DNA double strand break position leads to distinct gene expression changes and regulates VSG switching pathway choice

Author:

Thivolle AlixORCID,Mehnert Ann-KathrinORCID,Tihon Eliane,McLaughlin Emilia,Dujeancourt-Henry AnnickORCID,Glover LucyORCID

Abstract

Antigenic variation is an immune evasion strategy used by Trypanosoma brucei that results in the periodic exchange of the surface protein coat. This process is facilitated by the movement of variant surface glycoprotein genes in or out of a specialized locus known as bloodstream form expression site by homologous recombination, facilitated by blocks of repetitive sequence known as the 70-bp repeats, that provide homology for gene conversion events. DNA double strand breaks are potent drivers of antigenic variation, however where these breaks must fall to elicit a switch is not well understood. To understand how the position of a break influences antigenic variation we established a series of cell lines to study the effect of an I-SceI meganuclease break in the active expression site. We found that a DNA break within repetitive regions is not productive for VSG switching, and show that the break position leads to a distinct gene expression profile and DNA repair response which dictates how antigenic variation proceeds in African trypanosomes.

Funder

Institut Pasteur

Agence Nationale de la Recherche

Erasmus+

Horizon 2020

Foundation Recherché Médicale

Publisher

Public Library of Science (PLoS)

Subject

Virology,Genetics,Molecular Biology,Immunology,Microbiology,Parasitology

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