Affiliation:
1. Department of Pharmacology and Toxicology, Center for AIDS Research, Comprehensive Cancer Center, University of Alabama at Birmingham, Birmingham, Alabama 35294
Abstract
ABSTRACT
Intracellular
Toxoplasma gondii
grown in human foreskin fibroblast cells transported nitrobenzylthioinosine {NBMPR; 6-[(4-nitrobenzyl)mercapto]-9-β-
d
-ribofuranosylpurine}, an inhibitor of nucleoside transport in mammalian cells, as well as the nonphysiological β-
l
-enantiomers of purine nucleosides, β-
l
-adenosine, β-
l
-deoxyadenosine, and β-
l
-guanosine. The β-
l
-pyrimidine nucleosides, β-
l
-uridine, β-
l
-cytidine, and β-
l
-thymidine, were not transported. The uptake of NBMPR and the nonphysiological purine nucleoside β-
l
-enantiomers by the intracellular parasites also implies that
Toxoplasma
-infected cells can transport these nucleosides. In sharp contrast, under the same conditions, uninfected fibroblast cells did not transport NBMPR or any of the unnatural β-
l
-nucleosides. β-
d
-Adenosine and dipyridamole, another inhibitor of nucleoside transport, inhibited the uptake of NBMPR and β-
l
-stereoisomers of the purine nucleosides by intracellular
Toxoplasma
and
Toxoplasma
-infected cells. Furthermore, infection with a
Toxoplasma
mutant deficient in parasite adenosine/purine nucleoside transport reduced or abolished the uptake of β-
d
-adenosine, NBMPR, and purine β-
l
-nucleosides. Hence, the presence of the
Toxoplasma
adenosine/purine nucleoside transporters is apparently essential for the uptake of NBMPR and purine β-
l
-nucleosides by intracellular
Toxoplasma
and
Toxoplasma
-infected cells. These results also demonstrate that, in contrast to the mammalian nucleoside transporters, the
Toxoplasma
adenosine/purine nucleoside transporter(s) lacks stereospecificity and substrate specificity in the transport of purine nucleosides. In addition, infection with
T. gondii
confers the properties of the parasite's purine nucleoside transport on the parasitized host cells and enables the infected cells to transport purine nucleosides that were not transported by uninfected cells. These unique characteristics of purine nucleoside transport in
T. gondii
may aid in the identification of new promising antitoxoplasmic drugs.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Pharmacology (medical),Pharmacology
Reference29 articles.
1. Baer, H. P., A. El-Soofi, and A. Selim. 1988. Treatment of Schistosoma mansoni- and Schistosoma haematobium-infected mice with a combination of tubercidin and nucleoside transport inhibitor. Med. Sci. Res.16:919.
2. Bermudes, D., K. R. Peck, M. A. Afifi, C. J. M. Beckers, and K. A. Joiner. 1994. Tandemly repeated genes encode nucleoside triphosphate hydrolase isoforms secreted into parasitophorous vacuole of Toxoplasma gondii. J. Biol. Chem.269:29252-29260.
3. Carter, N. S., C. Ben Mamoun, W. Liu, E. O. Silva, S. M. Landfear, D. E. Goldberg, and B. Ullman. 2000. Isolation and functional characterization of the PfNT1 nucleoside transporter gene from Plasmodium falciparum. J. Biol. Chem.275:10683-10691.
4. Chiang, C.-W., N. Carter, W. J. Sullivan Jr., R. G. K. Donald, D. S. Roos, F. N. M. Naguib, M. H. el Kouni, B. Ullman, and C. M. Wilson. 1999. The adenosine transporter of Toxoplasma gondii. Identification by insertional mutagenesis, cloning, and recombinant expression. J. Biol. Chem.274:35255-35261.
5. de Koning, H. P., M. I. Al-Salabi, A. M. Cohen, G. H. Coombs, and J. M Wastling. 2003. Identification and characterization of high affinity nucleoside and nucleobase transporters in Toxoplasma gondii. Int. J. Parasitol.33:821-831.
Cited by
30 articles.
订阅此论文施引文献
订阅此论文施引文献,注册后可以免费订阅5篇论文的施引文献,订阅后可以查看论文全部施引文献