Isolation of Trypanosoma brucei gambiense from cured and relapsed sleeping sickness patients and adaptation to laboratory mice

Sleeping sickness due to Trypanosoma brucei (T.b.) gambiense is still a major public health problem in some central African countries. Historically, relapse rates around 5% have been observed for treatment with melarsoprol, widely used to treat second stage patients. Later, relapse rates of up to 50...

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Bibliographic Details
Published in:PLoS neglected tropical diseases 2011-04, Vol.5 (4), p.e1025-e1025
Main Authors: Pyana, Patient Pati, Ngay Lukusa, Ipos, Mumba Ngoyi, Dieudonné, Van Reet, Nick, Kaiser, Marcel, Karhemere Bin Shamamba, Stomy, Büscher, Philippe
Format: Article
Language:English
Subjects:
Adaptation
Adaptation, Biological
Animals
Antiprotozoal Agents - administration & dosage
Blood
Blood - parasitology
Cerebrospinal fluid
Cerebrospinal Fluid - parasitology
Cryopreservation
Diagnosis
Disease
Drug therapy
Female
Humans
Laboratories
Male
Medicine
Melarsoprol - administration & dosage
Mice
Parasites
Patients
Protozoa
Public health
Recurrence
Tropical diseases
Trypanosoma brucei gambiense - growth & development
Trypanosoma brucei gambiense - isolation & purification
Trypanosomiasis
Trypanosomiasis, African - drug therapy
Trypanosomiasis, African - parasitology
Vector-borne diseases
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Summary:Sleeping sickness due to Trypanosoma brucei (T.b.) gambiense is still a major public health problem in some central African countries. Historically, relapse rates around 5% have been observed for treatment with melarsoprol, widely used to treat second stage patients. Later, relapse rates of up to 50% have been recorded in some isolated foci in Angola, Sudan, Uganda and Democratic Republic of the Congo (DRC). Previous investigations are not conclusive on whether decreased sensitivity to melarsoprol is responsible for these high relapse rates. Therefore we aimed to establish a parasite collection isolated from cured as well as from relapsed patients for downstream comparative drug sensitivity profiling. A major constraint for this type of investigation is that T.b. gambiense is particularly difficult to isolate and adapt to classical laboratory rodents. From 360 patients treated in Dipumba hospital, Mbuji-Mayi, D.R. Congo, blood and cerebrospinal fluid (CSF) was collected before treatment. From patients relapsing during the 24 months follow-up, the same specimens were collected. Specimens with confirmed parasite presence were frozen in liquid nitrogen in a mixture of Triladyl, egg yolk and phosphate buffered glucose solution. Isolation was achieved by inoculation of the cryopreserved specimens in Grammomys surdaster, Mastomys natalensis and SCID mice. Thus, 85 strains were isolated from blood and CSF of 55 patients. Isolation success was highest in Grammomys surdaster. Forty strains were adapted to mice. From 12 patients, matched strains were isolated before treatment and after relapse. All strains belong to T.b. gambiense type I. We established a unique collection of T.b. gambiense from cured and relapsed patients, isolated in the same disease focus and within a limited period. This collection is available for genotypic and phenotypic characterisation to investigate the mechanism behind abnormally high treatment failure rates in Mbuji-Mayi, D.R. Congo.
ISSN:1935-2735
1935-2727
1935-2735
DOI:10.1371/journal.pntd.0001025