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Cis-dioxo-metal complex ( NH3CH2CH2NH2 ) 2.5 [ Mo0.5^(V)W0.5^(VI)O2 ( OC6H4O ) 2] 1 was obtained by the reaction of tetra-butyl ammonium hexamolybdotungstate with 1, 2-dihydroxybenzene in the mixed solvent of CH3OH, CH3CN and ethylenediamine,and characterized by X-ray diffraction, UV-vis and EPR analysis. Compared with its analogous complexes (NH3CH2CH2NH2)3[Mo^(V)O2(OC6H40)2] 2 and (NH3CH2CH2NH2)2[W^(VI)O2(OC6H4O)2] 3, the results show that tungsten(VI) is less active in redox than molybdenum (VI) and that the change of the valence induced by substitution of W(VI) for Mo(V) in EMO2(OC6H40)2]n- does not influence the coordination geometry of the complex anion in which the metal center exhibits distorted octahedral coordination with cis-dioxo catechol. The responses to EPR of complexes 1 and 2 are active but complex 3 is silent,and the UV-vis spectra exhibited by the three complexes are obvious different because of the different electronic configuration between the central Mo(V) and W(VI) ions in the complexes.It is noteworthy that complexes 1 and 2 have the similar EPR signal to flavoenzyme, suggesting that the three complexes have the same coordination geometry feature with the co-factor of flavoenzyme. 相似文献
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Crystal Structure and EPR Spectra of cis—Dioxo—molybdenum(V) Complex with o—Aminophenol 总被引:1,自引:0,他引:1
IntroductionMolybdenumiswidelyusedinbiologicalsystemsduetothetwobasicforms :nitrogenasesandoxotransferasesoroxomolybdoenzymes .Thelatterasthemononuclearactivesitesofamuchmorediversegroupofenzymesingeneralfunctioncatalyticallytransferanoxygenatomeithert… 相似文献
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拮抗状态下α1A,α1B和α1D-肾上腺素能受体的分子模拟研究 总被引:1,自引:0,他引:1
采用同源建模法对α1A-,α1B-和α1D-AR的三维结构进行了模拟,并采用分子力学、分子动力学方法对所得同源模型进行优化,然后分别采用训练集拮抗剂对接的方法得到拮抗状态下的α1A-,α1B-和α1D-AR三维结构模型.得到的模型再采用FRED对接软件对测试集中的18个化合物进行对接并打分,再将所得打分结果与其活性进行线性回归,其回归结果具有良好的拟合效果,由此回归方程预测的活性与化合物实验值较吻合,说明我们建立的拮抗状态下的α1A-,α1B-和α1D-AR的三维同源模型具有一定的合理性,可作为化合物虚拟筛选模型,对新化合物进行对接虚拟筛选. 相似文献
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采用同源建模法对α1A1,α1B和α1D-的三维结构进行了模拟,并采用分子力学、分子动力学方法对所得同源模型进行优化,然后分别采用训练集拮抗剂对接的方法得到拮抗状态下的α1A1,α1B和α1D-三维结构模型.得到的模型再采用FRED对接软件对测试集中的18个化合物进行对接并打分,再将所得打分结果与其活性进行线性回归,其回归结果具有良好的拟合效果,由此回归方程预测的活性与化合物实验值较吻合,说明我们建立的拮抗状态下的α1A1,α1B和α1D-的三维同源模型具有一定的合理性,可作为化合物虚拟筛选模型,对新化合物进行对接虚拟筛选. 相似文献
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(NH3CH2CH2NH2)3[Mo(Ⅴ)O2(O2C6H4)2] (1), (NH3CH2CH2NH2)2.5[Mo(Ⅴ)o.sW(Ⅵ)o.502(O2C6H4)2] (2) and(NH3CH2CH2NH2)2[VC(Ⅵ)O2(O2C6H4)2] (3) were synthesized, structurally characterized by X-ray diffraction analysis, and studied on their interactions with ATP, their DNA cleavage activities and antitumor properties. The redox state of molybdenum was not changed on going from crystal to aqueous solutions in complexes 1 and 2, while tungsten underwent reduction from W(VI) to W(V) in complexes 2 and 3. ATP promoted the oxidation of both molybdenum and tungsten from M(Ⅴ) to M(Ⅵ) and the hydrolysis of catecholate ligands in solution consisting of ATP and the complexes. Complex 1 possesses fairly good activity to DNA cleavage and against tumor S180 in mice, and is more effective than the control drug cyclophosphamide under the identical conditions. However, complexes 2 and 3 exhibited marginal effectiveness. The effectiveness of anti-tumor of the complexes was related positively to their DNA cleavage activities and their hydrolysis of catecholate ligands. 相似文献
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采用同源建模法对α1A-,α1B-和α1D-AR的三维结构进行了模拟,并采用分子力学、分子动力学方法对所得同源模型进行优化,然后分别采用训练集拮抗剂对接的方法得到拮抗状态下的α1A-,α1B-和α1D-AR三维结构模型.得到的模型再采用FRED对接软件对测试集中的18个化合物进行对接并打分,再将所得打分结果与其活性进行线性回归,其回归结果具有良好的拟合效果,由此回归方程预测的活性与化合物实验值较吻合,说明我们建立的拮抗状态下的α1A-,α1B-和α1D-AR的三维同源模型具有一定的合理性,可作为化合物虚拟筛选模型,对新化合物进行对接虚拟筛选. 相似文献
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本文用马来酰亚胺系列(MSL)及溴乙酰胺自旋标记物为探针,分别研究了透析液中1mmol/L浓度的Mg~(2+)对重建脂酶体上猪心线粒体H~+-ATP酶构象的影响。发现Mg~(2+)可以显著提高经标记后重建的H~+-ATP酶——L·(F_0·F_1)的ESR图谱中的强弱固定化比值(S/W)。用胰蛋白酶加尿素切下经MSL标记的L·(F_0·F_1)中的F_1部分,剩留的L·(F_0)部分的S/W值仍是有Mg~(2+)的比无Mg~(2+)的高。单独提纯的F_1经MSL标记后在无Mg~(2+)、有Mg~(2+)透析20h,二者ESR图谱无明显差异。上述结果支持我们前曾提出的模型,即Mg~(2+)通过与磷脂相互作用,改变其物理状态,引起H~+-ATP酶复合体中F_0部分的构象首先发生变化,然后这一变化再传递至复合体中活性中心所在的F_1部分。 相似文献
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人红细胞摄取环己二胺合铂(Ⅱ)配合物的手性选择性研究 总被引:9,自引:1,他引:8
合成了六种以不同手性的1,2-环己二胺(1,2-dach)作为载体配体的铂(Ⅱ)配合物,用元素分析、红外及分子图形方法对其组成和结构进行了表征.测定了它们跨人红细胞膜的一级反应动力学常数.用膜蛋白巯基滴定、荧光标记、自旋标记ESR谱等方法研究了它们与膜蛋白、膜脂的相互作用;用脂质体模拟了这些配合物的细胞摄入.结果表明:这些配合物主要通过简单扩散进入红细胞,其跨膜速率对环己二胺的手性具有明显的选择性.这种选择性主要来源于配合物与膜脂作用过程中的手性识别。 相似文献
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