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Characterization of α-conotoxin TxIB and TxID for smoking cessation and drug rehabilitation
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作者 ZHANGSUN Dong-ting ZHU Xiao-peng +8 位作者 ZHANGSUN Man-qi WU Yong LI Xiao-dan Sean CHRISTENSEN Quentin KAAS Peta J HARVEY David J CRAIK J Michael MCINTOSH LUO Su-lan 《中国药理学与毒理学杂志》 CAS CSCD 北大核心 2018年第9期711-713,共3页
Nicotinic acetylcholine receptors(nAChRs) are widely distributed ligand gated ion channels throughout the peripheral and central nervous systems of mammals.There are 16 different n AChR subunits,α1-α7,α9,α10 and ... Nicotinic acetylcholine receptors(nAChRs) are widely distributed ligand gated ion channels throughout the peripheral and central nervous systems of mammals.There are 16 different n AChR subunits,α1-α7,α9,α10 and β1-β4,as well as γ,δ,and ε,which assemble into pentamers to form different nAChR subtypes with distinct pharmacological properties in mammals.Among them α6β2*(*designates other possible subunit),α3β4 and α4β2 nAChR subtypes are potential therapeutic targets for the treatment of addiction.However,various n AChR subtypes are very difficult to pharmacologically distinguish from each other.The α6* n AChRs are expressed by dopaminergic neurons in the central nervous system,which modulate the release of dopamine and are believed to be important in mediating tobacco,morphine,cocaine and ethanol addiction.The α3β4 nAChRs present in the medial habenula with important role in influencing nicotine addiction.Blockage of α3β4 nAChRs in the medial habenula decreased the dose of nicotine that rodents would self-administer.Thus,new antagonists of α6β2* or α3β4 nA ChR subtypes are of considerable interest,which would give strategies to selectively modulate α6β2* or α3β4 nA ChR function.We characterized an α-conotoxin(α-CTx)TxIB with 16 amino acids and an α-CTx TxID with 15 amino acids from Conus textile.The sequence of TxIB is GCCSDPPCRNKHPDLCamide.The sequence of TxID is GCCSHPVCSAMSPIC with C-terminal amidation too.Both peptides with a Ⅰ-Ⅲ and Ⅱ-Ⅳ disulfide con-nectivity were chemically synthesized.The residues between Cys-Ⅱ and Cys-Ⅲ and Cys-Ⅲand Cys-Ⅳ of α-CTx are commonly referred to as loops 1 and 2,respectively.The number of residues in each of these loops is used to further classify the α-CTx.So TxIB is classified as a 4/7α-CTx,whereas the α-CTx TxIB has a 4/6 spacing.Both peptides were tested on rat nAChRs heterologously expressed in Xenopus laevis oocytes.The α-CTx TxIB blocked α6/α3β2β3 nAChR with an IC50 of 28 nmol·L^(-1),which showed little or no block of all the other tested subtypes at concentrations up to 10 μmol·L^(-1).TxIB blocking α6/α3β2β3 nAChR is rapidly reversed after toxin washout.The ability ofα-CTx TxIB to discriminate between α6/α3β2β3 and the other nAChR receptors is unique.There are no small molecules have this selectivity profile.Previously described α-CTx that potently blockα6/α3β2β3 nA ChR s also block either α6/α3β4 nAChRs,α3β2 nAChRs and(or) other nAChRs subtypes.TxID was the very potent α3β4 nAChR antagonists blocking rat α3β4 n AChRs with an IC-50 of 12.5 nmol·L1.However,TxID also blocked the closely related α6/α3β4 with an IC50 of 94 nmol·L^(-1).In fact,the expression profile ofα3β4 nAChRs and α6/α3β4 nAChRs overlap in a variety of tissues.So TxI D can′t differentiate α3β4 nA ChR from α6/α3β4 nA ChR effectively.To distinguish between these two close subtypes,positional-scanning mutagenesis of TxID was performed to identify critical residues that confer potency for α3β4 nAChRs,and hope to obtain more selective mutant to discriminate between these two close subtypes.The effects of 15 analogues and TxID were tested on both α3β4 and α6/α3β4 nAChRs.An analogue,ie [S9 A]TxID had46-fold greater potency for α3β4 versus α6/α3β4 nAChRs,which showed significantly improved selectivity for α3β4 versus α6/α3β4 nAChRs.Both TxI D and [S9 A]TxI D had little activity on other nA ChR subtypes.The three-dimensional solution structures of TxIB,TxID and [S9 A]TxID were determined using NMR spectroscopy.α-CTx TxI B,TxID and [S9 A]TxID represent uniquely selective ligand for probing the structure and function of α6β2*and α3β4 nA ChR s respectively.It is known about20% people have used drugs recreationally resulting in a substance use disorder finally.Therefore,structural insights derived from these ligands may facilitate the development of novel therapeutics for addiction involving α6β2* and α3β4 nA ChR s. 展开更多
关键词 ACETYLCHOLINE RECEPTORS smokingcessation DRUG REHABILITATION α-conotoxins
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Research Progress on the Influence of Structural Changes inμ-Conotoxins on Sodium Channel Receptors
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作者 Chengzhang LIN Yanling LIAO +1 位作者 Jiao CHEN Bingmiao GAO 《Agricultural Biotechnology》 2023年第6期99-105,共7页
The voltage-gated sodium channel(Na v)is widely present in mammals and can generate cell action potentials,which are related to many diseases.Theμ-Conotoxins(μ-CTx)isolated from the venom of cone snails can specific... The voltage-gated sodium channel(Na v)is widely present in mammals and can generate cell action potentials,which are related to many diseases.Theμ-Conotoxins(μ-CTx)isolated from the venom of cone snails can specifically block the voltage-gated sodium channel;it can be widely used as a necessary probe to distinguish the Na v channel subtypes.In this study,the effects of eightμ-CTx on different Na v channel isoforms were reviewed,and sequence alignment and protein homologous modeling were used to predict their biological activities,and the structure-activity relationship betweenμ-CTx and mutagenesis strategies. 展开更多
关键词 μ-conotoxins voltage-gated sodium channel homologous modeling structure-activity relationship
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α-芋螺毒素TxID异构体对人类乙酰胆碱受体的活性研究 被引量:1
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作者 长孙东亭 朱晓鹏 +3 位作者 吴勇 胡远艳 邴晖 罗素兰 《中国药科大学学报》 CAS CSCD 北大核心 2016年第4期483-490,共8页
研究α-芋螺毒素Tx ID 3个二硫键异构体对人类α3β4与α6/α3β4乙酰胆碱受体的阻断活性。采用Fmoc固相合成法,分别合成α-芋螺毒素Tx ID的3个二硫键异构体的线性肽,利用2步氧化法进行氧化折叠,获得具有定点连接二硫键的异构体多肽。... 研究α-芋螺毒素Tx ID 3个二硫键异构体对人类α3β4与α6/α3β4乙酰胆碱受体的阻断活性。采用Fmoc固相合成法,分别合成α-芋螺毒素Tx ID的3个二硫键异构体的线性肽,利用2步氧化法进行氧化折叠,获得具有定点连接二硫键的异构体多肽。利用非洲爪蟾卵母细胞表达人类α3β4与α6/α3β4乙酰胆碱受体亚型,测定3个异构体对该乙酰胆碱受体的电流与洗脱速率的影响情况。α-芋螺毒素Tx ID的3个二硫键异构体对人类α3β4与α6/α3β4乙酰胆碱受体亚型的阻断活性差异很大,阻断是可逆的,洗脱速率较快。其中具有天然构象的球状异构体活性最强,其半数阻断剂量(IC50)仅约为9.3 nmol/L;其次是带状异构体具有很微弱的抑制活性,其IC50大于5μmol/L;而珠子状异构体几乎没有阻断活性,其IC50大于10μmol/L。成功合成了α-芋螺毒素Tx ID的3个二硫键异构体,并获知了3个二硫键异构体分别对人类α3β4与α6/α3β4乙酰胆碱受体亚型的阻断活性,为α-芋螺毒素Tx ID后续海洋新药研发提供理论基础。 展开更多
关键词 α-芋螺毒素Tx ID 二硫键异构体 多肽人工合成 人类α3β4乙酰胆碱受体 人类α6/α3β4乙酰胆碱受体
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α-芋螺毒素TxID对肺癌的细胞毒性 被引量:1
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作者 钱江 孙志华 +3 位作者 刘益巧 谢品希 长孙东亭 罗素兰 《热带生物学报》 2019年第2期99-105,共7页
对α-芋螺毒素TxID在小细胞肺癌DMS114中的细胞毒性进行研究。使用两步氧化法对α-芋螺毒素TxID进行合成,质谱鉴定TxID,并通过高效液相色谱(HPLC)确定其纯度;对DMS114中的α3和β4 nAChR亚基进行克隆;使用MTT试验检测α-芋螺毒素TxID单... 对α-芋螺毒素TxID在小细胞肺癌DMS114中的细胞毒性进行研究。使用两步氧化法对α-芋螺毒素TxID进行合成,质谱鉴定TxID,并通过高效液相色谱(HPLC)确定其纯度;对DMS114中的α3和β4 nAChR亚基进行克隆;使用MTT试验检测α-芋螺毒素TxID单用或与阿霉素(ADM)联用对DMS114和HEL细胞的细胞毒性作用。本实验通过固相合成和两步氧化法,成功制备了α-芋螺毒素TxID;通过基因克隆实验,在DMS114细胞中检测到α3和β4 nAChR亚基;细胞毒性试验表明α-芋螺毒素TxID对肺癌细胞DMS114和正常细胞HEL都具有细胞毒性且在一定浓度TxID对肺癌细胞的毒性大于正常细胞;此外,TxID和ADM等比联用对DMS114细胞的毒性大于各自单独给药之和。本研究首次证明α3β4 nAChR特异性阻断剂α-芋螺毒素TxID能够抑制小细胞肺癌DMS114的增殖并具有细胞毒性作用,可为新型抗癌药物的研究与开发提供指导。 展开更多
关键词 α-芋螺毒素txid 小细胞肺癌 α3β4烟碱型乙酰胆碱受体 基因克隆 细胞毒性
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Alpha-芋螺毒素TxID合成方法的优化
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作者 吴勇 朱芙蓉 +2 位作者 刘倩 长孙东亭 罗素兰 《热带生物学报》 2014年第2期107-110,135,共5页
在常规两步氧化法合成的基础上,对芋螺毒素TxID第2对二硫键形成的条件进行了优化.优化条件包括有无氮气保护、氧化试剂中碘的浓度、三氟乙酸(TFA)含量、氧化时间等多个参数,研究其对TxID氧化折叠的影响.结果表明,氮气保护有利于TxID... 在常规两步氧化法合成的基础上,对芋螺毒素TxID第2对二硫键形成的条件进行了优化.优化条件包括有无氮气保护、氧化试剂中碘的浓度、三氟乙酸(TFA)含量、氧化时间等多个参数,研究其对TxID氧化折叠的影响.结果表明,氮气保护有利于TxID的氧化折叠,碘浓度需5~10倍于巯基浓度,TFA含量对氧化折叠影响不明显,氧化时间约5 min为宜. 展开更多
关键词 α-芋螺毒素txid 化学合成 碘氧化 优化 二硫键形成
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α-芋螺毒素TxID对亚基不同配比α3β4乙酰胆碱受体的敏感性研究 被引量:3
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作者 长孙东亭 吴勇 +1 位作者 朱晓鹏 罗素兰 《中国药学杂志》 CAS CSCD 北大核心 2016年第10期802-808,共7页
目的研究α-芋螺毒素TxID对具有不同亚基配比组成的大鼠α3β4乙酰胆碱受体(nAChRs)的阻断活性敏感性。方法利用非洲爪蟾卵母细胞表达大鼠α3β4乙酰胆碱受体亚型,将其亚基α3和β4的cRNA分别以3种不同比例,即1∶1、1∶10或10∶1注射到... 目的研究α-芋螺毒素TxID对具有不同亚基配比组成的大鼠α3β4乙酰胆碱受体(nAChRs)的阻断活性敏感性。方法利用非洲爪蟾卵母细胞表达大鼠α3β4乙酰胆碱受体亚型,将其亚基α3和β4的cRNA分别以3种不同比例,即1∶1、1∶10或10∶1注射到非洲爪蟾卵母细胞中进行表达,形成不同亚基配比的α3β4受体,分别检测和比较α-芋螺毒素TxID对这些不同亚基配比受体的阻断活性。结果成功表达了α3和β4亚基的3个不同配比的受体,且α-芋螺毒素TxID对它们的敏感性有较大差异,与常规的1∶1α3β4乙酰胆碱受体相比,1∶10α3β4乙酰胆碱受体对TxID的敏感度与之接近,其活性差异在2倍以内,而10∶1α3β4乙酰胆碱受体对TxID的敏感度显著下降,其活性差异超过了5倍。结论α-芋螺毒素TxID对不同亚基配比的α3β4乙酰胆碱受体有不同的敏感性,并能反应该受体的α和β亚基不同的组成方式,这对于研究α3β4乙酰胆碱受体的结构和生理功能具有很重要的指导意义。 展开更多
关键词 α-芋螺毒素txid α3β4乙酰胆碱受体 非洲爪蟾卵母细胞 α和β亚基配比 活性敏感性
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A novel ω-conotoxin Bu8 inhibiting N-type voltage-gated calcium channels displays potent analgesic activity 被引量:4
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作者 Jinqin Chen Xinhong Liu +5 位作者 Shuo Yu Jia Liu Rongfang Chen Yunxiao Zhang Ling Jiang Qiuyun Dai 《Acta Pharmaceutica Sinica B》 SCIE CAS CSCD 2021年第9期2685-2693,共9页
ω-Conotoxins inhibit N-type voltage-gated calcium(Ca_(v)2.2)channels and exhibit efficacy in attenuating neuropathic pain but have a low therapeutic index.Here,we synthesized and characterized a novelω-conotoxin,Bu8... ω-Conotoxins inhibit N-type voltage-gated calcium(Ca_(v)2.2)channels and exhibit efficacy in attenuating neuropathic pain but have a low therapeutic index.Here,we synthesized and characterized a novelω-conotoxin,Bu8 from Conus bullatus,which consists of 25 amino acid residues and three disulfide bridges.Bu8 selectively and potently inhibits depolarization-activated Ba^(2+ )currents mediated by rat Ca_(v)2.2 expressed in HEK293 T cells(IC_(50)=89 nmol/L).Bu8 is two-fold more potent thanω-conotoxin MVIIA,aω-conotoxin currently used for the treatment of severe chronic pain.It also displays potent analgesic activity in animal pain models of hot plate and acetic acid writhing but has fewer side effects on mouse motor function and lower toxicity in goldfish.Its lower side effects may be attributed to its faster binding rate and higher recovery ratios.The NMR structure demonstrates that Bu8 contains a small irregular tripleβ-strand.The structure-activity relationships of Bu8 Ala mutants and Bu8/MVIIA hybrid mutants demonstrate that the binding mode of Ca_(v)2.2 with the amino acid residues in loop 1 and loop 2 of Bu8 is different from that of MVIIA.This study characterizes a novel,more potentω-conotoxin and provides new insights for designing Ca_(v)2.2 antagonists. 展开更多
关键词 N-type calcium ion channel ω-conotoxin Bu8 Analgesic activity Structure-activity relationship
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Watermark in the Digital Video Broadcasting Handheld Transmission Signal
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作者 胡玲娜 蒋铃鸽 +1 位作者 何晨 杨峰 《Journal of Shanghai Jiaotong university(Science)》 EI 2009年第2期149-153,共5页
Transmitter identification(TxID) technique is used to diagnose the operation status of radio transmitters in DTV distributed transmission network.A new TxID method for digital video broadcasting-handheld (DVB-H) syste... Transmitter identification(TxID) technique is used to diagnose the operation status of radio transmitters in DTV distributed transmission network.A new TxID method for digital video broadcasting-handheld (DVB-H) system is proposed.Watermark is embedded in the DVB-H signal to form the composite signal.According to watermarking theory we demonstrate the required signal level for watermarking signal to achieve given bit error probability under different circumstance.By selecting the reference pattern to generate watermarking signal,peak-to-average power ratio(PAPR) of the transmitted signal can be improved.Simulation results show that even in wireless situation the receiver can distinguish the watermarking signal with low embedding strength, and distortion to the host signal can also be ignored. 展开更多
关键词 transmitter identification txid WATERMARK peak-to-average power ratio (PAPR)
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