Plasmodium: Difference between revisions

Revision as of 19:20, 25 November 2019

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
Schizonts develop in the erythrocytes, then rupture

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 Presentation

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

WHO Criteria (2010)

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 ≤ 50)
- Hypoglycemia (< 2.2)
- Acidosis (pH < 7.25 or bicarb < 15)
- Renal impairment (creatinine > 265)
- Hyperlactatemia
- Hyperparasitemia (≥ 2%)

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 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
Rapid diagnostic test (RDT) for antigens
- 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
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 severity, including the level of parasitemia, and country of acquisition, which predicts susceptibilities
- Most of the world is resistant; when in doubt, treat all P. falciparum malaria as chloroquine-resistant
All patients with P. falciparum malaria should be considered for hospital admission
- If severe, advocate for ICU-level care

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
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 following 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 & 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
- 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
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

Clindamycin, not doxycycline or atovaquone-proguanil, should be added to artesunate or quinine
Quinine and chloroquine is safe in pregnancy; artesunate safe after first trimester
So for chloroquine-resistant malaria in pregnancy is treated with quinine and clindamycin

Prevention and Chemoprophylaxis

Behavioural interventions

Mosquito avoidance (Anopheles mosquitoes are evening biters)
- Long sleeves & pants
- Insecticide-treated clothing
- Bed nets, screens on doors & windows

Chemoprophylaxis

Chemoprophylaxis is recommended for travelers to endemic areas
Agent chosen based on the local drug-resistance, patient age, and pregnancy status

Chloroquine-sensitive regions

Regions include Haiti, the Dominican Republic, Central America north of the Panama Canal, parts of Mexico, parts of South America, north Africa, parts of the Middle East, and west/central China
- See the CATMAT list for specific countries
Drugs of choice
- Chloroquine (Aralen) preferred, though hydroxychloroquine (Plaquenil) is also acceptable
- Chloroquine or hydroxychloroquine once a week, from 1 week before to 4 weeks after exposure
- Alternatives: atovaquone-proguanil, doxycycline or mefloquine

Chloroquine-resistant regions

Regions include most of sub-Saharan Africa, South America, Oceania and Asia
- See the CATMAT list for specific countries
- Some areas of Thailand, Myanmar (Burma), Laos and Cambodia, and southern Vietnam are both chloroquine-resistant and mefloquine-resistant
Drugs of choice
- Atovaquone-proguanil daily, from 1 day before to 1 week after exposure (because it treats the liver phase)
- Doxycycline daily, from 1 day before to 4 weeks after exposure (does not treat the liver phase)
- Mefloquine weekly, from 1 week before to 4 weeks after exposure
- Alternatives: primaquine daily, from 1 day before to 7 days after exposure
  - Primaquine contraindicated in G6PD deficiency and pregnancy

Chloroquine-and mefloquine-resistant regions

Regions include Asia, Africa and the Amazon basin, specifically in rural, wooded regions on the Thai borders with Myanmar, Cambodia, and Laos, as well as in southern Vietnam
Drugs of choice
- Atovaquone-proguanil daily, from 1 day before to 1 week after exposure
- Doxycycline daily, from 1 day before to 4 weeks after exposure
- No approved drugs for pregnancy or children less than 5 kg, though atovaquone-proguanil may be considered after the first trimester

Pregnancy

Mefloquine can be used, if they cannot avoid travelling to malaria-endemic areas
- Can cause neuropsychiatric symptoms

@@ Line 1: / Line 1: @@
 * Mosquito-borne protozoon that causes '''malaria'''
-== Microbiology ==
+== 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)
@@ Line 8: / Line 8: @@
 * Identified on thick-and-thin Giemsa-stained blood films
-== Life Cycle ==
+=== Life Cycle ===
-[[File:Malaria_LifeCycle_1-20181031193024771.gif|Malaria lifecycle]]
 * Infected mosquito injects sporozoites into human
 * Sporozoites infect the hepatocytes, which develop intracellular schizonts
@@ Line 18: / Line 15: @@
 * Schizonts develop in the erythrocytes, then rupture
-== Pathogenesis ==
+=== 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
@@ Line 28: / Line 24: @@
 ** In adults, hyperinsulin state and quinine also contributes
+=== Epidemiology ===
-[[File:image-20181101092857464.png|image-20181101092857464]]
-== 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
-[[File:image-20181031172205815.png|Distribution of Anopheles]]
 * Distribution varies by species
 ** ''P. falciparum'' in tropical and subtropical Americas, Africa, and Southeast Asia
@@ Line 55: / Line 45: @@
 ** Doxycycline has no known resistance
-== Presentation ==
+== Clinical Presentation ==
 * History of travel to an endemic country
 * Non-specific febrile illness with headaches, myalgias, and malaise
@@ Line 65: / Line 54: @@
 === Severe malaria ===
 * Mostly caused by ''P. falciparum'', though can also be caused by ''P. vivax''
 ==== WHO Criteria (2010) ====
 * Clinical
 ** Prostration / impaired consciousness
@@ Line 88: / Line 75: @@
 === 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 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
@@ Line 119: / Line 102: @@
 == Management ==
 * All returned travellers with fever should have thick and thin smears to rule out malaria
 * Management depends on severity, including the level of parasitemia, and country of acquisition, which predicts susceptibilities
@@ Line 127: / Line 109: @@
 === 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
@@ Line 141: / Line 122: @@
 === Severe malaria ===
 * Usually due to ''P. falciparum'', though can also be caused by ''P. vivax'' or ''P. knowlesi''
 * Admit to hospital, ideally ICU
@@ Line 169: / Line 149: @@
 === Pregnancy ===
 * Clindamycin, not doxycycline or atovaquone-proguanil, should be added to artesunate or quinine
 * Quinine and chloroquine is safe in pregnancy; artesunate safe after first trimester
 * So for chloroquine-resistant malaria in pregnancy is treated with quinine and clindamycin
-=== Prevention and Chemoprophylaxis ===
+== Prevention and Chemoprophylaxis ==
 === Behavioural interventions ===
 * Mosquito avoidance (''Anopheles'' mosquitoes are evening biters)
 ** Long sleeves &amp; pants
@@ Line 184: / Line 161: @@
 === Chemoprophylaxis ===
 * Chemoprophylaxis is recommended for travelers to endemic areas
 * Agent chosen based on the local drug-resistance, patient age, and pregnancy status
 ==== Chloroquine-sensitive regions ====
 * Regions include Haiti, the Dominican Republic, Central America north of the Panama Canal, parts of Mexico, parts of South America, north Africa, parts of the Middle East, and west/central China
 ** See [https://www.canada.ca/en/public-health/services/travel-health/about-catmat/appendix-malaria-risk-recommended-chemoprophylaxis-geographic.html#tbl1 the CATMAT list] for specific countries
@@ Line 198: / Line 173: @@
 ==== Chloroquine-resistant regions ====
 * Regions include most of sub-Saharan Africa, South America, Oceania and Asia
 ** See [https://www.canada.ca/en/public-health/services/travel-health/about-catmat/appendix-malaria-risk-recommended-chemoprophylaxis-geographic.html#tbl1 the CATMAT list] for specific countries
@@ Line 210: / Line 184: @@
 ==== Chloroquine-and mefloquine-resistant regions ====
 * Regions include Asia, Africa and the Amazon basin, specifically in rural, wooded regions on the Thai borders with Myanmar, Cambodia, and Laos, as well as in southern Vietnam
 * Drugs of choice
@@ Line 218: / Line 191: @@
 ==== Pregnancy ====
 * Mefloquine can be used, if they cannot avoid travelling to malaria-endemic areas
 ** Can cause neuropsychiatric symptoms
-=== Bases and Salts ===
-[[File:image-20181031221258061.png|image-20181031221258061]]
 == Further Reading ==
 * Boggild A, ''et al''. [https://www.canada.ca/en/public-health/services/reports-publications/canada-communicable-disease-report-ccdr/monthly-issue/2014-40/ccdr-volume-40-7-april-3-2014/ccdr-volume-40-7-april-3-2014.html 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).