Structure and dynamics of the chromatin remodeler ALC1 bound to a PARylated nucleosome

Author:

Bacic Luka1ORCID,Gaullier Guillaume1ORCID,Sabantsev Anton1ORCID,Lehmann Laura C1ORCID,Brackmann Klaus1,Dimakou Despoina1ORCID,Halic Mario2ORCID,Hewitt Graeme3,Boulton Simon J3,Deindl Sebastian1ORCID

Affiliation:

1. Department of Cell and Molecular Biology, Science for Life Laboratory, Uppsala University

2. Department of Structural Biology, St Jude Children's Research Hospital

3. The Francis Crick Institute

Abstract

The chromatin remodeler ALC1 is recruited to and activated by DNA damage-induced poly(ADP-ribose) (PAR) chains deposited by PARP1/PARP2/HPF1 upon detection of DNA lesions. ALC1 has emerged as a candidate drug target for cancer therapy as its loss confers synthetic lethality in homologous recombination-deficient cells. However, structure-based drug design and molecular analysis of ALC1 have been hindered by the requirement for PARylation and the highly heterogeneous nature of this post-translational modification. Here, we reconstituted an ALC1 and PARylated nucleosome complex modified in vitro using PARP2 and HPF1. This complex was amenable to cryo-EM structure determination without cross-linking, which enabled visualization of several intermediate states of ALC1 from the recognition of the PARylated nucleosome to the tight binding and activation of the remodeler. Functional biochemical assays with PARylated nucleosomes highlight the importance of nucleosomal epitopes for productive remodeling and suggest that ALC1 preferentially slides nucleosomes away from DNA breaks.

Funder

European Research Council

Knut och Alice Wallenbergs Stiftelse

Vetenskapsrådet

Cancerfonden

Francis Crick Institute

Wellcome Trust

Cancer Research UK

Publisher

eLife Sciences Publications, Ltd

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,General Medicine,General Neuroscience

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