Viral hemorrhagic fever
This article needs more reliable medical references for verification or relies too heavily on primary sources. (July 2020) |
Viral hemorrhagic fever | |
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Other names | viral haemorrhagic fever |
Two nurses standing near Mayinga N'Seka, a nurse with Ebola virus disease in the 1976 outbreak in Zaire. N'Seka died a few days later due to severe internal hemorrhage. | |
Specialty | Infectious disease |
Viral hemorrhagic fevers (VHFs) are a diverse group of animal and human illnesses. VHFs may be caused by five distinct families of RNA viruses: the families Filoviridae, Flaviviridae, Rhabdoviridae, and several member families of the Bunyavirales order such as Arenaviridae, and Hantaviridae. All types of VHF are characterized by fever and bleeding disorders and all can progress to high fever, shock and death in many cases. Some of the VHF agents cause relatively mild illnesses, such as the Scandinavian nephropathia epidemica (a hantavirus), while others, such as Ebola virus, can cause severe, life-threatening disease.
Signs and symptoms
[edit]Signs and symptoms of VHFs include (by definition) fever and bleeding:
- Flushing of the face and chest, small red or purple spots (petechiae), bleeding, swelling caused by edema, low blood pressure (hypotension), and circulatory shock.
- Malaise, muscle pain, headache, vomiting, and diarrhea occur frequently.
The severity of symptoms varies with the type of virus. The "VHF syndrome" (capillary leak, bleeding diathesis, and circulatory compromise leading to shock) appears in a majority of people with filoviral hemorrhagic fevers (e.g., Ebola and Marburg virus), Crimean–Congo hemorrhagic fever (CCHF), and the South American hemorrhagic fevers caused by arenaviruses, but only in a small minority of patients with dengue or Rift Valley fever.
Causes
[edit]Five families of RNA viruses have been recognised as being able to cause hemorrhagic fevers.[citation needed]
- The order Bunyavirales includes the families Arenaviridae, Fimoviridae, and all members of the former family Bunyaviridae, especially Peribunyaviridae.
- The family Arenaviridae include the viruses responsible for Lassa fever (Lassa virus), Lujo virus, Argentine (Junin virus), Bolivian (Machupo virus), Brazilian (Sabiá virus), Chapare hemorrhagic fever (Chapare virus), Venezuelan (Guanarito virus) and Whitewater Arroyo virus hemorrhagic fevers.
- The former family Bunyaviridae includes
- the causative agents of Hantavirus hemorrhagic fever with renal syndrome (HV-HFRS) (Hantaviridae),
- the Crimean-Congo hemorrhagic fever (CCHF) virus from the genus Orthonairovirus (Nairoviridae),
- Garissa virus and Ilesha virus from the genus Orthobunyavirus (Peribunyaviridae), and
- the Rift Valley fever (RVF) virus from the genus Phlebovirus (Phenuiviridae).
- The family Filoviridae (order Mononegavirales) includes Ebola virus and Marburg virus.
- The family Flaviviridae (order Amarillovirales) includes dengue, yellow fever, and two viruses in the tick-borne encephalitis group that cause VHF: Omsk hemorrhagic fever virus and Kyasanur Forest disease virus.
- The family Togaviridae (order Martellivirales) includes Chikungunya virus which causes Chikungunya fever.
- Family Rhabdoviridae (order Mononegavirales): In September 2012 scientists writing in the journal PLOS Pathogens reported the isolation of a member of the Rhabdoviridae responsible for two fatal and two non-fatal cases of hemorrhagic fever in the Bas-Congo district of the Democratic Republic of Congo. The virus was named Bas-Congo virus. The non-fatal cases occurred in healthcare workers involved in the treatment of the other two, suggesting the possibility of person-to-person transmission.[1] This virus is related to the Ephemerovirus and Tibrovirus genera.
The pathogen that caused the cocoliztli epidemics in Mexico of 1545 and 1576 is still unknown, and the 1545 epidemic may have been bacterial rather than viral.[2][3]
Pathophysiology
[edit]Different hemorrhagic fever viruses act on the body in different ways, resulting in different symptoms. In most VHFs, it is likely that several mechanisms contribute to symptoms, including liver damage, disseminated intravascular coagulation (DIC), and bone marrow dysfunction. In DIC, small blood clots form in blood vessels throughout the body, removing platelets necessary for clotting from the bloodstream and reducing clotting ability. DIC is thought to cause bleeding in Rift Valley, Marburg, and Ebola fevers. For filoviral hemorrhagic fevers, there are four general mechanisms of pathogenesis. The first mechanism is dissemination of virus due to suppressed responses by macrophages and dendritic cell (antigen presenting cells). The second mechanism is prevention of antigen specific immune response. The third mechanism is apoptosis of lymphocytes. The fourth mechanism is when infected macrophages interact with toxic cytokines, leading to diapedesis and coagulation deficiency. From the vascular perspective, the virus will infect vascular endothelial cells, leading to the reorganization of the VE-cadherin catenin complex (a protein important in cell adhesion). This reorganization creates intercellular gaps in endothelial cells. The gaps lead to increased endothelial permeability and allow blood to escape from the vascular circulatory system.[citation needed]
The reasons for variation among patients infected with the same virus are unknown but stem from a complex system of virus-host interactions. Dengue fever becomes more virulent during a second infection by means of antibody-dependent enhancement. After the first infection, macrophages display antibodies on their cell membranes specific to the dengue virus. By attaching to these antibodies, dengue viruses from a second infection are better able to infect the macrophages, thus reducing the immune system's ability to fight off infection.[citation needed]
Diagnosis
[edit]Definitive diagnosis is usually made at a reference laboratory with advanced biocontainment capabilities. The findings of laboratory investigation vary somewhat between the viruses but in general, there is a decrease in the total white cell count (particularly the lymphocytes), a decrease in the platelet count, an increase in the blood serum liver enzymes, and reduced blood clotting ability measured as an increase in both the prothrombin (PT) and activated partial thromboplastin times (PTT). The hematocrit may be elevated. The serum urea and creatine may be raised but this is dependent on the hydration status of the patient. The bleeding time tends to be prolonged.[citation needed]
Prevention
[edit]With the exception of yellow fever vaccine and Ebola vaccines, vaccines for VHF-associated viruses are generally not available. Post-exposure prophylactic (preventive) ribavirin may be effective for some bunyavirus and arenavirus infections.[4][5]
VHF isolation guidelines dictate that all VHF patients (with the exception of dengue patients) should be cared for using strict contact precautions, including hand hygiene, double gloves, gowns, shoe and leg coverings, and face shield or goggles. Lassa, CCHF, Ebola, and Marburg viruses may be particularly prone to nosocomial (hospital-based) spread. Airborne precautions should be utilized including, at a minimum, a fit-tested, HEPA filter-equipped respirator (such as an N95 mask), a battery-powered, air-purifying respirator, or a positive pressure supplied air respirator to be worn by personnel coming within 1.8 meter (six feet) of a VHF patient. Groups of patients should be cohorted (sequestered) to a separate building or a ward with an isolated air-handling system. Environmental decontamination is typically accomplished with hypochlorite (e.g. bleach) or phenolic disinfectants.[6]
Management
[edit]Medical management of VHF patients may require intensive supportive care. Antiviral therapy with intravenous ribavirin may be useful in Bunyaviridae and Arenaviridae infections (specifically Lassa fever, RVF, CCHF, and HFRS due to Old World Hantavirus infection) and can be used only under an experimental protocol as IND approved by the U.S. Food and Drug Administration (FDA). Interferon may be effective in Argentine or Bolivian hemorrhagic fevers (also available only as IND).[citation needed] A potential novel treatment, the NMT inhibitor, has been shown to completely inhibit lassa infection in cells based assays.[7]
Epidemiology
[edit]- Cocoliztli in Mexico 1545 and 1576 (suspected)[2][8][9][10][11]
- The Great Yellow Fever Epidemic of 1793 in Philadelphia, PA, US. Nearly 10% of the population of 50,000 died from the disease.
- Mékambo in Gabon is the site of several outbreaks of Ebola virus disease.
- Orientale Province, Democratic Republic of the Congo villages of Durba and Watsa were the epicenter of the 1998–2000 outbreak of Marburg virus disease.
- Uíge Province in Angola was the site of another outbreak of Marburg virus disease in 2005, the largest one to date of this disease.[12]
- A VHF outbreak in the village of Mweka, Democratic Republic of the Congo (DRC) that started in August 2007, and that has killed 103 people (100 adults and three children), has been shown to be caused (at least partially) by Ebola virus.
- A viral hemorrhagic fever is a possible cause of the Plague of Athens during the Peloponnesian War.[13]
- A viral hemorrhagic fever is an alternate theory of the cause of the Black Death and the Plague of Justinian[14]
- The initial, and currently only, outbreak of Lujo virus in September–October 2008 left four of five patients dead.[15]
- The 2014 West Africa Ebola outbreak, which was the biggest outbreak in history.
Biowarfare potential
[edit]The VHF viruses are spread in a variety of ways. Some may be transmitted to humans through a respiratory route.[citation needed] The viruses are considered by military medical planners to have a potential for aerosol dissemination, weaponization, or likelihood for confusion with similar agents that might be weaponized.[16][17]
See also
[edit]- Biosafety
- Jordi Casals-Ariet
- Dr. Matthew Lukwiya (1957–2000)
- C. J. Peters
References
[edit]- ^ Grard G, Fair JN, Lee D, et al. (September 2012). "A novel rhabdovirus associated with acute hemorrhagic fever in central Africa". PLOS Pathog. 8 (9): e1002924. doi:10.1371/journal.ppat.1002924. PMC 3460624. PMID 23028323.
- ^ a b Acuna-Soto R, Stahle DW, Cleaveland MK, Therrell MD (April 2002). "Megadrought and megadeath in 16th century Mexico". Emerging Infect. Dis. 8 (4): 360–62. doi:10.3201/eid0804.010175. PMC 2730237. PMID 11971767.
- ^ "500 years later, scientists discover what probably killed the Aztecs". The Guardian. Agence France-Presse. 2018-01-16.
- ^ Ergönül Ö, Keske Ş, Çeldir MG, Kara İA, Pshenichnaya N, Abuova G, et al. (2018). "Systematic Review and Meta-analysis of Postexposure Prophylaxis for Crimean-Congo Hemorrhagic Fever Virus among Healthcare Workers". Emerg Infect Dis. 24 (9): 1642–1648. doi:10.3201/eid2409.171709. PMC 6106438. PMID 30124196.
{{cite journal}}
: CS1 maint: multiple names: authors list (link) - ^ Hadi CM, Goba A, Khan SH, Bangura J, Sankoh M, Koroma S, et al. (2010). "Ribavirin for Lassa fever postexposure prophylaxis". Emerg Infect Dis. 16 (12): 2009–11. doi:10.3201/eid1612.100994. PMC 3294560. PMID 21122249.
{{cite journal}}
: CS1 maint: multiple names: authors list (link) - ^ Woods LC, ed. (2005). USAMRIID's Medical Management of Biological Casualties Handbook (PDF) (6th ed.). Fort Detrick MA: U.S. Army Medical Institute of Infectious Diseases. pp. 143–44. Archived from the original (PDF) on 2007-06-09. Retrieved 2007-06-09.
- ^ Witwit H, Betancourt CA, Cubitt B, Khafaji R, Kowalski H, Jackson N, Ye C, Martinez-Sobrido L, de la Torre JC (2024-08-26). "Cellular N-Myristoyl Transferases Are Required for Mammarenavirus Multiplication". Viruses. 16 (9): 1362. doi:10.3390/v16091362. ISSN 1999-4915. PMC 11436053. PMID 39339839.
- ^ "Was the Huey Cocoliztli a Haemorrhagic Fever?" (PDF). Archived from the original (PDF) on 2010-06-17. Retrieved 2010-07-25.
- ^ Indigenous Hemorrhagic Fever and The Spanish Conquest
- ^ Acuna-Soto R, Romero LC, Maguire JH (June 2000). "Large Epidemics of Hemorrhagic Fevers in Mexico 1545–1815" (PDF). Am J Trop Med Hyg. 62 (6): 733–39. doi:10.4269/ajtmh.2000.62.733. PMID 11304065. Archived from the original (PDF) on 2007-03-20. Retrieved 2006-12-04.
- ^ "Epidemics in New Spain". Archived from the original on 2010-06-14. Retrieved 2010-07-25.
- ^ Towner JS, Khristova ML, Sealy TK, Vincent MJ, Erickson BR, Bawiec DA, Hartman AL, Comer JA, Zaki SR, Ströher U, Gomes Da Silva F, Del Castillo F, Rollin PE, Ksiazek TG, Nichol ST (2006). "Marburgvirus Genomics and Association with a Large Hemorrhagic Fever Outbreak in Angola". Journal of Virology. 80 (13): 6497–516. doi:10.1128/JVI.00069-06. PMC 1488971. PMID 16775337.
- ^ Olson PE, Hames CS, Benenson AS, Genovese EN (1996). "The Thucydides syndrome: Ebola déjà vu? (or Ebola reemergent?)". Emerging Infect. Dis. 2 (2): 155–56. doi:10.3201/eid0202.960220. PMC 2639821. PMID 8964060.
- ^ Scott, Susan and Duncan, Christopher. (2004). Return of the Black Death: The World's Greatest Serial Killer West Sussex; John Wiley and Sons. ISBN 0-470-09000-6.
- ^ Briese T, Paweska J, McMullan L, Hutchison S, Street C, Palacios G, Khristova M, Weyer J, Swanepoel R, Engholm M, Nichol S, Lipkin W (2009). "Genetic Detection and Characterization of Lujo Virus, a New Hemorrhagic Fever–Associated Arenavirus from Southern Africa". PLOS Pathog. 5 (5): e1000455. doi:10.1371/journal.ppat.1000455. PMC 2680969. PMID 19478873.
- ^ Woods 2005, p. 145
- ^ Peters C (2000). "Are Hemorrhagic Fever Viruses Practical Agents for Biological Terrorism?". In Scheld WM, Craig WA, Hughes JM (eds.). Emerging Infections. Vol. 4. Washington, D.C.: ASM Press. pp. 201–09. ISBN 978-1555811976.
External links
[edit]- "Viral Haemorrhagic Fever". The National Archives of United Kingdom. Public Health England (PHE). Archived from the original on 2014-07-14.
- "Viral Haemorrhagic Fevers". World Health Organization (WHO). United Nations (UN). Archived from the original on August 23, 2004.
- "Viral Hemorrhagic Fevers (VHFs) Virus Families". National Center for Emerging and Zoonotic Infectious Diseases (NCEZID). U.S. Centers for Disease Control and Prevention (CDC). 2019-09-24.