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Behind Base J: The Roles of JBP1 and JBP2 on Trypanosomatids.


ABSTRACT: β-D-glucopyranosyloxymethiluracil (Base J) is a modified thymidine base found in kinetoplastids and some related organisms. Interestingly, Base J distribution into the genome can vary depending on the organism and its life stage. Base J is reported to be found mostly at telomeric repeats, on inactive variant surface glycoproteins (VSG's) expression sites (e.g., T. brucei), in RNA polymerase II termination sites and sub-telomeric regions (e.g., Leishmania). This hypermodified nucleotide is synthesized in two steps with the participation of two distinct thymidine hydroxylases, J-binding protein 1 and 2 (JBP1 and JBP2, respectively) and a β-glucosyl transferase. A third J-binding protein, named JBP3, was recently identified as part of a multimeric complex. Although its structural similarities with JBP1, it seems not to be involved in J biosynthesis but to play roles in gene expression regulation in trypanosomatids. Over the years, with the characterization of JBP1 and JBP2 mutant lines, Base J functions have been targeted and shone a light on that matter, showing genus-specific features. This review aims to explore Base J's reported participation as a regulator of RNA polymerase II transcription termination and to summarize the functional and structural characteristics and similarities of the remarkable JBP proteins in pathogenic trypanosomatids.

SUBMITTER: Assis LHC 

PROVIDER: S-EPMC10057400 | biostudies-literature | 2023 Mar

REPOSITORIES: biostudies-literature

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Behind Base J: The Roles of JBP1 and JBP2 on Trypanosomatids.

Assis Luiz Henrique de Castro LHC   de Paiva Stephany Cacete SC   Cano Maria Isabel Nogueira MIN  

Pathogens (Basel, Switzerland) 20230316 3


β-D-glucopyranosyloxymethiluracil (Base J) is a modified thymidine base found in kinetoplastids and some related organisms. Interestingly, Base J distribution into the genome can vary depending on the organism and its life stage. Base J is reported to be found mostly at telomeric repeats, on inactive variant surface glycoproteins (VSG's) expression sites (e.g., <i>T. brucei</i>), in RNA polymerase II termination sites and sub-telomeric regions (e.g., <i>Leishmania</i>). This hypermodified nucleo  ...[more]

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