Mastadenovirus

Mastadenovirus is a genus of viruses, in the family Adenoviridae. Human and other mammals serve as natural hosts. There are currently 50 species in this genus, including the type species human mastadenovirus C. The genus as a whole includes many very common causes of human infection, estimated to be responsible for 2-5% of all respiratory infections, as well as gastrointestinal and eye infections. Symptoms are usually mild.

Mastadenovirus
Virus classification
(unranked): Virus
Realm: Varidnaviria
Kingdom: Bamfordvirae
Phylum: Preplasmiviricota
Class: Tectiliviricetes
Order: Rowavirales
Family: Adenoviridae
Genus: Mastadenovirus
Type species
Human Mastadenovirus C
Species

see text

Specific tropisms include: serotypes 3, 5 and 7: lower respiratory tract infections, serotypes 8, 19, and 37: epidemic keratoconjunctivitis, serotypes 4 and 7: acute respiratory disease, serotypes 40 and 41: gastroenteritis, serotype 14: can cause potentially fatal adenovirus infections.

Canine adenovirus 1 (CAdV-1) can lead to death in puppies, or encephalitis in other carnivore species.[1][2][3]

Etymology

The name mastadenovirus is derived from the Greek word mastos for breast (hence mammal) and adenovirus named for the human adenoids from which the virus was first isolated.[4][5]

Taxonomy

The following species are recognized:

  • Bat mastadenovirus A
  • Bat mastadenovirus B
  • Bat mastadenovirus C
  • Bat mastadenovirus D
  • Bat mastadenovirus E
  • Bat mastadenovirus F
  • Bat mastadenovirus G
  • Bat mastadenovirus H
  • Bat mastadenovirus I
  • Bat mastadenovirus J
  • Bovine mastadenovirus A
  • Bovine mastadenovirus B
  • Bovine mastadenovirus C
  • Canine mastadenovirus A
  • Deer mastadenovirus B
  • Dolphin mastadenovirus A
  • Dolphin mastadenovirus B
  • Equine mastadenovirus A
  • Equine mastadenovirus B
  • Human mastadenovirus A
  • Human mastadenovirus B
  • Human mastadenovirus C, the type species
  • Human mastadenovirus D
  • Human mastadenovirus E
  • Human mastadenovirus F
  • Human mastadenovirus G
  • Murine mastadenovirus A
  • Murine mastadenovirus B
  • Murine mastadenovirus C
  • Ovine mastadenovirus A
  • Ovine mastadenovirus B
  • Ovine mastadenovirus C
  • Platyrrhini mastadenovirus A
  • Polar bear mastadenovirus A
  • Porcine mastadenovirus A
  • Porcine mastadenovirus B
  • Porcine mastadenovirus C
  • Sea lion mastadenovirus A
  • Simian mastadenovirus A
  • Simian mastadenovirus B
  • Simian mastadenovirus C
  • Simian mastadenovirus D
  • Simian mastadenovirus E
  • Simian mastadenovirus F
  • Simian mastadenovirus G
  • Simian mastadenovirus H
  • Simian mastadenovirus I
  • Skunk mastadenovirus A
  • Squirrel mastadenovirus A
  • Tree shrew mastadenovirus A

Human serotypes

Structure

Viruses in mastadenovirus are non-enveloped, with icosahedral geometries, and T=25 symmetry. The diameter is around 90 nm. Genomes are linear and non-segmented, around 35-36kb in length. The genome codes for 40 proteins.[1][6]

GenusStructureSymmetryCapsidGenomic arrangementGenomic segmentation
MastadenovirusPolyhedralPseudo T=59Non-envelopedLinearMonopartite

Life cycle

Viral replication is nuclear. Entry into the host cell is achieved by attachment of the viral fibers to the host CAR adhesion receptor. Subsequent binding of the penton protein to host integrin entry receptors mediates internalization into the host cell by clathrin-mediated endocytosis of the virus and fiber shedding. Some serotypes also seem to use macropinocytosis. Disruption of host endosomal membrane by lytic protein VI releases the viral capsid in the cytosol. Microtubular transport toward nucleus of the viral genome still protected by the core protein VII and a partial capsid mainly composed of hexons and protein IX. Docking at the NPC and capsid disruption. Import of the viral genome into host nucleus mediated by core protein VII. Transcription of early genes (E genes) by host RNA pol II: these proteins optimize the cellular milieu for viral replication, and counteract a variety of antiviral defenses. Intermediate genes activate replication of the DNA genome by DNA strand displacement in the nucleus. Expression of L4-22K and L4-33K causes early to late switch. Transcription of late genes (L genes) by host RNA pol II, mostly encoding structural proteins. Host translation shutoff performed by the viral 100K protein. Assembly of new virions in the nucleus. Virions are released by lysis of the cell. Virion maturation by the viral proteasehost receptors, which mediates clathrin-mediated endocytosis. Replication follows the DNA strand displacement model. DNA templated transcription, with some alternative splicing mechanism is the method of transcription. Translation takes place by ribosomal shunting. The virus exits the host cell by nuclear envelope breakdown, viroporins, and lysis. Human, mammals, and vertebrates serve as the natural host. Transmission routes are fecal-oral and respiratory. [1]

GenusHost detailsTissue tropismEntry detailsRelease detailsReplication siteAssembly siteTransmission
MastadenovirusHumans; mammalsNoneGlycoprotiensLysisNucleusNucleusUnknown

References

  1. "Viral Zone". ExPASy. Retrieved 1 July 2015.
  2. ICTV. "Virus Taxonomy: 2014 Release". Retrieved 1 July 2015.
  3. taxonomy. "Taxonomy browser (Mastadenovirus)". Ncbi.nlm.nih.gov. Retrieved 16 January 2014.
  4. Rowe, W. P.; Huebner, R. J.; Gilmore, L. K.; Parrott, R. H.; Ward, T. G. (December 1953). "Isolation of a cytopathogenic agent from human adenoids undergoing spontaneous degeneration in tissue culture". Proceedings of the Society for Experimental Biology and Medicine (New York, N.Y.). 84 (3): 570–573. doi:10.3181/00379727-84-20714. ISSN 0037-9727. PMID 13134217. S2CID 3097955.
  5. Pereira, H. G. (September 1959). "Adenoviruses". British Medical Bulletin. 15 (3): 225–230. doi:10.1093/oxfordjournals.bmb.a069769. ISSN 0007-1420. PMID 14431746.
  6. Rivailler, Pierre; Mao, Naiying; Zhu, Zhen; Xu, Wenbo (18 February 2019). "Recombination analysis of Human mastadenovirus C whole genomes". Scientific Reports. 9 (1): 2182. Bibcode:2019NatSR...9.2182R. doi:10.1038/s41598-019-38719-z. ISSN 2045-2322. PMID 30778154.
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