Severity of Human African Trypanosomiasis in East Africa Is Associated with Geographic Location, Parasite Genotype, and Host Inflammatory Cytokine Response Profile

Author:

MacLean Lorna1,Chisi John E.2,Odiit Martin3,Gibson Wendy C.4,Ferris Vanessa4,Picozzi Kim5,Sternberg Jeremy M.1

Affiliation:

1. School of Biological Sciences, University of Aberdeen, Aberdeen, United Kingdom

2. College of Medicine, University of Malawi, Blantyre, Malawi

3. Sleeping Sickness Special Programme, LIRI, Tororo, Uganda

4. School of Biological Sciences, University of Bristol, Bristol

5. CTVM, University of Edinburgh, Easter Bush, Roslin

Abstract

ABSTRACT The mechanisms underlying virulence in human African trypanosomiasis are poorly understood, although studies with experimental mice suggest that unregulated host inflammatory responses are associated with disease severity. We identified two trypanosomiasis foci with dramatically different disease virulence profiles. In Uganda, infections followed an acute profile with rapid progression to the late stage (meningoencephalitic infection) in the majority of patients (86.8%). In contrast, infections in Malawi were of a chronic nature, in which few patients progressed to the late stage (7.1%), despite infections of several months' duration. All infections were confirmed to be Trypanosoma brucei rhodesiense by testing for the presence of the serum resistance-associated ( SRA ) gene, but trypanosomes isolated from patients in Uganda or Malawi were distinguished by an SRA gene polymorphism. The two disease profiles were associated with markedly different levels of tumor necrosis factor alpha (TNF-α) and transforming growth factor β (TGF-β) in plasma. In Uganda but not Malawi early-stage TNF-α was elevated, while in Malawi but not Uganda early-stage TGF-β was elevated. Thus, rapid disease progression in Uganda is associated with TNF-α-mediated inflammatory pathology, whereas in the milder disease observed in Malawi this may be ameliorated by counterinflammatory cytokines. These differing host responses may result either from differing virulence phenotypes of northern and southern trypanosomes or from immune response polymorphisms in the different host populations.

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Immunology,Microbiology,Parasitology

Reference27 articles.

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3. Cattand, P., B. T. Miezan, and P. de Raadt. 1988. Human African trypanosomiasis: use of double centrifugation of cerebrospinal fluid to detect trypanosomes. Bull. W. H. O.66:83-86.

4. de Almeida, P. P., M. Ndao, N. Van Meirvenne, and S. Geerts. 1998. Diagnostic evaluation of PCR on dried blood samples from goats experimentally infected with Trypanosoma brucei brucei. Acta Trop.70:269-276.

5. Duggan, A. J., and M. P. Hutchinson. 1966. Sleeping sickness in Europeans: a review of 109 cases. J. Trop. Med. Hyg.69:124-131.

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