Proteome-wide Map of Targets of T790M-EGFR-Directed Covalent Inhibitors

Niessen, Sherry; Dix, Melissa M.; Barbas, Sabrina; Potter, Zachary E.; Lu, Shuyan; Brodsky, Oleg; Planken, Simon; Behenna, Douglas C.; Almaden, Chau; Gajiwala, K.S.; Ryan, Kevin; Ferre, RoseAnn; Lazear, Michael R.; Hayward, Matthew M.; Kath, John C.; Cravatt, Benjamin F.

doi:10.1016/j.chembiol.2017.08.017

Cited by 86 publications

(67 citation statements)

References 58 publications

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“…To assess the structural impact of the EGFR G724S mutation on the EGFR kinase we performed structural analysis based on a previously published co-crystal structure of rociletinib bound to EGFR (PDB ID: 5UWD) (Fig. 3a ) 30 . As described before the glycine-rich loop is an essential element for ligand binding and the glycine at position 724 is in direct contact with the adjacent ELREA motif that is subject to deletion mutations in affected patients.…”

Section: Resultsmentioning

confidence: 99%

“…As described before the glycine-rich loop is an essential element for ligand binding and the glycine at position 724 is in direct contact with the adjacent ELREA motif that is subject to deletion mutations in affected patients. The ELREA sequence plays a crucial role in the alignment of the regulatory helix αC that is a key element in the transition between the active and inactive kinase domain conformations 30 . It is therefore conceivable that the EGFR G724S mutation influences structure and dynamics of the binding site and thereby the affinity toward third-generation EGFR inhibitors.…”

Section: Resultsmentioning

confidence: 99%

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Overcoming EGFRG724S-mediated osimertinib resistance through unique binding characteristics of second-generation EGFR inhibitors

et al. 2018

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The emergence of acquired resistance against targeted drugs remains a major clinical challenge in lung adenocarcinoma patients. In a subgroup of these patients we identified an association between selection of EGFRT790M-negative but EGFRG724S-positive subclones and osimertinib resistance. We demonstrate that EGFRG724S limits the activity of third-generation EGFR inhibitors both in vitro and in vivo. Structural analyses and computational modeling indicate that EGFRG724S mutations may induce a conformation of the glycine-rich loop, which is incompatible with the binding of third-generation TKIs. Systematic inhibitor screening and in-depth kinetic profiling validate these findings and show that second-generation EGFR inhibitors retain kinase affinity and overcome EGFRG724S-mediated resistance. In the case of afatinib this profile translates into a robust reduction of colony formation and tumor growth of EGFRG724S-driven cells. Our data provide a mechanistic basis for the osimertinib-induced selection of EGFRG724S-mutant clones and a rationale to treat these patients with clinically approved second-generation EGFR inhibitors.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Overcoming EGFRG724S-mediated osimertinib resistance through unique binding characteristics of second-generation EGFR inhibitors

et al. 2018

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“…Dacomitinib is a pan-erythroblastic leukemia viral oncogene homologue (ERBB) inhibitor which targets wildtype and mutant forms of EGFR that possess activating L858R or exon 19 deletion mutations in addition to T790M mutation 42,43 . For the purpose of our study, we utilized the A431 epidermoid cancer cell line as it was previously reported to be characterized by a high expression of wildtype EGFR 44 , and has been utilized in experiments profiling EGFR covalent inhibitors 45,46 .…”

Section: Resultsmentioning

confidence: 99%

Evaluation and Optimization of Chemically-Cleavable Linkers for Quantitative Mapping of Small Molecule-Protein Interactomes

Rabalski

Bogdan

Baranczak

2019

Preprint

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Numerous reagents have been developed to enable chemical proteomic analysis of small molecule-protein interactomes. However, the performance of these reagents has not been systematically evaluated and compared. Herein, we report our efforts to conduct a parallel assessment of two widely-used chemically-cleavable linkers equipped with dialkoxydiphenylsilane (DADPS linker) and azobenzene (AZO linker) moieties. Profiling a cellular cysteinome using iodoacetamide alkyne probe demonstrated a significant discrepancy between the experimental results obtained through the application of each of the reagents. To better understand the source of observed discrepancy, a mass tolerant database search strategy using MSFragger software was performed. This resulted in identifying a previously unreported artifactual modification on the residual mass of the azobenzene linker. Furthermore, we conducted a comparative analysis of enrichment modes using both cleavable linkers. This effort determined that enrichment of proteolytic digests yielded a far greater number of identified cysteine residues than the enrichment conducted prior to protein digest. Inspired by recent studies where multiplexed quantitative labeling strategies were applied to cleavable biotin linkers, we combined this further optimized protocol using the DADPS cleavable linker with tandem mass tag (TMT) labeling to profile the FDA-approved covalent EGFR kinase inhibitor dacomitinib against the cysteinome of an epidermoid cancer cell line. Our analysis resulted in the detection and quantification of over 10,000 unique cysteine residues, a nearly 3-fold increase over previous studies that used cleavable biotin linkers for enrichment. Critically, cysteine residues corresponding to proteins directly as well as indirectly modulated by dacomitinib treatment were identified. Overall, our study suggests that the dialkoxydiphenylsilane linker could be broadly applied wherever chemically cleavable linkers are required for chemical proteomic characterization of cellular proteomes.

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“…Derivatisation of ABX‐1431 with an alkyne enrichment handle (ABX‐1431_ABP, Figure B) confirmed CNS penetrance and in vivo target engagement by ABX‐1431 in the mouse brain after a 4 h treatment with a single 25 mg kg −1 oral dose . This general approach has also been used to profile the cysteine‐targeted covalent drugs afatinib (EGFR inhibitor) and ibrutinib (BTK inhibitor), as well as the newly developed third generation EGFR inhibitors osimertinib, PF‐06747775 and rociletinib . Additionally, a dichlorotriazine‐based probe has been utilised recently to label bromodomains on lysine and tyrosine residues, and the high selectivity profile of a lysine‐targeted covalent inhibitor of the lipid kinase PI3Kδ was also determined using similar strategies …”

Section: Target Engagement and Selectivity Profilingmentioning

confidence: 87%