Papp Ferenc, Batista Cesar V F, Varga Zoltan, Herceg Monika, Román-González Sergio A, Gaspar Rezso, Possani Lourival D, Panyi Gyorgy
Department of Biophysics and Cell Biology, Medical and Health Science Center, University of Debrecen, Nagyerdei krt. 98, Debrecen 4012, Hungary.
Toxicon. 2009 Sep 15;54(4):379-89. doi: 10.1016/j.toxicon.2009.05.023. Epub 2009 Jun 3.
Using high-performance liquid chromatography Tst26, a novel potassium channel blocker peptide, was purified from the venom of the Brazilian scorpion Tityus stigmurus. Its primary structure was determined by means of automatic Edman degradation and mass spectrometry analysis. The peptide is composed of 37 amino acid residues and tightly folded through three disulfide bridges, similar to other K(+) channel blocking peptides purified from scorpion venoms. It contains the "essential dyad" for K(+) channel recognition comprised of a lysine at position 27 and a tyrosine at position 36. Electrophysiological assays revealed that Tst26 blocked hKv1.2 and hKv1.3 channels with high affinity (K(d)=1.9 nM and 10.7 nM, respectively) while it did not affect several other ion channels (mKv1.1, hKv1.4, hKv1.5, hERG, hIKCa1, hBK, hNav1.5) tested at 10 nM concentration. The voltage-dependent steady-state parameters of K(+) channel gating were unaffected by the toxin in both channels, but due to the fast association and dissociation kinetics Tst26 slowed the rate of inactivation of Kv1.3 channels. Based on the primary structure, the systematic nomenclature proposed for this peptide is alpha-KTx 4.6.
使用高效液相色谱法,从巴西蝎子Tityus stigmurus的毒液中纯化出一种新型钾通道阻断肽Tst26。通过自动Edman降解和质谱分析确定了其一级结构。该肽由37个氨基酸残基组成,并通过三个二硫键紧密折叠,类似于从蝎毒中纯化出的其他钾离子通道阻断肽。它含有钾离子通道识别的“必需二元组”,由第27位的赖氨酸和第36位的酪氨酸组成。电生理分析表明,Tst26以高亲和力阻断hKv1.2和hKv1.3通道(K(d)分别为1.9 nM和10.7 nM),而在10 nM浓度下对其他几种离子通道(mKv1.1、hKv1.4、hKv1.5、hERG、hIKCa1、hBK、hNav1.5)没有影响。毒素对两种通道中钾离子通道门控的电压依赖性稳态参数没有影响,但由于快速的结合和解离动力学,Tst26减缓了Kv1.3通道的失活速率。基于一级结构,为该肽提出的系统命名是α-KTx 4.6。
