Discovery of a Potent Dual SLK/STK10 Inhibitor Based on a Maleimide Scaffold

Ricardo A. M. Serafim; Fiona J. Sorrell; Benedict-Tilman Berger; Ross J. Collins; Stanley N. S. Vasconcelos; Katlin B. Massirer; Stefan Knapp; James Bennett; Oleg Fedorov; Hitesh Patel; William J. Zuercher; Jonathan M. Elkins

doi:10.1021/acs.jmedchem.0c01579

Discovery of a Potent Dual SLK/STK10 Inhibitor Based on a Maleimide Scaffold

Ricardo A. M. Serafim, Fiona J. Sorrell, Benedict-Tilman Berger, Ross J. Collins, Stanley N. S. Vasconcelos, Katlin B. Massirer, Stefan Knapp, James Bennett, Oleg Fedorov, Hitesh Patel, William J. Zuercher, Jonathan M. Elkins

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Resum

SLK (STE20-like kinase) and STK10 (serine/threonine kinase 10) are closely related kinases whose enzymatic activity is linked to the regulation of ezrin, radixin, and moesin function and to the regulation of lymphocyte migration and the cell cycle. We identified a series of 3-anilino-4-arylmaleimides as dual inhibitors of SLK and STK10 with good kinome-wide selectivity. Optimization of this series led to multiple SLK/STK10 inhibitors with nanomolar potency. Crystal structures of exemplar inhibitors bound to SLK and STK10 demonstrated the binding mode of the inhibitors and rationalized their selectivity. Cellular target engagement assays demonstrated the binding of the inhibitors to SLK and STK10 in cells. Further selectivity analyses, including analysis of activity of the reported inhibitors against off-targets in cells, identified compound 31 as the most potent and selective inhibitor of SLK and STK10 yet reported.

Idioma original	Anglès
Pàgines (de-a)	13259-13278
Nombre de pàgines	20
Revista	Journal of Medicinal Chemistry
Volum	64
Número	18
Data online anticipada	31 d’ag. 2021
DOIs	https://doi.org/10.1021/acs.jmedchem.0c01579
Estat de la publicació	Publicada - 23 de set. 2021
Publicat externament	Sí

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10.1021/acs.jmedchem.0c01579

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Serafim, R. A. M., Sorrell, F. J., Berger, B.-T., Collins, R. J., Vasconcelos, S. N. S., Massirer, K. B., Knapp, S., Bennett, J., Fedorov, O., Patel, H., Zuercher, W. J., & Elkins, J. M. (2021). Discovery of a Potent Dual SLK/STK10 Inhibitor Based on a Maleimide Scaffold. Journal of Medicinal Chemistry, 64(18), 13259-13278. https://doi.org/10.1021/acs.jmedchem.0c01579

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title = "Discovery of a Potent Dual SLK/STK10 Inhibitor Based on a Maleimide Scaffold",

abstract = "SLK (STE20-like kinase) and STK10 (serine/threonine kinase 10) are closely related kinases whose enzymatic activity is linked to the regulation of ezrin, radixin, and moesin function and to the regulation of lymphocyte migration and the cell cycle. We identified a series of 3-anilino-4-arylmaleimides as dual inhibitors of SLK and STK10 with good kinome-wide selectivity. Optimization of this series led to multiple SLK/STK10 inhibitors with nanomolar potency. Crystal structures of exemplar inhibitors bound to SLK and STK10 demonstrated the binding mode of the inhibitors and rationalized their selectivity. Cellular target engagement assays demonstrated the binding of the inhibitors to SLK and STK10 in cells. Further selectivity analyses, including analysis of activity of the reported inhibitors against off-targets in cells, identified compound 31 as the most potent and selective inhibitor of SLK and STK10 yet reported.",

keywords = "Ste20-like kinase slk, Binding, Domain, Phosphorylation, Activation, Apoptosis, Lok",

author = "Serafim, \{Ricardo A. M.\} and Sorrell, \{Fiona J.\} and Benedict-Tilman Berger and Collins, \{Ross J.\} and Vasconcelos, \{Stanley N. S.\} and Massirer, \{Katlin B.\} and Stefan Knapp and James Bennett and Oleg Fedorov and Hitesh Patel and Zuercher, \{William J.\} and Elkins, \{Jonathan M.\}",

year = "2021",

month = sep,

day = "23",

doi = "10.1021/acs.jmedchem.0c01579",

language = "English",

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T1 - Discovery of a Potent Dual SLK/STK10 Inhibitor Based on a Maleimide Scaffold

AU - Serafim, Ricardo A. M.

AU - Sorrell, Fiona J.

AU - Berger, Benedict-Tilman

AU - Collins, Ross J.

AU - Vasconcelos, Stanley N. S.

AU - Massirer, Katlin B.

AU - Knapp, Stefan

AU - Bennett, James

AU - Fedorov, Oleg

AU - Patel, Hitesh

AU - Zuercher, William J.

AU - Elkins, Jonathan M.

PY - 2021/9/23

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N2 - SLK (STE20-like kinase) and STK10 (serine/threonine kinase 10) are closely related kinases whose enzymatic activity is linked to the regulation of ezrin, radixin, and moesin function and to the regulation of lymphocyte migration and the cell cycle. We identified a series of 3-anilino-4-arylmaleimides as dual inhibitors of SLK and STK10 with good kinome-wide selectivity. Optimization of this series led to multiple SLK/STK10 inhibitors with nanomolar potency. Crystal structures of exemplar inhibitors bound to SLK and STK10 demonstrated the binding mode of the inhibitors and rationalized their selectivity. Cellular target engagement assays demonstrated the binding of the inhibitors to SLK and STK10 in cells. Further selectivity analyses, including analysis of activity of the reported inhibitors against off-targets in cells, identified compound 31 as the most potent and selective inhibitor of SLK and STK10 yet reported.

AB - SLK (STE20-like kinase) and STK10 (serine/threonine kinase 10) are closely related kinases whose enzymatic activity is linked to the regulation of ezrin, radixin, and moesin function and to the regulation of lymphocyte migration and the cell cycle. We identified a series of 3-anilino-4-arylmaleimides as dual inhibitors of SLK and STK10 with good kinome-wide selectivity. Optimization of this series led to multiple SLK/STK10 inhibitors with nanomolar potency. Crystal structures of exemplar inhibitors bound to SLK and STK10 demonstrated the binding mode of the inhibitors and rationalized their selectivity. Cellular target engagement assays demonstrated the binding of the inhibitors to SLK and STK10 in cells. Further selectivity analyses, including analysis of activity of the reported inhibitors against off-targets in cells, identified compound 31 as the most potent and selective inhibitor of SLK and STK10 yet reported.

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KW - Binding

KW - Domain

KW - Phosphorylation

KW - Activation

KW - Apoptosis

KW - Lok

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Discovery of a Potent Dual SLK/STK10 Inhibitor Based on a Maleimide Scaffold

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