Plasmodium: Difference between revisions
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Plasmodium
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*All returned travellers with fever should have thick and thin smears to rule out malaria |
*All returned travellers with fever should have thick and thin smears to rule out malaria |
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*Management depends on |
*Management depends on species and susceptibility (predicted by country of acquisition), and severity (including the level of parasitemia) |
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**Most of the world has chloroquine-resistant ''P. falciparum'', so when in doubt, treat all ''P. falciparum'' malaria as resistant |
**Most of the world has chloroquine-resistant ''P. falciparum'', so when in doubt, treat all ''P. falciparum'' malaria as resistant |
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*All patients with ''P. falciparum'' malaria should be considered for hospital admission |
*All patients with ''P. falciparum'' malaria should be considered for hospital admission |
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**If severe, advocate for ICU-level care |
**If severe, advocate for ICU-level care |
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===Concurrent Supportive Care=== |
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*Fluid resuscitation as needed (too much may be harmful in children) |
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*Rule out [[hypoglycemia]] if sudden change in clinical status (worsened with [[quinine]]) |
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*Avoid [[steroids]], which are associated with worse outcomes in cerebral malaria |
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*Correct coagulopathy and bleeding with blood products and [[vitamin K]] |
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*If [[shock]] develops, treat empirically with antibiotics while getting blood cultures to rule out intercurrent [[bacteremia]] |
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===Uncomplicated Malaria=== |
===Uncomplicated Malaria=== |
Revision as of 11:28, 21 August 2020
- Mosquito-borne protozoon that causes malaria
Background
Microbiology
- Intracellular protozoal parasite of red blood cells
- Species that cause human disease are: P. falciparum, P. vivax, P. ovale, P. malariae, and P. knowlesi (from the macaque monkey)
- P. knowlesi looks like P. malariae microscopically, but has a higher (>1%) parasitemia with a clinical course more like P. falciparum
- Identified on thick-and-thin Giemsa-stained blood films
Life Cycle
- Infected mosquito injects sporozoites into human
- Sporozoites infect the hepatocytes, which develop intracellular schizonts
- P. vivax and P. ovale can have prolonged (months to years) liver stages during which the patient is asymptomatic
- The hepatocytes rupture and release trophozoites, which infect erythrocytes and mature into trophozoites
- Trophozoites develop into schizonts, then rupture the erythrocyte to release more merozoites
- These cycles of merozoite to trophoziote to schizont to merozoite explain the periodic fevers
- Trophozoites can also develop into gametocytes (micro- or macro-gametocytes), which are taken up by the mosquito
- In the mosquito, the micro- and macro-gametocytes join to form a zygote, which matures into an ookinete then oocyst, which releases infective sporozoites
Pathophysiology
- Infected red blood cells adhere to endothelial cells, and clump, causing rosetting
- This causes microvascular obstruction and ischemia, which causes cerebral malaria and metabolic acidosis
- Can cause marrow suppression
- P. falciparum manages to avoid splenic sequestration
- Hypoglycemia
- In children, hypermetabolic and consumes glucose
- In adults, hyperinsulin state and quinine also contributes
Epidemiology
- Transmitted by female Anopheles mosquitoes, but can also be transmitted through blood transfusions
- Distribution is that of the Anopheles mosquito: tropical and subtropical regions worldwide with the exception of North America, Europe, and Australia
- Distribution varies by species
- P. falciparum in tropical and subtropical Americas, Africa, and Southeast Asia
- P. vivax in the Americas, India, and Southeast Asia
- P. malariae in tropical and subtropical Americas, Africa, and Southeast Asia
- P. ovale in sub-Saharan Africa
- P. knowlesi in Southeast Asia
- Resistance varies geographically
- Chloroquine-resistant P. falciparum is widespread in sub-Saharan Africa, Asia, and the Americas (except Mexico, regions west of the Panama Canal, Haiti, and the Dominican Republic)
- Chloroquine-resistant P. vivax is in Papua New Guinea and Indonesia, with case reports in many other countries
- Chloroquine-resistant P. malariae is found in Sumatra and Indonesia
- Amodiaquine-resistant P. falciparum can be found in Africa and Asia
- Mefloquine-resistant P. falciparum is in Thailand, Cambodia, Myanmar, and Vietnam, with case reports in Brazil and Africa
- Sulfadoxine-pyrimethamine resistance is widespread in Southeast Asia, the Amazon Basin, and Africa
- Atovaquone-proguanil resistance is increasing but still rare
- Reduced quinine susceptibility is reported in Southeast Asia, sub-Saharan Africa, and South America
- Reduced artemisinin susceptibility is reported in Cambodia, Thailand, Vietnam, and Myanmar
- Doxycycline has no known resistance
Clinical Manifestations
- History of travel to an endemic country
- Non-specific febrile illness with headaches, myalgias, and malaise
- Fevers are often periodic, appearing based on rupture of schizonts (tertian and quartan fever)
- q24h: P. falciparum
- q48h: P. vivax or P. ovale
- q72h: P. malariae
Severe Malaria
- Mostly caused by P. falciparum, though can also be caused by P. vivax
CATMAT Criteria (2019)
- Clinical
- Prostration / impaired consciousness
- Respiratory distress
- Multiple convulsions, which can be from cerebral malaria, hypoglycemia, severe metabolic acidosis, etc
- Circulatory collapse
- Pulmonary edema
- Abnormal bleeding
- Jaundice
- Hemoglobinuria
- Laboratory
- Severe anemia (Hb ≤ 70 or Hct <20%)
- Hypoglycemia (< 2.2)
- Acidosis (pH < 7.25 or bicarb < 15)
- Renal impairment (creatinine > 265)
- Hyperlactatemia
- Hyperparasitemia
- ≥ 2% for children < 5 years
- ≥5% for non-immune adults and children ≥ 5 years
- ≥10% for semi-immune adults and children ≥ 5 years
- Non-immune: born in non-endemic or low-transmission areas (e.g. as travellers), and those who are more than 6 to 12 months away from malaria exposure
- Semi-immune: birth and long-term residence in an endemic country and prior episodes of malaria
Cerebral Malaria
- Erythrocytes sequester in the cerebral microvessels
Malaria in Pregnancy
- Accumulation of infected erythrocytes in the placenta, causing IUGR, prematurity, and neonatal mortality
Late or Relapsing Malaria
- P. vivax and P. ovale can have liver stages (hypnozoites) that lie latent for months to years before causing relapses
- P. malariae can have a low-level asymptomatic parasitemia lasting for years before presentation
Diagnosis
Thick and Thin Peripheral Blood Films
- Thick for detecting parasites, thin for parasitemia and species
- P. knowlesi looks similar to P. malariae but presents like P. falciparum
- Usually done three times for improved sensitivity
Rapid Diagnostic Antigen Test (RDT)
- Good sensitivity and specificity for falciparum malaria, but lower sensitivity (66-88%) for non-falciparum or at low levels of parasitemia
- May cross-react with ANA and RF, and with dengue, hepatitis C, leishmaniasis, trypanosomiasis, schistosomiasis, tuberculosis, and toxoplasmosis
- May be positive up to 4 weeks after treatment from persistent gamecotyes and slow antigen clearance, so are not used to document treatment success
- BinaxNow is the only test in Canada
- T1 band: histidine-rich protein-2 (HRP-2) of P. falciparum
- T2 band: aldolase, a common antigen of four species of human malaria parasites
- C+ / T1+ / T2+: P. falciparum or mixed
- C+ / T1+ / T2–: P. falciparum
- C+ / T1– / T2+: non-falciparum
- C+ / T1– / T2–: no malaria
- Can remain positive for up to 4 weeks due to detection of dead organisms
Molecular Testing
- PCR is available
- Done reflexively in Ontario to confirm species and detect a mixed infection
Management
- All returned travellers with fever should have thick and thin smears to rule out malaria
- Management depends on species and susceptibility (predicted by country of acquisition), and severity (including the level of parasitemia)
- Most of the world has chloroquine-resistant P. falciparum, so when in doubt, treat all P. falciparum malaria as resistant
- All patients with P. falciparum malaria should be considered for hospital admission
- If severe, advocate for ICU-level care
Concurrent Supportive Care
- Fluid resuscitation as needed (too much may be harmful in children)
- Rule out hypoglycemia if sudden change in clinical status (worsened with quinine)
- Avoid steroids, which are associated with worse outcomes in cerebral malaria
- Correct coagulopathy and bleeding with blood products and vitamin K
- If shock develops, treat empirically with antibiotics while getting blood cultures to rule out intercurrent bacteremia
Uncomplicated Malaria
- Chloroquine-sensitive P. falciparum (Mexico, Central America west of the Panama Canal, Haiti, the Dominican Republic, and most of the Middle East), P. vivax, P. ovale, P. malariae, and P. knowlesi
- Oral chloroquine 600 mg base po once, followed by 300 mg base po at 6, 24, and 48 hours
- The dose for salt is 1000 mg and 500 mg
- Oral chloroquine 600 mg base po once, followed by 300 mg base po at 6, 24, and 48 hours
- Chloroquine-resistant P. falciparum (most of the world) or chloroquine-resistant P. vivax (Papua New Guinea and Indonesia)
- Atovaquone-proguanil 1000/400 mg (4 tablets) po daily for 3 days
- Alternative: quinine 542 mg base (650 mg salt) po q8h for 3 to 7 days, plus doxycycline 100 mg po bid for 7 days
- Prevention of relapsing P. vivax and P. ovale
- Indicated for patients with prolonged exposure
- Primaquine 30 mg base daily for 14 days started concurrent with chloroquine
- First rule out G6PD deficiency and pregnancy
- If pregnant, just treat intermittently until after delivery
Severe Malaria
- Usually due to P. falciparum, though can also be caused by P. vivax or P. knowlesi
- Admit to hospital, ideally ICU
- Frequent vitals and urine output
- Capillary glucose at least q4h
- Antimalarials
- Artesunate 2.4 mg/kg IV bolus over 1-2 minutes at 0, 12, 24, and 48 hours
- Four hours after the last dose, add one of the following
- Atovaquone-proguanil 1000/400 mg po daily for 3 days
- Doxycycline 100 mg po BID for 7 days
- Clindamycin 10 mg/kg IV followed by 5 mg/kg IV q8h for 7 days
- Four hours after the last dose, add one of the following
- Quinine 5.8 mg/kg IV loading dose over 30 min followed by 8.3 mg/kg IV infused over 4 hours q8h for 7 days
- Dose of quinine dihydrochloride would be 7 mg/kg and 10 mg/kg
- Do not use loading dose if they had quinine within 24 hours or mefloquine within 2 weeks
- Switch to oral tablets as soon as able to swallow
- If no infusion pump, run the loading dose as quinine 16.7 mg/kg IV over 4 hours
- Concurrent to last dose of quinine
- Atovaquone-proguanil 1000/400 mg po daily for 3 days
- Doxycycline 100 mg po BID for 7 days
- Clindamycin 10mg/kg IV load followed by 5 mg/kg q8h for 7 days
- Clindamycin is the preferred treatment in pregnant women and children under 8 years
- Artesunate 2.4 mg/kg IV bolus over 1-2 minutes at 0, 12, 24, and 48 hours
- Treat seizures with benzos; No role for seizure prophylaxis
- Avoid steroids in cerebral malaria (worse outcomes)
- Exchange transfusion has been investigated; it reduces parasitemia but has no clinically-important benefits
- CATMAT still recommends considering it if parasitemia ≥10%
- Usually 5 to 10 units of pRBC
Pregnancy
- Uncomplicated chloroquine-susceptible malaria:
- Chloroquine, or artemether-lumefantrine after the first trimester
- Rather than terminal
- Uncomplicated chloroquine-resistant P. falciparum or P. vivax:
- Mefloquine, quinine and clindamycin, or artemether-lumefantrine after the first trimester
- Prevention of relapsing P. vivax and P. ovale:
- Maintained chloroquine prophylaxis 300 mg base (500 mg salt) po weekly for the duration of their pregnancy
- Reassess for terminal with primaquine or tafenoquine prophylaxis after delivery
- Primaquine preferred if breastfeeding
- Severe malaria:
- Preferred is artesunate followed by clindamycin
- Alternative is quinine followed by clindamycin
- There are few data on artesunate in first trimester, but it appears safe, and the overall risk-benefit assessment favours treatment
- Other antimalarials
- Atovaquone-proguanil is likely safe and can be used after the first trimester for any of the above regimens
- Doxycycline, primaquine, and tafenoquine should be avoided in pregnancy
Prevention
Behavioural Interventions
- Mosquito avoidance (Anopheles mosquitoes are evening biters)
- Long sleeves & pants
- Insecticide-treated clothing
- Bed nets, screens on doors & windows
Chemoprophylaxis
Further Reading
- Boggild A, et al. Summary of recommendations for the diagnosis and treatment of malaria by the Committee to Advise on Tropical Medicine and Travel (CATMAT). CCDR 2014;40(7).
- A continuously-updated version is maintained online.
- CDC Treatment of Malaria: Guidelines For Clinicians (United States)