Deregulated DNA ADP-ribosylation impairs telomere replication

Author:

Wondisford Anne R.,Lee JunyeopORCID,Lu Robert,Schuller Marion,Groslambert JosephineORCID,Bhargava Ragini,Schamus-Haynes Sandra,Cespedes Leyneir C.,Opresko Patricia L.ORCID,Pickett Hilda A.ORCID,Min JaewonORCID,Ahel IvanORCID,O’Sullivan Roderick J.ORCID

Abstract

AbstractThe recognition that DNA can be ADP ribosylated provides an unexpected regulatory level of how ADP-ribosylation contributes to genome stability, epigenetics and immunity. Yet, it remains unknown whether DNA ADP-ribosylation (DNA-ADPr) promotes genome stability and how it is regulated. Here, we show that telomeres are subject to DNA-ADPr catalyzed by PARP1 and removed by TARG1. Mechanistically, we show that DNA-ADPr is coupled to lagging telomere DNA strand synthesis, forming at single-stranded DNA present at unligated Okazaki fragments and on the 3′ single-stranded telomere overhang. Persistent DNA-linked ADPr, due to TARG1 deficiency, eventually leads to telomere shortening. Furthermore, using the bacterial DNA ADP-ribosyl-transferase toxin to modify DNA at telomeres directly, we demonstrate that unhydrolyzed DNA-linked ADP-ribose compromises telomere replication and telomere integrity. Thus, by identifying telomeres as chromosomal targets of PARP1 and TARG1-regulated DNA-ADPr, whose deregulation compromises telomere replication and integrity, our study highlights and establishes the critical importance of controlling DNA-ADPr turnover for sustained genome stability.

Publisher

Springer Science and Business Media LLC

Cited by 1 articles. 订阅此论文施引文献 订阅此论文施引文献,注册后可以免费订阅5篇论文的施引文献,订阅后可以查看论文全部施引文献

1. The risky business of ADP-ribosylating telomeric DNA;Nature Structural & Molecular Biology;2024-05

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