RAS-inhibiting biologics identify and probe druggable pockets including an SII-α3 allosteric site

Katarzyna Z. Haza; Heather L. Martin; Ajinkya Rao; Amy L. Turner; Sophie E. Saunders; Britta Petersen; Christian Tiede; Kevin W. Tipping; Anna A Tang; Modupe Ajayi; Michael J. McPherson; Darren C. Tomlinson

doi:https://doi.org/10.1038/s41467-021-24316-0

doi.org/10.1038/s41467-021-24316-0

RAS-inhibiting biologics identify and probe druggable pockets including an SII-α3 allosteric site

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..., Darren C. Tomlinson

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Nature Communications16.60

Volume: 12, Issue: 1

Published: Jun 30, 2021

Abstract

RAS mutations are the most common oncogenic drivers across human cancers, but there remains a paucity of clinically-validated pharmacological inhibitors of RAS, as druggable pockets have proven difficult to identify. Here, we identify two RAS-binding Affimer proteins, K3 and K6, that inhibit nucleotide exchange and downstream signaling pathways with distinct isoform and mutant profiles. Affimer K6 binds in the SI/SII pocket, whilst Affimer K3 is...

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Paper Details

Title

RAS-inhibiting biologics identify and probe druggable pockets including an SII-α3 allosteric site

DOI

doi.org/10.1038/s41467-021-24316-0

Published Date

Jun 30, 2021

Journal

Nature Communications

Volume

12

Issue

1

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