Cryo-EM structure of the Smc5/6 holo-complex

Author:

Hallett Stephen T1ORCID,Campbell Harry Isabella1,Schellenberger Pascale2ORCID,Zhou Lihong1ORCID,Cronin Nora B3,Baxter Jonathan1ORCID,Etheridge Thomas J1ORCID,Murray Johanne M1ORCID,Oliver Antony W1ORCID

Affiliation:

1. Genome Damage and Stability Centre, School of Life Sciences, University of Sussex , Falmer , UK

2. Electron Microscopy Imaging Centre, School of Life Sciences, University of Sussex , Falmer , UK

3. London Consortium for CryoEM (LonCEM) Facility, The Francis Crick Institute , London , UK

Abstract

Abstract The Smc5/6 complex plays an essential role in the resolution of recombination intermediates formed during mitosis or meiosis, or as a result of the cellular response to replication stress. It also functions as a restriction factor preventing viral replication. Here, we report the cryogenic EM (cryo-EM) structure of the six-subunit budding yeast Smc5/6 holo-complex, reconstituted from recombinant proteins expressed in insect cells – providing both an architectural overview of the entire complex and an understanding of how the Nse1/3/4 subcomplex binds to the hetero-dimeric SMC protein core. In addition, we demonstrate that a region within the head domain of Smc5, equivalent to the ‘W-loop’ of Smc4 or ‘F-loop’ of Smc1, mediates an important interaction with Nse1. Notably, mutations that alter the surface-charge profile of the region of Nse1 which accepts the Smc5-loop, lead to a slow-growth phenotype and a global reduction in the chromatin-associated fraction of the Smc5/6 complex, as judged by single molecule localisation microscopy experiments in live yeast. Moreover, when taken together, our data indicates functional equivalence between the structurally unrelated KITE and HAWK accessory subunits associated with SMC complexes.

Funder

Wellcome Trust

University of Sussex

Wellcome

Cancer Research UK

MRC

Publisher

Oxford University Press (OUP)

Subject

Genetics

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