- Adenoviridae
Taxobox | color=violet
name = Adenoviruses
image_caption = Transmission electron micrograph of two adenovirus particles
virus_group = i
familia = "Adenoviridae"
subdivision_ranks = Genera
subdivision = "Aviadenovirus "
"Atadenovirus "
"Mastadenovirus "
"Siadenovirus "Adenoviruses are medium-sized (90–100 nm),
nonenveloped (naked)icosahedral viruses composed of a nucleocapsid and a double-stranded linearDNA genome. There are over 52 differentserotype s in humans, which are responsible for 5–10% of upper respiratory infections in children, and many infections in adults as well.Virus es of the family "Adenoviridae" infect various species of animals, including humans. Adenoviruses were first isolated in humanadenoid s (tonsils), from which the name is derived, and are classified as group I under theBaltimore classification scheme. Adenoviruses represent the largest nonenveloped viruses, because they are the maximum size able to be transported through the endosome (i.e. envelope fusion is not necessary). The virion also has a unique "spike" orfiber associated with each penton base of thecapsid (see picture below) that aids in attachment to the host cell via the coxsackie-adenovirus receptor on the surface of the host cell. There are 51 immunologically distinct human adenovirus serotypes (6 species: "Human adenovirus A" through "F") that can cause human infections ranging fromrespiratory disease (mainly species HAdV-B and C), and conjunctivitis (HAdV-B and D), to gastroenteritis (HAdV-F serotypes 40 and 41). Adenoviruses are unusually stable tochemical or physical agents and adversepH conditions, allowing for prolonged survival outside of the body and water. Adenoviruses are primarily spread via respiratory droplets, however they can also be spread byfecal routes as well.Most infections with adenovirus result in infections of the upper respiratory tract. Adenovirus infections often show up as
conjunctivitis ,tonsilitis (which may look exactly likestrep throat and cannot be distinguished from strep except by throat culture), an ear infection, orcroup . Adenoviruses can also causegastroenteritis (stomach flu). A combination of conjunctivitis and tonsilitis is particularly common with adenovirus infections. Some children (especially small ones) can develop adenovirusbronchiolitis orpneumonia , both of which can be severe. In babies, adenoviruses can also cause coughing fits that look almost exactly likewhooping cough . Adenoviruses can also causeviral meningitis orencephalitis . Rarely, adenovirus can causecystitis (inflammation of the urinary bladder—a form ofurinary tract infection —with blood in the urine).Most people recover from adenovirus infections by themselves, but people with
immunodeficiency sometimes die of adenovirus infections, and—rarely—even previously healthy people can die of these infections. [cite news | url = http://www.cnn.com/2007/HEALTH/conditions/12/19/killer.cold/index.html | title = A killer cold? Even the healthy may be vulnerable | work =CNN | author = Amy Burkholder | date =2007-12-19 | accessdate = 2007-12-19 ]Adenoviruses are often transmitted by coughed-out droplets, but can also be transmitted by contact with an infected person, or by virus particles left on objects such as towels and faucet handles. Some people with adenovirus gastroenteritis may shed the virus in their stools for months after getting over the symptoms. The virus can be passed from one person to another through some sexual practices, and through water in swimming pools that do not have enough chlorine in them. As with many other illnesses, good handwashing is one way to lessen the spread of adenoviruses from one person to another. Heat and
bleach will kill adenoviruses on objects.Treatment and prevention
There are no antiviral drugs to treat adenoviral infections, so treatment is largely directed at the symptoms (such as acetaminophen for fever). A doctor may give antibiotic eyedrops for conjunctivitis, since it takes a while to test to see if the eye infection is bacterial or viral and to help prevent secondary bacterial infections.
In the past, US military recruits were vaccinated against two serotypes of adenotypes, with a corresponding decrease in illnesses caused by those serotypes. The vaccine is no longer manufactured, and there are currently no vaccines available to protect against the adenovirus. Good hygiene, including handwashing, is still the best way to avoid picking up the adenovirus from an infected person.
Genome
The adenovirus genome is linear, non-segmented double stranded (ds) DNA which is around 30–38 Kbp. This allows the virus to theoretically carry 30 to 40
genes . Although this is significantly larger than other viruses in its Baltimore group it is still a very simple virus and is heavily reliant on the host cell for survival and replication. An interesting feature of this viral genome is that it has a terminal 55 kDa protein associated with each of the 5' ends of the linear dsDNA, these are used as primers in viral replication and ensure that the ends of the virus' linear genome are adequately replicated.Replication
Adenoviruses possess a linear dsDNA
genome and are able to replicate in the nucleus ofmammal ian cells using the host’s replication machinery.
thumb|250px|right|The structure of adenovirus. 1 = penton capsomeres 2 = hexon capsomeres, and 3= viral genome (linear dsDNA) Entry of adenoviruses into the host cell involves two sets of interactions between the virus and the host cell. Entry into the host cell is initiated by the knob domain of the fiber protein binding to the cell receptor. The two currently established receptors are: CD46 for the group B human adenovirus serotypes and the coxsackievirus adenovirus receptor (CAR) for all other serotypes. There are some reports suggesting MHC molecules and sialic acid residues functioning in this capacity as well. This is followed by a secondary interaction, where a specialized motif in the penton base protein interacts with anintegrin molecule. It is the co-receptor interaction that stimulates internalization of the adenovirus. This co-receptor molecule is αv integrin. Binding to αv integrin results inendocytosis of the virus particle via clathrin-coated pits. Attachment to αv integrin stimulates cell signaling and thus induces actin polymerization resulting in entry of the virion into the host cell within anendosome .cite journal
author=Wu and Nemerow | title=Virus yoga: the role of flexibility in virus host cell recognition | journal=Trends Microbiol
year=2004
pages=162–168
volume=12
issue=
pmid=15051066
format=
doi=10.1016/j.tim.2004.02.005]Once the virus has successfully gained entry into the host cell the endosome acidifies, which alters virus topology by causing capsid components to disassociate. These changes as well as the toxic nature of the pentons results in the release of the virion into the cytoplasm. With the help of cellular
microtubules the virus is transported to the nuclear pore complex whereby the adenovirus particle disassembles. Viral DNA is subsequently released which can enter the nucleus via thenuclear pore .cite journal
author=Meier and Greber | title=Adenovirus endocytosis | journal=J Gene Med
year=2004
pages=S152–S163
volume=6
issue=
pmid=14978758
format=
doi=10.1002/jgm.553] After this the DNA associates withhistone molecules. Thus viral gene expression can occur and new virus particles can be generated.The adenovirus life cycle is separated, by the
DNA replication process, into two phases: an early and a late phase. In both phases aprimary transcript is generated which is alternatively spliced to generatemonocistronic mRNA s compatible with the host’sribosome , allowing for the products to be translated.The early genes are responsible for expressing mainly non-structural, regulatory
proteins . The goal of these proteins is threefold: to alter the expression of host proteins that are necessary for DNAsynthesis ; to activate other virus genes (such as the virus-encodedDNA polymerase ); and to avoid premature death of the infected cell by the host-immune defenses (blockage ofapoptosis , blockage ofinterferon activity, and blockage ofMHC class I translocation and expression).Some adenoviruses under specialized conditions can transform cells using their early gene products. E1a (binds Retinoblastoma tumor suppressor protein) has been found to immortalize primary cells "in vitro" allowing E1b (binds
p53 tumor suppressor) to assist and stably transform the cells. Nevertheless, they are reliant upon each other to successfully transform the host cell and formtumors .DNA replication separates the early and late phases. Once the early genes have liberated adequate virus proteins, replication machinery and replication substrates, replication of the adenovirus genome can occur. A terminal protein that is covalently bound to the 5’ end of the adenovirus genome acts as a primer for replication. The viral DNA polymerase then uses a strand displacement mechanism, as opposed to the conventional
Okazaki fragments used in mammalian DNA replication, to replicate the genome.The late phase of the adenovirus life cycle is focused on producing sufficient quantities of structural protein to pack all the genetic material produced by DNA replication. Once the viral components have successfully been replicated the virus is assembled into its protein shells and released from the cell as a result of virally induced cell
lysis .Genera
This family contains the following genera:
*Genus "Aviadenovirus "; type species: "Fowl adenovirus A "
*Genus "Atadenovirus "; type species: "Ovine adenovirus D "
*Genus "Mastadenovirus "; type species: "Human adenovirus C "; others includeAD-36
*Genus "Siadenovirus "; type species: "Frog adenovirus "Adenoviruses in humans
* See
Adenovirus infection
* SeeAdenovirus serotype 14 Adenoviruses in animals
Two types of canine adenoviruses are well known, type 1 and 2. Type 1 causes
infectious canine hepatitis , a potentially fatal disease involvingvasculitis andhepatitis . Type 1 infection also can cause respiratory and eye infections. "Canine adenovirus 2" (CAdV-2) is one of the potential causes ofkennel cough . Corevaccine s fordog s include attenuated live CAdV-2, which produces immunity to CAdV-1 and CAdV-2. CAdV-1 was initially used in a vaccine for dogs, butcornea ledema was a common complication.cite book|author=Fenner, Frank J.; Gibbs, E. Paul J.; Murphy, Frederick A.; Rott, Rudolph; Studdert, Michael J.; White, David O.|title=Veterinary Virology (2nd ed.)|publisher=Academic Press, Inc|year=1993|id=ISBN 0-12-253056-X]Adenoviruses are also known to cause respiratory infections in
horse s,cattle ,pig s,sheep , andgoat s. "Equine adenovirus 1" can also cause fatal disease in immunocompromised Arabian foals, involving pneumonia and destruction of pancreatic andsalivary gland tissue.cite book|author=Fenner, Frank J.; Gibbs, E. Paul J.; Murphy, Frederick A.; Rott, Rudolph; Studdert, Michael J.; White, David O.|title=Veterinary Virology (2nd ed.)|publisher=Academic Press, Inc|year=1993|id=ISBN 0-12-253056-X]ee also
*
Infectious canine hepatitis References
ources
[http://www.cdc.gov/ncidod/dvrd/revb/respiratory/eadfeat.htm Centers for Disease Control and Prevention--National Center for Diseases--Division of Viral and Rickettsial Diseases] , Respiratory and Enteric Viruses Branch
External links
* [http://www.microbiologybytes.com/virology/Adenoviruses.html MicrobiologyBytes: Adenoviruses]
* [http://gsbs.utmb.edu/microbook/ch067.htm Adenoviruses General Concepts]
* [http://pathmicro.med.sc.edu/mhunt/dna1.htm DNA virus replication strategies]
* [http://www.vmri.hu/~harrach/ADENOSEQ.HTM Sequenced adenoviruses]
* [http://www.genetherapynet.com Gene Therapy Net - Adenoviral vectors used in gene therapy]
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