Affiliation:
1. Laboratory of Molecular Parasitology, The Rockefeller University, New York, New York
Abstract
ABSTRACT
Putative TTAGGG repeat-binding factor (TRF) homologues in the genomes of
Trypanosoma brucei
,
Trypanosoma cruzi
, and
Leishmania major
were identified. They have significant sequence similarity to higher eukaryotic TRFs in their C-terminal DNA-binding myb domains but only weak similarity in their N-terminal domains.
T. brucei
TRF (tbTRF) is essential and was shown to bind to duplex TTAGGG repeats. The RNA interference-mediated knockdown of tbTRF arrested bloodstream cells at G
2
/M and procyclic cells partly at S phase. Functionally, tbTRF resembles mammalian TRF2 more than TRF1, as knockdown diminished telomere single-stranded G-overhang signals. This suggests that tbTRF, like vertebrate TRF2, is essential for telomere end protection, and this also supports the hypothesis that TRF rather than Rap1 is the more ancient DNA-binding component of the telomere protein complex. Identification of the first
T. brucei
telomere DNA-binding protein and characterization of its function provide a new route to explore the roles of telomeres in pathogenesis of this organism. This work also establishes
T. brucei
as an attractive model for telomere biology.
Publisher
American Society for Microbiology
Subject
Cell Biology,Molecular Biology
Cited by
75 articles.
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