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A Recombinant Approach For Stapled Peptide Discovery Yields Inhibitors of the RAD51 Recombinase

View ORCID ProfileTeodors Pantelejevs, Pedro Zuazua-Villar, View ORCID ProfileOliwia Koczy, View ORCID ProfileAndrew Counsell, View ORCID ProfileStephen J. Walsh, View ORCID ProfileNaomi S. Robertson, View ORCID ProfileDavid R. Spring, View ORCID ProfileJessica Downs, View ORCID ProfileMarko Hyvönen
doi: https://doi.org/10.1101/2023.02.24.529929
Teodors Pantelejevs
aDepartment of Biochemistry, University of Cambridge, CB2 1GA, UK
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  • ORCID record for Teodors Pantelejevs
  • For correspondence: teodors.pantelejevs@osi.lv mh256@cam.ac.uk
Pedro Zuazua-Villar
bDivision of Cancer Biology, The Institute of Cancer Research, London SW3 6JB, UK
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Oliwia Koczy
aDepartment of Biochemistry, University of Cambridge, CB2 1GA, UK
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Andrew Counsell
cYusuf Hamied Department of Chemistry, University of Cambridge, CB2 1EW, UK
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Stephen J. Walsh
cYusuf Hamied Department of Chemistry, University of Cambridge, CB2 1EW, UK
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Naomi S. Robertson
cYusuf Hamied Department of Chemistry, University of Cambridge, CB2 1EW, UK
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David R. Spring
cYusuf Hamied Department of Chemistry, University of Cambridge, CB2 1EW, UK
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Jessica Downs
cYusuf Hamied Department of Chemistry, University of Cambridge, CB2 1EW, UK
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Marko Hyvönen
aDepartment of Biochemistry, University of Cambridge, CB2 1GA, UK
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  • For correspondence: teodors.pantelejevs@osi.lv mh256@cam.ac.uk
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Abstract

Stapling is a macrocyclisation method that connects amino acid side chains of a peptide to improve its pharmacological properties. We describe an approach for stapled peptide preparation and biochemical evaluation that combines recombinant expression of fusion constructs of target peptides and cysteine-reactive divinyl-heteroaryl chemistry, as an alternative to solid-phase synthesis. We then employ this workflow to prepare and evaluate BRC-repeat-derived inhibitors of the RAD51 recombinase, showing that a diverse range of secondary structure elements in the BRC repeat can be stapled without compromising binding and function. Using X-ray crystallography, we elucidate the atomic-level features of the staple moieties. We then demonstrate that BRC-repeat-derived stapled peptides can disrupt RAD51 function in cells following ionising radiation treatment.

Competing Interest Statement

The authors have declared no competing interest.

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The copyright holder for this preprint is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity. It is made available under a CC-BY 4.0 International license.
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Posted February 24, 2023.
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A Recombinant Approach For Stapled Peptide Discovery Yields Inhibitors of the RAD51 Recombinase
Teodors Pantelejevs, Pedro Zuazua-Villar, Oliwia Koczy, Andrew Counsell, Stephen J. Walsh, Naomi S. Robertson, David R. Spring, Jessica Downs, Marko Hyvönen
bioRxiv 2023.02.24.529929; doi: https://doi.org/10.1101/2023.02.24.529929
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A Recombinant Approach For Stapled Peptide Discovery Yields Inhibitors of the RAD51 Recombinase
Teodors Pantelejevs, Pedro Zuazua-Villar, Oliwia Koczy, Andrew Counsell, Stephen J. Walsh, Naomi S. Robertson, David R. Spring, Jessica Downs, Marko Hyvönen
bioRxiv 2023.02.24.529929; doi: https://doi.org/10.1101/2023.02.24.529929

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