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7,9-二溴二氢二苯并呋喃作为一种有效的酪蛋白激酶2(CK2)抑制剂的发现:合成、生物学评价及对异构体的结构研究

Discovery of 7,9-Dibromo-dihydrodibenzofuran as a Potent Casein Kinase 2 (CK2) Inhibitor: Synthesis, Biological Evaluation, and Structural Studies on /-Isomers.

作者信息

Rumler Hendrik, Schmithals Claudia, Werner Christian, Bollacke Andre, Aichele Dagmar, Götz Claudia, Niefind Karsten, Wünsch Bernhard, Jose Joachim

机构信息

University of Münster, Institute of Pharmaceutical and Medicinal Chemistry, Pharmacampus, Münster 48149, Germany.

Institute of Biochemistry, University of Cologne, Cologne 50674, Germany.

出版信息

ACS Pharmacol Transl Sci. 2024 Nov 19;7(12):3846-3866. doi: 10.1021/acsptsci.4c00426. eCollection 2024 Dec 13.

DOI:10.1021/acsptsci.4c00426
PMID:39698287
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11651316/
Abstract

The human protein kinase CK2 is a promising target for cancer treatment. Only two CK2 inhibitors have reached clinical trials until today. Among others, a dibenzofuran scaffold has emerged as highly prospective for the development of new CK2 inhibitors. Thirty-three newly synthesized dibenzofuran-based compounds were tested on their inhibitory potential . 7,9-Dichloro-8-hydroxy-4-[(phenylamino)methylene]-1,2-dihydro-dibenzo[,]furan-3(4)-one () and 7,9-dibromo-8-hydroxy-4-[(phenylamino)methylene]-1,2-dihydro-dibenzo[,]furan-3(4)-one () showed the lowest IC values with 5.8 nM for both. The dibenzofuran-based CK2 inhibitors crossed the cell membrane of LNCaP human prostate carcinoma cells and reduced intracellular CK2 activity. Among 70 kinases from different representative subgroups of the human kinome, CK2 was most strongly inhibited by compound . Co-crystallization of together with CK2α indicated a π-halogen bond of the bromine at position C9 with the gatekeeper amino acid Phe113. CK2α could bind both the - and -isomers of . Our results provide new insights into the structure-activity relationships of dibenzofuran derivatives.

摘要

人类蛋白激酶CK2是癌症治疗中一个很有前景的靶点。截至目前,只有两种CK2抑制剂进入了临床试验阶段。其中,二苯并呋喃支架已成为开发新型CK2抑制剂的极具前景的结构。对33种新合成的基于二苯并呋喃的化合物进行了抑制潜力测试。7,9-二氯-8-羟基-4-[(苯胺基)亚甲基]-1,2-二氢-二苯并[,]呋喃-3(4)-酮()和7,9-二溴-8-羟基-4-[(苯胺基)亚甲基]-1,2-二氢-二苯并[,]呋喃-3(4)-酮()的IC值最低,均为5.8 nM。基于二苯并呋喃的CK2抑制剂能够穿过LNCaP人前列腺癌细胞的细胞膜并降低细胞内CK2活性。在人类激酶组不同代表性亚组的70种激酶中,化合物对CK2的抑制作用最强。与CK2α的共结晶表明,C9位的溴与守门氨基酸Phe113形成了π-卤键。CK2α可以结合的 -异构体和 -异构体。我们的结果为二苯并呋喃衍生物的构效关系提供了新的见解。