV-specific T cells were demonstrated; HBV DNA and HBV RNA levels remained undetectable throughout the study period. MyrB was well tolerated; patients remained fully asymptomatic despite a significant increase of bile acids. In conclusion, this report shows excellent safety and effectiveness of a 48-week course of MyrB 10 mg/day, combined with tenofovir disoproxil fumarate, for the treatment of HDV-related compensated cirrhosis. [ABSTRACT FROM AUTHOR]

Published

2019

102. Kinase inhibitors tyrphostin 9 and rottlerin block early steps of rabies virus cycle.

Author

Lama, Zoé, Gaudin, Yves, Blondel, Danielle, and Lagaudrière-Gesbert, Cécile

Subjects

*RABIES virus, *KINASE inhibitors, *VIRUS diseases, *VIRAL genomes, *VIRAL replication

Abstract

Rabies virus (RABV) is a neurotropic virus that causes fatal encephalitis in humans and animals and still kills up to 59,000 people worldwide every year. To date, only preventive or post-exposure vaccination protects against the disease but therapeutics are missing. After screening a library of 80 kinases inhibitors, we identified two compounds as potent inhibitors of RABV infection: tyrphostin 9 and rottlerin. Mechanism of action studies show that both inhibitors interfere with an early step of viral cycle and can prevent viral replication. In presence of tyrphostin 9, the viral entry through endocytosis is disturbed leading to improper delivery of viral particles in cytoplasm, whereas rottlerin is inhibiting the transcription, most likely by decreasing intracellular ATP concentration, and therefore the replication of the viral genome. • A library of 80 kinase inhibitors was screened for anti-rabies virus infection. • Tyrphostin 9 and Rottlerin inhibit early steps of rabies infection in vitro. • Tyrphostin 9 inhibits viral entry by blocking endosome acidification. • Rottlerin inhibits viral transcription, most likely by reducing intracellular ATP content. [ABSTRACT FROM AUTHOR]

Published

2019

103. Identification of a clinical compound losmapimod that blocks Lassa virus entry.

Author

Zhang, Xiaoyu, Yan, Feihu, Tang, Ke, Chen, Qing, Guo, Jiamei, Zhu, Wenjun, He, Shihua, Banadyga, Logan, Qiu, Xiangguo, and Guo, Ying

Subjects

*HEMORRHAGIC fever, *MITOGEN-activated protein kinases, *VIRUS diseases, *VIRUS inhibitors, *VIRUSES, *THERAPEUTICS, *LASSA fever virus

Abstract

Lassa virus (LASV) causes Lassa hemorrhagic fever in humans and poses a significant threat to public health in West Africa. Current therapeutic treatments for Lassa fever are limited, making the development of novel countermeasures an urgent priority. In this study, we identified losmapimod, a p38 mitogen-activated protein kinase (MAPK) inhibitor, from 102 screened compounds as an inhibitor of LASV infection. Losmapimod exerted its inhibitory effect against LASV after p38 MAPK down-regulation, and, interestingly, had no effect on other arenaviruses capable of causing viral hemorrhagic fever. Mechanistic studies showed that losmapimod inhibited LASV entry by affecting the stable signal peptide (SSP)-GP2 subunit interface of the LASV glycoprotein, thereby blocking pH-dependent viral fusion. As an aryl heteroaryl bis-carboxyamide derivative, losmapimod represents a novel chemical scaffold with anti-LASV activity, and it provides a new lead structure for the future development of LASV fusion inhibitors. • Losmapimod was identified as a Lassa virus entry inhibitor following the screening of 102 clinical compounds. • Losmapimod inhibited Lassa virus infection by affecting the SSP-GP2 interface of the Lassa virus glycoprotein. • Losmapimod preferentially inhibits the entry of Lassa virus among arenaviruses known to cause human disease. [ABSTRACT FROM AUTHOR]

Published

2019

104. Farnesoid X receptor agonist GW4064 indirectly inhibits HCV entry into cells via down-regulating scavenger receptor class B type I.

Author

Wu, Zhou-Yi, Li, Hu, Li, Jian-Rui, Lv, Xiao-Qin, Jiang, Jian-Dong, and Peng, Zong-Gen

Subjects

*FARNESOID X receptor, *HEPATITIS C virus, *CHEMICAL scavengers, *GLUCOSE metabolism, *ANTIVIRAL agents, *DRUG activation

Abstract

Farnesoid X receptor (FXR) agonists play important regulatory roles in bile acid, lipid and glucose metabolism in vitro and in vivo. Thus, FXR agonists exhibit potential therapeutic effects on metabolism-related diseases that are associated with extrahepatic manifestations induced by hepatitis C virus (HCV) infection. This study investigated the effect and mechanism of FXR agonist GW4064 against HCV in vitro to explore the potential application of FXR agonists. Results showed that GW4064 and other FXR agonists have potent antiviral activity against HCV in Huh7.5 cells. GW4064 down-regulated the expression of scavenger receptor class B type I protein via FXR and thereby indirectly inhibited HCV entry into cells, leading to interruption of HCV life cycle. GW4064 also exhibited synergistic anti-HCV effect with known direct-acting antiviral agents (DAAs) used in the clinic and remained sensitive to DAA-resistant HCV mutations. Therefore, FXR agonists are also a kind of antiviral agent, and might be helpful in treatment of HCV-induced hepatic and extrahepatic manifestations. [ABSTRACT FROM AUTHOR]

Published

2019

105. Anti-zika virus activity of polyoxometalates.

Author

Francese, Rachele, Civra, Andrea, Rittà, Massimo, Donalisio, Manuela, Argenziano, Monica, Cavalli, Roberta, Mougharbel, Ali S., Kortz, Ulrich, and Lembo, David

Subjects

*POLYOXOMETALATES, *ZIKA virus infections, *ANTIVIRAL agents, *GUILLAIN-Barre syndrome, *PUBLIC health

Abstract

Abstract Zika virus (ZIKV) is an emerging infectious viral pathogen associated with severe fetal cerebral anomalies and the paralytic Guillain-Barrè syndrome in adults. It was the cause of a recent global health crisis following its entrance into a naïve population in the Americas. Nowadays, no vaccine or specific antiviral against ZIKV is available. In this study, we identified three polyoxometalates (POMs), the Anderson-Evans type [TeW 6 O 24 ]6- (TeW 6), and the Keggin-type [TiW 11 CoO 40 ]8-_ (TiW 11 Co), and [Ti 2 PW 10 O 40 ]7- (Ti 2 PW 10), that inhibit ZIKV infection with EC 50 s in the low micromolar range. Ti 2 PW 10 , the POM with the greatest selectivity index (SI), was selected and the step of ZIKV replicative cycle putatively inhibited was investigated by specific antiviral assays. We demonstrated that Ti 2 PW 10 targets the entry process of ZIKV infection and it is able to significantly reduce ZIKV progeny production. These results suggest that the polyanion Ti 2 PW 10 could be a good starting point to develop an effective therapeutic to treat ZIKV infection. Highlights • No vaccine or specific antiviral against ZIKV is available. • The polyoxometalates TeW 6 , TiW 11 Co and Ti 2 PW 10 showed a marked anti-ZIKV activity in vitro. • TeW 6 , TiW 11 Co and Ti 2 PW 10 are not toxic for cells. • Ti 2 PW 10 inhibits the entry process of ZIKV into the host cell. • Ti 2 PW 10 is able to significantly reduce ZIKV progeny production. [ABSTRACT FROM AUTHOR]

Published

2019

106. Berberine inhibits hepatitis C virus entry by targeting the viral E2 glycoprotein.

Author

Hung, Ting-Chun, Jassey, Alagie, Liu, Ching-Hsuan, Lin, Chien-Ju, Lin, Chun-Ching, Wong, Shu Hui, Wang, Jonathan Y., Yen, Ming-Hong, and Lin, Liang-Tzung

Abstract

Background: Despite the advent of direct-acting antivirals (DAAs), HCV remains an important public health problem globally. There is at present no effective vaccine against the virus, and the DAAs in current use cannot prevent de novo infection, including in liver transplant setting wherein donor livers inevitably become re-infected. Developing inhibitors to HCV entry using nature-derived small molecules may help to expand/complement the current treatment options.Purpose: In this study, we explored the effect of the plant alkaloid berberine (BBR) on HCV early viral entry.Methods: Cell culture-derived HCV (HCVcc), viral pseudoparticles bearing HCV glycoproteins (HCVpp), and entry-related assays were employed to assess BBR's bioactivity. Molecular docking was used to predict BBR-HCV glycoproteins interaction, and the compound's antiviral activity was confirmed against HCVcc infection of primary human hepatocytes (PHHs).Results: BBR specifically impeded HCVcc attachment and entry/fusion steps without inactivating the free virus particles or affecting the expression of host cell entry factors and post-entry viral replication. BBR also effectively inhibited infection by viral pseudoparticles expressing HCV E1/E2 glycoproteins and molecular docking analysis pointed at potential interaction with HCV E2. Finally, BBR could suppress HCVcc infection of PHHs.Conclusions: We identified BBR as a potent HCV entry inhibitor, which merits further evaluation particularly for use in transplant setting against graft re-infection by HCV. [ABSTRACT FROM AUTHOR]

Published

2019

107. HIV-1 Entry and Prospects for Protecting against Infection

Author

Jean-François Bruxelle, Nino Trattnig, Marianne W. Mureithi, Elise Landais, and Ralph Pantophlet

Subjects

mucosal transmission, transmitted/founder virus, viral entry, neutralizing antibody, entry inhibitor, Biology (General), QH301-705.5

Abstract

Human Immunodeficiency Virus type-1 (HIV-1) establishes a latent viral reservoir soon after infection, which poses a major challenge for drug treatment and curative strategies. Many efforts are therefore focused on blocking infection. To this end, both viral and host factors relevant to the onset of infection need to be considered. Given that HIV-1 is most often transmitted mucosally, strategies designed to protect against infection need to be effective at mucosal portals of entry. These strategies need to contend also with cell-free and cell-associated transmitted/founder (T/F) virus forms; both can initiate and establish infection. This review will discuss how insight from the current model of HIV-1 mucosal transmission and cell entry has highlighted challenges in developing effective strategies to prevent infection. First, we examine key viral and host factors that play a role in transmission and infection. We then discuss preventive strategies based on antibody-mediated protection, with emphasis on targeting T/F viruses and mucosal immunity. Lastly, we review treatment strategies targeting viral entry, with focus on the most clinically advanced entry inhibitors.

Published

2021

108. Fangchinoline inhibits SARS-CoV-2 and MERS-CoV entry.

Author

Sadhu, Srikanth, Dandotiya, Jyotsna, Dalal, Rajdeep, Khatri, Ritika, Mykytyn, Anna Z., Batra, Aashima, Kaur, Manpreet, Chandwaskar, Rucha, Singh, Virendra, Kamboj, Aarzoo, Srivastava, Mitul, Mani, Shailendra, Asthana, Shailendra, Samal, Sweety, Rizvi, Zaigham Abbas, Salunke, Deepak B., Haagmans, Bart L., and Awasthi, Amit

Subjects

*COVID-19, *SARS-CoV-2, *CORONAVIRUS diseases, *MERS coronavirus, *COVID-19 pandemic, *SARS-CoV-2 Omicron variant

Abstract

The COVID-19 pandemic caused by SARS-CoV-2, lead to mild to severe respiratory illness and resulted in 6.9 million deaths worldwide. Although vaccines are effective in preventing COVID-19, they may not be sufficient to protect immunocompromised individuals from this respiratory illness. Moreover, novel emerging variants of SARS-CoV-2 pose a risk of new COVID-19 waves. Therefore, identification of effective antivirals is critical in controlling SARS and other coronaviruses, such as MERS-CoV. We show that Fangchinoline (Fcn), a bisbenzylisoquinoline alkaloid, inhibits replication of SARS-CoV, SARS-CoV-2, and MERS-CoV in a range of in vitro assays, by blocking entry. Therapeutic use of Fcn inhibited viral loads in the lungs, and suppressed associated airway inflammation in hACE2. Tg mice and Syrian hamster infected with SARS-CoV-2. Combination of Fcn with remdesivir (RDV) or an anti-leprosy drug, Clofazimine, exhibited synergistic antiviral activity. Compared to Fcn, its synthetic derivative, MK-04-003, more effectively inhibited SARS-CoV-2 and its variants B.1.617.2 and BA.5 in mice. Taken together these data demonstrate that Fcn is a pan beta coronavirus inhibitor, which possibly can be used to combat novel emerging coronavirus diseases. [Display omitted] • Fangchinoline (Fcn) is a pan beta coronavirus entry inhibitor. • Fcn treatment reduced viral load and inflammation in infected hACE2.Tg mice and Hamster model. • Combinatorial treatment of Fcn with Remdesivir or Clofazimine showed synergistic antiviral efficacy. • MK-04-003, a synthetic derivative of Fcn, surpassed Fcn in mice against SARS-CoV-2 and its variants B.1.617.2 and BA.5. [ABSTRACT FROM AUTHOR]

Published

2023

109. Novel mono- and multivalent N-acetylneuraminic acid glycoclusters as potential broad-spectrum entry inhibitors for influenza and coronavirus infection.

Author

Zhu, Xingxing, Yi, Yanliang, Fan, Zibo, Liu, Ruiwen, Chu, Xindang, Wang, Mengyang, Zhang, Jiayi, Tretyakova, Elena, Zhang, Yongmin, Zhang, Lihe, Zhou, Demin, and Xiao, Sulong

Subjects

*COVID-19, *SARS-CoV-2, *MIDDLE East respiratory syndrome, *MERS coronavirus, *INFLUENZA, *BIOSYNTHESIS, *INFLUENZA viruses

Abstract

N -acetylneuraminic acid (Neu5Ac) is a glycan receptor of viruses spread in many eukaryotic cells. The present work aimed to design, synthesis and biological evaluation of a panel of Neu5Ac derivatives based on a cyclodextrin (CD) scaffold for targeting influenza and coronavirus membrane proteins. The multivalent Neu5Ac glycoclusters efficiently inhibited chicken erythrocyte agglutination induced by intact influenza virus in a Neu5Ac density–dependent fashion. Compared with inhibition by Neu5Ac, the multivalent inhibitor with 21 Neu5Ac residues on the primary face of the β -CD scaffold afforded 1788-fold higher binding affinity inhibition for influenza virus hemagglutinin with a dissociation constant (K D) of 3.87 × 10−7 M. It showed moderate binding affinity to influenza virus neuraminidase, but with only about one-thirtieth the potency of that with the HA protein. It also exhibited strong binding affinity to the spike protein of three human coronaviruses (severe acute respiratory syndrome coronavirus, Middle East respiratory syndrome coronavirus, and severe acute respiratory syndrome coronavirus 2), with K D values in the low micromolar range, which is about 10-time weaker than that of HA. Therefore, these multivalent sialylated CD derivatives have possible therapeutic application as broad-spectrum antiviral entry inhibitors for many viruses by targeting the Neu5Ac of host cells. [Display omitted] • A series of mono-, tri-, hepta-, nona-, and 21-valent Neu5Ac glycoclusters were designed and synthesized. • Glycocluster interactions with influenza virus hemagglutinin protein were evaluated using HI and SPR assays. • Binding affinities of 41 with influenza virus neuraminidase and three coronavirus spike glycoproteins were determined using SPR assays. • Cyclodextrin scaffold–based multivalent Neu5Ac glycoclusters may be novel broad-spectrum antiviral entry inhibitors. [ABSTRACT FROM AUTHOR]

Published

2023

110. Nine-valent oleanolic acid conjugates as potent inhibitors blocking the entry of influenza A virus.

Author

Shao, Liang, Su, Yangqing, Zhang, Yuan, Yang, Fan, Zhang, Jihong, Tang, Tao, and Yu, Fei

Subjects

*INFLUENZA A virus, *INFLUENZA viruses, *VIRUS inhibitors, *VIRAL variation, *SIALIC acids

Abstract

The influenza pandemic remains a major public health challenge that endangers the lives of many vulnerable and immune-compromised individuals worldwide. The high infectivity and genetic variability of influenza virus make it particularly challenging to design effective drugs to inhibit the virus. In previous studies, we determined that oleanolic acid (OA) and its derivatives block interactions between influenza and host cells, thus endowing OA with anti-viral efficacy. Inspired by the role of cluster glycosides in the interactions between hemagglutinins (HA) and sialic acid receptors (SA), we designed and synthesized a series of OA nonamers via the CuAAC reaction, and evaluated their anti-viral activities in vitro. We determined that among these nonamers, compound 15 displayed the highest potency (IC 50 = 5.23 μM), equivalent to the antiviral drug oseltamivir which is routinely prescribed for influenza A virus strain A/WSN/33 (H1N1). In addition, these compounds also displayed antiviral activity against influenza B. Mechanistic experiments indicated that OA nonamers can effectively target the influenza HA protein. This study collectively demonstrates that multivalent structure-activity binding strategy is an effective method for designing influenza virus inhibitors. OA nonamers can inhibit the entry of influenza virus by targeting the HA protein more effectively than OA monomers. [Display omitted] • A series of OA nonamers were designed and synthesized via the CuAAC reaction and their anti-influenza virus activities were evaluated. • The SAR of these OA nonamers as influenza virus inhibitors was summarized. • Among these OA nonamers, 15 and 16 displayed the highest anti-influenza A/WSN/33 activity. • The mechanism study suggested that OA nonamers 15 and 16 might bind to HA protein. [ABSTRACT FROM AUTHOR]

Published

2023

111. Entry inhibitors: New advances in HCV treatment

Author

Xi-Jing Qian, Yong-Zhe Zhu, Ping Zhao, and Zhong-Tian Qi

Subjects

antiviral target, entry factor, entry inhibitor, hepatitis C virus, hepatocyte, Infectious and parasitic diseases, RC109-216, Microbiology, QR1-502

Abstract

Hepatitis C virus (HCV) infection affects approximately 3% of the world’s population and causes chronic liver diseases, including liver fibrosis, cirrhosis, and hepatocellular carcinoma. Although current antiviral therapy comprising direct-acting antivirals (DAAs) can achieve a quite satisfying sustained virological response (SVR) rate, it is still limited by viral resistance, long treatment duration, combined adverse reactions, and high costs. Moreover, the currently marketed antivirals fail to prevent graft reinfections in HCV patients who receive liver transplantations, probably due to the cell-to-cell transmission of the virus, which is also one of the main reasons behind treatment failure. HCV entry is a highly orchestrated process involving initial attachment and binding, post-binding interactions with host cell factors, internalization, and fusion between the virion and the host cell membrane. Together, these processes provide multiple novel and promising targets for antiviral therapy. Most entry inhibitors target host cell components with high genetic barriers and eliminate viral infection from the very beginning of the viral life cycle. In future, the addition of entry inhibitors to a combination of treatment regimens might optimize and widen the prevention and treatment of HCV infection. This review summarizes the molecular mechanisms and prospects of the current preclinical and clinical development of antiviral agents targeting HCV entry.

Published

2016

112. Hépatite Delta : épidémiologie, diagnostic, histoire naturelle et traitements

Author

Dimitri Loureiro, C.M. Bed, Tarik Asselah, and Corinne Castelnau

Subjects

Hepatitis B virus, Cirrhosis, biology, business.industry, viruses, Gastroenterology, virus diseases, RNA virus, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, medicine.disease, medicine.disease_cause, Virology, Virus, Entry inhibitor, Serology, Subcutaneous injection, Hepatocellular carcinoma, Internal Medicine, medicine, business, medicine.drug

Abstract

Hepatitis B virus is a small enveloped RNA virus, which replicates independently but requires the hepatitis B virus (HBV) to provide the envelope proteins necessary for the assembly of its own viral particles. Approximately 5% of chronic hepatitis B virus carriers are infected with HDV. HBV vaccination remains the best preventive treatment for HDV. All HBV patients should be screened for HDV (anti-HDV serology). In case of positive HDV serology, HDV replication (HDV RNA) should be investigated using a sensitive and specific technique. Hepatitis Delta is often complicated by cirrhosis and hepatocellular carcinoma (HCC). For this reason, every patient with Delta cirrhosis should be screened for HCC by abdominal ultrasound every 6 months. The historical treatment was based on PEG-IFN with many side effects. A new treatment has been approved, Bulevirtide (Hepcludex®) an HDV/HBV entry inhibitor, for any patient with chronic hepatitis Delta infection (CHD) with active replication (except in decompensated cirrhosis), at a dose of 2mg/day by subcutaneous injection. The exact duration on-treatment is unknown, thus treatment should be continued if clinical benefit is observed.

Published

2022

113. Structural Insight into Paramyxovirus and Pneumovirus Entry Inhibition

Author

Megha Aggarwal and Richard K Plemper

Subjects

respiratory syncytial virus, parainfluenzavirus, measles virus, nipah virus, pneumovirus, paramyxovirus, virus entry, antiviral therapeutic, entry inhibitor, Microbiology, QR1-502

Abstract

Paramyxoviruses and pneumoviruses infect cells through fusion (F) protein-mediated merger of the viral envelope with target membranes. Members of these families include a range of major human and animal pathogens, such as respiratory syncytial virus (RSV), measles virus (MeV), human parainfluenza viruses (HPIVs), and highly pathogenic Nipah virus (NiV). High-resolution F protein structures in both the metastable pre- and the postfusion conformation have been solved for several members of the families and a number of F-targeting entry inhibitors have progressed to advanced development or clinical testing. However, small-molecule RSV entry inhibitors have overall disappointed in clinical trials and viral resistance developed rapidly in experimental settings and patients, raising the question of whether the available structural information may provide a path to counteract viral escape through proactive inhibitor engineering. This article will summarize current mechanistic insight into F-mediated membrane fusion and examine the contribution of structural information to the development of small-molecule F inhibitors. Implications are outlined for future drug target selection and rational drug engineering strategies.

Published

2020

114. Protein-Protein Interaction Targets to Inhibit HIV-1 Infection

Author

Kadow, John F., Langley, David R., Meanwell, Nicholas A., Pracitto, Richard, Walker, Michael A., Yeung, Kap-Sun, and Wendt, Michael D., editor

Published

2012

115. Molecular Mechanisms of HIV Entry

Author

Wilen, Craig B., Tilton, John C., Doms, Robert W., Rossmann, Michael G., editor, and Rao, Venigalla B., editor

Published

2012

116. Identification of gp120 Residue His105 as a Novel Target for HIV-1 Neutralization by Small-Molecule CD4-Mimics

Author

Mohammadjavad Mohammadi, Junhua Chen, Joseph Sodroski, Wayne A. Hendrickson, Amos B. Smith, Shuaiyi Liang, Saumya Anang, Cameron F. Abrams, Christopher J. Fritschi, Francesca Moraca, and Navid Madani

Subjects

Stereochemistry, Organic Chemistry, Indane, Human immunodeficiency virus (HIV), Ring (chemistry), medicine.disease_cause, Biochemistry, Small molecule, Neutralization, Protein–protein interaction, Entry inhibitor, Residue (chemistry), chemistry.chemical_compound, chemistry, Drug Discovery, medicine, medicine.drug

Abstract

[Image: see text] The design and synthesis of butyl chain derivatives at the indane ring 3-position of our lead CD4-mimetic compound BNM-III-170 that inhibits human immunodeficiency virus (HIV-1) infection are reported. Optimization efforts were guided by crystallographic and computational analysis of the small-molecule ligands of the Phe43 cavity of the envelope glycoprotein gp120. Biological evaluation of 11–21 revealed that members of this series of CD4-mimetic compounds are able to inhibit HIV-1 viral entry into target cells more potently and with greater breadth compared to BNM-III-170. Crystallographic analysis of the binding pocket of 14, 16, and 17 revealed a novel hydrogen bonding interaction between His105 and a primary hydroxyl group on the butyl side chain. Further optimization of this interaction with the His105 residue holds the promise of more potent CD4-mimetic compounds.

Published

2021

117. Labyrinthopeptin A1 inhibits dengue and Zika virus infection by interfering with the viral phospholipid membrane

Author

Dominique Schols, Eef Meyen, Sam Noppen, Merel Oeyen, Sandra Claes, Jordi Doijen, Roderich D. Süssmuth, and Kurt Vermeire

Subjects

Cell Survival, viruses, Broad-spectrum, Torovirus, Dengue virus, medicine.disease_cause, Antiviral Agents, Viral envelope, Zika virus, Dengue fever, Labyrinthopeptin, Bacteriocins, Virology, medicine, Animals, Humans, Antiviral, Cells, Cultured, Phospholipids, Dose-Response Relationship, Drug, biology, Zika Virus, Dengue Virus, Virus Internalization, biology.organism_classification, medicine.disease, Entry inhibitor, Phospholipid, Mechanism of action, Cell culture, Viral Envelope, Viruses, Cytokines, medicine.symptom, Peptides, medicine.drug

Abstract

To date, there are no broad-spectrum antivirals available to treat infections with flaviviruses such as dengue (DENV) and Zika virus (ZIKV). In this study, we determine the broad antiviral activity of the lantibiotic Labyrinthopeptin A1. We show that Laby A1 inhibits all DENV serotypes and various ZIKV strains with IC50 around 1 μM. The structurally related Laby A2 also displayed a consistent, but about tenfold lower, antiviral activity. Furthermore, Laby A1 inhibits many viruses from divergent families such as HIV, YFV, RSV and Punta Torovirus. Of interest, Laby A1 does not show activity against non-enveloped viruses. Its antiviral activity is independent of the cell line or the used evaluation method, and can also be observed in MDDC, a physiologically relevant primary cell type. Furthermore, Laby A1 demonstrates low cellular toxicity and has a more favorable SI compared to duramycin, a well-described lantibiotic with broad-spectrum antiviral activity. Time-of-drug addition experiments demonstrate that Laby A1 inhibits infection and entry processes of ZIKV and DENV. We reveal that Laby A1 performs its broad antiviral activity by interacting with a viral factor rather than a cellular factor, and that it has virucidal properties. Finally, using SPR interaction studies we demonstrate that Laby A1 interacts with several phospholipids (i.e. PE and PS) present in the viral envelope. Together with other recent Labyrinthopeptin antiviral publications, this work validates the activity of Laby A1 as broad antiviral entry inhibitor with a unique mechanism of action and demonstrates its potential value as antiviral agent against emerging flaviviruses. ispartof: VIROLOGY vol:562 pages:74-86 ispartof: location:United States status: published

Published

2021

118. Intranasal Administration of Maleic Anhydride-Modified Human Serum Albumin for Pre-Exposure Prophylaxis of Respiratory Syncytial Virus Infection

Author

Zhiwu Sun, Qian Wang, Ran Jia, Shuai Xia, Yuan Li, Qi Liu, Wei Xu, Jin Xu, Lanying Du, Lu Lu, and Shibo Jiang

Subjects

human serum albumin (HSA), pre-exposure prophylaxis (PrEP), respiratory syncytial virus (RSV), entry inhibitor, antiviral, Microbiology, QR1-502

Abstract

Respiratory syncytial virus (RSV) is the leading cause of pediatric viral respiratory tract infections. Neither vaccine nor effective antiviral therapy is available to prevent and treat RSV infection. Palivizumab, a humanized monoclonal antibody, is the only product approved to prevent serious RSV infection, but its high cost is prohibitive in low-income countries. Here, we aimed to identify an effective, safe, and affordable antiviral agent for pre-exposure prophylaxis (PrEP) of RSV infection in children at high risk. We found that maleic anhydride (ML)-modified human serum albumin (HSA), designated ML-HSA, exhibited potent antiviral activity against RSV and that the percentages of the modified lysines and arginies in ML- are correlated with such anti-RSV activity. ML-HSA inhibited RSV entry and replication by interacting with viral G protein and blocking RSV attachment to the target cells, while ML-HAS neither bound to F protein, nor inhibited F protein-mediated membrane fusion. Intranasal administration of ML-HSA before RSV infection resulted in significant decrease of the viral titers in the lungs of mice. ML-HSA shows promise for further development into an effective, safe, affordable, and easy-to-use intranasal regimen for pre-exposure prophylaxis of RSV infection in children at high risk in both low- and high-income countries.

Published

2015

119. An engineered recombinant protein containing three structural domains in SARS-CoV-2 S2 protein has potential to act as a pan-human coronavirus entry inhibitor or vaccine antigen.

Author

Wang X, Sun L, Liu Z, Xing L, Zhu Y, Xu W, Xia S, Lu L, and Jiang S

Subjects

Humans, Animals, Mice, SARS-CoV-2 genetics, SARS-CoV-2 metabolism, Recombinant Proteins genetics, Spike Glycoprotein, Coronavirus chemistry, COVID-19 prevention & control, Coronavirus 229E, Human metabolism, Middle East Respiratory Syndrome Coronavirus genetics, Middle East Respiratory Syndrome Coronavirus metabolism

Abstract

The threat to global health caused by three highly pathogenic human coronaviruses (HCoV), SARS-CoV-2, MERS-CoV and SARS-CoV, calls for the development of pan-HCoV therapeutics and vaccines. This study reports the design and engineering of a recombinant protein designated HR1LS. It contains three linked molecules, each consisting of three structural domains, including a heptad repeat 1 (HR1), a central helix (CH), and a stem helix (SH) region, in the S2 subunit of SARS-CoV-2 spike (S) protein. It was found that HR1LS protein automatically formed a trimer able to bind with heptad repeat 2 (HR2) region in the SARS-CoV-2 S2 subunit, thus potently inhibiting HCoV fusion and entry into host cells. Furthermore, immunization of mice with HR1LS, when combined with CF501 adjuvant, resulted in the production of neutralizing antibodies against infection of SARS-CoV-2 and its variants, as well as SARS-CoV, MERS-CoV, HCoV-229E, HCoV-NL63 and MjHKU4r-CoV-1. These results suggest that HR1LS is a promising candidate for further development as a novel HR1-trimer-based pan-HCoV entry inhibitor or vaccine for the treatment and prevention of infection by SARS-CoV-2 and its variants, but also other HCoVs with the potential to cause future emerging and re-emerging infectious coronavirus diseases.

Published

2023

120. Tangeretin, an extract from Citrus peels, blocks cellular entry of arenaviruses that cause viral hemorrhagic fever.

Author

Tang, Ke, He, Shihua, Zhang, Xiaoyu, Guo, Jiamei, Chen, Qing, Yan, Feihu, Banadyga, Logan, Zhu, Wenjun, Qiu, Xiangguo, and Guo, Ying

Subjects

*FLAVONES, *ARENAVIRUSES, *HEMORRHAGIC fever, *VIRAL vaccines, *FRUIT skins

Abstract

Abstract The family Arenaviridae consists of numerous enveloped RNA viruses with ambisense coding strategies. Eight arenaviruses, including Lassa virus, are known to cause severe and fatal viral hemorrhagic fever (VHF) in humans, yet vaccines and treatments for disease caused by arenaviruses are very limited. In this study, we screened a natural product library consisting of 131 compounds and identified tangeretin, a polymethoxylated flavone widely present in citrus fruit peels, as a Lassa virus entry inhibitor that blocks viral fusion. Further analyses demonstrated the efficacy of tangeretin against seven other VHF-causing arenaviruses, suggesting that this compound, which has a history of medical usage, could be used to develop an effective therapeutic to treat infection and disease caused by Lassa virus and related viruses. Highlights • A natural product library consisting of 131 compounds was screened to identify inhibitors of Lassa virus. • Tangeretin inhibited Lassa virus entry by blocking viral fusion. • Tangeretin also showed efficacy against seven other VHF-causing arenaviruses. [ABSTRACT FROM AUTHOR]

Published

2018

121. Flexibility of small molecular CD4 mimics as HIV entry inhibitors.

Author

Kobayakawa, Takuya, Ohashi, Nami, Hirota, Yuki, Takahashi, Kohei, Yamada, Yuko, Narumi, Tetsuo, Yoshimura, Kazuhisa, Matsushita, Shuzo, Harada, Shigeyoshi, and Tamamura, Hirokazu

Subjects

*CD4 antigen, *INDOLE, *ANTI-HIV agents, *SMALL molecules, *PIPERIDINE

Abstract

Graphical abstract Abstract CD4 mimics such as YIR-821 and its derivatives are small molecules which inhibit the interaction between the Phe43 cavity of HIV-1 gp120 with host CD4, an interaction that is involved in the entry of HIV to cells. Known CD4 mimics generally possess three structural features, an aromatic ring, an oxalamide linker and a piperidine moiety. We have shown previously that introduction of a cyclohexyl group and a guanidine group into the piperidine moiety and a fluorine atom at the meta -position of the aromatic ring leads to a significant increase in the anti-HIV activity. In the current study, the effects of conformational flexibility were investigated by introduction of an indole-type group in the junction between the oxalamide linker and the aromatic moiety or by replacement of the oxalamide linker with a glycine linker. This led to the development of compounds with high anti-HIV activity, showing the importance of the junction region for the expression of high anti-HIV activity. The present data are expected to be useful in the future design of novel CD4 mimic molecules. [ABSTRACT FROM AUTHOR]

Published

2018

122. Potential targets for therapeutic intervention and structure based vaccine design against Zika virus.

Author

Qadir, Amina, Riaz, Muhammad, Saeed, Muhammad, and Shahzad-ul-Hussan, Syed

Subjects

*ZIKA virus, *DRUG therapy, *PROTEINS, *FLAVIVIRUSES, *THERAPEUTICS

Abstract

Continuously increasing number of reports of Zika virus (ZIKV) infections and associated severe clinical manifestations, including autoimmune abnormalities and neurological disorders such as neonatal microcephaly and Guillain-Barré syndrome have created alarming situation in various countries. To date, no specific antiviral therapy or vaccine is available against ZIKV. This review provides a comprehensive insight into the potential therapeutic targets and describes viral epitopes of broadly neutralizing antibodies (bNAbs) in vaccine design perspective. Interactions between ZIKV envelope glycoprotein E and cellular receptors mediate the viral fusion and entry to the target cell. Blocking these interactions by targeting cellular receptors or viral structural proteins mediating these interactions or viral surface glycans can inhibit viral entry to the cell. Similarly, different non-structural proteins of ZIKV and un-translated regions (UTRs) of its RNA play essential roles in viral replication cycle and potentiate for therapeutic interventions. Structure based vaccine design requires identity and structural description of the epitopes of bNAbs. We have described different conserved bNAb epitopes present in the ZIKV envelope as potential targets for structure based vaccine design. This review also highlights successes, unanswered questions and future perspectives in relation to therapeutic and vaccine development against ZIKV. [ABSTRACT FROM AUTHOR]

Published

2018

123. Novel cyclo-peptides inhibit Ebola pseudotyped virus entry by targeting primed GP protein.

Author

Li, Quanjie, Ma, Ling, Yi, Dongrong, Wang, Han, Wang, Jing, Zhang, Yongxin, Guo, Ying, Li, Xiaoyu, Zhou, Jinming, Shi, Yi, Gao, George F., and Cen, Shan

Subjects

*CYCLIC peptides, *EBOLA virus, *HEMORRHAGIC fever, *VIRAL proteins, *DEATH rate, *THERAPEUTICS

Abstract

Ebola virus (EBOV) causes fatal hemorrhagic fever with high death rates in human. Currently, there are no available clinically-approved prophylactic or therapeutic treatments. The recently solved crystal structure of cleavage-primed EBOV glycoprotein (GPcl) in complex with the C domain of endosomal protein Niemann-Pick C1 (NPC1) provides a new target for the development of EBOV entry inhibitors. In this work, a computational approach using docking and molecular dynamic simulations is carried out for the rational design of peptide inhibitors. A novel cyclo-peptide (Pep-3.3) was identified to target at the late stage of EBOV entry and exhibit specific inhibitory activity against EBOV-GP pseudotyped viruses, with 50% inhibitory concentration (IC50) of 5.1 μM. In vitro binding assay and molecular simulations revealed that Pep-3.3 binds to GPcl with a KD value of 69.7 μM, through interacting with predicted residues in the hydrophobic binding pocket of GPcl. Mutation of predicted residues T83 caused resistance to Pep-3.3 inhibition in viral infectivity, providing preliminary support for the model of the peptide binding to GPcl. This study demonstrates the feasibility of inhibiting EBOV entry by targeting GPcl with peptides. [ABSTRACT FROM AUTHOR]

Published

2018

124. Glycosyl-Phosphatidylinositol-Anchored Anti-HIV Env Single-Chain Variable Fragments Interfere with HIV-1 Env Processing and Viral Infectivity.

Author

Misra, Anisha, Gleeson, Emile, Weiming Wang, Chaobaihui Ye, Zhou, Paul, and Kimata, Jason T.

Subjects

*HIV infections, *THERAPEUTICS, *PHOSPHATIDYLINOSITOLS, *VIRION, *VIRAL replication, *ANTI-HIV agents, *VIRAL envelope proteins

Abstract

In previous studies, we demonstrated that single-chain variable fragments (scFvs) from anti-human immunodeficiency virus (HIV) Env monoclonal antibodies act as entry inhibitors when tethered to the surface of target cells by a glycosyl-phosphatidylinositol (GPI) anchor. Interestingly, even if a virus escapes inhibition at entry, its replication is ultimately controlled. We hypothesized that in addition to functioning as entry inhibitors, anti-HIV GPI-scFvs may also interact with Env in an infected cell, thereby interfering with the infectivity of newly produced virions. Here, we show that expression of the anti-HIV Env GPI-scFvs in virus-producing cells reduced the release of HIV from cells 5- to 22-fold, and infectivity of the virions that were released was inhibited by 74% to 99%. Additionally, anti-HIV Env GPI-scFv X5 inhibited virion production and infectivity after latency reactivation and blocked transmitter/founder virus production and infectivity in primary CD4+ T cells. In contrast, simian immunodeficiency virus (SIV) production and infectivity were not affected by the anti-HIV Env GPI-scFvs. Loss of infectivity of HIV was associated with a reduction in the amount of virion-associated Env gp120. Interestingly, an analysis of Env expression in cell lysates demonstrated that the anti-Env GPI-scFvs interfered with processing of Env gp160 precursors in cells. These data indicate that GPI-scFvs can inhibit Env processing and function, thereby restricting production and infectivity of newly synthesized HIV. Anti-Env GPI-scFvs therefore appear to be unique anti- HIV molecules as they derive their potent inhibitory activity by interfering with both early (receptor binding/entry) and late (Env processing and incorporation into virions) stages of the HIV life cycle. IMPORTANCE The restoration of immune function and persistence of CD4+ T cells in HIV-1-infected individuals without antiretroviral therapy requires a way to increase resistance of CD4+ T cells to infection by both R5- and X4-tropic HIV-1. Previously, we reported that anchoring anti-HIV-1 single-chain variable fragments (scFvs) via glycosyl-phosphatidylinositol (GPI) to the surface of permissive cells conferred a high level of resistance to HIV-1 variants at the level of entry. Here, we report that anti- HIV GPI-scFvs also derive their potent antiviral activity in part by blocking HIV production and Env processing, which consequently inhibits viral infectivity even in primary infection models. Thus, we conclude that GPI-anchored anti-HIV scFvs derive their potent blocking activity of HIV replication by interfering with successive stages of the viral life cycle. They may be effectively used in genetic intervention of HIV-1 infection. [ABSTRACT FROM AUTHOR]

Published

2018

125. Establishment of pseudovirus infection mouse models for in vivo pharmacodynamics evaluation of filovirus entry inhibitors.

Author

Chen, Qing, Tang, Ke, Zhang, Xiaoyu, Chen, Panpan, and Guo, Ying

Subjects

VIRAL vaccines, FILOVIRIDAE, ANTIVIRAL agents, BIOLUMINESCENCE, EBOLA virus, PHARMACODYNAMICS

Abstract

Filoviruses cause severe and fatal viral hemorrhagic fever in humans. Filovirus research has been extensive since the 2014 Ebola outbreak. Due to their high pathogenicity and mortality, live filoviruses require Biosafety Level-4 (BSL-4) facilities, which have restricted the development of anti-filovirus vaccines and drugs. An HIV-based pseudovirus cell infection assay is widely used for viral entry studies in BSL-2 conditions. Here, we successfully constructed nine in vitro pseudo-filovirus models covering all filovirus genera and three in vivo pseudo-filovirus-infection mouse models using Ebola virus, Marburg virus, and Lloviu virus as representative viruses. The pseudo-filovirus-infected mice showed visualizing bioluminescence in a dose-dependent manner. A bioluminescence peak in mice was reached on day 5 post-infection for Ebola virus and Marburg virus and on day 4 post-infection for Lloviu virus. Two known filovirus entry inhibitors, clomiphene and toremiphene, were used to validate the model. Collectively, our study shows that all genera of filoviruses can be well-pseudotyped and are infectious in vitro . The pseudo-filovirus-infection mouse models can be used for in vivo activity evaluation of anti-filovirus drugs. This sequential in vitro and in vivo evaluation system of filovirus entry inhibitors provides a secure and efficient platform for screening and assessing anti-filovirus agents in BSL-2 facilities. [ABSTRACT FROM AUTHOR]

Published

2018

126. Resistance to Enfuvirtide and Other HIV Entry Inhibitors

Author

Melby, Thomas, Heilek, Gabrielle, Cammack, Nick, Greenberg, Michael L., Georgiev, Vassil St., editor, and Mayers, Douglas L., editor

Published

2009

127. Inhibitors of Viral Entry

Author

Melby, Tom, Westby, Mike, Hofmann, F., editor, Kräusslich, Hans-Georg, editor, and Bartenschlager, Ralf, editor

Published

2009

128. A Recombinant Fragment of Human Surfactant Protein D Binds Spike Protein and Inhibits Infectivity and Replication of SARS-CoV-2 in Clinical Samples

Author

Uday Kishore, Ekta Gupta, Hrishikesh Pandit, Indra Kundu, Sheetalnath Rooge, Savneet Kaur, Reshu Agarwal, Sanjeev Gupta, Taruna Madan, Dinesh M. Tripathi, Susan Idicula-Thomas, Praveen M. Varghese, Rambhadur Subedi, and Barnali Biswas

Subjects

entry inhibition, Male, 0301 basic medicine, viruses, Clinical Biochemistry, Plasma protein binding, Virus Replication, spike protein, medicine.disease_cause, law.invention, 0302 clinical medicine, law, Chlorocebus aethiops, Receptor, skin and connective tissue diseases, Pulmonary Surfactant-Associated Protein D, Original Research, Coronavirus, Infectivity, Chemistry, virus diseases, Recombinant Proteins, Spike Glycoprotein, Coronavirus, Recombinant DNA, Female, Protein Binding, medicine.drug, Adult, Pulmonary and Respiratory Medicine, surfactant protein D, Protein subunit, Virus, 03 medical and health sciences, medicine, Animals, Humans, Gene, Vero Cells, Molecular Biology, entry inhibitor, SARS-CoV-2, fungi, COVID-19, Surfactant protein D, Cell Biology, Molecular biology, Virology, Entry inhibitor, body regions, 030104 developmental biology, 030228 respiratory system, Viral replication

Abstract

RationaleCOVID-19 is an acute infectious disease caused by the Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2). Human surfactant protein D (SP-D) is known to interact with spike protein of SARS-CoV, but its immune-surveillance against SARS-CoV-2 is not known.ObjectiveThis study aimed to examine the potential of a recombinant fragment of human SP-D (rfhSP-D) as an inhibitor of replication and infection of SARS-CoV-2.MethodsrfhSP-D interaction with spike protein of SARS-CoV-2 and hACE-2 receptor was predicted via docking analysis. The inhibition of interaction between spike protein and ACE-2 by rfhSP-D was confirmed using direct and indirect ELISA. The effect of rfhSP-D on replication and infectivity of SARS-CoV-2 from clinical samples was studied by measuring the expression of RdRp gene of the virus using qPCR.Measurements and Main ResultsIn-silico interaction studies indicated that three amino acid residues in the RBD of spike of SARS-CoV-2 were commonly involved in interacting with rfhSP-D and ACE-2. Studies using clinical samples of SARS-CoV-2 positive cases (asymptomatic, n=7 and symptomatic, n=8 and negative controls n=15) demonstrated that treatment with 5μM rfhSP-D inhibited viral replication by ~5.5 fold and was more efficient than Remdesivir (100 μM). Approximately, a 2-fold reduction in viral infectivity was also observed after treatment with 5μM rfhSP-D.ConclusionsThese results conclusively demonstrate that the calcium independent rfhSP-D mediated inhibition of binding between the receptor binding domain of the S1 subunit of the SARS-CoV-2 spike protein and human ACE-2, its host cell receptor, and a significant reduction in SARS-CoV-2 infection and replication in-vitro.

Published

2021

129. Development of broad-spectrum coronavirus therapeutics: identification of potent inhibitors of SARS-CoV-2 binding and entry

Author

McLaren, Paul (Medical Microbiology and Infectious Diseases), Drebot, Michael (Medical Microbiology and Infectious Diseases), Kindrachuk, Jason, Allardice, Meagan, McLaren, Paul (Medical Microbiology and Infectious Diseases), Drebot, Michael (Medical Microbiology and Infectious Diseases), Kindrachuk, Jason, and Allardice, Meagan

Abstract

Coronavirus outbreaks have been increasing in both frequency and magnitude for the last 20 years. Prior to 2002, there were two identified human coronaviruses. Now in 2022 there are seven, potentially eight. From severe acute respiratory syndrome coronavirus (SARS-CoV) in 2002, to Middle East respiratory syndrome coronavirus (MERS-CoV) in 2012 and SARS-CoV-2 in 2019, coronavirus outbreaks have continued to escalate, causing more infections and more deaths with each successive outbreak. SARS-CoV-2 was declared a pandemic on March 11, 2020, by the World Health Organization. To date, there have been around 460 million cases and over 6 million deaths, worldwide. The need for therapeutic interventions for SARS-CoV-2 is continuing, but even greater is the need for broad spectrum coronavirus therapeutics that may be used for this and other coronavirus outbreaks. Due to the critical role of ACE2 in the replication of SARS-CoV, SARS-CoV-2 and human coronavirus (HCoV)-NL63, ACE2 has become a prime target for therapeutic intervention. Groups have tested chimerics of ACE2 fused to an Fc peptide: ACE2-Fc as a decoy molecule that would bind the receptor binding domain (RBD) of SARS-CoV-2 with the same or greater affinity than ACE2 on the surface of cells. Here is described the production and evaluation of seven ACE2-Fc chimerics, and the down-selection to one lead candidate as a potent inhibitor of SARS-CoV-2 cell entry. All ACE2-Fc chimerics were sequence verified, their expression was confirmed in HEK293Ts using western blots and their relative neutralization capacity was tested in in vitro neutralization assays. Evaluation of these constructs led to the identification of a lead construct, which was a potent inhibitor of a SARS-CoV-2 D614G pseudotype luciferase reporter virus. Additional testing of the lead ACE2-Fc construct in wild-type SARS-CoV-2 also demonstrated potent neutralization. Further evaluation of this protein in vivo will allow for determination of dose range, and

Published

2022

130. Entry inhibition of HIV-1 subtype C isolates

Author

Morris, Lynn, Coetzer, Mia, Gray, Elin S., Cilliers, Tonie, Alexandre, Kabamba B., Moore, Penny L., Binley, James M., Parnham, Michael J., editor, Bruinvels, J., editor, Reeves, Jacqueline D., editor, and Derdeyn, Cynthia A., editor

Published

2007

131. Inhibitors that target fusion

Author

Wei, Wang, Weiss, Carol D., Parnham, Michael J., editor, Bruinvels, J., editor, Reeves, Jacqueline D., editor, and Derdeyn, Cynthia A., editor

Published

2007

132. The challenge of HIV sequence diversity in the envelope glycoprotein

Author

Vergne, Laurence, Peeters, Martine, Parnham, Michael J., editor, Bruinvels, J., editor, Reeves, Jacqueline D., editor, and Derdeyn, Cynthia A., editor

Published

2007

133. Inhibitors that target gp120-CD4 interactions

Author

Lin, Pin-fang, Kadow, John, Alexander, Louis, Parnham, Michael J., editor, Bruinvels, J., editor, Reeves, Jacqueline D., editor, and Derdeyn, Cynthia A., editor

Published

2007

134. Introduction to entry inhibitors in the management of HIV infection

Author

Tilton, John C., Doms, Robert W., Parnham, Michael J., editor, Bruinvels, J., editor, Reeves, Jacqueline D., editor, and Derdeyn, Cynthia A., editor

Published

2007

135. Enfuvirtide: from basic science to FDA approval

Author

Greenberg, Michael L., Parnham, Michael J., editor, Bruinvels, J., editor, Reeves, Jacqueline D., editor, and Derdeyn, Cynthia A., editor

Published

2007

136. Future clinical prospects for entry inhibitors

Author

Heath, Sonya L., Kilby, J. Michael, Parnham, Michael J., editor, Bruinvels, J., editor, Reeves, Jacqueline D., editor, and Derdeyn, Cynthia A., editor

Published

2007

137. Bulevirtide for patients with compensated chronic hepatitis delta: A review

Author

Elisabetta Degasperi, Maria P. Anolli, and Pietro Lampertico

Subjects

Settore MED/12 - Gastroenterologia, chronic delta hepatitis, Hepatology, HDV-RNA, HDV, combined response, virological response, Bulevirtide, clinically significant portal hypertension, compensated cirrhosis, entry inhibitor

Abstract

Chronic hepatitis delta (CHD) affects approximately 10-20 million people worldwide and represents the most severe form of chronic viral hepatitis, as it is characterized by high rates of progression to cirrhosis and its complications (end-stage liver disease, hepatocellular carcinoma). In the last 30 years, the only treatment option for CHD has been represented by the off-label administration of Interferon (or Pegylated Interferon)-alpha: antiviral treatment, however, resulted in suboptimal (20-30%) virological response and was burdened by several side effects, de facto contraindicating Interferon (IFN) administration in patients with more advanced liver disease. Recently, Bulevirtide (BLV), a first-in-class HBV-HDV entry inhibitor blocking Na

Published

2022

138. Phyllanthin and hypophyllanthin, the isolated compounds of Phyllanthus niruri inhibit protein receptor of corona virus (COVID-19) through in silico approach

Author

Achmad Fuad Hafid, Tri Widiandani, Aty Widyawaruyanti, Honey Dzikri Marhaeny, and Tutik Sri Wahyuni

Subjects

Pharmacology, 0303 health sciences, Protease, Phyllanthus, biology, Physiology, Chemistry, Drug discovery, medicine.medical_treatment, In silico, Hepatitis C virus, General Medicine, medicine.disease_cause, biology.organism_classification, Virus, Entry inhibitor, 03 medical and health sciences, 0302 clinical medicine, Viral entry, 030220 oncology & carcinogenesis, Drug Discovery, medicine, 030304 developmental biology, medicine.drug

Abstract

Objectives Phyllanthus niruri has been known as an immunomodulator and also reported to possess an antiviral activity against several RNA viruses, such as hepatitis B virus and hepatitis C virus by inhibiting viral entry and replication. Since the current situation of Coronavirus Disease 2019 (COVID-19) which infected among the world and caused severe disease and high morbidity, it urgently needed to find new agents against COVID-19. Therefore, in silico screening against COVID-19 receptors is carried out as an initial stage of drug discovery by evaluating the activity of phyllanthin and hypophyllanthin, an isolated from Phyllanthus niruri, in inhibiting spike glycoprotein (6LZG) and main protease (5R7Y) which play as target receptors of COVID-19. Methods Molegro Virtual Docker 6.0 used to determine the best binding energy through the rerank score which shows the total energy bonds calculation. Results Phyllanthin and hypophyllanthin demonstrated to possess greater binding affinity toward the COVID-19 inhibition sites than their native ligand. The rerank score of phyllanthin and hypophyllanthin are lower than the native ligands 6LZG and 5R7Y. This result indicated that phyllanthin and hypophyllanthin have a stronger interaction than the native ligands both in spike glycoprotein (entry inhibitor) and main protease (translation and replication inhibitor). Conclusions In conclusion, phyllanthin and hypophyllanthin are predicted to have strong activity against COVID-19 through inhibiting spike glycoprotein and main protease under in silico study. Further research is needed to support the development of P. niruri as inhibitor agents of COVID-19 through bioassay studies.

Published

2021

139. The entry inhibitor DS003 (BMS-599793): a BMS-806 analogue, provides superior activity as a pre-exposure prophylaxis candidate

Author

Jeremy Nuttall, Naomi Armanasco, Yoann Aldon, Daniel J. Stieh, Sarah Harman, Robin J. Shattock, Paul Rogers, Paul Ziprin, and Carolina Herrera

Subjects

Conformational change, Immunology, HIV Infections, HIV Envelope Protein gp120, Pharmacology, Article, Piperazines, Epitope, Piperidines, Viral envelope, HIV Fusion Inhibitors, In vivo, medicine, Humans, Immunology and Allergy, Binding site, Chemistry, Entry inhibitor, Infectious Diseases, Fostemsavir, Mechanism of action, Pyrazines, CD4 Antigens, Pre-Exposure Prophylaxis, medicine.symptom, medicine.drug

Abstract

Objective Small molecule inhibitors able to bind to gp120 and prevent CD4-induced HIV-1 envelope conformational change provide an important class of inhibitors. Currently, only Fostemsavir is approved for HAART, which makes this class of inhibitors attractive candidates for prevention. We assessed the activity of DS003 (BMS-599793), an analogue of BMS-378806, in different mucosal tissues and elucidated its mechanism of action. Design Pre-clinical analysis was performed with human mucosal tissue models as surrogates of in vivo activity. Methods Antiviral efficacy of DS003 was assessed in mucosal tissue explants (ecto-cervical, penile and colorectal) and in trans-infection models (co-cultures of dendritic or mucosal migratory cells with CD4+T cells) with several dosing times (2 h, 24 h and sustained) and in combination with a fusion inhibitor. Binding of DS003 to gp120 was assessed by flow cytometry and bio-layer interferometry and further probed in competitive studies using soluble CD4 (sCD4) and an anti-CD4 induced antibody, 17b. Results In all models, the inhibitory activity of DS003 was increased with longer periods of exposure and by combination with a fusion inhibitor. Pre-exposure to sCD4 impeded DS003 binding to viral envelope (Env). In contrast, DS003 did not impact subsequent binding of sCD4. Furthermore, sCD4-induced epitope exposure as assessed by 17b binding was significantly reduced in the presence of DS003. Conclusion DS003 inhibits HIV-1 infection by binding to or near the CD4 binding site of gp120, preventing CD4-induced conformational change essential for viral fusion. These data highlight the potential of DS003 for development as a pre-exposure prophylaxis candidate.

Published

2021

140. A Novel CXCR4 Targeting Protein SDF-1/54 as an HIV-1 Entry Inhibitor

Author

Suiyi Tan, Wenjuan Li, Zhaofeng Li, Yujing Li, Jiangyan Luo, Liangzhentian Yu, Jie Yang, Mengjie Qiu, Hongyan Cheng, Wei Xu, Shibo Jiang, Lu Lu, Shuwen Liu, and Weifeng Ma

Subjects

SDF-1/54, HIV-1, CXCR4, entry inhibitor, Microbiology, QR1-502

Abstract

CXC chemokine receptor 4 (CXCR4) is a co-receptor for HIV-1 entry into target cells. Its natural ligand, the chemokine SDF-1, inhibits viral entry mediated by this receptor. However, the broad expression pattern of CXCR4 and its critical roles in various physiological and pathological processes indicate that the direct application of SDF-1 as an entry inhibitor might have severe consequences. Previously, we constructed an effective SDF-1 mutant, SDF-1/54, by deleting the α-helix of the C-terminal functional region of SDF-1. Of note, SDF-1/54 shows remarkable decreased chemotoxic ability, but maintains a similar binding affinity to CXCR4, suggesting SDF-1/54 might better serve as a CXCR4 inhibitor. Here, we found that SDF-1/54 exhibited potent antiviral activity against various X4 HIV-1 strains, including the infectious clone HIV-1 NL4-3, laboratory-adapted strain HIV-1 IIIB, clinical isolates and even drug-resistant strains. By using time-of-addition assay, non-infectious and infectious cell−cell fusion assay and CXCR4 internalization assay, we demonstrated SDF-1/54 is an HIV-1 entry inhibitor. A combination of SDF-1/54 with several antiretroviral drugs exhibited potent synergistic anti-HIV-1 activity. Moreover, SDF-1/54 was stable and its anti-HIV-1 activity was not significantly affected by the presence of seminal fluid, vaginal fluid simulant and human serum albumin. SDF-1/54 showed limited in vitro cytotoxicity to lymphocytes and vaginal epithelial cells. Based on these findings, SDF-1/54 could have a therapeutic potential as an HIV-1 entry inhibitor.

Published

2019

141. Development of Protein- and Peptide-Based HIV Entry Inhibitors Targeting gp120 or gp41

Author

Jing Pu, Qian Wang, Wei Xu, Lu Lu, and Shibo Jiang

Subjects

HIV-1, gp120, gp41, entry inhibitor, peptide, antibody, recombinant protein, antiretroviral drugs, Microbiology, QR1-502

Abstract

Application of highly active antiretroviral drugs (ARDs) effectively reduces morbidity and mortality in HIV-infected individuals. However, the emergence of multiple drug-resistant strains has led to the increased failure of ARDs, thus calling for the development of anti-HIV drugs with targets or mechanisms of action different from those of the current ARDs. The first peptide-based HIV entry inhibitor, enfuvirtide, was approved by the U.S. FDA in 2003 for treatment of HIV/AIDS patients who have failed to respond to the current ARDs, which has stimulated the development of several series of protein- and peptide-based HIV entry inhibitors in preclinical and clinical studies. In this review, we highlighted the properties and mechanisms of action for those promising protein- and peptide-based HIV entry inhibitors targeting the HIV-1 gp120 or gp41 and discussed their advantages and disadvantages, compared with the current ARDs.

Published

2019

142. Purification and Study of CC Chemokine-Based Strategies to Combat Chronic Inflammation and HIV

Author

Nguyen, Anna Faith

Subjects

Biochemistry, Molecular biology, Biomedical engineering, Anti-Inflammatory, biotherapeutic, CC Chemokine, Entry Inhibitor, HIV, structural biology

Abstract

The human immune system is among one of the most complex organ systems in the human body. While it is responsible for healing wounds and protecting from disease, it can also have deleterious effects when over- or under-active. For example, many people who experience traumatic brain injury (TBI) suffer many of their ill effects due to the increased pressure on their brain, caused by an influx of immune cells. In another example, Auto-Immune Deficiency Syndrome (AIDS) is a progression of the Human Immunodeficiency Virus (HIV) that results in the death of immune cells, and thus, leaves the person open to opportunistic infections. Proteins involved in both these immune processes are known as chemokines (chemoattractant cytokines), which are small, secreted proteins that recruit and activate leukocytes, and can signal their movement towards a site of inflammation or infection (known as chemotaxis). As a result, more detailed study of the chemokine system is necessary in order to discover novel strategies to combat immune system-related ailments. This dissertation focuses on the broad applications involving utilizing certain segments of the chemokine system as biotherapeutics in chronic inflammation and HIV infection. First, the purification and structural study of the poxvirus viral CC Chemokine Inhibitor (vCCI) that naturally inhibits chemotaxis helps shed light on the mechanism behind this protein’s broadly-applicable method of binding CC Chemokines, revealing key residues that are likely vital for the mechanism behind the protein’s ability to broadly inhibit inflammation. Later, CC Chemokines are also studied in the context of HIV-inhibition, focusing on the N-terminal properties of a natural chemokine analog, 5P12-RANTES, which has been shown to inhibit HIV entry into the human cell. This inhibitory chemokine analog is also used to design and create second-generation HIV entry inhibitors, 5P12-Linker-T1144 and 5P12-Linker-T2635, which inhibit HIV at two separate stages of HIV entry process. And finally, chemokine analogs are suggested as a possible system for targeting cells likely to contain latent HIV DNA, to later activate transcription and allow the HIV-infected cells to be recognized by the immune system by utilizing the protein 5P14-Linker-Tat. Overall, this dissertation reveals structural insights into the proteins vCCI, vMIP-II and 5P12-RANTES that help elucidate the properties of the chemokine system, as well as offers three newly-engineered proteins, 5P12-Linker-T1144, 5P12-Linker-T2635 and 5P14-Linker-Tat to be used to combat HIV infection with preliminary results showing signs of efficacy.

Published

2017

143. Cellular electrical impedance to profile SARS-CoV-2 fusion inhibitors and to assess the fusogenic potential of spike mutants

Author

Emiel Vanhulle, Jordi Doijen, Joren Stroobants, Becky Provinciael, Sam Noppen, Dominique Schols, Annelies Stevaert, and Kurt Vermeire

Subjects

Pharmacology, Science & Technology, SARS-CoV-2, Virology, Spike, Pharmacology & Pharmacy, Cell-cell fusion, Entry inhibitor, Life Sciences & Biomedicine, Cellular electrical impedance

Abstract

Despite the vaccination campaigns for COVID-19, we still cannot control the spread of SARS-CoV-2, as evidenced by the ongoing circulation of the Omicron variants of concern. This highlights the need for broad-spectrum antivirals to further combat COVID-19 and to be prepared for a new pandemic with a (re-)emerging coronavirus. An interesting target for antiviral drug development is the fusion of the viral envelope with host cell membranes, a crucial early step in the replication cycle of enveloped viruses. In this study, we explored the use of cellular electrical impedance (CEI) to quantitatively monitor morphological changes in real time, resulting from cell-cell fusion elicited by SARS-CoV-2 spike. The impedance signal in CEI-quantified cell-cell fusion correlated with the expression level of SARS-CoV-2 spike in transfected HEK293T cells. For antiviral assessment, we validated the CEI assay with the fusion inhibitor EK1 and measured a concentration-dependent inhibition of SARS-CoV-2 spike mediated cell-cell fusion (IC50value of 0.13 μM). In addition, CEI was used to confirm the fusion inhibitory activity of the carbohydrate-binding plant lectin UDA against SARS-CoV-2 (IC50value of 0.55 μM), which complements prior in-house profiling activities. Finally, we explored the utility of CEI in quantifying the fusogenic potential of mutant spike proteins and in comparing the fusion efficiency of SARS-CoV-2 variants of concern. In summary, we demonstrate that CEI is a powerful and sensitive technology that can be applied to studying the fusion process of SARS-CoV-2 and to screening and characterizing fusion inhibitors in a label-free and non-invasive manner.ImportanceDespite the success of the vaccines against SARS-CoV-2, new variants of the virus are still emerging and spreading, underlining the need for additional effective antiviral countermeasures. An interesting antiviral target for enveloped viruses is the fusion of the viral envelope with host cell membranes, a crucial early step in the life cycle of coronaviruses like SARS-CoV-2. Here, we present a sensitive impedance-based method to monitor in real-time cell-cell fusion elicited by the SARS-CoV-2 spike protein. With this technique we can profile entry inhibitors and determine the inhibitory potential of fusion inhibitors for SARS-CoV-2. In addition, with cellular electrical impedance we can evaluate the fusogenic properties of new emerging SARS-CoV-2 variants. Overall, the impedance technology adds valuable information on the fusion process of circulating coronaviruses and helps unravel the mode of action of new antivirals, opening new avenues for the development of next generation fusion inhibitors with improved antiviral activity.

Published

2023

144. Therapeutic potential of HIV-1 entry inhibitor peptidomimetics

Author

Samuel K. Kwofie, Nneka Pu Korie, Osbourne Quaye, and Kwesi Z Tandoh

Subjects

0301 basic medicine, Anti-HIV Agents, Peptidomimetic, Human immunodeficiency virus (HIV), HIV Infections, HIV Antibodies, medicine.disease_cause, Bioinformatics, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 0302 clinical medicine, Drug Discovery, medicine, Humans, Drug discovery, business.industry, virus diseases, Virus Internalization, Antiretroviral therapy, Entry inhibitor, 030104 developmental biology, 030220 oncology & carcinogenesis, HIV-1, Peptidomimetics, Minireview, business, Broadly Neutralizing Antibodies, medicine.drug

Abstract

Human immunodeficiency virus 1 (HIV-1) infection remains a public health concern globally. Although great strides in the management of HIV-1 have been achieved, current highly active antiretroviral therapy is limited by multidrug resistance, prolonged use-related effects, and inability to purge the HIV-1 latent pool. Even though novel therapeutic options with HIV-1 broadly neutralizing antibodies (bNAbs) are being explored, the scalability of bNAbs is limited by economic cost of production and obligatory requirement for parenteral administration. However, these limitations can be addressed by antibody mimetics/peptidomimetics of HIV-1 bNAbs. In this review we discuss the limitations of HIV-1 bNAbs as HIV-1 entry inhibitors and explore the potential therapeutic use of antibody mimetics/peptidomimetics of HIV-1 entry inhibitors as an alternative for HIV-1 bNAbs. We highlight the reduced cost of production, high specificity, and oral bioavailability of peptidomimetics compared to bNAbs to demonstrate their suitability as candidates for novel HIV-1 therapy and conclude with some perspectives on future research toward HIV-1 novel drug discovery.

Published

2021

145. Therapeutic shutdown of HBV transcripts promotes reappearance of the SMC5/6 complex and silencing of the viral genome in vivo

Author

Katja Giersch, Marc Lütgehetmann, Stephan Urban, Rudolf K. F. Beran, A Pirosu, Tassilo Volz, Maura Dandri, Lena Allweiss, Robert C Muench, Simon P. Fletcher, and Hassan Javanbakht

Subjects

Hepatitis B virus, Chromosomal Proteins, Non-Histone, Cell Cycle Proteins, Genome, Viral, Biology, liver, medicine.disease_cause, Mice, Hepatitis B, Chronic, interferon-α, Viral entry, antiviral therapy, medicine, Animals, Humans, Gene silencing, Viral Regulatory and Accessory Proteins, Host factor, Hepatology, Chimera, Gastroenterology, RNA, cccDNA, Virology, digestive system diseases, Entry inhibitor, HBx, Trans-Activators, hepatitis B, DNA, Circular, medicine.drug

Abstract

ObjectiveTherapeutic strategies silencing and reducing the hepatitis B virus (HBV) reservoir, the covalently closed circular DNA (cccDNA), have the potential to cure chronic HBV infection. We aimed to investigate the impact of small interferring RNA (siRNA) targeting all HBV transcripts or pegylated interferon-α (peg-IFNα) on the viral regulatory HBx protein and the structural maintenance of chromosome 5/6 complex (SMC5/6), a host factor suppressing cccDNA transcription. In particular, we assessed whether interventions lowering HBV transcripts can achieve and maintain silencing of cccDNA transcription in vivo.DesignHBV-infected human liver chimeric mice were treated with siRNA or peg-IFNα. Virological and host changes were analysed at the end of treatment and during the rebound phase by qualitative PCR, ELISA, immunoblotting and chromatin immunoprecipitation. RNA in situ hybridisation was combined with immunofluorescence to detect SMC6 and HBV RNAs at single cell level. The entry inhibitor myrcludex-B was used during the rebound phase to avoid new infection events.ResultsBoth siRNA and peg-IFNα strongly reduced all HBV markers, including HBx levels, thus enabling the reappearance of SMC5/6 in hepatocytes that achieved HBV-RNA negativisation and SMC5/6 association with the cccDNA. Only IFN reduced cccDNA loads and enhanced IFN-stimulated genes. However, the antiviral effects did not persist off treatment and SMC5/6 was again degraded. Remarkably, the blockade of viral entry that started at the end of treatment hindered renewed degradation of SMC5/6.ConclusionThese results reveal that therapeutics abrogating all HBV transcripts including HBx promote epigenetic suppression of the HBV minichromosome, whereas strategies protecting the human hepatocytes from reinfection are needed to maintain cccDNA silencing.

Published

2021

146. In vitro inhibitory effect of maraviroc on the association of the simian immunodeficiency virus envelope glycoprotein with CCR5

Author

Ignacio Giraudy, Silvia A. González, José L. Affranchino, and César A. Ovejero

Subjects

viruses, Simian, medicine.disease_cause, 03 medical and health sciences, chemistry.chemical_compound, Viral envelope, Virology, Genetics, medicine, Molecular Biology, Immunodeficiency, 030304 developmental biology, Maraviroc, chemistry.chemical_classification, 0303 health sciences, biology, 030306 microbiology, virus diseases, General Medicine, Simian immunodeficiency virus, biology.organism_classification, medicine.disease, In vitro, Entry inhibitor, chemistry, Glycoprotein, medicine.drug

Abstract

Asian macaques infected with simian immunodeficiency viruses (SIVs) isolated from African non-human primates develop a disease similar to human AIDS. SIV enters its target cells by binding to CD4 and a coreceptor, typically CCR5. Maraviroc is an entry inhibitor of human immunodeficiency virus type 1 (HIV-1) that prevents the interaction between CCR5 and the surface subunit gp120 of the viral envelope glycoprotein (Env). Thus far, the activity of maraviroc on SIV entry has been poorly studied. Here, we determined in vitro pharmacological parameters of the effect of maraviroc on the SIV Env association with CCR5. Cell-to-cell fusion inhibition assays were used to compare the susceptibility to maraviroc of the SIVsmmPBj Env-CCR5 interaction with that of HIV-1BaL Env. Analysis of dose–response curves and determination of IC50 values demonstrate that increasing concentrations of maraviroc inhibit the membrane fusion activity of SIVsmmPBj Env in a manner and to an extent similar to that of HIV-1BaL Env.

Published

2021

147. Long-term trans-inhibition of the hepatitis B and D virus receptor NTCP by taurolithocholic acid

Author

Dieter Glebe, Nora Goldmann, Kira Alessandra At Lowjaga, Simon Franz Müller, Joachim Geyer, Michael Kirstgen, and Felix Lehmann

Subjects

Hepatology, Bile acid, Physiology, medicine.drug_class, Virus receptor, Gastroenterology, Transporter, Hepatitis B, medicine.disease, digestive system, Molecular biology, Entry inhibitor, chemistry.chemical_compound, Cholestasis, chemistry, Physiology (medical), medicine, Taurolithocholic acid, Receptor, medicine.drug

Abstract

Human hepatic bile acid transporter Na+/taurocholate cotransporting polypeptide (NTCP) represents the liver-specific entry receptor for the hepatitis B and D viruses (HBV/HDV). Chronic hepatitis B and D affect several million people worldwide, but treatment options are limited. Recently, HBV/HDV entry inhibitors targeting NTCP have emerged as promising novel drug candidates. Nevertheless, the exact molecular mechanism that NTCP uses to mediate virus binding and entry into hepatocytes is still not completely understood. It is already known that human NTCP mRNA expression is downregulated under cholestasis. Furthermore, incubation of rat hepatocytes with the secondary bile acid taurolithocholic acid (TLC) triggers internalization of the rat Ntcp protein from the plasma membrane. In the present study, the long-term inhibitory effect of TLC on transport function, HBV/HDV receptor function, and membrane expression of human NTCP were analyzed in HepG2 and human embryonic kidney (HEK293) cells stably overexpressing NTCP. Even after short-pulse preincubation, TLC had a significant long-lasting inhibitory effect on the transport function of NTCP, but the NTCP protein was still present at the plasma membrane. Furthermore, binding of the HBV/HDV myr-preS1 peptide and susceptibility for in vitro HDV infection were significantly reduced by TLC preincubation. We hypothesize that TLC rapidly accumulates in hepatocytes and mediates long-lasting trans-inhibition of the transport and receptor function of NTCP via a particular TLC-binding site at an intracellularly accessible domain of NTCP. Physiologically, this trans-inhibition might protect hepatocytes from toxic overload of bile acids. Pharmacologically, it provides an interesting novel NTCP target site for potential long-acting HBV/HDV entry inhibitors.NEW & NOTEWORTHY The hepatic bile acid transporter NTCP is a high-affinity receptor for hepatitis B and D viruses. This study shows that TLC rapidly accumulates in NTCP-expressing hepatoma cells and mediates long-lasting trans-inhibition of NTCP's transporter and receptor function via an intracellularly accessible domain, without substantially affecting its membrane expression. This domain is a promising novel NTCP target site for pharmacological long-acting HBV/HDV entry inhibitors.

Published

2021

148. RETRACTED ARTICLE: Thiophen urea derivatives as a new class of hepatitis C virus entry inhibitors

Author

Eun Kyu Lee, Tae Kon Kim, Inhee Choi, Hyung Chul Ryu, Marc P. Windisch, Jee Woong Lim, and Hye Hyun Yoo

Subjects

Drug, Hepatitis C virus, media_common.quotation_subject, small molecule, thiophen urea, RM1-950, Pharmacology, medicine.disease_cause, 01 natural sciences, chemistry.chemical_compound, Docking (dog), Pharmacokinetics, Drug Discovery, medicine, entry inhibitor, media_common, EC50, 010405 organic chemistry, General Medicine, hepatitis c virus, Small molecule, 0104 chemical sciences, Entry inhibitor, 010404 medicinal & biomolecular chemistry, chemistry, Therapeutics. Pharmacology, Lead compound, medicine.drug

Abstract

To develop unique small-molecule inhibitors of hepatitis C virus (HCV), thiophen urea (TU) derivatives were synthesised and screened for HCV entry inhibitory activities. Among them, seven TU compounds exhibited portent anti-viral activities against genotypes 1/2 (EC50 < 30 nM) and subsequently, they were further investigated; based on the pharmacological, metabolic, pharmacokinetic, and safety profiles, J2H-1701 was selected as the optimised lead compound as an HCV entry inhibitor. J2H-1701 possesses effective multi-genotypic antiviral activity. The docking results suggested the potential interaction of J2H-1701 with the HCV E2 glycoprotein. These results suggest that J2H-1701 can be a potential candidate drug for the development of HCV entry inhibitors.

Published

2021

149. Pentagalloylglucose, a highly bioavailable polyphenolic compound present in Cortex moutan, efficiently blocks hepatitis C virus entry.

Author

Behrendt, Patrick, Perin, Paula, Menzel, Nicolas, Banda, Dominic, Pfaender, Stephanie, Alves, Marco P., Thiel, Volker, Meuleman, Philip, Colpitts, Che C., Schang, Luis M., Vondran, Florian W.R., Anggakusuma, null, Manns, Michael P., Steinmann, Eike, and Pietschmann, Thomas

Subjects

*PENTAGALLOYLGLUCOSE, *POLYPHENOLS, *HEPATITIS C virus, *ANTIVIRAL agents, *LIVER transplantation

Abstract

Approximately 142 million people worldwide are infected with hepatitis C virus (HCV). Although potent direct acting antivirals are available, high costs limit access to treatment. Chronic hepatitis C virus infection remains a major cause of orthotopic liver transplantation. Moreover, re-infection of the graft occurs regularly. Antivirals derived from natural sources might be an alternative and cost-effective option to complement therapy regimens for global control of hepatitis C virus infection. We tested the antiviral properties of a mixture of different Chinese herbs/roots named Zhi Bai Di Huang Wan (ZBDHW) and its individual components on HCV. One of the ZBDHW components, Penta-O-Galloyl-Glucose (PGG), was further analyzed for its mode of action in vitro , its antiviral activity in primary human hepatocytes as well as for its bioavailability and hepatotoxicity in mice. ZBDHW, its component Cortex Moutan and the compound PGG efficiently block entry of HCV of all major genotypes and also of the related flavivirus Zika virus. PGG does not disrupt HCV virion integrity and acts primarily during virus attachment. PGG shows an additive effect when combined with the well characterized HCV inhibitor Daclatasvir. Analysis of bioavailability in mice revealed plasma levels above tissue culture IC 50 after a single intraperitoneal injection. In conclusion, PGG is a pangenotypic HCV entry inhibitor with high bioavailability. The low cost and wide availability of this compound make it a promising candidate for HCV combination therapies, and also emerging human pathogenic flaviviruses like ZIKV. [ABSTRACT FROM AUTHOR]

Published

2017

150. New Drugs in the Pipeline for the Treatment of HIV: a Review.

Author

Gravatt, Leigh Anne Hylton, Leibrand, Crystal R, Patel, Sulay, and McRae, MaryPeace

Abstract

Purpose of Review: The purpose of this paper is to review therapies with new mechanisms of action for the treatment of HIV that are at least in phase 2 clinical trials. Recent Findings: There are several new mechanisms of action being represented within clinical development, including histone deacetylase (HDAC) inhibitors, gene therapies, broadly neutralizing anti-HIV antibodies, immune modulation, and drugs with new mechanisms to block HIV entry. The new therapies are being developed for both as add-on therapy to existing combination antiretroviral therapy and as agents to be used during treatment interruption. The current drugs in development have had varying degrees of success in the early trials. Summary: Each of these new drugs may potentially fill a void in current antiretroviral therapy (ART) therapies, which will ultimately lead to improved outcomes in HIV-infected individuals. [ABSTRACT FROM AUTHOR]

Published

2017