UMSBP2 is chromatin remodeler that functions in regulation of gene expression and suppression of antigenic variation in trypanosomes

Author:

Soni Awakash1,Klebanov-Akopyan Olga1,Erben Esteban2,Plaschkes Inbar3,Benyamini Hadar3,Mitesser Vera1ORCID,Harel Amnon4,Yamin Katereena4ORCID,Onn Itay4ORCID,Shlomai Joseph1

Affiliation:

1. Department of Microbiology and Molecular Genetics, Institute for Medical Research Israel- Canada and the Kuvin Center for the Study of Infectious and Tropical Diseases, The Hebrew University of Jerusalem , Jerusalem  91120 , Israel

2. Heidelberg University Center for Molecular Biology at Heidelberg University, DKFZ-ZMBH Alliance, Im Neuenheimer Feld 282 , 69120 Heidelberg , Germany

3. The Info-Core Bioinformatics Unit, Faculty of Medicine, The Hebrew University of Jerusalem, Jerusalem 91120 , Israel

4. Azrieli Faculty of Medicine, Bar-Ilan University , 8 Henrietta Szold Street , Safed 1311502 , Israel

Abstract

Abstract Universal Minicircle Sequence binding proteins (UMSBPs) are CCHC-type zinc-finger proteins that bind the single-stranded G-rich UMS sequence, conserved at the replication origins of minicircles in the kinetoplast DNA, the mitochondrial genome of kinetoplastids. Trypanosoma brucei UMSBP2 has been recently shown to colocalize with telomeres and to play an essential role in chromosome end protection. Here we report that TbUMSBP2 decondenses in vitro DNA molecules, which were condensed by core histones H2B, H4 or linker histone H1. DNA decondensation is mediated via protein-protein interactions between TbUMSBP2 and these histones, independently of its previously described DNA binding activity. Silencing of the TbUMSBP2 gene resulted in a significant decrease in the disassembly of nucleosomes in T. brucei chromatin, a phenotype that could be reverted, by supplementing the knockdown cells with TbUMSBP2. Transcriptome analysis revealed that silencing of TbUMSBP2 affects the expression of multiple genes in T. brucei, with a most significant effect on the upregulation of the subtelomeric variant surface glycoproteins (VSG) genes, which mediate the antigenic variation in African trypanosomes. These observations suggest that UMSBP2 is a chromatin remodeling protein that functions in the regulation of gene expression and plays a role in the control of antigenic variation in T. brucei.

Funder

Israel Science Foundation

The Hebrew University of Jerusalem

Publisher

Oxford University Press (OUP)

Subject

Genetics

Reference90 articles.

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1. Deviating from the norm: Nuclear organisation in trypanosomes;Current Opinion in Cell Biology;2023-12

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