fbpx
Wikipedia

Viral neuraminidase

January 01, 1970

Viral neuraminidase is a type of neuraminidase found on the surface of influenza viruses that enables the virus to be released from the host cell. Neuraminidases are enzymes that cleave sialic acid (also called neuraminic acid) groups from glycoproteins. Viral neuraminidase was discovered by Alfred Gottschalk at the Walter and Eliza Hall Institute in 1957.[3] Neuraminidase inhibitors are antiviral agents that inhibit influenza viral neuraminidase activity and are of major importance in the control of influenza.[4]

Neuraminidase
Crystallographic structure of influenza neuraminidase in complex with the inhibitor 4-acetamido-3-hydroxy-5-nitro-benzoic acid.[1]
Identifiers
SymbolNeur
PfamPF00064
Pfam clanCL0434
InterProIPR001860
SCOP22bat / SCOPe / SUPFAM
CAZyGH34
CDDcd00260
Available protein structures:
Pfam  structures / ECOD  
PDBRCSB PDB; PDBe; PDBj
PDBsumstructure summary
PDB1a14​, 1a4g​, 1a4q​, 1b9s​, 1b9t​, 1b9v​, 1bji​, 1f8b​, 1f8c​, 1f8d​, 1f8e​, 1inf​, 1ing​, 1inh​, 1inv​, 1inw​, 1inx​, 1iny​, 1ivb​, 1ivc​, 1ivd​, 1ive​, 1ivf​, 1ivg​, 1l7f​, 1l7g​, 1l7h​, 1mwe​, 1nca​, 1ncb​, 1ncc​, 1ncd​, 1nma​, 1nmb​, 1nmc​, 1nn2​, 1nna​, 1nnb​, 1nnc​, 1nsb​, 1nsc​, 1nsd​, 1v0z​, 1vcj​, 1w1x​, 1w20​, 1w21​, 1xoe​, 1xog​, 2aep​, 2aeq​, 2b8h​, 2bat​, 2c4a​, 2c4l​, 2cml​, 2ht5​, 2ht7​, 2ht8​, 2htq​, 2htr​, 2htu​, 2htv​, 2htw​, 2hty​, 2hu0​, 2hu4​, 2qwa​, 2qwb​, 2qwc​, 2qwd​, 2qwe​, 2qwf​, 2qwg​, 2qwh​, 2qwi​, 2qwj​, 2qwk​, 3b7e​, 3beq​, 3ckz​, 3cl0​, 3cl2​, 3cye​, 3nn9​, 4nn9​, 5nn9​, 6nn9​, 7nn9
The structure of the influenza virus neuraminidase.[2]
Structure of Influenza, showing neuraminidase marked as NA and hemagglutinin as HA
Influenza virus replication, showing how in step 6 the neuraminidase and hemagglutinin proteins incorporated into the host cell's membrane are used to escape.

Viral neuraminidases are the members of the glycoside hydrolase family 34 CAZY GH_34 which comprises enzymes with only one known activity; sialidase or neuraminidase EC 3.2.1.18. Neuraminidases cleave the terminal sialic acid residues from carbohydrate chains in glycoproteins. Sialic acid is a negatively charged sugar associated with the protein and lipid portions of lipoproteins.[citation needed]

To infect a host cell, the influenza virus attaches to the exterior cell surface using hemagglutinin, a molecule found on the surface of the virus that binds to sialic acid groups. Sialic acids are found on various glycoproteins at the host cell surface. The virus then moves from sialic acid group to sialic acid group until it finds the proper cell surface receptor (whose identity remains unknown).[5] Neuraminadase enables this movement by cleaving sialic acid groups that hemagglutinin was attached to. After the virus has entered the cell and has replicated, new viral particles bud from the host cell membrane. The hemagglutinin on new viral particles remains attached to sialic acid groups of glycoproteins on the external cell surface and the surface of other viral particles; neuraminadase cleaves these groups and thereby allows the release of viral particles[6] and prevents self-aggregation.[5] Neuraminadase also facilitates the movement of virus particles in the presence of mucus rich in silicic acid.[5]

A single hemagglutinin-neuraminidase protein can combine neuraminidase and hemagglutinin functions, such as in mumps virus and human parainfluenza virus.[citation needed]

Function edit

The enzyme helps viruses to be released after budding from the plasma membrane of a host cell. Influenza virus membranes contain two glycoproteins: hemagglutinin and neuraminidase. While the hemagglutinin on the surface of the virion is needed for infection, its presence inhibits release of the particle after budding. Viral neuraminidase cleaves terminal sialic acid residues from glycan structures on the surface of the infected cell. This promotes the release of progeny viruses and the spread of the virus from the host cell to uninfected surrounding cells. Neuraminidase also cleaves sialic acid residues from viral proteins, preventing aggregation of viruses.[medical citation needed]

Inhibitors edit

Main article: Neuraminidase inhibitors

Neuraminidase has been targeted in structure-based enzyme inhibitor design programmes that have resulted in the production of two drugs, zanamivir (Relenza) and oseltamivir (Tamiflu). Administration of neuraminidase inhibitors is a treatment that limits the severity and spread of viral infections. Neuraminidase inhibitors are useful for combating influenza infection: zanamivir, administered by inhalation; oseltamivir, administered orally; and under research is peramivir administered parenterally, that is through intravenous or intramuscular injection.[citation needed]

Neuraminidase inhibition resistance edit

On February 27, 2005, a 14-year-old Vietnamese girl was documented to be carrying an H5N1 influenza virus strain that was resistant to the drug oseltamivir. The drug is used to treat patients that have contracted influenza. However, the Vietnamese girl who had received a prophylactic dose (75 mg once a day) was found to be non-responsive to the medication. In growing fears of a global avian flu pandemic, scientists began to look for a cause of resistance to the Tamiflu medication. The cause was determined to be a histidine-to-tyrosine (amino acid) substitution at position 274 in its neuraminidase protein.[citation needed]

As strains of influenza are continuously mutating, it is essential that scientists quickly and efficiently determine the correct neuraminidase subtype that is responsible for the drug resistance in order to develop medications that will combat specific strains of influenza.[citation needed]

A new class of neuraminidase inhibitors that covalently attach to the enzyme have shown activity against drug-resistant virus in vitro.[7][8]

Specificity edit

In ideal circumstances, influenza virus neuraminidase (NA) should act on the same type of receptor the virus hemagglutinin (HA) binds to, a phenomenon that does not always happen. It is not quite clear how the virus manages to function when there is no close match between the specificities of NA and HA.[citation needed]

Exo- and endo- edit

Neuraminidase enzymes can have endo- or exo-glycosidase activity, and are classified as EC 3.2.1.29 (endo-neuraminidase)[9] and EC 3.2.1.18 (exo-neuraminidases).[10] In general, mammalian sialic acid residues are at terminal positions (non-reducing end) in complex glycans, and so viral neuraminidases - which are exo-glycosidase enzymes - use these terminal residues as their substrates.[citation needed]

See also edit

References edit

  1. ^ Jedrzejas, MJ; Singh, S; Brouillette, WJ; Laver, WG; Air, GM; Luo, M (14 March 1995). "Structures of aromatic inhibitors of influenza virus neuraminidase". Biochemistry. 34 (10): 3144–51. doi:10.1021/bi00010a003. PMID 7880809.
  2. ^ Varghese, J. N.; McKimm-Breschkin, J. L.; Caldwell, J. B.; Kortt, A. A.; Colman, P. M. (1992). "The structure of the complex between influenza virus neuraminidase and sialic acid, the viral receptor". Proteins: Structure, Function, and Genetics. 14 (3): 327–32. doi:10.1002/prot.340140302. PMID 1438172. S2CID 41743465.
  3. ^ "WEHI History: 1957 Discovery of Neuraminidase - Key Flu Molecule". WEHI. Retrieved 2023-11-08.
  4. ^ Couch RB (1999). "Measures for control of influenza". PharmacoEconomics. 16 (Suppl 1): 41–5. doi:10.2165/00019053-199916001-00006. PMID 10623375. S2CID 41844816.
  5. ^ a b c Dou, Dan; Revol, Rebecca; Östbye, Henrik; Wang, Hao; Daniels, Robert (2018-07-20). "Influenza A Virus Cell Entry, Replication, Virion Assembly and Movement". Frontiers in Immunology. 9: 1581. doi:10.3389/fimmu.2018.01581. ISSN 1664-3224. PMC 6062596. PMID 30079062.
  6. ^ Huang IC, Li W, Sui J, Marasco W, Choe H, Farzan M (May 2008). "Influenza A virus neuraminidase limits viral superinfection". J. Virol. 82 (10): 4834–43. doi:10.1128/JVI.00079-08. PMC 2346733. PMID 18321971.
  7. ^ BBC News: Flu drug 'shows promise' in overcoming resistance (accessed 22 February 2013)
  8. ^ Kim J-H et al. Mechanism-based covalent neuraminidase inhibitors with broad spectrum influenza antiviral activity. Science doi:10.1126/science.1232552
  9. ^ "EC 3.2.1.129".
  10. ^ "EC 3.2.1.18".

External links edit

 
Wikimedia Commons has media related to Influenza neuraminidase.
  • Influenza Research Database Database of influenza sequences (including neuraminidase).
  • Proteopedia Influenza Neuraminidase, Tamiflu and Relenza Avian Influenza Neuraminidase, Tamiflu and Relenza

January 01, 1970
viral, neuraminidase, type, neuraminidase, found, surface, influenza, viruses, that, enables, virus, released, from, host, cell, neuraminidases, enzymes, that, cleave, sialic, acid, also, called, neuraminic, acid, groups, from, glycoproteins, discovered, alfre. Viral neuraminidase is a type of neuraminidase found on the surface of influenza viruses that enables the virus to be released from the host cell Neuraminidases are enzymes that cleave sialic acid also called neuraminic acid groups from glycoproteins Viral neuraminidase was discovered by Alfred Gottschalk at the Walter and Eliza Hall Institute in 1957 3 Neuraminidase inhibitors are antiviral agents that inhibit influenza viral neuraminidase activity and are of major importance in the control of influenza 4 NeuraminidaseCrystallographic structure of influenza neuraminidase in complex with the inhibitor 4 acetamido 3 hydroxy 5 nitro benzoic acid 1 IdentifiersSymbolNeurPfamPF00064Pfam clanCL0434InterProIPR001860SCOP22bat SCOPe SUPFAMCAZyGH34CDDcd00260Available protein structures Pfam structures ECOD PDBRCSB PDB PDBe PDBjPDBsumstructure summaryPDB1a14 1a4g 1a4q 1b9s 1b9t 1b9v 1bji 1f8b 1f8c 1f8d 1f8e 1inf 1ing 1inh 1inv 1inw 1inx 1iny 1ivb 1ivc 1ivd 1ive 1ivf 1ivg 1l7f 1l7g 1l7h 1mwe 1nca 1ncb 1ncc 1ncd 1nma 1nmb 1nmc 1nn2 1nna 1nnb 1nnc 1nsb 1nsc 1nsd 1v0z 1vcj 1w1x 1w20 1w21 1xoe 1xog 2aep 2aeq 2b8h 2bat 2c4a 2c4l 2cml 2ht5 2ht7 2ht8 2htq 2htr 2htu 2htv 2htw 2hty 2hu0 2hu4 2qwa 2qwb 2qwc 2qwd 2qwe 2qwf 2qwg 2qwh 2qwi 2qwj 2qwk 3b7e 3beq 3ckz 3cl0 3cl2 3cye 3nn9 4nn9 5nn9 6nn9 7nn9 The structure of the influenza virus neuraminidase 2 Structure of Influenza showing neuraminidase marked as NA and hemagglutinin as HA Influenza virus replication showing how in step 6 the neuraminidase and hemagglutinin proteins incorporated into the host cell s membrane are used to escape Viral neuraminidases are the members of the glycoside hydrolase family 34 CAZY GH 34 which comprises enzymes with only one known activity sialidase or neuraminidase EC 3 2 1 18 Neuraminidases cleave the terminal sialic acid residues from carbohydrate chains in glycoproteins Sialic acid is a negatively charged sugar associated with the protein and lipid portions of lipoproteins citation needed To infect a host cell the influenza virus attaches to the exterior cell surface using hemagglutinin a molecule found on the surface of the virus that binds to sialic acid groups Sialic acids are found on various glycoproteins at the host cell surface The virus then moves from sialic acid group to sialic acid group until it finds the proper cell surface receptor whose identity remains unknown 5 Neuraminadase enables this movement by cleaving sialic acid groups that hemagglutinin was attached to After the virus has entered the cell and has replicated new viral particles bud from the host cell membrane The hemagglutinin on new viral particles remains attached to sialic acid groups of glycoproteins on the external cell surface and the surface of other viral particles neuraminadase cleaves these groups and thereby allows the release of viral particles 6 and prevents self aggregation 5 Neuraminadase also facilitates the movement of virus particles in the presence of mucus rich in silicic acid 5 A single hemagglutinin neuraminidase protein can combine neuraminidase and hemagglutinin functions such as in mumps virus and human parainfluenza virus citation needed Contents 1 Function 2 Inhibitors 2 1 Neuraminidase inhibition resistance 3 Specificity 4 Exo and endo 5 See also 6 References 7 External linksFunction editThe enzyme helps viruses to be released after budding from the plasma membrane of a host cell Influenza virus membranes contain two glycoproteins hemagglutinin and neuraminidase While the hemagglutinin on the surface of the virion is needed for infection its presence inhibits release of the particle after budding Viral neuraminidase cleaves terminal sialic acid residues from glycan structures on the surface of the infected cell This promotes the release of progeny viruses and the spread of the virus from the host cell to uninfected surrounding cells Neuraminidase also cleaves sialic acid residues from viral proteins preventing aggregation of viruses medical citation needed Inhibitors editMain article Neuraminidase inhibitors Neuraminidase has been targeted in structure based enzyme inhibitor design programmes that have resulted in the production of two drugs zanamivir Relenza and oseltamivir Tamiflu Administration of neuraminidase inhibitors is a treatment that limits the severity and spread of viral infections Neuraminidase inhibitors are useful for combating influenza infection zanamivir administered by inhalation oseltamivir administered orally and under research is peramivir administered parenterally that is through intravenous or intramuscular injection citation needed Neuraminidase inhibition resistance edit On February 27 2005 a 14 year old Vietnamese girl was documented to be carrying an H5N1 influenza virus strain that was resistant to the drug oseltamivir The drug is used to treat patients that have contracted influenza However the Vietnamese girl who had received a prophylactic dose 75 mg once a day was found to be non responsive to the medication In growing fears of a global avian flu pandemic scientists began to look for a cause of resistance to the Tamiflu medication The cause was determined to be a histidine to tyrosine amino acid substitution at position 274 in its neuraminidase protein citation needed As strains of influenza are continuously mutating it is essential that scientists quickly and efficiently determine the correct neuraminidase subtype that is responsible for the drug resistance in order to develop medications that will combat specific strains of influenza citation needed A new class of neuraminidase inhibitors that covalently attach to the enzyme have shown activity against drug resistant virus in vitro 7 8 Specificity editIn ideal circumstances influenza virus neuraminidase NA should act on the same type of receptor the virus hemagglutinin HA binds to a phenomenon that does not always happen It is not quite clear how the virus manages to function when there is no close match between the specificities of NA and HA citation needed Exo and endo editNeuraminidase enzymes can have endo or exo glycosidase activity and are classified as EC 3 2 1 29 endo neuraminidase 9 and EC 3 2 1 18 exo neuraminidases 10 In general mammalian sialic acid residues are at terminal positions non reducing end in complex glycans and so viral neuraminidases which are exo glycosidase enzymes use these terminal residues as their substrates citation needed See also editH5N1 genetic structure Antigenic shift Influenza research HemagglutininReferences edit Jedrzejas MJ Singh S Brouillette WJ Laver WG Air GM Luo M 14 March 1995 Structures of aromatic inhibitors of influenza virus neuraminidase Biochemistry 34 10 3144 51 doi 10 1021 bi00010a003 PMID 7880809 Varghese J N McKimm Breschkin J L Caldwell J B Kortt A A Colman P M 1992 The structure of the complex between influenza virus neuraminidase and sialic acid the viral receptor Proteins Structure Function and Genetics 14 3 327 32 doi 10 1002 prot 340140302 PMID 1438172 S2CID 41743465 WEHI History 1957 Discovery of Neuraminidase Key Flu Molecule WEHI Retrieved 2023 11 08 Couch RB 1999 Measures for control of influenza PharmacoEconomics 16 Suppl 1 41 5 doi 10 2165 00019053 199916001 00006 PMID 10623375 S2CID 41844816 a b c Dou Dan Revol Rebecca Ostbye Henrik Wang Hao Daniels Robert 2018 07 20 Influenza A Virus Cell Entry Replication Virion Assembly and Movement Frontiers in Immunology 9 1581 doi 10 3389 fimmu 2018 01581 ISSN 1664 3224 PMC 6062596 PMID 30079062 Huang IC Li W Sui J Marasco W Choe H Farzan M May 2008 Influenza A virus neuraminidase limits viral superinfection J Virol 82 10 4834 43 doi 10 1128 JVI 00079 08 PMC 2346733 PMID 18321971 BBC News Flu drug shows promise in overcoming resistance accessed 22 February 2013 Kim J H et al Mechanism based covalent neuraminidase inhibitors with broad spectrum influenza antiviral activity Science doi 10 1126 science 1232552 EC 3 2 1 129 EC 3 2 1 18 External links edit nbsp Wikimedia Commons has media related to Influenza neuraminidase Influenza Research Database Database of influenza sequences including neuraminidase Proteopedia Influenza Neuraminidase Tamiflu and Relenza Avian Influenza Neuraminidase Tamiflu and Relenza Portal nbsp Biology Retrieved from https en wikipedia org w index php title Viral neuraminidase amp oldid 1200818865, wikipedia, wiki, book, books, library,

article

, read, download, free, free download, mp3, video, mp4, 3gp, jpg, jpeg, gif, png, picture, music, song, movie, book, game, games.