Metacaspases of Trypanosoma cruzi: Possible candidates for programmed cell death mediators
The genome of Trypanosoma cruzi, the Protozoan parasite causing the American Trypanosomiasis, Chagas disease, contains two genes, TcMCA3 and TcMCA5, with homology to those encoding metacaspases, distantly related to the caspases involved in programmed cell death (PCD) in higher eukaryotes. TcMCA3 is...
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Veröffentlicht in: | Molecular and biochemical parasitology 2006, Vol.145 (1), p.18-28 |
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Zusammenfassung: | The genome of
Trypanosoma cruzi, the Protozoan parasite causing the American Trypanosomiasis, Chagas disease, contains two genes,
TcMCA3 and
TcMCA5, with homology to those encoding metacaspases, distantly related to the caspases involved in programmed cell death (PCD) in higher eukaryotes.
TcMCA3 is present in the CL Brener clone at 16 copies per haploid genome, arrayed in two tandems located in chromosomes of 0.54 and 0.98
Mbp.
TcMCA5, on the other hand, is present as a single copy gene. The proteins encoded were expressed in
Escherichia coli BL21 [DE3] cells, and used to generate antibodies, which allowed demonstrating that
TcMCA3 is expressed in the four major developmental stages of the parasite, whereas
TcMCA5 is expressed only in the epimastigote form. Moreover, recombinant
TcMCA3, but not
TcMCA5, was recognized by most sera from chronic Chagasic patients, showing that the protein is expressed during natural infections. All attempts to show processing and enzyme activity in the recombinant proteins have been unsuccesful so far; however, indirect evidence suggests that the metacaspases might be involved in PCD of the parasite. (1) Immunofluorescence experiments showed that both proteins change their subcellular localization during fresh human serum (FHS)-induced PCD migrating into the nucleus. (2) Epimastigotes over-expressing
TcMCA5 were more sensitive to FHS-induced PCD than the controls. (3) PCD was paralelled by an increase in peptidase activity against Z-YVAD-AFC, a typical caspase substrate, and the apoptotic nuclei cells were labeled in vivo with the pan-caspase fluorescent inhibitor SR-VAD-FMK. Further experiments will be required to complete the characterization of these proteins and elucidate their role in the parasite. |
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ISSN: | 0166-6851 1872-9428 |
DOI: | 10.1016/j.molbiopara.2005.09.001 |