Literature DB >> 32084124

Identification of a novel base J binding protein complex involved in RNA polymerase II transcription termination in trypanosomes.

Rudo Kieft1, Yang Zhang1, Alexandre P Marand2, Jose Dagoberto Moran1, Robert Bridger1, Lance Wells1, Robert J Schmitz2, Robert Sabatini1.   

Abstract

Base J, β-D-glucosyl-hydroxymethyluracil, is a modification of thymine DNA base involved in RNA Polymerase (Pol) II transcription termination in kinetoplastid protozoa. Little is understood regarding how specific thymine residues are targeted for J-modification or the mechanism of J regulated transcription termination. To identify proteins involved in J-synthesis, we expressed a tagged version of the J-glucosyltransferase (JGT) in Leishmania tarentolae, and identified four co-purified proteins by mass spectrometry: protein phosphatase (PP1), a homolog of Wdr82, a potential PP1 regulatory protein (PNUTS) and a protein containing a J-DNA binding domain (named JBP3). Gel shift studies indicate JBP3 is a J-DNA binding protein. Reciprocal tagging, co-IP and sucrose gradient analyses indicate PP1, JGT, JBP3, Wdr82 and PNUTS form a multimeric complex in kinetoplastids, similar to the mammalian PTW/PP1 complex involved in transcription termination via PP1 mediated dephosphorylation of Pol II. Using RNAi and analysis of Pol II termination by RNA-seq and RT-PCR, we demonstrate that ablation of PNUTS, JBP3 and Wdr82 lead to defects in Pol II termination at the 3'-end of polycistronic gene arrays in Trypanosoma brucei. Mutants also contain increased antisense RNA levels upstream of transcription start sites, suggesting an additional role of the complex in regulating termination of bi-directional transcription. In addition, PNUTS loss causes derepression of silent Variant Surface Glycoprotein genes involved in host immune evasion. Our results suggest a novel mechanistic link between base J and Pol II polycistronic transcription termination in kinetoplastids.

Entities:  

Year:  2020        PMID: 32084124     DOI: 10.1371/journal.pgen.1008390

Source DB:  PubMed          Journal:  PLoS Genet        ISSN: 1553-7390            Impact factor:   5.917


  11 in total

1.  ZC3H4 restricts non-coding transcription in human cells.

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Authors:  Wei Wang; Duo Peng; Rodrigo P Baptista; Yiran Li; Jessica C Kissinger; Rick L Tarleton
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3.  Genetic Interaction Between Site-Specific Epigenetic Marks and Roles of H4v in Transcription Termination in Trypanosoma brucei.

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Review 4.  Impact of Genetic Diversity and Genome Plasticity of Leishmania spp. in Treatment and the Search for Novel Chemotherapeutic Targets.

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5.  Target highlights in CASP14: Analysis of models by structure providers.

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6.  Common and unique features of glycosylation and glycosyltransferases in African trypanosomes.

Authors:  Samuel M Duncan; Michael A J Ferguson
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Review 7.  Read, Write, Adapt: Challenges and Opportunities during Kinetoplastid Genome Replication.

Authors:  Jeziel D Damasceno; Catarina A Marques; Jennifer Black; Emma Briggs; Richard McCulloch
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Review 8.  Histone Modifications and Other Facets of Epigenetic Regulation in Trypanosomatids: Leaving Their Mark.

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Journal:  mBio       Date:  2020-09-01       Impact factor: 7.867

Review 9.  A nuclear enterprise: zooming in on nuclear organization and gene expression control in the African trypanosome.

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Journal:  Parasitology       Date:  2021-01-07       Impact factor: 3.234

Review 10.  Genetic and immunological basis of human African trypanosomiasis.

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