All the mutations that are fit to die

Emma Gebauer,Markus A. Seeliger

CELL CHEMICAL BIOLOGY(2024)

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摘要
In this issue of Cell Chemical Biology, Chakraborty et al.1 employ a deep mutational screening analysis of 3,500 single point mutations in every residue in Src kinase’s catalytic domain to determine which residues are critical for conferring ATP-competitive inhibitor resistance. They identify a dynamically controlled resistance site.
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