Human granulocytic anaplasmosis

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Human granulocytic anaplasmosis
Classification and external resources
Specialty Lua error in Module:Wikidata at line 446: attempt to index field 'wikibase' (a nil value).
ICD-10 A79.8
ICD-9-CM 083.8
DiseasesDB 31663
MedlinePlus 001381
eMedicine med/3391 ped/655 emerg/159
Patient UK Human granulocytic anaplasmosis
MeSH D016873
[[[d:Lua error in Module:Wikidata at line 863: attempt to index field 'wikibase' (a nil value).|edit on Wikidata]]]
Anaplasma phagocytophilum cultured in human

Human granulocytic anaplasmosis (HGA) (previously known as Human granulocytic ehrlichiosis, or HGE[1][2]) is a tick-borne, infectious disease caused by Anaplasma phagocytophilum, an obligate intracellular bacterium that is typically transmitted to humans by at least three kinds of ticks, Ixodes scapularis, Ixodes pacificus, and Dermacentor variabilis. These ticks also transmit Lyme disease and other tick borne diseases.[3]

The bacteria infect white blood cells called neutrophils, causing changes in gene expression that prolong the life of these otherwise short-lived cells.[4]

History

The first outbreak of Human Granulocytic Anaplasmosis (HGA) in the United States was in a patient in early 1990 in Wisconsin. He was kept in the hospital in Minnesota for testing, but died without a diagnosis.[5] Over the next couple of years, many people within the same area of Wisconsin and Minnesota had come down with the same symptoms.[5] It was discovered in 1994 that it was Human Granulocytic Ehrlichiosis (HGE), later to be known as HGA.[6]

Ecology and Epidemiology

A. phagocytophilum is transmitted to humans by Ixodes ticks. These ticks are found in the US, Europe, and Asia. In the US, I. scapularis is the tick vector in the East and Midwest states, and I. pacificus in the Pacific Northwest.[7] In Europe, the I. ricinus is the main tick vector, and I. persulcatus is the currently known tick vector in Asia.[5]

The major mammalian reservoir for A. phagocytophilum in the eastern United States is the white-footed mouse, Peromyscus leucopus. Although white-tailed deer and other small mammals harbor A. phagocytophilum, evidence suggests that they are not a reservoir for the strains that cause HGA.[8][9] A tick that has a blood meal from an infected reservoir becomes infected themselves. If an infected tick then latches onto a human the disease is then transmitted to the human host and A. phagocytophilum symptoms can arise.[6]

Anaplasma phagocytophilum shares its tick vector with other human pathogens, and about 10% of patients with HGA show serologic evidence of coinfection with Lyme disease, babesiosis, or tick-borne meningoencephalitis.[10]

Statistics

From the first reported case in 1994 until 2010, HGA's rates of incidence have exponentially increased.[11] This is likely because HGA is found where there are ticks that carry and transmit Lyme disease, also known as Borrelia burgdorferi, and babesiosis, which is found in the northeastern and midwestern parts of the United States, which has seemingly increased in the past couple of decades.[11] Before 2000, there were less than 300 cases reported per year. In 2000, there were only 350 reported cases.[11] From 2009-2010, HGA experienced a 52% increase in the number of cases reported.[11]

Signs and Symptoms

Signs and symptoms may include:

  • fever
  • severe headache
  • muscle aches (myalgia)
  • chills and shaking, similar to the symptoms of influenza
  • nausea
  • vomiting
  • loss of appetite
  • unintentional weight loss
  • abdominal pain
  • cough
  • diarrhea,
  • aching joints
  • sensitivity to light
  • weakness
  • fatigue
  • change in mental status (extreme confusion, memory loss, inability to comprehend environment- interaction, reading, etc.)
  • temporary loss of basic motor skills

Symptoms may be minor, as evidenced by surveillance studies in high-risk areas. Gastrointestinal tract symptoms occur in less than half of patients and a skin rash is seen in less than 10% of patients.[12] It is also characterized by a low number of platelets, a low number of white blood cells, and elevated serum transaminase levels in the majority of infected patients.[12] Even though people of any age can get HGA, it is usually more severe in the aging or immune-compromised. Some severe complications may include respiratory failure, kidney failure, and secondary infections.

Diagnosis

Clinically, HGA is essentially indistinguishable from Human monocytic ehrlichiosis, the infection caused by Ehrlichia chaffeensis, and other tick-borne illnesses such as Lyme disease may be suspected.[13] As Ehrlichia serologies can be negative in the acute period, PCR is very useful for diagnosis.[14]

Treatment and Prevention

Doxycycline is the treatment of choice. If anaplasmosis is suspected, treatment should not be delayed while waiting for a definitive laboratory confirmation, as prompt doxycycline therapy has been shown to improve outcomes.[13] Presentation during early pregnancy can complicate treatment. Doxycycline compromises dental enamel during development.[15] Although rifampin is indicated for post-delivery pediatric and some doxycycline-allergic patients, it is teratogenic. Rifampin is contraindicated during conception and pregnancy.[16] Currently, there is no vaccine against human granulocytic anaplasmosis, so antibiotics are the only form of treatment.[5] The best way to prevent HGA is to prevent getting tick bites.[17] If the disease is not treated with antibiotics quickly, sometimes before the diagnosis, the patient has a high chance of mortality.[5] Most patients make a complete recovery, though some patients are intensively cared for after treatment.[5] A reason for a patient needing intensive care is if the patient goes too long without seeing a doctor or being diagnosed.[5] The majority of patients, though, make a 100% recovery with no residual damage.[5]

Terminology

Although the infectious agent is known to be from the Anaplasma genus, the term "human granulocytic ehrlichiosis" (HGE) is often used, reflecting the prior classification of the organism. E. phagocytophilum and E. equi were reclassified as Anaplasma phagocytophilum.

Major Surface Proteins (MSPs)

Lots of MSPs are found in Anaplasma and the ones that interact with Anaplasma can mainly be found in A. marginale and A. phagocytophilum.[18] There are many different phenotypic traits that are associated with MSPs, because each MSP can only infect certain animals in certain conditions.[18] A. phagocytophilum infects the most vast array of living things, including humans, and all around the world.[18] A. marginale evolved to be more specific in infecting animals, such as deer and cattle in the subtropics and tropics.[18] The main difference between these two MSPs is that the host cell for A. phagocytophilum is the granulocyte, while the host cell for A. marginale is erythrocytes. [18] It is likely that these MSPs coevolved, because they had previously interacted via tick-pathogen interaction. [18]

Anaplasma MSPs can not only cooperate with vertebrates, but also invertebrates, which make these phenotypes evolve faster than others, because they have a lot of selective forces acting on them.[18]

See also

External links

References

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  2. Human Anaplasmosis Basics - Minnesota Dept. of Health
  3. http://www.bioone.org/doi/abs/10.1603/0022-2585%282003%29040%5B0534%3ADOBBEC%5D2.0.CO%3B2
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  12. 12.0 12.1 Murray, Patrick R.; Rosenthal, Ken S.; Pfaller, Michael A. Medical Microbiology, Fifth Edition. United States: Elsevier Mosby, 2005
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