新型N-型钙通道抑制剂的发现、优化及作用机理研究
基本信息
结项摘要
N-type calcium channel modulates the release of neurotransmitters in the pre-synaptic nerve terminals in lamina I and II of the dorsal horn of the spinal cord, and is the important target for the analgesics of neuropathic pain, inflammatory pain, allodynia and hyperalgesia. Recently, a potent analgesic alpha-conopeptide T5, which derived from Conus snail of China South Sea, have been firstly found to be a potent blocker of N-type calcium channel expressed in human embryonic kidney cell HEK 293, but it is weak for neuronal nicotinic acetylcholine receptors (nAChR). On the base of the above discovery, this project will use several methods, such as patch-clamp technique, molecular biology, molecular docking and dynamics simulations and chronic pain models, to investigate the selectivity of T5 to GABAb receptor-mediated N-type calcium channels and other voltage-dependent calcium channels and its effects on some typical signal molecules involved in pain, and elucidate the difference of this kind of N-type calcium channel inhibitors from omega-conopeptide N-type calcium channel inhibitors. This project will also screen new N-type calcium channel inhibitors among other alpha-conopeptides and other conopeptides that do not belong to omega-conopetides. Based on the structures of new N-type calcium channel inhibitors and molecular simulations, the structures of specific N-type calcium channel inhibitors and bifunctional inhibitors for N-type calcium channel and nAChR subtypes, such as alpha3beta2 and alpha9alpha10, will be optimized.After this work, the highly potent analgesics for chronic pain will be found.
N-型钙通道调控脊柱背角I及II的突触前神经末端等的神经递质释放,是治疗病理性慢性疼痛、炎症痛、异常疼等重要靶点。前期我们首次发现来自我国南海芋螺的一个α-芋螺镇痛多肽T5对人胚肾细胞HEK293表达的N-型钙通道具有较高活性,但对神经元烟碱型乙酰胆碱受体亚型很弱。本课题拟在已有工作的基础上,应用膜片钳、分子生物学、分子计算模拟及慢性疼痛模型等,开展该新型N-型钙通道抑制剂对GABAb介导的N-型钙通道、其他钙通道等的选择性及对有关镇痛信号通路的影响,阐明其与ω-芋螺多肽型N-型钙通道抑制剂的作用机制区别,进一步筛选其他α-芋螺多肽、非ω-芋螺多肽是否也作用于N-型钙通道,并结合α-、ω-芋螺多肽型抑制剂与N-型钙通道作用的分子模拟结果,优化特异作用于新型N-型钙通道抑制剂或作用于神经元型乙酰胆碱受体亚型及N-型钙通道的多靶点抑制剂,以期获得对慢性疼痛镇痛活性更高先导化合物。
项目摘要
为获得具有镇痛活性新型N-型钙通道(Cav2.2)抑制剂,本课题开展了如下四个方面研究:(1)α-芋螺多肽T5(Eb1.6)作用靶标、结构活性关系、镇痛活性、副作用以及对镇痛信号通路研究;(2)α-芋螺多肽Eb1.6与Vt1.27与ω-芋螺多肽Cav2.2抑制剂崁合肽设计合成及活性评价;(3)新型ω-芋螺多肽类Cav2.2抑制剂筛选及优化;(4)ω-芋螺多肽SO-3、MVIIA结构活性关系、毒副作用研究。取得如下主要结果:(1)确定了α-芋螺多肽T5(Eb1.6)作用靶标为Cav2.2,该肽对大鼠慢性疼痛模型具有很高的镇痛活性(nmol/kg级),且副作用低;(2)合成了35个α-芋螺毒素Eb1.6(T5)、Vt1.27及上述多肽与SO-3 loop2崁合体,发现一些多肽对Cav2.2抑制率较高,10 microM多肽的抑制率为25-37%;(3)研究了Eb1.6(T5)给药后对镇痛有关的信号通路分子的影响,如NMDAR、C-fos、ATF3、GABAR、PICK1、AMPAR、PKC-γ、BDNF、TRPV1、GAP-43、NGF-β、TPH1等,结果表明Eb1.6能显著提高BDNF、NGF-β及NMDAR基因表达量,显著降低AMPAR、GABAR基因及蛋白的表达量以及CaMKII-β蛋白的表达量;(4)合成了10个含三对二硫键可能作用于Cav2.2的新型多肽,完成了其对Cav2.2的抑制活性测定,发现了一条多肽Bu8比MVIIA活性高两倍,且专一性作用于Cav2.2,不作用于Nav1.7、Nav1.8,对P/Q型、L型钙离子通道的活性低;(5)系统地研究了Bu8结构活性关系,溶液NMR结构及CD谱显示Bu8含有典型β折叠,Ser6、Ser7、Ser12、Asn22氨基酸对Cav2.2结合活性影响不显著,而Bu8[R3A]、Bu8[R9A]、Bu8[T11A]结合活性与Bu8相比分别下降了2倍、5倍和10倍,说明Arg3、Arg9、Thr11是与Cav2.2结合关键氨基酸。(6)获得较SO-3活性高的突变体两个;(7)研究了SO-3与MVIIA崁合肽的镇痛活性(包括PNL模型)、毒副作用(金鱼毒性、自发活动,运动协同性),发现了MVIIA的毒副作用关键残基Met12。目前发表Sci论文3篇(2篇大于4),中文2篇(还有一篇在审),参与编写专著2部。
项目成果
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数据更新时间:2023-05-31
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