H_8[P_2Mo_(17)Co(OH_2)O_(61)]和H_8[P_2Mo_(17)Ni(OH_2)O_(61)]的抑酶活性研究

合成了2种过渡金属取代的多酸H_8[P_2Mo_(17)Co(OH_2)O_(61)]和H_8[P_2Mo_(17)Ni(OH_2)O_(61)],并对其抑酶活性进行了研究.结果表明,这2种化合物对酪氨酸酶均有有效的抑制效果.抑制机理表明2种化合物均是可逆竞争型抑制剂.H_8[P_2Mo_(17)Co(OH_2)O_(61)]和H_8[P_2Mo_(17)Ni(OH_2)O_(61)]的半抑制率IC_(50)值分别为(0.434 0±0.000 4)和(0.466 5±0.012 0)mmol/L,抑制常数K_Ⅰ分别为0.216 7和0.220 4mmol/L.该研究能够扩大多金属氧酸盐的应用范围.     

钒取代的多酸盐对酪氨酸酶抑制机理的研究

合成了2种不同的钒取代Keggin型多金属氧酸盐(Na4PMo11VO40和(HGly)4PMo11VO40,以下分别简写为PMo11V和Gly-PMo11V),并用紫外光谱和红外光谱对其进行结构表征.以这2种化合物为效应物,采用酶动力学方法研究其对酪氨酸酶二酚酶的抑制效果、抑制机理和抑制类型.结果表明:PMo11V和Gly-PMo11V对酪氨酸酶均有明显的抑制效果,其IC50分别为0.522和0.447mmol/L.其中,PMo11V对酪氨酸酶的抑制过程属可逆的竞争型抑制,抑制常数KI为2.629mmol/L,而Gly-PMo11V对酪氨酸酶的抑制属不可逆的抑制.综合比较,Gly-PMo11V对蘑菇酪氨酸酶的抑制效果优于PMo11V.     

双2:17钼磷系列稀土杂多蓝的合成和性质研究

首次合成和离析了八种以缺位型Dawson结构钼磷杂多阴离子为配体的稀土杂多蓝K_(17)H_2[Ln-(P_2Mo_(17)O_(61))_2]·nH_2O和K_(17)H_4[Ln(P_2Mo_(17)O_(61))_2]·nH_2O(Ln=La,Pr,Sm,Yb).通过元素分析、电位滴定、红外光谱、紫外光谱、极谱、循环伏安、X射线光电子能谱、热重-差热分析和电子顺磁共振对杂多蓝进行了表征.实验结果表明,杂多阴离子还原为杂多蓝后,性质发生了某些变化,但结构基本不变,配体P_2Mo_(17)O_(61)~(10-)仍为a_2型.     

轮型和球型高核钼簇对酪氨酸酶的抑制作用

对3种高核钼簇Mo_(57)V_6,Mo_(154)(轮型)和Mo_(132)(球型)进行合成和结构表征,通过酶动力学方法得知这3种高核钼簇对酪氨酸酶二酚酶均具有很强的抑制作用,其抑制作用均为可逆竞争性抑制;高核钼簇对酪氨酸酶二酚酶活性的抑制作用和抑制效果均优于其他简单多阴离子的多酸化合物.其中球型高核钼簇的抑酶作用明显强于轮型高核钼簇.     

SYNTHESES AND SPECTRA OF HETEROPOLY BLUES OF DOUBLE 2:17 MOLYBDOPHOSPHATES LANTHANIDE COMPLEXES

The present paper reports eight heteropoty blues of double 2:17 motybdophosphates tanthanide comptexes with tacunary Dawson structure, i.e., K_(17)H_2[Ln(P_2Mo_2~ⅤMo_(15)~ⅥO_(16))_2], nH_2O and K_(17)H_4 [Ln(P_2Mo~Ⅴ_4Mo_(13)~ⅥO_(61))_2], nH_2O(Ln=La, Pr, Sm, Yb). They were characterized by etementat anatyses, potentiometric titration, IR, UV, potarography, cyclic vottammetry, X-ray photoelectron spectra, X-ray powder diffraction, thermat analyses and ESR. The results show that the properties of these heteropoty btues are different from those of heteropoty blues with saturated Dawson structure and other tacunary series. They are more stabte than their parent heteropoty acids in aqueous sotution and have the abitity of anti-base decomposition.     

钒取代型多金属氧酸盐对酪氨酸酶的抑制作用

测定了自制的α-1,2,3-K6H[SiW9V3O40]、α-1,2-K6[SiW10V2O40]和α-K5[SiW11VO40](以下分别简写为α-SiW9V3、α-SiW10V2和α-SiW11V)钒取代多金属氧酸盐对蘑菇酪氨酸酶活性的抑制作用。 结果表明,在pH=6.8的NaH2PO4-Na2HPO4缓冲溶液中,α-SiW9V3对酪氨酸酶有较强的抑制作用,表现为对酶稳态活力的抑制作用和对迟滞时间的延长作用,在DMSO溶液中,其IC50为0.6841 mmol/L,0.7 mmol/L α-SiW9V3可使单酚酶的迟滞时间由235 s延长至650 s,增加了2.77倍。 α-SiW9V3对酪氨酸酶单酚酶的抑制为可逆作用过程,抑制类型为混合型,其抑制常数KI、KIS分别为4.22和2.39 mmol/L。 α-SiW10V2不溶于DMSO,故未研究其对酶的抑制作用,α-SiW11V对酪氨酸酶抑制作用很弱。     

Dawson结构钼磷酸的合成与表征

合成了H_6P_2Mo_(18)O_(62)杂多酸及其四丁基铵盐和四丁基鏻盐,用IR、~(31)P NMR、GV等手段核查其纯度并研究了热稳定性、酸性和氧化还原性。结果表明,Dawson结构钼磷酸较Keggin结构钼磷酸有更强的氧化性。     

曲酸对马铃薯酪氨酸酶的抑制作用研究

曲酸等几种化合物对马铃薯酪氨酸酶的抑制作用表明：巯基类化合物、抗坏血酸和曲酸具有较强的抑制作用。预水浴温度和时间对曲酸的抑制作用并没有显著影响,曲酸通过延长L-tyrosine加氧羟化的迟滞时间,从而抑制单酚酶活性,以L—DOPA为底物测得曲酸为竞争性抑制,抑制常数艏为0．17mM。紫外光谱表明曲酸能将二酚酶催化的产物o-醌还原成二酚,从而抑制黑色素的生成。     

多酸/Pt-Ni合金纳米粒子复合膜电极的制备及其对H_2O_2电催化性能研究

选用Dawson型多酸K_6[P_2W_(18)O_(62)]·14H_2O (P_2W_(18))和Pt-Ni合金纳米粒子作为电化学活性组分,制备了P_2W_(18)/Pt-Ni合金纳米粒子复合膜电极,采用循环伏安法研究了复合膜电极的电化学行为。实验结果表明,P_2W_(18)/Pt-Ni合金纳米粒子复合膜电极具有良好的重复性和稳定性,并展现出较P_2W_(18)电极更好的对H_2O_2的电催化活性。     

钒取代的Dawson型磷钼酸对酪氨酸酶的抑制作用

采用酶动力学方法研究了5种钒取代的Dawson型磷钼酸H₇[P₂Mo₁₇VO₆₂]、H₈[P₂Mo₁₆V₂O₆₂]、H₉[P₂Mo₁₅V₃O₆₂]、H₈[P₂Mo₁₄V₄O₆₂H₂]和H₉[P₂Mo₁₃V₅O₆₂H₂](分别简写为P₂Mo₁₇V、P₂Mo₁₆V₂、P₂Mo₁₅V₃、P₂Mo₁₄V₄和P₂Mo₁₃V₅)对蘑菇酪氨酸酶二酚酶的抑制作用,结果表明,效应物P₂Mo₁₇V、P₂Mo₁₆V₂和P₂Mo₁₅V₃能够明显地抑制酪氨酸酶的活性,其半抑制浓度(IC₅₀)值分别为0.409、0.386和0.386 mmol/L,且均表现为可逆的竞争型抑制,效应物P₂Mo₁₇V、P₂Mo₁₆V₂和P₂Mo₁₅V₃对游离酶的抑制常数K_I分别为0.234、0.391和0.249 mmol/L。 而效应物P₂Mo₁₄V₄在0~1.0 mmol/L浓度范围内,对酪氨酸酶二酚酶无明显抑制作用,效应物P₂Mo₁₃V₅对酪氨酸酶二酚酶表现为激活作用。     

Inhibition of α/β-K6P2W18O62·10H2O on the Activity of Mushroom Tyrosinase and Its Antimicrobial Effects

Dawson-type phosphotungstic polyoxometalate α/β-K₆P₂W₁₈O₆₂·10H₂O(P₂W₁₈) was synthesized and its inhibitory effect on the mushroom tyrosinase was investigated. It could inhibit diphenolase activity of mushroom tyrosinase as an irreversible inhibitor. When the concentration of the enzyme reached 0.0176 mg/mL, the concentration of P₂W₁₈ leading to 50% activity lost(IC₅₀) was 0.05 mmol/L for monophenolase and 0.64 mmol/L for diphenolase. In addition, the antimicrobial activity of P₂W₁₈ was evaluated by zone of inhibition test. The results show that P₂W₁₈ possesses effective antimicrobial ability against Escherichia coli, Bacillus subtilis, yeast, especially Escherichia coli and yeast.     

两种多酸型酪氨酸酶抑制剂的性能研究

以H₃PW₁₂O₄₀和H₄SiW₁₂O₄₀(简写为PW₁₂和SiW₁₂)为效应物, 测定其对酪氨酸酶活力的抑制作用. 通过非变性聚丙烯凝胶(Native-PAGE)电泳确定酪氨酸酶是多家族基因编码, 其分子量为3×10⁴~3.4×10⁴, 4.2×10⁴~4.6×10⁴, 6.4×10⁴~6.8×10⁴, 且均具有活性, 测定PW₁₂和SiW₁₂对酪氨酸酶的抑制效果, 并结合酶动力学法研究其抑制机理. 结果表明, 当PW₁₂和SiW₁₂浓度分别达到13和25 mmol/L时, 酪氨酸酶的活力完全被抑制, 即PW₁₂和SiW₁₂对酪氨酸酶二酚酶具有不同程度的抑制效果. 当所加酶量为0.0173 mg/mL时, PW₁₂和SiW₁₂对酪氨酸酶二酚酶活力的半抑制率 (IC₅₀)分别为1.57和2.31 mmol/L, 它们对酪氨酸酶二酚酶的抑制均为可逆过程. 其中, PW₁₂对二酚酶的抑制类型为混合型, 其K_I及K_IS分别为0.34和0.43 mmol/L, SiW₁₂对二酚酶的抑制类型表现为竞争型, 其K_I为0.59 mmol/L. 综合考虑IC₅₀值和抑制常数等参数, PW₁₂对酪氨酸酶二酚酶的抑制能力优于SiW₁₂.     

Hydrothermal Synthesis,Structure and Properties of a New Phosphomolybdate Based on Novel [Co(H2O)4(HP2Mo5O23)]8- Anions and [H8(H2O)16]8+ Water Cluster Cations

A pure inorganic [P₂Mo₅O₂₃]^6- based cobalt complex [H₈(H₂O)₁₆][Co(H₂O)₄(HP₂Mo₅O₂₃)₂] with a sandglass-like shape was synthesized and characterized by means of single-crystal X-ray diffraction, powder X-ray diffraction(PXRD), infrared spectroscopy(IR), thermogravimetry/differential scanning calorimetry(TG/DSC), ultraviolet-visible spectroscopy(UV-Vis) and cyclic voltammogram(CV). Single-crystal X-ray diffraction analysis reveals that the asymmetric unit of compound 1 consists of a half cobalt ion, one [P₂Mo₅O₂₃]^6- anion, two coordinated water molecules and eight lattice water molecules. It is especially intriguing to note that two [P₂Mo₅O₂₃]^6- clusters are symmetrical about the Co ion, like a sandglass. And a chair-like water cluster with an unprecedented centrosymmetric [H₈(H₂O)₁₆]⁸⁺ can be observed in compound 1. Additionally, the electrochemical and catalytic properties of compound 1 were also investigated.     

具有Dawson结构的钼钒磷杂多酸氧化还原性质的研究

通过SnCl₂电位滴定、极谱和循环伏安方法,详细研究了2:18系列钼钒磷杂多酸H_(6+n)[P₂Mo^13-nV_nO₆₂]·xH₂O(n=1～3)和H^_4+n[P₂Mo_18-nV_nO₆₂H₂]·xH₂O(n=4,5)在溶液中的氧化还原性质,证实它们的还原为三步分别加合n,2,2个电子,同时加合n,2,2个质子的过程,总结了循环伏安峰电位与pH的关系,提出了还原机理。     

Development of bis-thiobarbiturates as successful urease inhibitors and their molecular modeling studies

Bis-thiobarbiturate derivatives 1–15 have been synthesized, characterized by1 HNMR and EI-MS and screened for urease inhibition. All compounds showed various degree of urease inhibitory activity with IC_(50) values ranging 7.45 0.12 74.24 0.81 mmol/L while the standard thiourea behaved normally(IC_(50) = 21.10 0.12). Compounds 1(IC_(50) = 7.45 0.12 μmol/L), 9(IC_(50) = 18.17 1.03 μmol/L) and 13(IC_(50) = 8.61 0.45 μmol/L) showed excellent urease inhibitory activity in the series. Molecular modeling studies were performed to understand the binding site with the bimetallic nickel center of the enzyme.Structure-activity relationship has also been established for these compounds. This study identified bisthiobarbiturate as a novel class of urease inhibitors.     

Pillaring of Zn2Al Layered Double Hydroxide by Dawson Polyoxometalate Anions

Zn2Al layered double hydroxide pillared with Dawson polyoxometalates, P₂W₁₇ZO₆₁^8-(Z=Mn²⁺, Co ²⁺, Ni²⁺, Cu²⁺, Zn²⁺) was prepared. A basal space of ca. 16 nm indicates the intercalated Dawson ions to be oriented with their C₂ axis perpendicular to the double hydroxide layers(with the exception of P₂W₁₇Zn-LDH). The IR and¹³P MASNMR spectral reveal that the Dawson ions retain their integrity in the interlayer space of LDH. A preliminary study shows that these compounds are highly active catalysts for the oxidation of cyclohexene with molecular oxygen.     

Synthesis and α-glucosidase inhibitory activity of chrysin,diosmetin, apigenin,and luteolin derivatives

Several derivatives have been synthesized from chrysin, diosmetin, apigenin, and luteolin, which were isolated from diverse natural plants. The α-glucosidase inhibitory activity of these compounds was evaluated. The glucosidase inhibitory activity of all derivatives （IC50 〈 24.396 μmol]L） was higher compared with that of the reference drug, acarbose （IC50=563.601 ±40.492μmol/L）, and 1- deoxynojirimycin （IC50 = 226.912± 12.573 μmol/L）. O3＇,O7-Hexyl diosmetin （IC50 = 2.406 ± 0.101μmol/L） was the most potent inhibitor identified. These compounds showed a higher inhibitory ability compared with their precursors except the luteolin derivatives. In general, the inhibitory activity of the synthetic derivatives was enhanced with long alkyl chains at positions 3＇, 4＇ and 7 of the flavonoid.     

新型双杂环修饰的酰胺硫醚衍生物的合成和生物活性

首次设计并合成了16个新型1,2,4-三唑与1,3,4-噻二唑双杂环修饰的酰胺硫醚衍生物,并对其进行了结构表征。分别评价了目标分子对蛋白酪氨酸磷酸酶1B(PTP1B)和细胞分裂周期25磷酸酶B(Cdc25B)抑制活性,结果发现:16个目标分子对PTP1B具有良好的抑制活性,其中8-C-d和8-D-c的抑制作用最佳,半抑制浓度(IC_(50)值)分别为(1.19±0.22)mg/L和(1.08±0.09)mg/L,优于阳性参照物齐墩果酸(IC_(50)=(1.27±0.19)mg/L),有望作为抗糖尿病药物先导物;对Cdc25B抑制活性测试中,11个目标分子表现出良好的活性,其中8-A-d、8-C-d和8-D-c抑制活性的IC_(50)值分别为(0.97±0.05)、(1.06±0.03)和(0.94±0.11)mg/L,低于阳性参照物Na_3VO_4(IC_(50)=(1.25±0.14)mg/L),有望作为抗肿瘤药物先导物。     

Esterification of phthalic anhydride with 1-butanol and 2-ethylhexanol catalyzed by heteropolyacids

Esterification of phthalic anhydride with 2-ethylhexanol and 1-butanol and ester decomposition of dioctyl phthalate (DOP) in presence of Keggin; H₃PW₁₂O₄₀, H₄SiW₁₂O₄₀, H₄SiMo₁₂O₄₀, Wells–Dawson; H₆P₂W₁₈O₆₂, H₆P₂W₁₇MoO₆₂ and Preyssler; H₁₄[NaP₅W₂₉MoO₁₁₀], H₁₄[NaP₅W₃₀O₁₁₀], type heteropolyacids have been investigated. The heteropolyacids with Preyssler and Wells–Dawson structures and their molybdenum substituted derivatives show higher activity in esterification and ester decomposition reactions than Keggin type heteropolyacids. A complete conversion of phthalic anhydride to dioctyl phthalate and dibutyl phthalate are achieved in 2 h in presence of molybdenum substituted Preyssler heteropolyacid. In the decomposition of dioctyl phthalate in the presence of Preyssler heteropolyacid, 2-ethylhexene is formed in quantitative yield.