6-Amino-2,4,5-trimethylpyridin-3-ol and 2-amino-4,6-dimethylpyrimidin-5-ol derivatives as selective fibroblast growth factor receptor 4 inhibitors: design, synthesis, molecular docking, and anti-hepatocellular carcinoma efficacy evaluation.

Szczegóły
Abstrakt

Tytuł:: 6-Amino-2,4,5-trimethylpyridin-3-ol and 2-amino-4,6-dimethylpyrimidin-5-ol derivatives as selective fibroblast growth factor receptor 4 inhibitors: design, synthesis, molecular docking, and anti-hepatocellular carcinoma efficacy evaluation.
Autorzy:: Chaudhary CL; College of Pharmacy, Yeungnam University, Gyeongsan, Republic of Korea.
Lim D; Innovo Therapeutics Inc, Daejeon, Republic of Korea.
Chaudhary P; College of Pharmacy, Yeungnam University, Gyeongsan, Republic of Korea.
Guragain D; College of Pharmacy, Yeungnam University, Gyeongsan, Republic of Korea.
Awasthi BP; College of Pharmacy, Yeungnam University, Gyeongsan, Republic of Korea.
Park HD; Innovo Therapeutics Inc, Daejeon, Republic of Korea.
Kim JA; College of Pharmacy, Yeungnam University, Gyeongsan, Republic of Korea.
Jeong BS; College of Pharmacy, Yeungnam University, Gyeongsan, Republic of Korea.
Źródło:: Journal of enzyme inhibition and medicinal chemistry [J Enzyme Inhib Med Chem] 2022 Dec; Vol. 37 (1), pp. 844-856.
Typ publikacji:: Journal Article
Język:: English
Imprint Name(s):: Original Publication: Basingstoke, UK : Taylor & Francis, c2002-
MeSH Terms:: Drug Design*
Antineoplastic Agents/*pharmacology
Carcinoma, Hepatocellular/*drug therapy
Liver Neoplasms/*drug therapy
Pyridines/*pharmacology
Pyrimidines/*pharmacology
Animals ; Antineoplastic Agents/chemical synthesis ; Antineoplastic Agents/chemistry ; Carcinoma, Hepatocellular/pathology ; Cell Proliferation/drug effects ; Chickens ; Dose-Response Relationship, Drug ; Humans ; Liver Neoplasms/pathology ; Liver Neoplasms, Experimental/drug therapy ; Liver Neoplasms, Experimental/pathology ; Models, Molecular ; Molecular Structure ; Pyridines/chemical synthesis ; Pyridines/chemistry ; Pyrimidines/chemical synthesis ; Pyrimidines/chemistry ; Structure-Activity Relationship ; Tumor Cells, Cultured
References:: Oncotarget. 2016 Sep 6;7(36):57633-57650. (PMID: 27192118)
Proc Natl Acad Sci U S A. 2002 Aug 20;99(17):11369-74. (PMID: 12172009)
Bioorg Med Chem Lett. 2017 Jun 1;27(11):2420-2423. (PMID: 28433531)
J Med Chem. 2011 Oct 27;54(20):7066-83. (PMID: 21936542)
Cancer Cell. 2011 Mar 8;19(3):347-58. (PMID: 21397858)
Chem Rev. 1996 Dec 19;96(8):3147-3176. (PMID: 11848856)
Mol Cancer Ther. 2019 Dec;18(12):2194-2206. (PMID: 31409633)
ACS Med Chem Lett. 2020 Mar 06;11(10):1899-1904. (PMID: 33062171)
Cancer Discov. 2015 Apr;5(4):424-37. (PMID: 25776529)
J Med Chem. 2020 Oct 22;63(20):11484-11497. (PMID: 33030342)
Int J Cancer. 1995 Apr 10;61(2):170-6. (PMID: 7705943)
Eur J Med Chem. 2014 May 6;78:126-39. (PMID: 24681390)
Future Med Chem. 2018 Oct;10(20):2457-2470. (PMID: 30325210)
Cancer Sci. 2018 Oct;109(10):3024-3031. (PMID: 30070748)
J Chem Inf Model. 2008 Dec;48(12):2371-85. (PMID: 19007114)
Curr Med Chem. 2005;12(1):23-49. (PMID: 15638729)
Sci Rep. 2021 Mar 5;11(1):5303. (PMID: 33674622)
Br J Cancer. 2005 Jan 31;92(2):320-7. (PMID: 15655558)
ACS Med Chem Lett. 2017 Mar 31;8(5):543-548. (PMID: 28523108)
Cancers (Basel). 2019 Jun 18;11(6):. (PMID: 31216701)
Cancer Discov. 2015 Apr;5(4):355-7. (PMID: 25847957)
Cancer Discov. 2019 Dec;9(12):1696-1707. (PMID: 31575541)
Oncotarget. 2016 Mar 22;7(12):13575-86. (PMID: 26498355)
J Enzyme Inhib Med Chem. 2021 Dec;36(1):1884-1897. (PMID: 34340602)
Cancer Discov. 2012 Dec;2(12):1118-33. (PMID: 23002168)
Cancer Cell. 2018 Apr 9;33(4):581-598. (PMID: 29634946)
Thorac Cancer. 2017 Nov;8(6):655-665. (PMID: 28906590)
Int J Mol Sci. 2021 Sep 07;22(18):. (PMID: 34575841)
ACS Med Chem Lett. 2019 Jul 03;10(8):1180-1186. (PMID: 31413803)
EMBO J. 1991 Jun;10(6):1347-54. (PMID: 1709094)
Clin Cancer Res. 2017 Oct 1;23(19):5720-5728. (PMID: 28698202)
Clin Cancer Res. 2016 Jan 1;22(1):259-67. (PMID: 26373574)
CA Cancer J Clin. 2018 Nov;68(6):394-424. (PMID: 30207593)
Pathobiology. 2015;82(6):280-9. (PMID: 26551585)
Cancer Res. 2017 Dec 15;77(24):6999-7013. (PMID: 29247039)
J Hepatol. 2009 Jan;50(1):118-27. (PMID: 19008009)
Contributed Indexing:: Keywords: Aminotrimethylpyri(mi)dinol; FGFR4 kinase; anti-tumour; hepatocellular carcinoma; molecular docking
Substance Nomenclature:: 0 (Antineoplastic Agents)
0 (Pyridines)
0 (Pyrimidines)
Entry Date(s):: Date Created: 20220317 Date Completed: 20220321 Latest Revision: 20220322
Update Code:: 20240105
PubMed Central ID:: PMC8933034
DOI:: 10.1080/14756366.2022.2048378
PMID:: 35296193
: Czasopismo naukowe

Pełny tekst

A novel series of aminotrimethylpyridinol and aminodimethylpyrimidinol derivatives were designed and synthesised for FGFR4 inhibitors. Structure-activity relationship on the FGFR4 inhibitory activity of the new compounds was clearly elucidated by an intensive molecular docking study. Anti-cancer activity of the compounds was evaluated using hepatocellular carcinoma (HCC) cell lines and a chick chorioallantoic membrane (CAM) tumour model. Compound 6O showed FGFR4 inhibitory activity over FGFR1 - 3. Compared to the positive control BLU9931, compound 6O exhibited at least 8 times higher FGFR4 selectivity. Strong anti-proliferative activity of compound 6O was observed against Hep3B, an HCC cell line which was a much more sensitive cell line to BLU9931. In vivo anti-tumour activity of compound 6O against Hep3B-xenografted CAM tumour model was almost similar to BLU9931. Overall, compound 6O , a novel derivative of aminodimethylpyrimidinol, was a selective FGFR4 kinase inhibitor blocking HCC tumour growth.

Informacja