Strategic Fluorination to Achieve a Potent, Selective, Metabolically Stable, and Orally Bioavailable Inhibitor of CSNK2

被引:0
|
作者
Ong, Han Wee [1 ,2 ,3 ]
Yang, Xuan [1 ,2 ,3 ]
Smith, Jeffery L. [2 ,3 ]
Taft-Benz, Sharon [1 ,4 ]
Howell, Stefanie [2 ,3 ]
Dickmander, Rebekah J. [1 ,5 ,6 ,7 ]
Havener, Tammy M. [2 ,3 ]
Sanders, Marcia K. [1 ,4 ]
Brown, Jason W. [8 ]
Counago, Rafael M. [2 ,3 ,9 ]
Chang, Edcon [8 ]
Kraemer, Andreas [10 ]
Moorman, Nathaniel J. [1 ,5 ,6 ]
Heise, Mark [1 ,4 ]
Axtman, Alison D. [1 ,2 ,3 ]
Drewry, David H. [1 ,2 ,3 ,6 ]
Willson, Timothy M. [1 ,2 ,3 ]
机构
[1] Rapidly Emerging Antiviral Drug Dev Initiat READDI, Chapel Hill, NC 27599 USA
[2] Univ North Carolina Chapel Hill, Eshelman Sch Pharm, Struct Genom Consortium SGC, Chapel Hill, NC 27599 USA
[3] Univ North Carolina Chapel Hill, Eshelman Sch Pharm, Div Chem Biol & Med Chem, Chapel Hill, NC 27599 USA
[4] Univ North Carolina Chapel Hill, Dept Genet, Chapel Hill, NC 27599 USA
[5] Univ North Carolina Chapel Hill, Dept Microbiol & Immunol, Chapel Hill, NC 27599 USA
[6] Univ North Carolina Chapel Hill, Lineberger Comprehens Canc Ctr, Chapel Hill, NC 27599 USA
[7] Univ North Carolina Chapel Hill, Dept Chem, Chapel Hill, NC 27599 USA
[8] Takeda Dev Ctr Amer Inc, San Diego, CA 92121 USA
[9] Univ Estadual Campinas, Ctr Biol Mol & Engn Genet CBMEG, Ctr Quim Med CQMED, BR-13083875 Campinas, SP, Brazil
[10] Goethe Univ Frankfurt Main, Inst Pharmaceut Chem, Struct Genom Consortium SGC, Max von Laue Str 9, D-60438 Frankfurt, Germany
来源
MOLECULES | 2024年 / 29卷 / 17期
关键词
CSNK2; pyrazolo[1,5-a]pyrimidine; fluorination; antiviral; SARS-CoV-2; beta-coronavirus; CK2; KINASE;
D O I
10.3390/molecules29174158
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The host kinase casein kinase 2 (CSNK2) has been proposed to be an antiviral target against beta-coronaviral infection. To pharmacologically validate CSNK2 as a drug target in vivo, potent and selective CSNK2 inhibitors with good pharmacokinetic properties are required. Inhibitors based on the pyrazolo[1,5-a]pyrimidine scaffold possess outstanding potency and selectivity for CSNK2, but bioavailability and metabolic stability are often challenging. By strategically installing a fluorine atom on an electron-rich phenyl ring of a previously characterized inhibitor 1, we discovered compound 2 as a promising lead compound with improved in vivo metabolic stability. Compound 2 maintained excellent cellular potency against CSNK2, submicromolar antiviral potency, and favorable solubility, and was remarkably selective for CSNK2 when screened against 192 kinases across the human kinome. We additionally present a co-crystal structure to support its on-target binding mode. In vivo, compound 2 was orally bioavailable, and demonstrated modest and transient inhibition of CSNK2, although antiviral activity was not observed, possibly attributed to its lack of prolonged CSNK2 inhibition.
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页数:23
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