Nipah virus: Difference between revisions
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| title = Fact sheet N°262: Nipah virus | | title = Fact sheet N°262: Nipah virus | ||
| date = September 2001 | | date = September 2001 | ||
|url = http://www.who.int/mediacentre/factsheets/fs262/en/}}</ref> it is an [[overlap agent]] under the [[Select Agent Program]] due to high lethality and a wide range of susceptible hosts. | |url = http://www.who.int/mediacentre/factsheets/fs262/en/}}</ref> it is an [[overlap agent]] under the [[Select Agent Program]] due to high lethality and a wide range of susceptible hosts. It is in [[CDC Bioterrorism Agents-Disease list]] category C. | ||
Several zoonotic and vectorborne viral diseases have emerged, since the mid-1990s, in Southeast Asia and the Western Pacific, among them Nipah virus, which caused an outbreak of fatal pneumonia in pigs and encephalitis in humans in the Malay Peninsula.<ref name=Mackenzie2001>{{citation | Several zoonotic and vectorborne viral diseases have emerged, since the mid-1990s, in Southeast Asia and the Western Pacific, among them Nipah virus, which caused an outbreak of fatal pneumonia in pigs and encephalitis in humans in the Malay Peninsula.<ref name=Mackenzie2001>{{citation | ||
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The mode of transmission from animal to animal, and from animal to human is uncertain, but appears to require close contact with contaminated tissue or body fluids from infected animals. Nipah antibodies have been detected in pigs, other domestic and wild animals. The role of species other than pigs in transmitting infection to other animals has not yet been determined. | The mode of transmission from animal to animal, and from animal to human is uncertain, but appears to require close contact with contaminated tissue or body fluids from infected animals. Nipah antibodies have been detected in pigs, other domestic and wild animals. The role of species other than pigs in transmitting infection to other animals has not yet been determined. | ||
==Taxonomy and genetics== | ==Taxonomy and genetics== | ||
Hendra and [[Nipah virus]]es have been placed into a new genus of the family ''[[Paramyxoviridae]]'', ''Henipavirus.''<ref name=Wang2000>{{citation | |||
| journal = Journal of Virology | |||
| date = November 2000 | |||
|pages = 9972-9979 | |||
| volume = 74 | |||
|issue = 21 | |||
| title = The Exceptionally Large Genome of Hendra Virus: Support for Creation of a New Genus within the Family ''Paramyxoviridae'' | |||
| author = Wang LF ''et al.'' | |||
| url = http://jvi.asm.org/cgi/content/full/74/21/9972}}</ref> | |||
<ref name=CIDRAPnipah>{{citation | They are single-stranded RNA viruses, approximately 15000 nucleotides long. <ref name=CIDRAPnipah>{{citation | ||
| title = Nipah virus | | title = Nipah virus | ||
| date = 2007 | | date = 2007 | ||
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(see References: Bossart 2002, Mackenzie 2001) | (see References: Bossart 2002, Mackenzie 2001) | ||
==Morphology= | ==Laboratory presentation== | ||
===Morphology=== | |||
* Helical | * Helical | ||
* Enveloped with distinct surface projections | * Enveloped with distinct surface projections | ||
* 150 to 200 nm in diameter; 10,000 to 10,040 nm long | * 150 to 200 nm in diameter; 10,000 to 10,040 nm long | ||
* Spherical or filamentous, but pleomorphic forms occur | * Spherical or filamentous, but pleomorphic forms occur | ||
===Metabolic=== | |||
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The incubation period is between 4 and 18 days. In many cases the infection is mild or inapparent (sub-clinical). In symptomatic cases, the onset is usually with "influenza-like" symptoms, with high fever and muscle pains (myalgia). The disease may progress to inflammation of the brain (encephalitis) with drowsiness, disorientation, convulsions and coma. Fifty percent of clinically apparent cases die. | The incubation period is between 4 and 18 days. In many cases the infection is mild or inapparent (sub-clinical). In symptomatic cases, the onset is usually with "influenza-like" symptoms, with high fever and muscle pains (myalgia). The disease may progress to inflammation of the brain (encephalitis) with drowsiness, disorientation, convulsions and coma. Fifty percent of clinically apparent cases die. | ||
==References== | ==References== | ||
{{reflist}} | {{reflist}}[[Category:Suggestion Bot Tag]] |
Latest revision as of 06:01, 26 September 2024
Nipah virus, first identified in Malaysia in 1999, is a zoonotic virus that can cause disease in humans and animals;[1] it is an overlap agent under the Select Agent Program due to high lethality and a wide range of susceptible hosts. It is in CDC Bioterrorism Agents-Disease list category C.
Several zoonotic and vectorborne viral diseases have emerged, since the mid-1990s, in Southeast Asia and the Western Pacific, among them Nipah virus, which caused an outbreak of fatal pneumonia in pigs and encephalitis in humans in the Malay Peninsula.[2]
Ecology
The virus is named after the location where it was first detected in Malaysia.
Reservoir
It is currently believed that certain species of fruit bats are the natural hosts of both Nipah and Hendra viruses. They are distributed across an area encompassing northern, eastern and south-eastern areas of Australia, Indonesia, Malaysia, the Philippines and some of the Pacific Islands. The bats appear to be susceptible to infection with these viruses, but do not themselves become ill. It is not known how the virus is transmitted from bats to animals.
Transmission
The mode of transmission from animal to animal, and from animal to human is uncertain, but appears to require close contact with contaminated tissue or body fluids from infected animals. Nipah antibodies have been detected in pigs, other domestic and wild animals. The role of species other than pigs in transmitting infection to other animals has not yet been determined.
Taxonomy and genetics
Hendra and Nipah viruses have been placed into a new genus of the family Paramyxoviridae, Henipavirus.[3]
They are single-stranded RNA viruses, approximately 15000 nucleotides long. [4]
Formerly in the genus Morbillivirus, now classified in a new genus along with the similar Hendra virus (70% to 88% nucleotide homology, 67% to 92% amino acid homology): Henipavirus [5] (see References: Bossart 2002, Mackenzie 2001)
Laboratory presentation
Morphology
- Helical
- Enveloped with distinct surface projections
- 150 to 200 nm in diameter; 10,000 to 10,040 nm long
- Spherical or filamentous, but pleomorphic forms occur
Metabolic
Clinical features
It is unlikely that Nipah virus is easily transmitted to man, although previous outbreak reports suggest that Nipah virus is transmitted from animals to humans more readily than Hendra virus. Despite frequent contact between fruit bats and humans there is no serological evidence of human infection among bat carers. Pigs were the apparent source of infection among most human cases in the Malaysian outbreak of Nipah, but other sources, such as infected dogs and cats, cannot be excluded. Human-to-human transmission of Nipah virus has not been reported.
The incubation period is between 4 and 18 days. In many cases the infection is mild or inapparent (sub-clinical). In symptomatic cases, the onset is usually with "influenza-like" symptoms, with high fever and muscle pains (myalgia). The disease may progress to inflammation of the brain (encephalitis) with drowsiness, disorientation, convulsions and coma. Fifty percent of clinically apparent cases die.
References
- ↑ World Health Organization (September 2001), Fact sheet N°262: Nipah virus
- ↑ Mackenzie JS, Chua KB, Ua PW, et al. (2001 Jun), "Emerging viral diseases of Southeast Asia and the Western Pacific", Emerg Infect Dis 7(3 Suppl): 497-505
- ↑ Wang LF et al. (November 2000), "The Exceptionally Large Genome of Hendra Virus: Support for Creation of a New Genus within the Family Paramyxoviridae", Journal of Virology 74 (21): 9972-9979
- ↑ Center for Infectious Disease Research and Policy (2007), Nipah virus, University of Minnesota
- ↑ Bossart KN et al. (November 2002), "Membrane Fusion Tropism and Heterotypic Functional Activities of the Nipah Virus and Hendra Virus Envelope Glycoproteins", Journal of Virology 76: 11186-11198, DOI:10.1128/JVI.76.22.11186-11198.2002