在HEK-293F细胞中对组成型激活的人野生型和S267K 5-HT6受体上配体效力的全谱分析。
Whole spectrum analysis of ligand efficacy at constitutively active human wild-type and S267K 5-HT6 receptors in HEK-293F cells.
作者信息
Romero Gonzalo, Pujol Marta, Pérez Pilar, Buschmann Helmut, Pauwels Petrus J
机构信息
Laboratorios Dr. Esteve S.A., Av. Mare de Déu de Montserrat 221, 08041 Barcelona, Spain.
出版信息
J Pharmacol Toxicol Methods. 2007 Mar-Apr;55(2):144-50. doi: 10.1016/j.vascn.2006.04.007. Epub 2006 May 9.
INTRODUCTION
Modulation of constitutive activity by the recombinant wild-type human 5-HT6 receptor was investigated with a series of 5-HT6 receptor ligands by monitoring the cAMP signalling pathway. The impact of the mutation S267K near the B(261)BXXB(265) CIII-loop motif was analyzed on the magnitude of constitutive receptor activity as previously conflicting results have been reported.
METHODS
The wild-type 5-HT6 receptor plasmid was obtained by PCR and the mutant S267K5-HT6 receptor was constructed by site-directed mutagenesis and stably transfected in HEK-293F cells by electroporation. The cAMP signalling pathway was monitored as a functional read-out to investigate ligands' responses using homogeneous time resolved fluorescence.
RESULTS
Constitutive activity was present both at wild-type and mutant S267K 5-HT6 receptors. Negative efficacy (E(max), % versus basal) as observed at nanomolar concentrations with SB-271046 was larger for mutant (-92+/-1%) than wild-type 5-HT6 receptor (-45+/-1%). Ro 04-6790 also demonstrated negative efficacy at the wild-type 5-HT6 receptor with a magnitude similar to SB-271046 but with a 36-fold lower potency. MS-245 demonstrated at nanomolar concentrations intermediate negative efficacy; -48+/-3% and -16+/-2% at mutant and wild-type 5-HT6 receptor, respectively. The 5-HT-mediated cAMP response was blocked by SB-271046, MS-245 and Ro 04-6790 to their respective level of negative efficacy with pKB values fitting with their binding pK(i) values. E-6801 was a highly potent (pEC50: 10.17 to 10.19) and efficacious agonist (+98 to +102% versus 5-HT) at both wild-type and mutant 5-HT6 receptors.
DISCUSSION
The recombinant wild-type human 5-HT6 receptor is constitutively active in HEK-293F cells and displays a high resolution to monitor efficacy properties of 5-HT6 receptor ligands. The resolution capacity to differentiate between efficacy properties of 5-HT6 receptor ligands, in particular for negative efficacy, can be further enhanced by monitoring the mutant S267K 5-HT6 receptor.
引言
通过监测环磷酸腺苷(cAMP)信号通路,利用一系列5-羟色胺6(5-HT6)受体配体研究重组野生型人5-HT6受体组成性活性的调节。由于之前报道的结果相互矛盾,因此分析了靠近B(261)BXXB(265) CIII环模体的S267K突变对受体组成性活性大小的影响。
方法
通过聚合酶链反应(PCR)获得野生型5-HT6受体质粒,并通过定点诱变构建突变型S267K 5-HT6受体,然后通过电穿孔稳定转染至人胚肾293F(HEK-293F)细胞中。监测cAMP信号通路作为功能读数,使用均相时间分辨荧光来研究配体的反应。
结果
野生型和突变型S267K 5-HT6受体均存在组成性活性。在纳摩尔浓度下,与野生型5-HT6受体(-45±1%)相比,突变型(-92±1%)对SB-271046的负向效力(E(max),相对于基础水平的百分比)更大。Ro 04-6790在野生型5-HT6受体上也表现出负向效力,其大小与SB-271046相似,但效力低36倍。MS-245在纳摩尔浓度下表现出中等负向效力;在突变型和野生型5-HT6受体上分别为-48±3%和-16±2%。5-羟色胺(5-HT)介导的cAMP反应被SB-271046、MS-245和Ro 04-6790阻断至各自的负向效力水平,其平衡解离常数(pKB)值与它们的结合解离常数(pK(i))值相符。E-6801在野生型和突变型5-HT6受体上均为高效能激动剂(半数有效浓度的负对数:10.17至10.19)且有效(相对于5-HT为+98至+102%)。
讨论
重组野生型人5-HT6受体在HEK-293F细胞中具有组成性活性,并对监测5-HT6受体配体的效力特性具有高分辨率。通过监测突变型S267K 5-HT6受体,可以进一步提高区分5-HT6受体配体效力特性的分辨能力,特别是对于负向效力。
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