Trypanosoma brucei: Difference between revisions
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Trypanosoma brucei
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==Background== |
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= ''Trypanosoma brucei'' (African trypanosomiasis) = |
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also known as African sleeping sickness |
*Causes '''African trypanosomiasis''', also known as '''African sleeping sickness''' |
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{| class="wikitable" |
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{| |
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! |
! |
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! |
!West African |
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! |
!East African |
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|- |
|- |
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|Organism |
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|''T. b. gambiense'' |
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|''T. b. rhodesiense'' |
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|- |
|- |
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|Vector |
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|tsetse fly, ''palpalis'' group |
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|tsetse fly, ''morsitans'' group |
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|- |
|- |
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|Habitat |
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| Primary reservoir |
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|forests and wooded areas |
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| Humans |
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|savanna and woodlands |
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|- |
|- |
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|Primary reservoir |
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| Human illness |
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|humans |
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| Chronic (late CNS disease) |
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|antelope and cattle |
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| Acute (early CNS disease) |
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|- |
|- |
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| |
|Human illness |
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|chronic (late CNS disease) |
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| Months to years |
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|acute (early CNS disease) |
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| < 9 months |
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|- |
|- |
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|Duration of illness |
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| Lymphadenopathy |
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|months to years |
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| Prominent |
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|< 9 months |
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| Minimal |
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|- |
|- |
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|Lymphadenopathy |
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| Parasitemia |
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|prominent |
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| Low |
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|minimal |
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| High |
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|- |
|- |
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|Parasitemia |
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| Epidemiology |
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|low |
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| Rural |
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|high |
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| Tourists and workers in game parks/wild areas; rural |
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|- |
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|Epidemiology |
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|rural |
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|tourists and workers in game parks/wild areas; rural |
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|- |
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|Treatment |
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|[[pentamidine]] (non-CNS) or [[eflornithin]] (CNS) |
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|[[suramin]] (non-CNS) or [[melarsoprol]] (CNS) |
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|} |
|} |
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== |
===Microbiology=== |
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* |
*Vector-borne flagellated protozoan parasite transmitted by the tsetse fly belonging to the genus ''Trypanosoma'', subgenus ''Trypanozoon'' |
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* |
*Two subspecies that are morphologically indistinguishable |
||
** |
**''T. b. gambiense'', causing chronic African trypanosomiasis (“West African sleeping sickness”) |
||
** |
**''T. b. rhodesiense'', causing acute African trypanosomiasis (“East African sleeping sickness”) |
||
** |
**Also, ''T. b. brucei'', which infects cattle and occasionally other animals |
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* |
*No intracellular phase, in contrast to Chagas disease |
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== |
===Epidemiology=== |
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*Present only in sub-Saharan Africa |
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[[File:SleepingSick_LifeCycle_19.jpg|T. brucei life cycle]] |
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*Transmitted by flies in the genus [[Vector::Glossina species|Glossina]] (tsetse flies) in their saliva during feeding |
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**Tsetse flies exists only in Africa |
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*Animal reservoirs include cattle and possibly wild ungulates (''T. b. rhodesiense''); non-human animals are less important for ''T. b. gambiense'' |
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===Pathophysiology=== |
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== Epidemiology == |
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*Procyclic trypomastigotes develop in the midgut then migrate to the salivary glands, where they develop into epimastigotes and then metacyclic trypomastigotes |
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* Present only in sub-Saharan Africa |
|||
* |
*Metacyclic trypomastigotes are transmitted in the saliva during feeding |
||
**Local replication in the trypanosomal chancre followed by lymphatic and hematogenous dissemination |
|||
** Tsetse fly exists only in Africa |
|||
*They multiply in the bloodstream and are thus exposed continuously to the immune system |
|||
* Animal reservoirs include cattle and possibly wild ungulates (''T. b. rhodesiense''); non-human animals are less important for ''T. b. gambiense'' |
|||
**They undergo antigenic variation to periodically change their external glycoprotein structures (VATs) |
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**VAT: variant antigen type |
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==Clinical Manifestations== |
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== Pathophysiology == |
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*Almost all cases lead to death if not treated |
|||
* Procyclic trypomastigotes develop in the midgut then migrate to the salivary glands, where they develop into epimastigotes and then metacyclic trypomastigotes |
|||
* Metacyclic trypomastigotes are transmitted in the saliva during feeding |
|||
** Local replication in the trypanosomal chancre followed by lymphatic and hematogenous dissemination |
|||
* They multiply in the bloodstream and are thus exposed continuously to the immune system |
|||
** They undergo antigenic variation to periodically change their external glycoprotein structures (VATs) |
|||
** VAT: variant antigen type |
|||
===West African trypanosomiasis=== |
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== Clinical Presentation == |
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*Typically more chronic than East African trypanosomiasis |
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* Almost all cases lead to death if not treated |
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====Trypanosomal chancre==== |
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=== West African trypanosomiasis === |
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*Incubation period of 1 to 2 weeks |
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* Typically more chronic than East African trypanosomiasis |
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*Painful, indurated trypanosomal chancre, which resolves after several weeks |
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**May ulcerate |
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**May have regional lymphadenopathy |
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**Often not present |
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==== |
====Stage 1 disease (hemolymphatic)==== |
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* |
*Incubation period [[Usual incubation period::weeks to months]] |
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*Intermittent high fever lasting days, with intervening afebrile periods |
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* Painful, indurated trypanosomal chancre, which resolves after several weeks |
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*Lymphadenopathy develops |
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** May ulcerate |
|||
** |
**'''Winterbottom sign''': enlargement of posterior cervical lymphadenopathy |
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*Hepatosplenomegaly |
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** Often not present |
|||
*Transient edema in face, hands, feed, and periarticular areas |
|||
*Pruritis, often with an irregular erythematous circinate rash on trunk, shoulders, buttocks, and thighs (5-10 cm with central clearing) |
|||
*May also have malaise, headache, weakness, weight loss/cachexia, arthralgias, and tachycardia |
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*Anemia, thrombocytopenia |
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*Mott cells on tissue biopsy |
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==== |
====Stage 2 disease (meningoencephalitic)==== |
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*Multiple neurological manifestations are possible, following months to years of infection |
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* Incubation period weeks to months |
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**Irritability, personality changes, and loss of concentration may be the earliest symptoms |
|||
* Intermittent high fever lasting days, with intervening afebrile periods |
|||
**Progressive indifference with daytime somnolence and sometimes restlessness and insomnia at night |
|||
* Lymphadenopathy develops |
|||
**Headache is common |
|||
** '''Winterbottom sign''': enlargement of posterior cervical lymphadenopathy |
|||
**Extrapyramidal signs with choreiform movements, tremors, fasciculations |
|||
* Hepatosplenomegaly |
|||
**Ataxia |
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* Transient edema in face, hands, feed, and periarticular areas |
|||
**Parkinsonian features |
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* Pruritis, often with an irregular erythematous circinate rash on trunk, shoulders, buttocks, and thighs (5-10 cm with central clearing) |
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**Coma and death over weeks to months |
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* May also have malaise, headache, weakness, weight loss/cachexia, arthralgias, and tachycardia |
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*CSF should be abnormal, with elevated protein and WBCs |
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* Anemia, thrombocytopenia |
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*Extraneurological symptoms may include hypothyroidism and adrenal insufficiency (not necessarily confirmed on bloodwork) |
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* Mott cells on tissue biopsy |
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===East African trypanosomiasis=== |
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==== Stage 2 disease (meningoencephalitic) ==== |
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*Typically more acute than West African trypanosomiasis |
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* Multiple neurological manifestations are possible, following months to years of infection |
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*Incubation period of days to weeks |
|||
** Irritability, personality changes, and loss of concentration may be the earliest symptoms |
|||
*In returned travelers, may present with fever, malaise, and headache |
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** Progressive indifference with daytime somnolence and sometimes restlessness and insomnia at night |
|||
*Fever becomes intermittent and a rash develops |
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** Headache is common |
|||
*Lymphadenopathy is less prominent |
|||
** Extrapyramidal signs with choreiform movements, tremors, fasciculations |
|||
*Persistent tachycardia |
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** Ataxia |
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*No clear distinction between hemolymphatic and meningoencephalitic stages |
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** Parkinsonian features |
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*Patients may die from arrhythmias or heart failure related to pancarditis |
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** Coma and death over weeks to months |
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*Untreated, death within weeks to months |
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* CSF should be abnormal, with elevated protein and WBCs |
|||
* Extraneurological symptoms may include hypothyroidism and adrenal insufficiency (not necessarily confirmed on bloodwork) |
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==Diagnosis== |
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=== East African trypanosomiasis === |
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*Diagnosis requires demonstration of parasite in tissue or fluid on microscopy, '''including CSF in all patients''' |
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* Typically more acute than West African trypanosomiasis |
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**For chancre, express fluid and examine under light microscopy for motile trypanosomes |
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* Incubation period of days to weeks |
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**Fix and stain with Giemsa |
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* In returned travelers, may present with fever, malaise, and headache |
|||
**Aspiration of lymph nodes with kneading (may need multiple aspirates) |
|||
* Fever becomes intermittent and a rash develops |
|||
**Thin and thick Giemsa stained blood films is most useful in hemolymphatic stage |
|||
* Lymphadenopathy is less prominent |
|||
*PCR and LAMP may be sensitive and specific but is not currently well-enough developed |
|||
* Persistent tachycardia |
|||
* No clear distinction between hemolymphatic and meningoencephalitic stages |
|||
* Patients may die from arrhythmias or heart failure related to pancarditis |
|||
* Untreated, death within weeks to months |
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== |
==Management== |
||
*Treatment is more toxic in meningoencephalitic stage |
|||
* Diagnosis requires parasite in tissue or fluid on microscopy, '''including CSF in all patients''' |
|||
*Monitor for side effects during treatment (common) |
|||
** For chancre, express fluid and examine under light microscopy for motile trypanosomes |
|||
** Fix and stain with Giemsa |
|||
** Aspiration of lymph nodes with kneading (may need multiple aspirates) |
|||
** Thin and thick Giemsa stained blood films is most useful in hemolymphatic stage |
|||
* PCR and LAMP may be sensitive and specific but is not currently well-enough developed |
|||
== |
===CDC Guidelines=== |
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{| class="wikitable" |
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* Treatment is more toxic in meningoencephalitic stage |
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!Species |
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!Drug |
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== Side effects of treatment are many == |
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!Adult Dosage |
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!Pediatric Dosage |
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=== CDC Guidelines === |
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{| |
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! Species |
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! Drug |
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! Adult Dosage |
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! Pediatric Dosage |
|||
|- |
|- |
||
| |
|''T. b. rhodesiense'', hemolymphatic stage |
||
| |
|[[Suramin]] |
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| |
|1 gm IV on days 1, 3, 7 ,14, and 21 |
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|20 mg/kg IV on days 1, 3, 7, 14, and 21 |
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|- |
|- |
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| |
|''T. b. rhodesiense'', CNS involvement |
||
| |
|[[Melarsoprol]] |
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| |
|2-3.6 mg/kg/day IV x 3 days. After 7 days, 3.6 mg/kg/day x 3 days. Give a 3rd series of 3.6 mg/kg/d after 7 days. |
||
| |
|2-3.6 mg/kg/day IV x 3 days. After 7 days, 3.6 mg/kg/day x 3 days. Give a 3rd series of 3.6 mg/kg/d after 7 days. |
||
|- |
|- |
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| |
|''T. b. gambiense'', Hemolymphatic stage |
||
| |
|[[Pentamidine]] |
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| |
|4 mg/kg/day IM or IV x 7-10 days |
||
| |
|4 mg/kg/day IM or IV x 7-10 days |
||
|- |
|- |
||
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|''T. b. gambiense'', CNS involvement |
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|[[Eflornithine]] |
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|400 mg/kg/day in 4 doses x 14 days |
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| |
|400 mg/kg/day in 4 doses x 14 days |
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|} |
|} |
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* |
*Patients should be followed with a lumbar puncture every 6 months (or sooner, if symptoms return) for 2 years after treatment to detect a relapse should it occur |
||
* |
*New treatment, [[fexinidazole]], may be a reasonable oral treatment |
||
==Prevention== |
|||
*Vector control programs |
|||
== Prevention == |
|||
*Treatment of infected humans and animals |
|||
*Vector avoidance with insect repellant, long-sleeve clothes, and avoiding known endemic areas |
|||
{{DISPLAYTITLE:''Trypanosoma brucei''}} |
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* Vector control programs |
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[[Category:Protozoa]] |
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* Treatment of infected humans and animals |
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* Vector avoidance with insect repellant, long-sleeve clothes, and avoiding known endemic areas |
|||
Latest revision as of 12:08, 21 August 2020
Background
- Causes African trypanosomiasis, also known as African sleeping sickness
| West African | East African | |
|---|---|---|
| Organism | T. b. gambiense | T. b. rhodesiense |
| Vector | tsetse fly, palpalis group | tsetse fly, morsitans group |
| Habitat | forests and wooded areas | savanna and woodlands |
| Primary reservoir | humans | antelope and cattle |
| Human illness | chronic (late CNS disease) | acute (early CNS disease) |
| Duration of illness | months to years | < 9 months |
| Lymphadenopathy | prominent | minimal |
| Parasitemia | low | high |
| Epidemiology | rural | tourists and workers in game parks/wild areas; rural |
| Treatment | pentamidine (non-CNS) or eflornithin (CNS) | suramin (non-CNS) or melarsoprol (CNS) |
Microbiology
- Vector-borne flagellated protozoan parasite transmitted by the tsetse fly belonging to the genus Trypanosoma, subgenus Trypanozoon
- Two subspecies that are morphologically indistinguishable
- T. b. gambiense, causing chronic African trypanosomiasis (“West African sleeping sickness”)
- T. b. rhodesiense, causing acute African trypanosomiasis (“East African sleeping sickness”)
- Also, T. b. brucei, which infects cattle and occasionally other animals
- No intracellular phase, in contrast to Chagas disease
Epidemiology
- Present only in sub-Saharan Africa
- Transmitted by flies in the genus Glossina (tsetse flies) in their saliva during feeding
- Tsetse flies exists only in Africa
- Animal reservoirs include cattle and possibly wild ungulates (T. b. rhodesiense); non-human animals are less important for T. b. gambiense
Pathophysiology
- Procyclic trypomastigotes develop in the midgut then migrate to the salivary glands, where they develop into epimastigotes and then metacyclic trypomastigotes
- Metacyclic trypomastigotes are transmitted in the saliva during feeding
- Local replication in the trypanosomal chancre followed by lymphatic and hematogenous dissemination
- They multiply in the bloodstream and are thus exposed continuously to the immune system
- They undergo antigenic variation to periodically change their external glycoprotein structures (VATs)
- VAT: variant antigen type
Clinical Manifestations
- Almost all cases lead to death if not treated
West African trypanosomiasis
- Typically more chronic than East African trypanosomiasis
Trypanosomal chancre
- Incubation period of 1 to 2 weeks
- Painful, indurated trypanosomal chancre, which resolves after several weeks
- May ulcerate
- May have regional lymphadenopathy
- Often not present
Stage 1 disease (hemolymphatic)
- Incubation period weeks to months
- Intermittent high fever lasting days, with intervening afebrile periods
- Lymphadenopathy develops
- Winterbottom sign: enlargement of posterior cervical lymphadenopathy
- Hepatosplenomegaly
- Transient edema in face, hands, feed, and periarticular areas
- Pruritis, often with an irregular erythematous circinate rash on trunk, shoulders, buttocks, and thighs (5-10 cm with central clearing)
- May also have malaise, headache, weakness, weight loss/cachexia, arthralgias, and tachycardia
- Anemia, thrombocytopenia
- Mott cells on tissue biopsy
Stage 2 disease (meningoencephalitic)
- Multiple neurological manifestations are possible, following months to years of infection
- Irritability, personality changes, and loss of concentration may be the earliest symptoms
- Progressive indifference with daytime somnolence and sometimes restlessness and insomnia at night
- Headache is common
- Extrapyramidal signs with choreiform movements, tremors, fasciculations
- Ataxia
- Parkinsonian features
- Coma and death over weeks to months
- CSF should be abnormal, with elevated protein and WBCs
- Extraneurological symptoms may include hypothyroidism and adrenal insufficiency (not necessarily confirmed on bloodwork)
East African trypanosomiasis
- Typically more acute than West African trypanosomiasis
- Incubation period of days to weeks
- In returned travelers, may present with fever, malaise, and headache
- Fever becomes intermittent and a rash develops
- Lymphadenopathy is less prominent
- Persistent tachycardia
- No clear distinction between hemolymphatic and meningoencephalitic stages
- Patients may die from arrhythmias or heart failure related to pancarditis
- Untreated, death within weeks to months
Diagnosis
- Diagnosis requires demonstration of parasite in tissue or fluid on microscopy, including CSF in all patients
- For chancre, express fluid and examine under light microscopy for motile trypanosomes
- Fix and stain with Giemsa
- Aspiration of lymph nodes with kneading (may need multiple aspirates)
- Thin and thick Giemsa stained blood films is most useful in hemolymphatic stage
- PCR and LAMP may be sensitive and specific but is not currently well-enough developed
Management
- Treatment is more toxic in meningoencephalitic stage
- Monitor for side effects during treatment (common)
CDC Guidelines
| Species | Drug | Adult Dosage | Pediatric Dosage |
|---|---|---|---|
| T. b. rhodesiense, hemolymphatic stage | Suramin | 1 gm IV on days 1, 3, 7 ,14, and 21 | 20 mg/kg IV on days 1, 3, 7, 14, and 21 |
| T. b. rhodesiense, CNS involvement | Melarsoprol | 2-3.6 mg/kg/day IV x 3 days. After 7 days, 3.6 mg/kg/day x 3 days. Give a 3rd series of 3.6 mg/kg/d after 7 days. | 2-3.6 mg/kg/day IV x 3 days. After 7 days, 3.6 mg/kg/day x 3 days. Give a 3rd series of 3.6 mg/kg/d after 7 days. |
| T. b. gambiense, Hemolymphatic stage | Pentamidine | 4 mg/kg/day IM or IV x 7-10 days | 4 mg/kg/day IM or IV x 7-10 days |
| T. b. gambiense, CNS involvement | Eflornithine | 400 mg/kg/day in 4 doses x 14 days | 400 mg/kg/day in 4 doses x 14 days |
- Patients should be followed with a lumbar puncture every 6 months (or sooner, if symptoms return) for 2 years after treatment to detect a relapse should it occur
- New treatment, fexinidazole, may be a reasonable oral treatment
Prevention
- Vector control programs
- Treatment of infected humans and animals
- Vector avoidance with insect repellant, long-sleeve clothes, and avoiding known endemic areas
