Zhou Zhen, Wang Xiaohui, Li Min, Sohma Yoshiro, Zou Xiaoqin, Hwang Tzyh-Chang
Department of Medical Pharmacology, University of Missouri-Columbia, Columbia, MO 65211, USA.
J Physiol. 2005 Dec 1;569(Pt 2):447-57. doi: 10.1113/jphysiol.2005.095083. Epub 2005 Oct 13.
Previous studies using non-hydrolysable ATP analogues and hydrolysis-deficient cystic fibrosis transmembrane conductance regulator (CFTR) mutants have indicated that ATP hydrolysis precedes channel closing. Our recent data suggest that ATP binding is also important in modulating the closing rate. This latter hypothesis predicts that ATP analogues with higher binding affinities should stabilize the open state more than ATP. Here we explore the possibility of using N6-modified ATP/ADP analogues as high-affinity ligands for CFTR gating, since these analogues have been shown to be more potent than native ATP/ADP in other ATP-binding proteins. Among the three N6-modified ATP analogues tested, N6-(2-phenylethyl)-ATP (P-ATP) was the most potent, with a K(1/2) of 1.6 +/- 0.4 microm (>50-fold more potent than ATP). The maximal open probability (P(o)) in the presence of P-ATP was approximately 30% higher than that of ATP, indicating that P-ATP also has a higher efficacy than ATP. Single-channel kinetic analysis showed that as [P-ATP] was increased, the opening rate increased, whereas the closing rate decreased. The fact that these two kinetic parameters have different sensitivities to changes of [P-ATP] suggests an involvement of two different ATP-binding sites, a high-affinity site modulating channel closing and a low affinity site controlling channel opening. The effect of P-ATP on the stability of open states was more evident when ATP hydrolysis was abolished, either by mutating the nucleotide-binding domain 2 (NBD2) Walker B glutamate (i.e. E1371) or by using the non-hydrolysable ATP analogue AMP-PNP. Similar strategies to develop nucleotide analogues with a modified adenine ring could be valuable for future studies of CFTR gating.
以往使用不可水解的ATP类似物和水解缺陷型囊性纤维化跨膜电导调节因子(CFTR)突变体的研究表明,ATP水解先于通道关闭。我们最近的数据表明,ATP结合在调节关闭速率方面也很重要。后一种假设预测,具有更高结合亲和力的ATP类似物应该比ATP更能稳定开放状态。在这里,我们探讨了使用N6修饰的ATP/ADP类似物作为CFTR门控的高亲和力配体的可能性,因为这些类似物在其他ATP结合蛋白中已被证明比天然ATP/ADP更有效。在所测试的三种N6修饰的ATP类似物中,N6-(2-苯乙基)-ATP(P-ATP)最有效,其K(1/2)为1.6±0.4微摩尔(比ATP强50倍以上)。在P-ATP存在下的最大开放概率(P(o))比ATP高约30%,表明P-ATP也比ATP具有更高的效能。单通道动力学分析表明,随着[P-ATP]的增加,开放速率增加,而关闭速率降低。这两个动力学参数对[P-ATP]变化具有不同敏感性这一事实表明涉及两个不同的ATP结合位点,一个高亲和力位点调节通道关闭,一个低亲和力位点控制通道开放。当通过突变核苷酸结合结构域2(NBD2)的沃克B谷氨酸(即E1371)或使用不可水解的ATP类似物AMP-PNP消除ATP水解时,P-ATP对开放状态稳定性的影响更明显。开发具有修饰腺嘌呤环的核苷酸类似物的类似策略可能对未来CFTR门控的研究有价值。