Competitive binding of MatP and topoisomerase IV to the MukB hinge domain

Author:

Fisher Gemma LM1ORCID,Bolla Jani R23ORCID,Rajasekar Karthik V1ORCID,Mäkelä Jarno1,Baker Rachel1,Zhou Man1,Prince Josh P1ORCID,Stracy Mathew1,Robinson Carol V23,Arciszewska Lidia K1ORCID,Sherratt David J1ORCID

Affiliation:

1. Department of Biochemistry, University of Oxford

2. Physical and Theoretical Chemistry Laboratory, University of Oxford

3. The Kavli Institute for Nanoscience Discovery

Abstract

Structural Maintenance of Chromosomes (SMC) complexes have ubiquitous roles in compacting DNA linearly, thereby promoting chromosome organization-segregation. Interaction between the Escherichia coli SMC complex, MukBEF, and matS-bound MatP in the chromosome replication termination region, ter, results in depletion of MukBEF from ter, a process essential for efficient daughter chromosome individualization and for preferential association of MukBEF with the replication origin region. Chromosome-associated MukBEF complexes also interact with topoisomerase IV (ParC2E2), so that their chromosome distribution mirrors that of MukBEF. We demonstrate that MatP and ParC have an overlapping binding interface on the MukB hinge, leading to their mutually exclusive binding, which occurs with the same dimer to dimer stoichiometry. Furthermore, we show that matS DNA competes with the MukB hinge for MatP binding. Cells expressing MukBEF complexes that are mutated at the ParC/MatP binding interface are impaired in ParC binding and have a mild defect in MukBEF function. These data highlight competitive binding as a means of globally regulating MukBEF-topoisomerase IV activity in space and time.

Funder

Wellcome Trust

Medical Research Council

Publisher

eLife Sciences Publications, Ltd

Subject

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

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