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New Neuraminidase Inhibitory Alkaloids from the Mangrove Soil-Derived Fungus Arthrinium sp.SCSIO 41305
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作者 HU Yiwei ZHAO Kai +6 位作者 ZHU Junheng QI Xin CHEN Weihao SONG Yingying PANG Xiaoyan LIU Yonghong WANG Junfeng 《Journal of Ocean University of China》 SCIE CAS CSCD 2023年第5期1446-1451,共6页
New alkaloid,(E)-2-(hydroxyimino)-4-methylpentanamide(1)and a new cyclopentano[b]pyridine,4-hydroxy-7-methyl-6,7-dihydro-5H-cyclopenta[c]pyridin-5-one(2),together with ten known compounds(3–12)were isolated from the ... New alkaloid,(E)-2-(hydroxyimino)-4-methylpentanamide(1)and a new cyclopentano[b]pyridine,4-hydroxy-7-methyl-6,7-dihydro-5H-cyclopenta[c]pyridin-5-one(2),together with ten known compounds(3–12)were isolated from the mangrove soil-derived fungus Arthrinium sp.SCSIO 41305.Extensive spectroscopic analysis and X-Ray crystallographic analysis were used to elucidate the structure of(E)-2-(hydroxyimino)-4-methylpentanamide(1),including its absolute configuration.All the isolated compounds(1–12)were evaluated for their antimicrobial and enzyme inhibitory activities against acetylcholinesterase(ACh E),neuraminidase(NAs),and phosphatidylinositol 3-kinase(PI3K).Among them,compounds 1 and 3 exhibited strong neuraminidase inhibitory activity with IC_(50)values of 12.04,1.92μmol L^(-1)(IC_(50)20μmol L^(-1)for oseltamivir acid),while compounds 5,6,8,and 10showed moderate neuraminidase inhibitory activity,and compounds 6–10 displayed weak enzyme inhibitory activities against PI3K. 展开更多
关键词 Arthrinium ALKALOID pyridine neuraminidasE ACETYLCHOLINESTERASE
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Compound heterozygous mutations in the neuraminidase 1 gene in type 1 sialidosis: A case report and review of literature 被引量:4
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作者 Lan-Xiao Cao Ying Liu +3 位作者 Zhao-Jun Song Bao-Rong Zhang Wen-Ying Long Guo-Hua Zhao 《World Journal of Clinical Cases》 SCIE 2021年第3期623-631,共9页
BACKGROUND Type 1 sialidosis,also known as cherry-red spot-myoclonus syndrome,is a rare autosomal recessive lysosomal storage disorder presenting in the second decade of life.The most common symptoms are myoclonus,ata... BACKGROUND Type 1 sialidosis,also known as cherry-red spot-myoclonus syndrome,is a rare autosomal recessive lysosomal storage disorder presenting in the second decade of life.The most common symptoms are myoclonus,ataxia and seizure.It is rarely encountered in the Chinese mainland.CASE SUMMARY A 22-year-old male presented with complaints of progressive myoclonus,ataxia and slurred speech,without visual symptoms;the presenting symptoms began at the age of 15-year-old.Whole exome sequencing revealed two pathogenic heterozygous missense variants[c.239C>T(p.P80L)and c.544A>G(p.S182G)in the neuraminidase 1(NEU1)gene],both of which have been identified previously in Asian patients with type 1 sialidosis.All three patients identified in China's Mainland come from three unrelated families,but all three show the NEU1 mutations p.S182G and p.P80L pathogenic variants.Increasing sialidase activity through chaperones is a promising therapeutic target in sialidosis.CONCLUSION Through retrospective analysis and summarizing the clinical and genetic characteristics of type 1 sialidosis,we hope to raise awareness of lysosomal storage disorders among clinicians and minimize the delay in diagnosis. 展开更多
关键词 Sialidosis MYOCLONUS ATAXIA neuraminidase 1 Case report Mucolipidoses
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Analysis of correlated mutations, stalk motifs, and phylogenetic relationship of the 2009 influenza A virus neuraminidase sequences 被引量:4
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作者 Wei Hu 《Journal of Biomedical Science and Engineering》 2009年第7期550-558,共9页
The 2009 H1N1 influenza pandemic has attracted worldwide attention. The new virus first emerged in Mexico in April, 2009 was identified as a unique combination of a triple- reassortant swine influenza A virus, compose... The 2009 H1N1 influenza pandemic has attracted worldwide attention. The new virus first emerged in Mexico in April, 2009 was identified as a unique combination of a triple- reassortant swine influenza A virus, composed of genetic information from pigs, hu- mans, birds, and a Eurasian swine influenza virus. Several recent studies on the 2009 H1N1 virus util-ized small datasets to conduct analysis. With new sequences available up to date, we were able to extend the previous research in three areas. The first was finding two networks of co-mutations that may po-tentially affect the current flu-drug binding sites on neuraminidase (NA), one of the two surface proteins of flu virus. The second was discovering a special stalk motif, which was dominant in the H5N1 strains in the past, in the 2009 H1N1 strains for the first time. Due to the high virulence of this motif, the second finding is significant in our current research on 2009 H1N1. The third was updating the phylogenetic an- alysis of current NA sequences of 2009 H1N1 and H5N1, which demonstrated that, in clear contrast to previous findings, the N1 sequences in 2009 are di-verse enough to cover different major branches of the phylogenetic tree of those in previous years. As the novel influenza A H1N1 virus continues to spread globally, our results highlighted the importance of performing timely analysis on the 2009 H1N1 virus. 展开更多
关键词 Entropy Co-mutation MUTATION Mutual Information neuraminidasE Phylogenetic ANALYSIS Random Forest STALK Motif Swine Flu
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Production and application of recombinant haemagglutinin neuraminidase of Newcastle disease virus 被引量:1
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作者 Selvan Nallaiyan Ranjit Singh Amirtha Jacob Abbadorai +2 位作者 Sukumar Sundaramoorthy Jeyakumar Nelson Suryanarayana Veluvarthy Venkata Sanyasi 《Asian Pacific Journal of Tropical Medicine》 SCIE CAS 2010年第8期629-632,共4页
Objective:To discuss the possibility of expressing the haemagglutinin-neuraminidase(HN) protein in prokaryotic system such as Escherichia coli(E.coli) cells by cloning the full length HN gene.Methods:The full leng... Objective:To discuss the possibility of expressing the haemagglutinin-neuraminidase(HN) protein in prokaryotic system such as Escherichia coli(E.coli) cells by cloning the full length HN gene.Methods:The full length HN gene of Newcastle Disease Virus(NDV) of size 1 734 bp was preciously isolated by RT-PCR.The sequence was assessed and submitted to Nucleic Acid Databank(NCBI) and the gene ID was EU215390.1 after cloning and sequencing.Now the assessed HN gene was subcloned into pET 32 a+ expression vector for production the HN protein in E.coli, BL21(DE3) P<sup>LYS</sup>S cells following standard protocols.The crude lysate protein from the induced positive clone was size assessed by sodium dodecyl sulfale-polyacrylamide gel electrophoresis (SDS-PAGE) and their haemagglutination(HA) property against chicken RBC was assessed by standard micro HA test.Results:The molecular size of the full HN gene of NDV as assessed by cloning and digesting the positive clone to release the insert was 1.7 kb.The expressed protein in both crude and pure form was assessed to be 63 kDa and 81 kDa,respectively.The HA activity of the crude protein of the positive clone was 1 in 40.Conclusions:This finding indicates that the fusion protein retains the biological activity of native protein in the crude form and therefore could be used as a diagnostic reagent for antibody detection and for routine assessment of immune status in commercial layer forms. 展开更多
关键词 Newcastle disease VIRUS HAEMAGGLUTININ neuraminidasE Surface GLYCOPROTEIN Diagnostic REAGENT
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Activity of T Cells Stimulated by Hemagglutinin-neuraminidase of Newcastle Disease Virus in vivo 被引量:3
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作者 PIAO Bing-guo LI Xiao +9 位作者 SUN Li-li KAN Shi-fu LIU Lei HUANG Hai-yan YANG Guo-hua WANG Yu-hang WANG Zhuo-yue SUN Jiu-hua PIAO Yun-feng JIN Ning-yi 《Chemical Research in Chinese Universities》 SCIE CAS CSCD 2011年第3期455-460,共6页
To investigate the stimulated activity of T cells and the anti-tumor properties of hemagglutinin-neuraminidase(HN) of Newcastle disease virus(NDV) strain Changchun(NDVcc), the expression of HN gene in hepatoma c... To investigate the stimulated activity of T cells and the anti-tumor properties of hemagglutinin-neuraminidase(HN) of Newcastle disease virus(NDV) strain Changchun(NDVcc), the expression of HN gene in hepatoma cells(human HepG-2 and mouse H22 cells) infected with the recombinant adenovirus(Ad-HN) was identified by Western blot analysis and flow cytometry. Sialidase activity of NDVcc HN expressed by Ad-HN was assayed by the periodate-resorcinol method. The in vivo anti-tumor effects of NDVcc HN were evaluated in the H22 solid tumor model. Regional lymph nodes of the mouse model treated with Ad-HN were removed to harvest T lymphocytes and evaluating the specific cytotoxicity of cytotoxic T lymphocyte(CTL) and natural killer(NK) cells by an L-lactate dehydrogenase(LDH) assay, in the mean time, the secretion of cytokines was analyzed by enzyme linked immunosorbent assays(ELISA). The results show that NDVcc HN was effectively expressed by Ad-HN in HepG-2 and H22 cells. The sialidase activity assay showed that Ad-HN significantly reduced sialic acid level of the hepatoma cells compared with the cells infected the empty adenovirus vector(Ad-mock). When treated with Ad-HN, the growth of subcutaneous H22 primary tumors in C57BL/6 mice was suppressed, and the mean mice survival increased. In addition, the treatment of Ad-HN elicited strong NK and CTL responses, and high levels of Th1 cytokines, such as IL-2 and IFN-γ. In conclusion, NDVcc HN effectively elicits T cell-mediate anti-tumor cytotoxicity via sialidase activity and may be a novel strategy for cancer immunotherapy. 展开更多
关键词 Newcastle disease virus HEMAGGLUTININ-neuraminidasE HEPATOMA T Cell Anti-tumor immunity
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In Vitro Anti-viral Activities and Structureactivity Relationship Studies of Flavones and Dihydroflavone Derivatives as Influenza Virus Potential Neuraminidase Inhibitors 被引量:1
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作者 孙家英 何云清 +3 位作者 杜惠蓉 刘长路 陈安银 梅虎 《Chinese Journal of Structural Chemistry》 SCIE CAS CSCD 2015年第11期1641-1651,共11页
From the bioassay tests, 14 neuraminidase inhibitors (NIs) flavones and dihydroflavones derivatives from natural plants displayed different degree of inhibitory activities. Further- more, compounds No. 8 and 14 show... From the bioassay tests, 14 neuraminidase inhibitors (NIs) flavones and dihydroflavones derivatives from natural plants displayed different degree of inhibitory activities. Further- more, compounds No. 8 and 14 showed good inhibitory activity against influenza A virus with IC50 = 835.4 and 860.6 μg/mL. Then, to investigate interactions between NIs and neuraminidase (NA), molecular docking was performed. Docking results indicated that Arg118, Asp151, Arg292 and Arg371 were the key residues in the active pocket of 2ht8. Main influencing factors of interactions between NIs and NA were hydrogen bond and electrostatic, then hydrophobic factor. Moreover, experimental activities of NIs were consistent with total scores of the docking. In order to understand the chemical-biological interactions governing their activities toward NA, QSAR models of 14 NIs were developed. The obtained HQSAR (hologram quantitative structure activity relationship), PLS (partial least squares) and SRA (stepwise regression analysis) models were robust and had good exterior predictive capabilities. Moreover, squared multiple correlation coefficients (R2) and squared cross-validated correlation coefficients (Q2) of HQSAR and PLS models based on descriptors by Gaussian and Sarchitect were 0.832 and 0.721, 0.925 and 0.688, 0.892 and 0.692, respectively. R2 and SE (standard error) of SRA model based on descriptors by Gaussian were 0.922 and 0.072. Therefore, these models may be further used to design and evaluate the bioactivity of new compounds. 展开更多
关键词 neuraminidase inhibitors ACTIVITIES flavones and dihydroflavones DOCKING QSAR
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Pathogenicity and amino acid sequences of hemagglutinin cleavage site and neuraminidase stalk of differently passaged H9N2-avian influenza virus in broilers 被引量:1
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作者 Houssam A. Shaib Nelly Cochet +4 位作者 Thierry Ribeiro Afif M. Abdel Nour Georges Nemer Maya F. Saade Elie K. Barbour 《Advances in Bioscience and Biotechnology》 2011年第4期198-206,共9页
Low pathogenic Avian Influenza (AI) virus has the ability to evolve to high pathogenic viruses resulting in significant economic losses in the poultry sector. This study aims at assessing the impact of H9N2 viral pass... Low pathogenic Avian Influenza (AI) virus has the ability to evolve to high pathogenic viruses resulting in significant economic losses in the poultry sector. This study aims at assessing the impact of H9N2 viral passaging in broilers and its relatedness to pathogenicity and amino acid (a.a) sequences of the hemagglutinin (HA) cleavage site and neuraminidase (NA) stalk. The original H9N2 AI virus (P0) was used to challenge ten-21 days old broilers. Individual recovery of H9N2 virus from homogenates of trachea, lungs and airsacs was attempted in 9 days old chicken embryos, as a conclusion of the first passage (P1). Tracheal isolates of H9N2 were passaged for a second (P2) and a third (P3) time in broilers, followed by a similar embryonic recovery procedure. The a.a. sequence of a part of HA1 cleavage site and Neuraminidase stalk were compared among the differently passaged viruses;an assessement of the relatedness of the determined a.a. sequences to the pathogenicity in broilers, based on frequency of mortality, morbidity signs, gross and microscopic lesions at 3 days post challenge with the P1, P2, and P3-H9N2, is concluded. An increase in certain morbidity signs and specific lesions was observed in P2- and P3-H9N2 challenged broilers compared to birds challenged with P1-H9N2. A conserved R-S-S-R amino acid sequence at the HA1 cleavage site was observed in the differently passaged H9N2, associated with a variability in the NA stalk-a.a sequences. The passaging of the low pathogenic H9N2 virus in broilers leads to a trend of increase in pathogenicity, manifested in higher frequency of morbidity signs, and of specific gross and microscopic lesions of the examined organs. This passaging was associated with a conserved a.a. sequence of the hemaglutinin cleavage site and a variability in the sequence of the neuraminidase stalk. A detailed study of the potential of the detected variability in the neuraminidase stalk of H9N2 in induction of a higher pathogenicity in broilers will be the subject of future investigations. 展开更多
关键词 H9N2 Avian Influenza PATHOGENICITY Passaging BROILERS Amino Acid Sequences HEMAGGLUTININ (HA) neuraminidasE (NA) STALK
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Indonesian avian influenza H274Y mutant neuraminidase homology models assessment 被引量:1
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作者 Sigit Jaya Herlambang Rosari Saleh 《Journal of Biophysical Chemistry》 2011年第3期345-352,共8页
Five models of Indonesian H274Y mutant neuralminidase type 1 (N1) were generated from the template 3CKZ by homology modeling. The template has the best similarity percentage 97% with the model sequence. The models was... Five models of Indonesian H274Y mutant neuralminidase type 1 (N1) were generated from the template 3CKZ by homology modeling. The template has the best similarity percentage 97% with the model sequence. The models was evaluated to search the best model with DOPE, 3D-profiles and PROCHECK in a good rank. The results show model 3 as a potential model to be used in the simulation with the lowest DOPE score, highest verify-3D score and from Ramachandran plots we inferred that it also shared the 1st rank with model 4 based on the 99.4% of the residues found, without Glycine and Proline, at the most favoured and additionally allowed region of both model structures. 展开更多
关键词 neuraminidasE MODEL Assessment HOMOLOGY MODEL MUTANT AVIAN Influenza
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Mutation-induced spatial differences in neuraminidase structure and sensitivity to neuraminidase inhibitors
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作者 杨志伟 郝东晓 +3 位作者 车一卓 杨嘉辉 张磊 张胜利 《Chinese Physics B》 SCIE EI CAS CSCD 2018年第1期145-153,共9页
Neuraminidase (NA), a major surface glycoprotein of influenza virus with well-defined active sites, is an ideal plat- form for the development of antiviral drugs. However, a growing number of NA mutations have drug ... Neuraminidase (NA), a major surface glycoprotein of influenza virus with well-defined active sites, is an ideal plat- form for the development of antiviral drugs. However, a growing number of NA mutations have drug resistance to today's inhibitors. Numerous efforts are made to explore the resistance mechanisms through understanding the structural changes in mutated NA proteins and the associated different binding profiles of inhibitors, via x-ray, nuclear magnetic resonance, electron microscopy, and molecular dynamics methods. This review presents the architectural features of mutated NA proteins, as well as the respective inhibitor sensitivities arising from these spatial differences. Finally, we summarize the resistance mechanisms of today's neuraminidase inhibitors and the outlook tbr the development of novel inhibitors. 展开更多
关键词 MUTATION active sites neuraminidasE inhibitor sensitivity
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Sheng Jiang San, traditional multi-herb formulation, exerts anti-influenza effects in vitro and in vivo via neuraminidaseinhibition and immune regulation
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作者 ZHANG Tian-bo XIAO Meng-jie +4 位作者 Chun-Kwok WONG Ka-Pun CHRIS MOK ZHAO Xin TI Hui-hui Pang-Chui SHAW 《中国药理学与毒理学杂志》 CAS 北大核心 2019年第9期738-739,共2页
OBJECTIVE Sheng Jiang San(SJS),a multi-herb formulation,is used in treating high fever,thirsty and anxiety in ancient China and it is sometimes used to treat seasonal influenza in modern.However,there is no evidenceba... OBJECTIVE Sheng Jiang San(SJS),a multi-herb formulation,is used in treating high fever,thirsty and anxiety in ancient China and it is sometimes used to treat seasonal influenza in modern.However,there is no evidencebased investigation and mechanism research to support SJS′s anti-influenza efficacy.This study aims to investigate the anti-influenza effect of SJS and its possible mechanisms.METHODS In this study,we examined the inhibitory effect of SJS against different influenza viruses on Madin-Darby canine kidney cells.Influenza virus infected BALB/c mice were employed as in vivo model to evaluate the efficacy.Mice challenged with A/PR/8/34(H1N1)were orally administrated SJS 1 g·kg^-1 daily for seven days and monitored for 14 d.The survival rate,body mass changes,lung index,lung viral load,histopathologic changes and immune-regulation of the mice were measured.The underlying anti-influenza virus mechanisms were studied by a series of biological assays in vitro to determine if hemagglutinin,ribonucleoprotein complex or nerauminidase were targets of SJS.RESULTS SJS exerted a broad spectrum of inhibitory effects on multiple influenza strains in a dose-dependent manner.And IC50 of SJS against A/WSN/33(H1N1)was lower than 35 mg·L^-1.SJS also protected 50%of mice from influenza virus PR8 infection.The lung index and the lung viral load of SJS treated mice were signifi⁃cantly decrease compared with untreated mice.SJS 2 g·L^-1 inhibited 80%of neuraminidase enzymatic activity.SJS also up-regulated TNF-αand IFN-αand down-regulated IL-2 of influenza virus induced mice.CONCLUSION SJS is a useful formulation for treating influenza virus infection. 展开更多
关键词 Sheng Jiang San anti-influenza activity neuraminidase inhibition immuno-regulation
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QSAR Studies on Influenza Neuraminidase Inhibitors——Acylthiourea Analogue
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作者 景举华 梁桂兆 +3 位作者 梅虎 张巧霞 李志良 吕凤林 《Chinese Journal of Structural Chemistry》 SCIE CAS CSCD 2009年第2期200-204,共5页
The quantitative structure-activity relationship (QSAR) of 30 acylthiourea analogues was studied by using a three-dimensional holographic vector of atomic interaction field (3D-HoVAIF) to describe their chemical s... The quantitative structure-activity relationship (QSAR) of 30 acylthiourea analogues was studied by using a three-dimensional holographic vector of atomic interaction field (3D-HoVAIF) to describe their chemical structures. The descriptors obtained were screened by stepwise multiple regression (SMR) and a partial least-squares (PLS) regression model was built. The correlation coefficient r^2 of the established model and Leave-One-Out (LOO) Cross-Validation (CV) correlation coefficient q^2 are 0.624 and 0.409, respectively. The model has favorable stability and good prediction capability, and further QSAR analysis showed that hydrophobic interaction has the most important effect on the activity of acylthiourea analogue and 3D-HoVAIF was applicable to the molecular structural characterization and biologicalactivity prediction. 展开更多
关键词 ACYLTHIOUREA neuraminidase inhibitors three-dimensional holographic vector of atomic interaction field (3D-HoVAIF) quantitative structure-activity relationship (QSAR)
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Analysis of Oseltamivir Resistance Substitutions in Influenza Virus Glycoprotein Neuraminidase using a Lentivirus-Based Surrogate Assay System
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作者 Jennifer Tisoncik-Go Katie S Cordero Lijun Rong 《Virologica Sinica》 SCIE CAS CSCD 2013年第2期81-91,共11页
Influenza A virus poses a great threat to global health, and oseltamivir (trade marked as Tamiflu), which targets influenza surface glycoprotein neuraminidase (NA), is used clinically as a major anti-influenza treatme... Influenza A virus poses a great threat to global health, and oseltamivir (trade marked as Tamiflu), which targets influenza surface glycoprotein neuraminidase (NA), is used clinically as a major anti-influenza treatment. However, certain substitutions in NA can render an influenza virus resistant to this drug. In this study, using a lentiviral pseudotyping system, which alleviates the safety concerns of studying highly pathogenic influenza viruses such as avian influenza H5N1, that utilizes influenza surface glycoproteins (hemagglutinin or HA, and NA) and an HIV-core combined with a luciferase reporter gene as a surrogate assay, we first assessed the functionality of NA by measuring pseudovirion release in the absence or presence of oseltamivir. We demonstrated that oseltamivir displays a dose-dependent inhibition on NA activity. In contrast, a mutant NA (H274Y) is more resistant to oseltamivir treatment. In addition, the effects of several previously reported substitution NA mutants were examined as well. Our results demonstrate that this lentivirus-based pseudotyping system provides a quick, safe, and effective way to assess resistance to neuraminidase inhibitors. And we believe that as new mutations appear in influenza isolates, their impact on the effectiveness of current and future anti-NA can be quickly and reliably evaluated by this assay. 展开更多
关键词 Influenza virus neuraminidase (NA) OSELTAMIVIR Drug resistance
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Molecular docking investigation for Indonesian H274Y mutant neuraminidase type 1 with neuraminidase inhibitors
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作者 Sigit Jaya Herlambang Rosari Saleh 《American Journal of Molecular Biology》 2012年第1期49-59,共11页
The aim of this study is to get insight the interaction between Indonesian H274Y mutant neuraminidase with four inhibitors. Not only to seek preferable inhibitor to be used, but also to investigate the interaction occ... The aim of this study is to get insight the interaction between Indonesian H274Y mutant neuraminidase with four inhibitors. Not only to seek preferable inhibitor to be used, but also to investigate the interaction occurred, especially hydrogen bonds formed. Hydrogen bonds analysis and its interaction energies calculation showed that zanamivir is the most preferable inhibitor with 13 hydrogen bonds formed and –439.96 kcal/mol. Laninamivir would be an alternative inhibitor since it has 10 hydrogen bonds and –307.19 kcal/mol. The investigation of ΔSAS showed almost all active site residues buried when interacted with inhibitors. Only a few residues have an increases ΔSAS. Lipinski rule analysis showed that zanamivir and laninamivir would be best taken by injection or inhalation. 展开更多
关键词 MOLECULAR DOCKING neuraminidasE INHIBITOR Resistance
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Evidence of Synergistic Activity of Medicinal Plant Extracts against Neuraminidase Inhibitor Resistant Strains of Influenza Viruses
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作者 Dhivya Rajasekaran Enzo A. Palombo +4 位作者 Tiong Chia Yeo Diana Lim Siok Ley Chu Lee Tu Francois Malherbe Lara Grollo 《Advances in Microbiology》 2014年第16期1260-1277,共18页
The frequent emergence of drug resistant influenza viral strains emphasizes the urgent and continual need to develop new antiviral drugs. Given the encouraging findings of previous studies on antiviral compounds from ... The frequent emergence of drug resistant influenza viral strains emphasizes the urgent and continual need to develop new antiviral drugs. Given the encouraging findings of previous studies on antiviral compounds from plant sources, this study focused on medicinal plants from Borneo that were traditionally used to treat symptoms of influenza infection. Following the promising results of earlier investigations, four plant extracts that demonstrated multiple modes of viral inhibition were studied against wild-type and neuraminidase (NA) inhibitor-resistant strains of Types A and B influenza viruses. The extracts exhibited more pronounced activities against the wild-type viruses than the NA inhibitor-resistant strains. Variations in the antiviral potential of the extracts collected from different parts of the same plant were also evidenced in the in vitro micro-inhibition assays. Even though all plant extracts affected NA activity of all viruses, only two extracts demonstrated hemagglutination inhibitory (HI) activities against Type A pandemic H1N1 and Type B viruses. Furthermore, Receptor Destroying Enzyme (RDE) treatments of extracts exhibiting HI activities indicated the presence of sialic acid (SA)-like component(s) that may be responsible for HI activity. Since the antiviral potential of extracts was not completely suppressed by RDE, the possibility of non SA-like antiviral components cannot be ruled out. Therefore, synergistic activity between SA-like and non SA-like components contained in the plant extracts may be responsible for the demonstrated antiviral potential. The results also indicated the presence of non SA-like components that may act against other viral proteins apart from hemagglutinin (HA) and NA. Hence, this study supports the presence of multiple antiviral components that act against different viral proteins or interfere with different stages of viral replication. Our results suggest that these plant extracts have the potential to be developed as therapeutic agents for the treatment of influenza and could be a solution to the global occurrence of viral strains resistant to NA inhibitors. 展开更多
关键词 Influenza ANTIVIRALS MEDICINAL Plant Extracts HEMAGGLUTINATION INHIBITION neuraminidasE INHIBITION Sialic Acid-Like RDE
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Substrate specificity of avian influenza H5N1 neuraminidase
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作者 Naruthai Onsirisakul Shin-ichi Nakakita +7 位作者 Chompunuch Boonarkart Alita Kongchanagul Ornpreya Suptawiwat Pilaipan Puthavathana Krisada Chaichuen Kanokwan Kittiniyom Yasuo Suzuki Prasert Auewarakul 《World Journal of Virology》 2014年第4期30-36,共7页
AIM: To characterise neuraminidase(NA) substrate specificity of avian influenza H5N1 strains from humans and birds comparing to seasonal influenza virus.METHODS: Avian influenza H5N1 strains from humans and birds were... AIM: To characterise neuraminidase(NA) substrate specificity of avian influenza H5N1 strains from humans and birds comparing to seasonal influenza virus.METHODS: Avian influenza H5N1 strains from humans and birds were recruited for characterising their NA substrate specificity by using a modified commercial fluorescence Amplex Red assay. This method can identify the preference of α2,6-linked sialic acid or α2,3-linked sialic acid. Moreover, to avoid the bias of input virus, reverse genetic virus using NA gene from human isolated H5N1 were generated and used to compare with the seasonal influenza virus. Lastly, the substrate specificity profile was further confirmed by high-performance liquid chromatography(HPLC) analysis of the enzymatic product. RESULTS: The H5N1 NA showed higher activity on α2,3-linked sialic acid than α2,6-linked(P < 0.0001). To compare the NA activity between the H5N1 and seasonal influenza viruses, reverse genetic viruses carrying the NA of H5N1 viruses and NA from a seasonal H3N2 virus was generated. In these reverse genetic viruses, the NA activity of the H5N1 showed markedly higher activity against α2,3-linked sialic acid than that of the H3N2 virus, whereas the activities on α2,6-linkage were comparable. Interestingly, NA from an H5N1 human isolate that was previously shown to have heamagglutinin(HA) with dual specificity showed reduced activity on α2,3-linkage. To confirm the substrate specificity profile, HPLC analytic of enzymatic product was performed. Similar to Amplex red assay, H5N1 virus showed abundant preference on α2,3-linked sialic acid.CONCLUSION: H5N1 virus maintains the avian specific NA and NA changes may be needed to accompany changes in HA receptor preference for the viral adaptation to humans. 展开更多
关键词 H5N1 AVIAN INFLUENZA VIRUS neuraminidasE Sialic acid Adaptation Substrate PREFERENCE
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The Comparison of Substrate Stability in Neuraminidase Type 2 (N2) Active Site between A/Tokyo/3/67 and A/Pennsylvania/10218/84 with Heating Dynamics Simulation
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作者 Sigit Jaya Herlambang Rosari Saleh 《World Journal of Condensed Matter Physics》 2011年第3期77-87,共11页
A molecular dynamics simulation of two neuraminidase-sialic acid (NA-SA) complexes show a difference of the level of stability between sialic acid and neuraminidases that originated from viruses A/Tokyo/3/67 (Structur... A molecular dynamics simulation of two neuraminidase-sialic acid (NA-SA) complexes show a difference of the level of stability between sialic acid and neuraminidases that originated from viruses A/Tokyo/3/67 (Structure A) dan A/Pennsylvania/10218/84 (Structure B). Analyses of sialic acid RMSD and the change of torsional angles suggest that the sialic acid in Structure A is much more twisted and able to be influenced more by the binding of the neuraminidase functional residues than Structure B. Moreover, analyses upon hydrogen bond occupancy and binding free energy of both complexes showed that Structure A had more stable hydrogen bonds and each complex’s binding free energy were calculated to be –1.37 kcal/mol and 17.97 kcal/mol for Structure A and Structure B, respectively, further suggesting stability more dominant in Structure A than Structure B. Overall, Structure A has a more stable enzyme-substrate than Structure B. 展开更多
关键词 neuraminidasE Sialic Acid BIND Stability Functional Residues AVIAN INFLUENZA
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Vitisin B inhibits influenza A virus replication by multi-targeting neuraminidase and virusinduced oxidative stress 被引量:3
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作者 Eun-Bin Kwon Wei Li +8 位作者 Young Soo Kim Buyun Kim Hwan-Suck Chung Younghoon Go Hyun-Jeong Ko Jae-Hyoung Song Young Ho Kim Chun Whan Choi Jang-Gi Choi 《Acta Pharmaceutica Sinica B》 SCIE CAS CSCD 2023年第1期174-191,共18页
The development of drug-resistant influenza and new pathogenic virus strains underscores the need for antiviral therapeutics.Currently,neuraminidase(NA)inhibitors are commonly used antiviral drugs approved by the US F... The development of drug-resistant influenza and new pathogenic virus strains underscores the need for antiviral therapeutics.Currently,neuraminidase(NA)inhibitors are commonly used antiviral drugs approved by the US Food and Drug Administration(FDA)for the prevention and treatment of influenza.Here,we show that vitisin B(VB)inhibits NA activity and suppresses H1N1 viral replication in MDCK and A549 cells.Reactive oxygen species(ROS),which frequently occur during viral infection,increase virus replication by activating the NF-κB signaling pathway,downmodulating glucose-6-phosphate dehydrogenase(G6PD)expression,and decreasing the expression of nuclear factor erythroid2-related factor 2(Nrf2)antioxidant response activity.VB decreased virus-induced ROS generation by increasing G6PD expression and Nrf2 activity,and inhibiting NF-κB translocation to the nucleus through IKK dephosphorylation.In addition,VB reduced body weight loss,increased survival,decreased viral replication and the inflammatory response in the lungs of influenza A virus(IAV)-infected mice.Taken together,our results indicate that VB is a promising therapeutic candidate against IAV infection,complements existing drug limitations targeting viral NA.It modulated the intracellular ROS by G6PD,Nrf2 antioxidant response pathway,and NF-κB signaling pathway.These results demonstrate the feasibility of a multi-targeting drug strategy,providing new approaches for drug discovery against IAV infection. 展开更多
关键词 INFLUENZA Vitisin B Vitis vinifera L. neuraminidasE Reactive oxygen species NF-κB Multi-targeting Nrf2 G6PD
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神经氨酶1在脂多糖诱导的心肌损伤中的作用及机制研究
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作者 王秀昆 陈小丽 杨波 《中国心血管病研究》 CAS 2024年第3期284-288,共5页
目的探讨神经氨酸酶1(NEU1)对脂多糖(LPS)诱导的大鼠心肌损伤的作用及分子机制。方法选取2023年6-7月于武汉市第三医院动物房饲养24只6~7周雄性Sprague-Dawley大鼠,大鼠购自湖北省疾控中心实验中心,首先采取NUE1抑制剂OSE(20 mg/kg)或... 目的探讨神经氨酸酶1(NEU1)对脂多糖(LPS)诱导的大鼠心肌损伤的作用及分子机制。方法选取2023年6-7月于武汉市第三医院动物房饲养24只6~7周雄性Sprague-Dawley大鼠,大鼠购自湖北省疾控中心实验中心,首先采取NUE1抑制剂OSE(20 mg/kg)或等量生理盐水连续灌胃预处理3 d后,腹腔注射LPS(10 mg/kg)或等量生理盐水,12 h后行心脏离体灌流检查。取血清,ELISA检测心肌损伤标志物cTnT、CK-MB;取心脏,Western检测心肌组织中Bcl-2、Bax蛋白表达水平。结果超声心动图结果显示,LPS组大鼠心脏射血分数及缩短分数明显降低,而LPS+OSE组大鼠的心脏功能得到改善。血清酶学结果显示,LPS组大鼠心肌损伤标志物较对照组明显升高,而NEU1抑制剂OSE组则显著降低心肌损伤标志物的水平。心脏电生理结果显示,LPS腹腔注射后,大鼠心脏的动作电位(APD)及有效不应期(ERP)显著缩短;与LPS组相比,LPS+OSE组大鼠的平均ERP及APD50、APD90水平显著增加。Western结果示LPS腹腔注射后,大鼠心肌组织中Bax的蛋白水平表达明显升高,Bcl-2蛋白则表达较少;与LPS组相比,LPS+OSE组大鼠心肌组织中的Bcl-2表达增加,Bax蛋白水平降低。结论NEU1抑制剂预处理可通过减轻炎症和细胞凋亡,改善LPS诱导造成的心肌损伤,从而保护心脏功能。 展开更多
关键词 神经氨酸酶1 脂多糖 凋亡
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基于FAERS的神经氨酸酶抑制剂药品不良事件信号挖掘
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作者 阴敏 陈佳丽 +2 位作者 刘皓天 菅凌燕 刘晓东 《中国药业》 CAS 2024年第19期122-126,共5页
目的为临床安全使用神经氨酸酶抑制剂提供参考。方法采用OpenVigil 2.1平台检索美国食品和药物管理局不良事件报告系统(FAERS)中2004年第1季度至2022年第3季度奥司他韦、扎那米韦、帕拉米韦的相关药品不良事件(ADE)报告(其中帕拉米韦只... 目的为临床安全使用神经氨酸酶抑制剂提供参考。方法采用OpenVigil 2.1平台检索美国食品和药物管理局不良事件报告系统(FAERS)中2004年第1季度至2022年第3季度奥司他韦、扎那米韦、帕拉米韦的相关药品不良事件(ADE)报告(其中帕拉米韦只有2015年至2022年的数据),采用报告比值比(ROR)法和英国药品和保健品管理局(MHRA)综合标准法挖掘ADE信号,采用《国际医学用语词典(25.0版)》(MedDRA 25.0)中的首选语(PT)对检索到的药品不良反应(ADR)进行编码,按系统器官分类(SOC)进行归类。结果共获得以神经氨酸酶抑制剂为首要怀疑药物的ADE报告14646份,其中奥司他韦12223份、扎那米韦2377份、帕拉米韦46份。共挖掘到ADE信号228个,涉及15个SOC,SOC主要集中在精神病类、胃肠系统疾病、各类神经系统疾病等。发生频次较多的ADR,奥司他韦为呕吐、异常行为、幻觉、失眠、意识模糊状态等,扎那米韦为异常行为、幻觉、谵妄、意识丧失、意识状态改变等,帕拉米韦为休克和急性肾损伤;信号强度较大的ADR,奥司他韦为婴儿痤疮、热性谵妄、病态人格、出血性小肠结肠炎、睡惊症等,扎那米韦为热性谵妄、热性惊厥、眼黏膜皮肤综合征、异常行为、梦话,帕拉米韦为休克和急性肾损伤;未列入药品说明书的ADR,奥司他韦有失眠、上腹痛、攻击、意识丧失、心动过缓等,扎那米韦有意识丧失、意识水平下降、惊厥发作、攻击、激越等。结论临床使用神经氨酸酶抑制剂时,应关注精神病类、胃肠系统疾病和各类神经系统疾病的ADR,以保障患者的用药安全。 展开更多
关键词 神经氨酸酶抑制剂 美国食品和药物管理局不良事件报告系统 药品不良事件 报告比值比法 英国药品和保健品管理局(MHRA)综合标准法
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Drug screening for influenza neuraminidase inhibitors 被引量:7
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作者 LIU Ailin, CAO Hongpeng & DU Guanhua Institute of Materia Medica, Chinese Academy of Medical Sciences and Peking Union Medical College, Beijing 100050, China Institute of Medicinal Biotechnology, Chinese Academy of Medical Sciences and Peking Union Medical College, Beijing 100050, China 《Science China(Life Sciences)》 SCIE CAS 2005年第1期1-5,共5页
Neuraminidase (NA) is one of the most important targets to screen the drugs of anti-influenza virus A and B. After virtual screening approaches were applied to a compound database which possesses more than 10000 compo... Neuraminidase (NA) is one of the most important targets to screen the drugs of anti-influenza virus A and B. After virtual screening approaches were applied to a compound database which possesses more than 10000 compound structures, 160 compounds were selected for bioactivity assay, then a High Throughput Screening (HTS) model established for influenza virus NA inhibitors was applied to detect these compounds. Finally, three compounds among them displayed higher inhibitory activities, the range of their IC5o was from 0.1 μmol/L to 3 μmol/L. Their structural scaffolds are novel and different from those of NA inhibitors approved for influenza treatment, and will be useful for the design and research of new NA inhibitors. The result indicated that the combination of virtual screening with HTS was very significant to drug screening and drug discovery. 展开更多
关键词 neuraminidasE (NA) inhibitor high THROUGHPUT SCREENING (HTS) INFLUENZA virus virtual screening.
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