Design and characterization of a novel structural class of Kv1.3 inhibitors

被引:7
|
作者
Hendrickx, Louise Antonia [1 ]
Dobricic, Vladimir [2 ]
Toplak, Zan [3 ]
Peigneur, Steve [1 ]
Masic, Lucija Peterlin [3 ]
Tomasic, Tihomir [3 ]
Tytgat, Jan [1 ]
机构
[1] Univ Leuven KUL, Toxicol & Pharmacol, Campus Gasthuisberg,Onderwijs & Navorsing 2, B-3000 Leuven, Belgium
[2] Univ Belgrade, Fac Pharm, Dept Pharmaceut Chem, Vojvode Stepe 450, Belgrade 11221, Serbia
[3] Univ Ljubljana, Fac Pharm, Askerceva 7, Ljubljana 1000, Slovenia
关键词
MEMORY T-CELLS; GAUSSIAN DESCRIPTION; K+ CHANNEL; TARGET; BLOCKERS;
D O I
10.1016/j.bioorg.2020.103746
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 voltage-gated potassium channel K(v)1.3 is involved in multiple autoimmune diseases, such as multiple sclerosis, rheumatoid arthritis, diabetes mellitus type 1 and psoriasis. In many auto-immune diseases better treatment options are desired as existing therapies are often ineffective or become less effective over time, for which K(v)1.3 inhibitors arise as promising candidates. In this study, five compounds were selected based on a 3D similarity searching methodology and subsequently screened ex vivo on the K(v)1.3 channel. The screening resulted in two compounds inhibiting the K(v)1.3 channel, of which TVS-12 was the most potent compound, while TVS-06 -although less potent- showed an excellent selectivity for K(v)1.3 For both compounds the mechanism of action was investigated by an electrophysiological characterization on the K(v)1.3 channel and three K(v)1.3 mutants, designed to resemble the pore region of K(v)1.2 channels. Structurally, the presence of a benzene ring and/or an oxane ring seems to cause a better interaction with the K(v)1.3 channel, resulting in a 20-fold higher potency for TVS-12.
引用
收藏
页数:9
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