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style="background:#Template:Taxobox colour;"\|Lassa Virus (LASV)
	; TEM micrograph of Lassa virus virions.
style="background:#Template:Taxobox colour;" \| Virus classification
Group:	Group V ((-)ssRNA)
Order:	Unassigned;
Family:	Arenaviridae;
Genus:	Arenavirus;
Species:	Lassa virus;

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Revision as of 12:22, 8 June 2015

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [5]; Associate Editor(s)-in-Chief: Ammu Susheela, M.D. [6]

Synonyms and keywords: Lassa hemorrhagic fever; LHF

Overview

Lassa fever is caused by the Lassa virus, a member of the Arenaviridae family. It is an enveloped, single-stranded, bisegmented RNA virus. Mastomysrodents shed the virus in urine and droppings. The direct contact with these materials or ingestion or inhalation, can lead to infection. Lassa virus enters the cell by the receptor-mediated endocytosis and undergoes very rapid replication and manifest the disease.

Virus

Taxonomy

Viruses; ssRNA viruses; ssRNA negative-strand viruses; Arenaviridae; Mammarenavirus ^[1]

Biology

Lassa virus belongs to Arenaviridae ^[2].
The Arenaviridae are a family of viruses whose members are generally associated with rodent-transmitted diseases in humans. Each virus usually is associated with a particular rodent host species in which it is maintained. Arenavirus infections are relatively common in humans in some areas of the world and can cause severe illnesses.

Structure and genome

Lassa viruses are enveloped, single-stranded, bisegmented, ambisense RNA viruses. Their genome^[3] is contained in two RNA segments that code for two proteins each, one in each sense, for a total of four viral proteins.^[4] The large segment encodes a small zinc-binding protein (Z) that regulates transcription and replication,^[5]^[6] and the RNA polymerase (L). The small segment encodes the nucleoprotein (NP) and the surface glycoprotein precursor (GP, also known as the viral spike), which is proteolytically cleaved into the envelope glycoproteins GP1 and GP2 that bind to the alpha-dystroglycan receptor and mediate host cell entry.^[7]

Outbreak Distribution Map Lassa Fever CDC.png[1]^[8]

Lassa fever causes hemorrhagic fever frequently shown by immunosuppression. Replication for Lassa virus is very rapid, while also demonstrating temporal control in replication.^[9] The first replication step is transcription of mRNA copies of the negative- or minus-sense genome. This ensures an adequate supply of viral proteins for subsequent steps of replication, as the NP and L proteins are translated from the mRNA. The positive- or plus-sense genome, then makes viral complementary RNA (vcRNA)copies of itself. The RNA copies are a template for producing negative-sense progeny, but mRNA is also synthesized from it. The mRNA synthesized from vcRNA are translated to make the GP and Z proteins. This temporal control allows the spike proteins to be produced last, and therefore, delay recognition by the host immune system.
Nucleotide studies of the genome have shown that Lassa has four lineages: three found in Nigeria and the fourth in Guinea, Liberia, and Sierra Leone. The Nigerian strains seem likely to have been ancestral to the others but additional work is required to confirm this.^[10] One book that explains about this disease is The Lassa Ward by Ross I. Donaldson. He describes what it is like being a doctor and taking care of the Sierra Leone people who have contracted the virus.

Receptors

The Lassa virus gains entry into the host cell by means of the cell-surface receptor the alpha-dystroglycan (alpha-DG),^[10] a versatile receptor for proteins of the extracellular matrix. It shares this receptor with the prototypic Old World arenavirus lymphocytic choriomeningitis virus. Receptor recognition depends on a specific sugar modification of alpha-dystroglycan by a group of glycosyltransferases known as the LARGE proteins. Specific variants of the genes encoding these proteins appear to be under positive selection inWest Africa where Lassa is endemic. Alpha-dystroglycan is also used as a receptor by viruses of the New World clade C arenaviruses (Oliveros and Latino viruses). In contrast, the New World arenaviruses of clades A and B, which include the important viruses Machupo, Guanarito, Junin, and Sabia in addition to the non pathogenic Amapari virus, use the transferrin receptor 1. A small aliphatic amino acid at the GP1 glycoprotein amino acid position 260 is required for high-affinity binding to alpha-DG. In addition, GP1 amino acid position 259 also appears to be important, since all arenaviruses showing high-affinity alpha-DG binding possess a bulky aromatic amino acid (tyrosine or phenylalanine) at this position.
Unlike most enveloped viruses which use clathrin coated pits for cellular entry and bind to their receptors in a pH dependent fashion, Lassa and lymphocytic choriomeningitis virus instead use an endocytotic pathway independent of clathrin, caveolin, dynamin and actin. Once within the cell the viruses are rapidly delivered to endosomes via vesicular trafficking albeit one that is largely independent of the small GTPases Rab5 and Rab7. On contact with the endosome pH-dependent membrane fusion occurs mediated by the envelope glycoprotein, which at the lower pH of the endosome binds the lysosome protein LAMP1 which results in membrane fusion and escape from the endosome.

Life cycle

The life cycle of Lassa virus is similar to the Old World arenaviruses^[11]. Lassa virus enters the cell by the receptor-mediated endocytosis. Which endocytotic pathway is used is not known yet, but at least the cellular entry is sensitive to cholesterol depletion. It was reported that virus internalization is limited upon cholesterol depletion. The receptor used for cell entry is alpha-dystroglycan, a highly conserved and ubiquitously expressed cell surface receptor for extracellular matrix proteins.
Dystroglycan, which is later cleaved into alpha-dystroglycan and beta-dystroglycan is originally expressed in most cells to mature tissues, and it provides molecular link between the ECM and the actin-based cytoskeleton^[12]. After virus enters the cell by alpha-dystroglycan mediated endocytosis, low-pH environment triggers pH-dependent membrane fusion and releases RNP (viral ribonucleoprotein) complex into the cytoplasm.
Viral RNA is unpacked, and replication and transcription initiate in the cytoplasm.^[12] As the replication starts, both S and L RNA genomes synthesize the antigenomic S and L RNAs, and from the antigenomic RNAs, genomic S and L RNA are synthesized. Both genomic and antigenomic RNAs are needed for transcription and translation. S RNA encodes GP and NP (viral nucleocapsid protein) proteins, and L RNA encodes Z and L proteins. L protein most likely represents the viral RNA-dependent RNA polymerase.^[13].
When the cell is infected by the virus, L polymerase is associated with the viral RNP and initiates the transcription of the genomic RNA. The 5’ and 3’ terminal 19 nt viral promoter regions of both RNA segments are necessary for recognition and binding of the viral polymerase. The primary transcription first transcribes mRNAs from the genomic S and L RNAs, which code NP and L proteins, respectively. Transcription terminates at the stem-loop (SL) structure within the intergenomic region. Arenaviruses use a cap snatching strategy to gain the cap structures from the cellular mRNAs, and it is mediated by the endonuclease activity of the L polymerase and the cap binding activity of NP. Antigenomic RNA transcribes viral genes GPC and Z, encoded in genomic orientation, from S and L segments respectively. The antigenomic RNA also serves as the template for the replication.^[14] After translation of GPC, it is posttranslationally modified in the endoplasmic reticulum.
GPC is cleaved into GP1 and GP2 at the later stage of the secretory pathway. It is reported the cellular protease SKI-1/S1P was responsible for the cleavage. Cleaved glycoproteins are incorporated into the virion envelope when the virus buds and release from the cell membrane.^[13]

Natural Reservoir

The reservoir, or host, of Lassa virus is a rodent known as the "multimammate rat" (Mastomys natalensis). Once infected, this rodent is able to excrete virus in urine for an extended time period, maybe for the rest of its life. Mastomys rodents breed frequently, produce large numbers of offspring, and are numerous in the savannas and forests of west, central, and east Africa. In addition, Mastomys readily colonize human homes and areas where food is stored. All of these factors contribute to the relatively efficient spread of Lassa virus from infected rodents to humans.

Mastomys natalensis or the natal multimammate mouse.[3]^[15]

Mastomys natalensis is commonly known as the “multimammate rat” due to the female’s multiple and prominent mammary glands.[4]^[15]

Mastomysrodents shed the virus in urine and droppings and direct contact with these materials, through touching soiled objects, eating contaminated food, or exposure to open cuts or sores, can lead to infection. Because Mastomys rodents often live in and around homes and scavenge on leftover human food items or poorly stored food, direct contact transmission is common. Mastomys rodents are sometimes consumed as a food source and infection may occur when rodents are caught and prepared. Contact with the virus may also occur when a person inhales tiny particles in the air contaminated with infected rodent excretions.

Gallery

The images below display key features of the Lassa virus.

This transmission electron micrograph (TEM) depicted numbers of Lassa virus virions adjacent to some cell debris. Source: CDC microbiologist C. S. Goldsmith, P. Rollin, M. Bowen.Adapted from Public Health Image Library (PHIL), Centers for Disease Control and Prevention.^[16]
This highly magnified transmission electron micrograph (TEM) depicted some of the ultrastructural details of three Lassa virus virions.Adapted from Public Health Image Library (PHIL), Centers for Disease Control and Prevention.^[16]
This transmission electron micrograph depicted eight virions (viral particles) of a newly-discovered virus, which was determined to be a member of the genus, Arenavirus. A cause of fatal hemorrhagic fever, it was confirmed that this virus was responsible for causing illness in five South Africans, four of whom died having succumbed to its devastating effects. Source: CDC microbiologist Charles HumphreyAdapted from Public Health Image Library (PHIL), Centers for Disease Control and Prevention.^[16]

References

↑ "Taxonomy browser (Lassavirus)".
↑ "The Centers for Disease Control and Prevention".
↑ "Genome:The autobiography of a species in 23 chapters". Nat Genet. 24 (1): 21. 2000. doi:10.1038/71638. PMID 10615121.
↑ Moshkoff DA, Salvato MS, Lukashevich IS (2007). "Molecular characterization of a reassortant virus derived from Lassa and Mopeia viruses". Virus Genes. 34 (2): 169–76. doi:10.1007/s11262-006-0050-3. PMC 1892610. PMID 17143722.
↑ Cornu TI, de la Torre JC (2001). "RING finger Z protein of lymphocytic choriomeningitis virus (LCMV) inhibits transcription and RNA replication of an LCMV S-segment minigenome". J Virol. 75 (19): 9415–26. doi:10.1128/JVI.75.19.9415-9426.2001. PMC 114509. PMID 11533204.CS1 maint: PMC format (link)
↑ Djavani M, Lukashevich IS, Sanchez A, Nichol ST, Salvato MS (1997). "Completion of the Lassa fever virus sequence and identification of a RING finger open reading frame at the L RNA 5' End". Virology. 235 (2): 414–8. doi:10.1006/viro.1997.8722. PMID 9281522.
↑ Smelt SC, Borrow P, Kunz S, Cao W, Tishon A, Lewicki H; et al. (2001). "Differences in affinity of binding of lymphocytic choriomeningitis virus strains to the cellular receptor alpha-dystroglycan correlate with viral tropism and disease kinetics". J Virol. 75 (1): 448–57. doi:10.1128/JVI.75.1.448-457.2001. PMC 113937. PMID 11119613.
↑ ^8.0 ^8.1 "Center for Disease Control and Prevention (CDC)".
↑ Lashley FR (2006). "Emerging infectious diseases at the beginning of the 21st century". Online J Issues Nurs. 11 (1): 2. PMID 16629503.
↑ ^10.0 ^10.1 Bowen MD, Rollin PE, Ksiazek TG, Hustad HL, Bausch DG, Demby AH; et al. (2000). "Genetic diversity among Lassa virus strains". J Virol. 74 (15): 6992–7004. PMC 112216. PMID 10888638.
↑ "Wikipedia lassa virus".
↑ ^12.0 ^12.1 Rojek JM, Kunz S (2008). "Cell entry by human pathogenic arenaviruses". Cell Microbiol. 10 (4): 828–35. doi:10.1111/j.1462-5822.2007.01113.x. PMID 18182084.
↑ ^13.0 ^13.1 Drosten C, Kümmerer BM, Schmitz H, Günther S (2003). "Molecular diagnostics of [[viral hemorrhagic fevers]]". Antiviral Res. 57 (1–2): 61–87. PMID 12615304. URL–wikilink conflict (help)
↑ Yun NE, Walker DH (2012). "Pathogenesis of Lassa fever". Viruses. 4 (10): 2031–48. doi:10.3390/v4102031. PMC 3497040. PMID 23202452.CS1 maint: PMC format (link)
↑ ^15.0 ^15.1 "Wikipedia Natal multimammate mouse".
↑ ^16.0 ^16.1 ^16.2 "Public Health Image Library (PHIL), Centers for Disease Control and Prevention".

Template:WikiDoc Sources

[1] "Taxonomy browser (Lassavirus)".

[NCCN-2] "The Centers for Disease Control and Prevention".

[pmid10615121-3] "Genome:The autobiography of a species in 23 chapters". Nat Genet. 24 (1): 21. 2000. doi:10.1038/71638. PMID 10615121.

[pmid17143722-4] Moshkoff DA, Salvato MS, Lukashevich IS (2007). "Molecular characterization of a reassortant virus derived from Lassa and Mopeia viruses". Virus Genes. 34 (2): 169–76. doi:10.1007/s11262-006-0050-3. PMC 1892610. PMID 17143722.

[pmid11533204-5] Cornu TI, de la Torre JC (2001). "RING finger Z protein of lymphocytic choriomeningitis virus (LCMV) inhibits transcription and RNA replication of an LCMV S-segment minigenome". J Virol. 75 (19): 9415–26. doi:10.1128/JVI.75.19.9415-9426.2001. PMC 114509. PMID 11533204.CS1 maint: PMC format (link)

[pmid9281522-6] Djavani M, Lukashevich IS, Sanchez A, Nichol ST, Salvato MS (1997). "Completion of the Lassa fever virus sequence and identification of a RING finger open reading frame at the L RNA 5' End". Virology. 235 (2): 414–8. doi:10.1006/viro.1997.8722. PMID 9281522.

[pmid11119613-7] Smelt SC, Borrow P, Kunz S, Cao W, Tishon A, Lewicki H; et al. (2001). "Differences in affinity of binding of lymphocytic choriomeningitis virus strains to the cellular receptor alpha-dystroglycan correlate with viral tropism and disease kinetics". J Virol. 75 (1): 448–57. doi:10.1128/JVI.75.1.448-457.2001. PMC 113937. PMID 11119613.

[CDC-8] 8.0 ^8.1 "Center for Disease Control and Prevention (CDC)".

[pmid16629503-9] Lashley FR (2006). "Emerging infectious diseases at the beginning of the 21st century". Online J Issues Nurs. 11 (1): 2. PMID 16629503.

[pmid10888638-10] 10.0 ^10.1 Bowen MD, Rollin PE, Ksiazek TG, Hustad HL, Bausch DG, Demby AH; et al. (2000). "Genetic diversity among Lassa virus strains". J Virol. 74 (15): 6992–7004. PMC 112216. PMID 10888638.

[Wikipedia-11] "Wikipedia lassa virus".

[pmid18182084-12] 12.0 ^12.1 Rojek JM, Kunz S (2008). "Cell entry by human pathogenic arenaviruses". Cell Microbiol. 10 (4): 828–35. doi:10.1111/j.1462-5822.2007.01113.x. PMID 18182084.

[pmid12615304-13] 13.0 ^13.1 Drosten C, Kümmerer BM, Schmitz H, Günther S (2003). "Molecular diagnostics of [[viral hemorrhagic fevers]]". Antiviral Res. 57 (1–2): 61–87. PMID 12615304. URL–wikilink conflict (help)

[pmid23202452-14] Yun NE, Walker DH (2012). "Pathogenesis of Lassa fever". Viruses. 4 (10): 2031–48. doi:10.3390/v4102031. PMC 3497040. PMID 23202452.CS1 maint: PMC format (link)

[Wikipedia_Natal_multimammate_mouse-15] 15.0 ^15.1 "Wikipedia Natal multimammate mouse".

[PHIL-16] 16.0 ^16.1 ^16.2 "Public Health Image Library (PHIL), Centers for Disease Control and Prevention".

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@@ Line 51: / Line 51: @@
 | [[File:Mastomys natalensis mammary.jpg|thumb|center|400 px|Mastomys natalensis is commonly known as the “multimammate rat” due to the female’s multiple and prominent mammary glands.<SMALL><SMALL>''[http://en.wikipedia.org/wiki/Natal_multimammate_mouse]''<ref name="Wikipedia Natal multimammate mouse">{{Cite web | title = Wikipedia Natal multimammate mouse| url =  http://en.wikipedia.org/wiki/Natal_multimammate_mouse}}</ref></SMALL></SMALL>]]
 |}
-* [[Transmission]] of Lassa virus to humans occurs most commonly through [[ingestion]] or [[inhalation]]. Mastomysrodents shed the [[virus]] in [[urine]] and droppings and direct contact with these materials, through touching soiled objects, eating contaminated [[food]], or exposure to open [[cuts]] or [[sores]], can lead to [[infection]].
+* Mastomysrodents shed the [[virus]] in [[urine]] and droppings and direct contact with these materials, through touching soiled objects, eating contaminated [[food]], or exposure to open [[cuts]] or [[sores]], can lead to [[infection]]. Because Mastomys rodents often live in and around homes and scavenge on leftover human food items or poorly stored food, direct contact [[transmission]] is common. Mastomys [[rodents]] are sometimes consumed as a food source and [[infection]] may occur when [[rodents]] are caught and prepared. Contact with the [[virus]] may also occur when a person inhales tiny particles in the air contaminated with infected [[rodent]] excretions.
-* Because Mastomys rodents often live in and around homes and scavenge on leftover human food items or poorly stored food, direct contact [[transmission]] is common. Mastomys [[rodents]] are sometimes consumed as a food source and [[infection]] may occur when [[rodents]] are caught and prepared. Contact with the [[virus]] may also occur when a person inhales tiny particles in the air contaminated with infected [[rodent]] excretions. This [[aerosol]] or airborne [[transmission]] may occur during cleaning activities, such as sweeping.
-* [[Direct]] contact with infected rodents is not the only way in which people are [[infected]]; person-to-person [[transmission]] may occur after exposure to [[virus]] in the [[blood]], [[tissue]], [[secretions]], or excretions of a Lassa virus-infected individual. Casual contact (including [[skin]]-to-[[skin]] contact without exchange of [[body fluids]]) does not spread Lassa virus. Person-to-person [[transmission]] is common in health care settings (called [[nosocomial transmission]]) where proper [[personal protective equipment]] (PPE) is not available or not used. Lassa virus may be spread in contaminated [[medical equipment]], such as reused needles.
 ==Gallery==