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Imaging A frican trypanosomes
Author(s) -
M L.,
Myburgh E.,
Rodgers J.,
Price H. P.
Publication year - 2013
Publication title -
parasite immunology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.795
H-Index - 75
eISSN - 1365-3024
pISSN - 0141-9838
DOI - 10.1111/pim.12046
Subject(s) - african trypanosomiasis , biology , trypanosoma brucei , trypanosomiasis , eflornithine , immunology , disease , trypanosoma , virology , pathology , medicine , biochemistry , gene , enzyme , spermidine
Summary T rypanosoma brucei are extracellular kinetoplastid parasites transmitted by the blood‐sucking tsetse fly. They are responsible for the fatal disease human African trypanosomiasis ( HAT ), also known as sleeping sickness. In late‐stage infection, trypanosomes cross the blood–brain barrier ( BBB ) and invade the central nervous system ( CNS ) invariably leading to coma and death if untreated. There is no available vaccine and current late‐stage HAT chemotherapy consists of either melarsoprol, which is highly toxic causing up to 8% of deaths, or nifurtimox–eflornithine combination therapy ( NECT ), which is costly and difficult to administer. There is therefore an urgent need to identify new late‐stage HAT drug candidates. Here, we review how current imaging tools, ranging from fluorescent confocal microscopy of live immobilized cells in culture to whole‐animal imaging, are providing insight into T. brucei biology, parasite‐host interplay, trypanosome CNS invasion and disease progression. We also consider how imaging tools can be used for candidate drug screening purposes that could lead to new chemotherapies.

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