Vinylpyridine as a Tunable Covalent Warhead Targeting C797 in EGFR

Vinylpyridine as a Tunable Covalent Warhead Targeting C797 in EGFR

To further facilitate the discovery of cysteine reactive covalent inhibitors, there is a need to develop new reactive groups beyond the traditional acrylamide-type warheads. Herein we describe the design and synthesis of covalent EGFR inhibitors that use vinylpyridine as the reactive group. Structur...

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Veröffentlicht in:ACS medicinal chemistry letters 2024-05, Vol.15 (5), p.583-589
Hauptverfasser: Pemberton, Nils, Compagne, Nina, Argyrou, Argyrides, Evertsson, Emma, Gunnarsson, Anders, Kettle, Jason G., Orme, Jonathan P., Ward, Richard A.
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container_end_page 589
container_issue 5
container_start_page 583
container_title ACS medicinal chemistry letters
container_volume 15
creator Pemberton, Nils
Compagne, Nina
Argyrou, Argyrides
Evertsson, Emma
Gunnarsson, Anders
Kettle, Jason G.
Orme, Jonathan P.
Ward, Richard A.
description To further facilitate the discovery of cysteine reactive covalent inhibitors, there is a need to develop new reactive groups beyond the traditional acrylamide-type warheads. Herein we describe the design and synthesis of covalent EGFR inhibitors that use vinylpyridine as the reactive group. Structure-based design identified the quinazoline-containing vinylpyridine 6 as a starting point. Further modifications focused on reducing reactivity resulted in substituted vinyl compound 12, which shows high EGFR potency and good kinase selectivity, as well as significantly reduced reactivity compared to the starting compound 6, confirming that vinylpyridines can be applied as an alternative cysteine reactive warhead with tunable reactivity.
doi_str_mv 10.1021/acsmedchemlett.3c00425
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title Vinylpyridine as a Tunable Covalent Warhead Targeting C797 in EGFR
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