1998
DOI: 10.1128/mcb.18.10.5643
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Biosynthesis and Function of the Modified DNA Base β-d-Glucosyl-Hydroxymethyluracil in Trypanosoma brucei

Abstract: β-d-Glucosyl-hydroxymethyluracil, also called J, is a modified DNA base conserved among kinetoplastid flagellates. InTrypanosoma brucei, the majority of J is present in repetitive DNA but the partial replacement of thymine by J also correlates with transcriptional repression of the variant surface glycoprotein (VSG) genes in the telomeric VSG gene expression sites. To gain a better understanding of the function of J, we studied its biosynthesis in T. brucei and found that it is made in two steps. In the first … Show more

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Cited by 72 publications
(76 citation statements)
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“…ES derepression was interpreted as a consequence of reduction in J, as incubation with BrdUrd resulted in a 12-fold decrease in the levels of J. However, overproduction of J by incubation with hydroxymethyldeoxyuridine also resulted in derepression of silent sites, making it possible that perturbance of the DNA structure was the critical factor rather than the amount of J itself (65). Although incubation of our T. brucei GFP reporter strain with up to 400 M BrdUrd resulted in silent ES upregulation, levels were not as striking as with the other treatments shown here (results not shown).…”
Section: Up-regulation Of Silent Ess Correlates With a Block In Smentioning
confidence: 99%
“…ES derepression was interpreted as a consequence of reduction in J, as incubation with BrdUrd resulted in a 12-fold decrease in the levels of J. However, overproduction of J by incubation with hydroxymethyldeoxyuridine also resulted in derepression of silent sites, making it possible that perturbance of the DNA structure was the critical factor rather than the amount of J itself (65). Although incubation of our T. brucei GFP reporter strain with up to 400 M BrdUrd resulted in silent ES upregulation, levels were not as striking as with the other treatments shown here (results not shown).…”
Section: Up-regulation Of Silent Ess Correlates With a Block In Smentioning
confidence: 99%
“…This reaction is not specific to the sequence or life cycle-stage as demonstrated by the random placement of base J in the bloodstream and procyclic forms of cells grown with HOMedU included in the medium. 43 A J binding protein (JBP1) was identified in T. brucei and shown to specifically bind to base J in DNA. 49 Subsequently, another trypanosomal protein was discovered to share some N-terminal sequence identity with JBP1 (along with exhibiting homology to the SWI2/SNF2 chromatin remodeling protein family) and named JBP2 even though it does not bind to J-containing DNA.…”
Section: Polynucleotide Hydroxylases 41 Thymidine Hydroxylase Of Promentioning
confidence: 99%
“…41,42 The modified base is thought to induce chromatin compaction and thereby stabilize the chromosome from rearrangements within these repetitive sequences. 43,44 Moreover, base J is suggested to play a role in gene silencing related to the process of antigenic variation. 51 Mutation of putative active-site residues in JBP1 yielded protein that was unable to complement a JBP1 null mutant to restore base J levels.…”
mentioning
confidence: 99%
“…Only one of the 20 expression sites is active at any given time. The presence of J within the ~19 inactive telomeric VSG gene expression sites but not in the active site suggests that J may be involved in the transcriptional repression of VSG gene expression sites and thus, antigenic variation [3,5,6].…”
Section: Introductionmentioning
confidence: 99%
“…In order to analyze the biological function of base J in T. brucei, we need to first characterize the factor(s) regulating Jbiosynthesis. Substantial indirect evidence [6][7][8] indicates that the modification of thymine in trypanosome DNA occurs in two steps: a thymine is oxidized to hydroxymethyluracil (HOMeUra) by a putative thymine-7-hydroxylase (TH), followed by glucosylation of the new base by a putative glucosyltransferase (GT). All current data suggests that the stage specific regulation occurs at the first step, since procyclic-form trypanosomes are able to synthesize J when grown in the presence of hydroxymethyldeoxyuridine (HOMedU), the intermediate in the J-biosysnthesis pathway.…”
Section: Introductionmentioning
confidence: 99%