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  2. Development of a Model for Chemical Screening Based on Collateral Sensitivity to Target BTK C481S Mutant

Development of a Model for Chemical Screening Based on Collateral Sensitivity to Target BTK C481S Mutant

  • Cancers (Basel). 2020 Apr 7;12(4):901. doi: 10.3390/cancers12040901.
Camille Libre 1 Ludovic Moro-Sibilot 1 Stéphane Giraud 2 Laetitia Martin 2 Els Verhoeyen 3 4 Caroline Costa 3 Amel Chebel 1 Nathalie Bissay 1 Gilles Salles 1 Laurent Genestier 1 Pierre Sujobert 1
Affiliations

Affiliations

  • 1 Cancer Research Center of Lyon, INSERM U1052 UMR CNRS 5286, Equipe labellisée Ligue Contre le Cancer, Université de Lyon, 69008 Lyon, France.
  • 2 Center for Drug Discovery and Development (C3D), Fondation Synergie Lyon Cancer, Cancer Research Center of Lyon (CRCL, UMR INSERM 1052 CNRS 5286-Centre Léon Bérard), 69008 Lyon, France.
  • 3 CIRI-International Center for Infectiology Research, Inserm, U1111, Ecole Normale Supérieure de Lyon, Université Lyon 1, CNRS, 69364 UMR5308 Lyon, France.
  • 4 C3M, Université Côte d'Azur, INSERM, 06204 Nice, France.
Abstract

Targeted therapies have improved the outcome of Cancer, but their efficacy is intrinsically limited by the emergence of subclones with a mutation in the gene encoding the target protein. A few examples of collateral sensitivity have demonstrated that the conformational changes induced by these mutations can create unexpected sensitivity to other kinase inhibitors, but whether this concept can be generalized is unknown. Here is described the development of a model to screen a library of kinase inhibitors for collateral sensitivity drugs active on the Bruton Tyrosine Kinase (Btk) protein with the ibrutinib resistance mutation C481S. First, we demonstrate that overexpression of the constitutively active mutant of Btk harboring the E41K mutation in Ba/F3 cells creates an oncogenic addiction to Btk. Then, we have exploited this phenotype to perform a screen of a kinase inhibitor library on cells with or without the ibrutinib resistance mutation. The Btk inhibitors showed the expected sensitivity profile, but none of the drugs tested had a specific activity against the C481S mutant of Btk, suggesting that extending the collateral sensitivity paradigm to all kinases targeted by Cancer therapy might not be trivial.

Keywords

BTK; chemical screen; collateral sensitivity; ibrutinib resistance.

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