Hydrophobic Derivatives of Glycopeptide Antibiotics as Inhibitors of Protein Kinases

被引:0
|
作者
G. Cozza
M. Fortuna
F. Meggio
S. Sarno
M. H. G. Kubbutat
F. Totzke
C. Schaechtele
L. A. Pinna
E. N. Olsufyeva
M. N. Preobrazhenskaya
机构
[1] University of Padova,Department of Molecular Medicine
[2] University of Padova,Department of Biological Chemistry
[3] University of Padova,Department of Biomedical Sciences
[4] ProQinase GmbH,undefined
[5] Center for Neuroscience Research Neuroscience Institute,undefined
[6] Gause Institute of New Antibiotics,undefined
来源
Biochemistry (Moscow) | 2018年 / 83卷
关键词
polycyclic glycopeptide derivatives; protein kinases; antiviral activity;
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学科分类号
摘要
As key regulators of cell signaling, protein kinases (PKs) are attractive targets for therapeutic intervention in a variety of diseases. Herein, we report for the first time the inhibitory activity of polycyclic peptides, particularly, derivatives of glycopeptide antibiotics teicoplanin and eremomycin, against a panel of 12 recombinant human protein kinases and two protein kinases (CK1 and CK2) isolated from rat liver. Several of the investigated compounds inhibited various PKs with IC50 values below 10 μM and caused >90% suppression of the enzyme activity at 10 μM concentration. Kinetic analysis of the protein kinase CK2α inhibition by the teicoplanin aglycon analogue (7) demonstrated the non-competitive mechanism of inhibition (with regard to ATP). Interestingly, the inhibitory activity of some investigated compounds correlated with the earlier described antiviral activity against HIV, HCV, and other corona- and flaviviruses.
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页码:1222 / 1230
页数:8
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