Discovery of a novel template, 7-substituted 7-deaza-4′-thioadenosine derivatives as multi-kinase inhibitors

Karishma K. Mashelkar; Woong Sub Byun; Hyejin Ko; Kisu Sung; Sushil K. Tripathi; Seungchan An; Yun A. Yum; Jee Youn Kwon; Minjae Kim; Gibae Kim; Eun Ji Kwon; Hyuk Woo Lee; Minsoo Noh; Sang Kook Lee; Lak Shin Jeong

doi:10.3390/ph14121290

Discovery of a novel template, 7-substituted 7-deaza-4^′-thioadenosine derivatives as multi-kinase inhibitors

Karishma K. Mashelkar
, Woong Sub Byun
, Hyejin Ko
, Kisu Sung
, Sushil K. Tripathi
, Seungchan An
, Yun A. Yum
, Jee Youn Kwon
, Minjae Kim
, Gibae Kim
, Eun Ji Kwon
, Hyuk Woo Lee
, Minsoo Noh
, Sang Kook Lee
, Lak Shin Jeong

Department of Pharmacy

Research output: Contribution to journal › Article › peer-review

11 Scopus citations

Abstract

The development of anticancer drugs remains challenging owing to the potential for drug resistance. The simultaneous inhibition of multiple targets involved in cancer could overcome resistance, and these agents would exhibit higher potency than single-target inhibitors. Protein kinases represent a promising target for the development of anticancer agents. As most multi-kinase inhibitors are heterocycles occupying only the hinge and hydrophobic region in the ATP binding site, we aimed to design multi-kinase inhibitors that would occupy the ribose pocket, along with the hinge and hydrophobic region, based on ATP-kinase interactions. Herein, we report the discovery of a novel 4^′-thionucleoside template as a multi-kinase inhibitor with potent anticancer activity. The in vitro evaluation revealed a lead 1g (7-acetylene-7-deaza-4^′-thioadenosine) with potent anticancer activity, and marked inhibition of TRKA, CK1δ, and DYRK1A/1B kinases in the kinome scan assay. We believe that these findings will pave the way for developing anticancer drugs.

Original language	English
Article number	1290
Journal	Pharmaceuticals
Volume	14
Issue number	12
DOIs	https://doi.org/10.3390/ph14121290
State	Published - Dec 2021

Keywords

7-deaza-4-thioadenosine derivatives
Anticancer
Multi-kinase inhibitor
Nucleoside

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.3390/ph14121290

Cite this

Mashelkar, K. K., Byun, W. S., Ko, H., Sung, K., Tripathi, S. K., An, S., Yum, Y. A., Kwon, J. Y., Kim, M., Kim, G., Kwon, E. J., Lee, H. W., Noh, M., Lee, S. K., & Jeong, L. S. (2021). Discovery of a novel template, 7-substituted 7-deaza-4^′-thioadenosine derivatives as multi-kinase inhibitors. Pharmaceuticals, 14(12), Article 1290. https://doi.org/10.3390/ph14121290

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title = "Discovery of a novel template, 7-substituted 7-deaza-4′-thioadenosine derivatives as multi-kinase inhibitors",

abstract = "The development of anticancer drugs remains challenging owing to the potential for drug resistance. The simultaneous inhibition of multiple targets involved in cancer could overcome resistance, and these agents would exhibit higher potency than single-target inhibitors. Protein kinases represent a promising target for the development of anticancer agents. As most multi-kinase inhibitors are heterocycles occupying only the hinge and hydrophobic region in the ATP binding site, we aimed to design multi-kinase inhibitors that would occupy the ribose pocket, along with the hinge and hydrophobic region, based on ATP-kinase interactions. Herein, we report the discovery of a novel 4′-thionucleoside template as a multi-kinase inhibitor with potent anticancer activity. The in vitro evaluation revealed a lead 1g (7-acetylene-7-deaza-4′-thioadenosine) with potent anticancer activity, and marked inhibition of TRKA, CK1δ, and DYRK1A/1B kinases in the kinome scan assay. We believe that these findings will pave the way for developing anticancer drugs.",

keywords = "7-deaza-4-thioadenosine derivatives, Anticancer, Multi-kinase inhibitor, Nucleoside",

author = "Mashelkar, \{Karishma K.\} and Byun, \{Woong Sub\} and Hyejin Ko and Kisu Sung and Tripathi, \{Sushil K.\} and Seungchan An and Yum, \{Yun A.\} and Kwon, \{Jee Youn\} and Minjae Kim and Gibae Kim and Kwon, \{Eun Ji\} and Lee, \{Hyuk Woo\} and Minsoo Noh and Lee, \{Sang Kook\} and Jeong, \{Lak Shin\}",

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AU - Mashelkar, Karishma K.

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AU - Ko, Hyejin

AU - Sung, Kisu

AU - Tripathi, Sushil K.

AU - An, Seungchan

AU - Yum, Yun A.

AU - Kwon, Jee Youn

AU - Kim, Minjae

AU - Kim, Gibae

AU - Kwon, Eun Ji

AU - Lee, Hyuk Woo

AU - Noh, Minsoo

AU - Lee, Sang Kook

AU - Jeong, Lak Shin

PY - 2021/12

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N2 - The development of anticancer drugs remains challenging owing to the potential for drug resistance. The simultaneous inhibition of multiple targets involved in cancer could overcome resistance, and these agents would exhibit higher potency than single-target inhibitors. Protein kinases represent a promising target for the development of anticancer agents. As most multi-kinase inhibitors are heterocycles occupying only the hinge and hydrophobic region in the ATP binding site, we aimed to design multi-kinase inhibitors that would occupy the ribose pocket, along with the hinge and hydrophobic region, based on ATP-kinase interactions. Herein, we report the discovery of a novel 4′-thionucleoside template as a multi-kinase inhibitor with potent anticancer activity. The in vitro evaluation revealed a lead 1g (7-acetylene-7-deaza-4′-thioadenosine) with potent anticancer activity, and marked inhibition of TRKA, CK1δ, and DYRK1A/1B kinases in the kinome scan assay. We believe that these findings will pave the way for developing anticancer drugs.

AB - The development of anticancer drugs remains challenging owing to the potential for drug resistance. The simultaneous inhibition of multiple targets involved in cancer could overcome resistance, and these agents would exhibit higher potency than single-target inhibitors. Protein kinases represent a promising target for the development of anticancer agents. As most multi-kinase inhibitors are heterocycles occupying only the hinge and hydrophobic region in the ATP binding site, we aimed to design multi-kinase inhibitors that would occupy the ribose pocket, along with the hinge and hydrophobic region, based on ATP-kinase interactions. Herein, we report the discovery of a novel 4′-thionucleoside template as a multi-kinase inhibitor with potent anticancer activity. The in vitro evaluation revealed a lead 1g (7-acetylene-7-deaza-4′-thioadenosine) with potent anticancer activity, and marked inhibition of TRKA, CK1δ, and DYRK1A/1B kinases in the kinome scan assay. We believe that these findings will pave the way for developing anticancer drugs.

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