高效液相色谱法测定金属配合物｛Fe［3-(2-吡啶基)-5,6-二苯基-1,2,4-三嗪］3｝2+两种几何异构体的动力学转变

通过高效液相色谱法研究了3-(2-吡啶基)-5,6-二苯基-1,2,4-三嗪(PDT)和Fe(Ⅱ)的配合物［Fe(PDT)3］2+的面式和经式两种几何异构体之间的动力学平衡过程。结果表明:不同温度(30,35,40,45 ℃)下,两种几何异构体含量(x)之间的相互转变均符合动力学一级反应,其xeln［(xe-x0)/(xe-x)］值和反应时间t(min)之间的关系分别为:xeln［(xe-x0)/(xe-x)］=0.082t+0.729 (r2=0.9911,T=45 ℃),xeln［(xe-x0)/(xe-x)］=0.049t+0.598 (r2=0.9987,T=40 ℃),xeln［(xe-x0)/(xe-x)］=0.022t+0.586 (r2=0.9987,T=35 ℃),xeln［(xe-x0)/(xe-x)］=0.012t+0.591(r2=0.9988,T=30 ℃)。两种异构体之间的动力学相互转变过程中的活化焓(ΔH)、活化熵(ΔS)和活化能(ΔEa)分别为:ΔH=103.84 kJ·mol-1,ΔS=271.93 J·mol-1·K-1,ΔEa=86.74 kJ·mol-1 (面式异构体向经式异构体转变);ΔH=106.47 kJ·mol-1,ΔS=257.65 J·mol-1·K-1,ΔEa=94.43 kJ·mol-1 (经式异构体向面式异构体转变)。     

8-羟基喹啉钐配合物与鲱鱼精DNA的作用研究

在pH=7.4的Tris-HCl缓冲溶液中,采用荧光光谱法研究表明8-羟基喹啉(HQ)能与稀土金属Sm(III)形成比例为3∶1的配合物。综合运用荧光光谱法、热力学方法、粘度法等分析方法研究了8-羟基喹啉钐配合物与鲱鱼精DNA的作用方式与作用部位,通过EB探针、粘度、磷酸盐、寡聚核苷酸以及Scatchard分析得出了Sm(III)(HQ)3与DNA之间是以部分嵌插以及沟渠作用发生相互作用,且以部分嵌插作用为主。热力学实验表明,Sm(III)(HQ)3能够自发地与DNA发生相互作用,而且这自发过程是焓为主要驱动力,各热力学函数值为ΔrHmΘ=-3.19×105J·mol-1,ΔrGmΘ300.15 K=-9.075×103J·mol-1,ΔrSmΘ=-1.033×103J·mol-1·K-1。Sm(III)(HQ)3能够与DNA以5∶1的比例形成复合物,在300.15和310.15 K形成复合物的结合常数为KΘ300.15 K=1.52×104L·mol-1,KΘ310.15 K=2.48×102L·mol-1。     

季铵型阳离子纤维素对水中腐殖酸的吸附

以异丙醇为分散剂,碱纤维与3-氯-2-羟丙基三甲基氯化铵反应,醚化接枝制得一种环境功能材料-季铵型阳离子纤维素(QACC)。用红外光谱、X-射线衍射和电镜扫描对材料的结构进行了表征:红外光谱中1 644 cm-1处存在明显的季铵基的弯曲振动。经过改性的QACC结晶度下降,比表面积增加。研究了QACC对腐殖酸的吸附性能:pH=8、318 K时,QACC对腐殖酸的饱和吸附容量为622 mg·g-1;其表观活化能为6.45 kJ·mol-1;吸附符合Lagergren二级动力学方程,吸附速率随温度升高而加快;吸附等温模型符合Langmuir等温式,为单分子层吸附;吸附腐殖酸的ΔH、ΔS、ΔG分别为:31.7 kJ·mol-1、119 J·mol-1·K-1、-5.34 kJ·mol-1,吸附主要为化学吸附。     

盐酸异丙肾上腺素与牛血清蛋白相互作用的光谱研究

本研究采用紫外和荧光光谱分析法研究了生理pH条件下盐酸异丙肾上腺素(HAI)与牛血清白蛋白(BSA)在不同温度(25℃和37℃)下的相互作用。实验结果表明,HAI使BSA紫外吸收峰增强,并使BSA的特征荧光峰猝灭,表明HAI与BSA形成结合物。HAI对BSA荧光猝灭机制为静态猝灭,属于单位点结合。25℃时两者之间的结合常数为7.41×103L·mol-1,ΔG为-22.10 kJ·mol-1,ΔH为25.86 kJ·mol-1,ΔS为940 J·mol-1。37℃时的结合常数为4.26×105L·mol-1,ΔH和ΔS与25℃时相同,ΔG为-33.41 kJ·mol-1。以上热力学参数表明HAI与BSA之间的结合属自发过程,两者之间的作用力以疏水作用为主。根据Fster非辐射能量转移理论计算出HAI与BSA间的结合距离为2.503nm。     

中国化学会第21届全国高中学生化学竞赛（决赛）理论试题答案

第1题计算A、B两条直线的斜率:直线A的斜率为-3.76×104直线B的斜率为-1.01×104由Clausius-Clapeyron方程lnp=-ΔvRapTHm C及直线A和直线B的斜率分别得到:ΔHA=84.0kJ.mol-1ΔHB=312.6kJ.mol-1ΔH=ΔHB-ΔHA=312.6kJ.mol-1-84.0kJ.mol-1=229kJ.mol-11-4设xA、xB分别为为DEAA三     

三类引发剂引发苯乙烯聚合特性的比较研究和理论分析

用膨胀计法分别测定了氮 氮键引发剂偶氮二异丁腈 (AIBN)、氧 氧键引发剂过氧化二苯甲酰 (BPO)、碳 碳键引发剂 2 ,3 二氰基 2 ,3 二苯基丁二酸二乙酯的内消旋体 (I)和外消旋体 (II)在苯乙烯中的分解动力学参数 ,分解活化能分别为 :Ed(AIBN) =1 40 0 6kJ·mol-1,Ed(BPO) =1 2 0 3 3kJ·mol-1,Ed(I) =1 0 4 5 2kJ·mol-1,Ed(II) =89 5 6kJ·mol-1;分解活化熵分别为 :ΔS≠(AIBN) =76 3 2J·mol-1·K-1,ΔS≠(BPO) =1 2 76J·mol-1·K-1,ΔS≠(I) =-3 5 2 3J·mol-1·K-1,ΔS≠(II) =-80 84J·mol-1·K-1,并且II的极限转化率α∞ 表现出随温度升高而升高 ,I的α∞ 随温度升高先减小而后趋于平稳的趋势 ,这与AIBN和BPO引发苯乙烯聚合的极限转化率α∞ 随温度的升高而降低的规律有明显不同。对此用动力学链长综合常数k对T的微分结果并结合过渡态理论进行了分析。     

光谱法研究硝基苯与牛血清蛋白的相互作用

本文应用荧光分析法研究了不同酸度、温度和反应时间条件下,硝基苯对牛血清蛋白(BSA)的荧光猝灭作用。实验结果表明在激发波长λex=280nm,发射波长λem=342nm,浓度为0.05 mol·L-1,pH=7.50的TrisHCl缓冲溶液中,猝灭效果最为明显。计算289,304和318 K温度下二者的结合常数分别为:1.25×104、1.00×104和0.833×104L·mol-1。通过Gibbs-Helmholtz方程对其相互作用的热力学参数进行计算(ΔH=-10.7 kJ·moL-1;ΔS=41.4 J·moL-1·K-1),表明二者之间是静电相互作用。实验结果表明,硝基苯对牛血清蛋白荧光猝灭方式为静态猝灭,最后使用紫外吸收光谱法对其作用机理进一步确认。     

镉(Ⅱ)与牛血清蛋白相互作用的分子光谱研究

在模拟生理条件下,采用分子荧光、紫外光谱法研究了水溶液中Cd2+与牛血清蛋白(BSA)的相互作用.研究表明,在pH=7.0缓冲液中,以280nm作为激发波长,342nm作为发射波长,Cd2+对BSA的荧光发射有较强猝灭作用.实验测定了Cd2+与BSA在289K,306K和319K温度下的结合常数Ka分别为5.31×104,5.22×104,4.70×104,其热力学参数ΔHm=-3.07kJ·mol-1;ΔSm=79.83J·mol-1·K-1.结果表明导致BSA荧光猝灭是由于分子内的非辐射能量转移而引起的静态猝灭,他们之间的主要作用力是静电作用力.     

柚皮苷与人血清白蛋白相互作用的研究

用荧光、紫外光谱、分子对接研究了柚皮苷与人血清白蛋白(HSA)在pH=7.40的Tris-HCl缓冲溶液中相互作用的情况。结果表明,柚皮苷对人血清白蛋白的内源荧光有明显的猝灭作用,猝灭过程为动态猝灭。根据Stern-Volmer方程计算得到柚皮苷与HSA在293、298和310 K下的结合常数分别为2.472×105、2.210×105和1.392×104L·mol-1,结合位点数约为1。由实验计算出热力学参数焓变ΔH为-16.8 kJ·mol-1,ΔS为46.0 J·mol-1·K-1,推断出柚皮苷与人血清白蛋白之间主要靠疏水作用和静电引力结合,与分子模拟的结果相同。同时采用同步荧光技术考察了柚皮苷对HSA构象的影响。     

二甲基胺取代-烃基膦酸树脂对钆(Ⅲ)的吸附性能

用二甲基胺取代 烃基膦酸树脂对钆的吸附行为进行研究,试验结果表明,在pH4.90时,树脂对钆的静态饱和吸附容量为219mg·g-1(树脂);用2mol·L-1HCl可以定量洗脱;表观吸附速率常数k298=1.81×10-4s-1,测得吸附热力学参数分别为:ΔH=77.46kJ·mol-1,ΔG=-32.417kJ·mol-1,ΔS=368.69J·mol-1·K-1;等温吸附服从Frenndlich曲线;树脂功能基与Gd(Ⅲ)的配位比为2∶1;并用红外光谱探讨了树脂与钆的成键情况。     

Spectroscopic study on acid-induced unfolding and refolding of apo-neuroglobin

pH-induced unfolding and refolding of apo-neuroglobin (apo-Ngb) were investigated by UV, fluorescence, circular dichroism (CD) spectra and light scattering measurements. Results revealed that apo-Ngb became partially unfolded at around pH 5.0, with evidences from a red shift in the fluorescence spectra, a decrease in the far-UV CD and a sharp peak in the light scattering intensity. Further lowering of the pH reversed these effects, suggesting that apo-Ngb folds back to a compact state. At pH 2.0, the apo-Ngb forms a folding intermediate known as molten globule (MG), which is possessed of native-like secondary structure and almost complete loss of tertiary structure. Based on these results, the acid-induced denaturation pathway of apo-Ngb can be illustrated from the native state (N), via a partially unfolded state (U_A) to the molten globule state (MG).     

水合和pH对蛋白酶K热诱发转变影响的量热法研究

用差示扫描量热法, 在310～450 K温度范围、0.048～4.39克水/克干酶以及pH3～9范围内研究了蛋白酶K(EC 3.4.21.14)的热变性。分别提出表征热变性过程的三个主要热力学参数: 热变性温度T_d、比变性焓△H_d及超额表观比热C_(ex)~(max)和总水量h以及pH的关系。除Td和h的关系属于Flory-Garrett类型外, 蛋白酶K的热变性热力学特征和已报道的球蛋白、双螺旋蛋白及三螺旋蛋白不相同。一级水合水对蛋白酶K热变性热力学特征有最大的影响, pH也是影响该酶热稳定性的重要因素。     

牛血红蛋白与双十二烷基二甲基溴化铵相互作用的光谱研究(英文)

运用荧光光谱、紫外-可见吸收光谱和圆二色谱法研究了双十二烷基二甲基溴化铵(DDAB)与牛血红蛋白(Hb)的相互作用。从紫外-可见吸收光谱观察到,随着DDAB的浓度增大,Hb在406nm处的特征吸收峰强度下降,且峰位蓝移,说明DDAB导致血红素辅基微观环境变化。由荧光光谱研究可以得出随着DDAB的浓度增大,Hb在340nm处的荧光强度逐渐增强,说明导致色氨酸荧光淬灭的血红素辅基与色氨酸的距离增大。由Scatchard方程计算了不同温度下该反应的表观结合常数、结合位点数及结合热力学参数,热力学参数的变化表明DDAB与Hb之间以疏水作用力为主。圆二色谱的研究进一步表明DDAB使Hb产生轻微的二级结构改变,α-螺旋含量增加.     

Fluorescence Quenching Study on the Interaction of Some Schiff Base Complexes with Bovine Serum Albumin

The interaction of Schiff base ligand A and its three metal complexes [A‐Fe(II), A‐Cu(II), and A‐Zn(II)] with bovine serum albumin (BSA) was investigated using a tryptophan fluorescence quenching method. The Schiff base ligand A and its three metal complexes all showed quenching of BSA fluorescence in a Tris‐HCl buffer. Quenching constants were determined for quenching BSA by the Schiff base ligand A and its metal complexes in a Tris‐HCl buffer (pH=7.4) at different temperatures. The experimental results show that the dynamic quenching constant (K_SV) was increased with increasing temperature, whereas the association constant (K) was decreased with the increase of temperature. The thermodynamic parameters ΔH, ΔG and ΔS at different temperatures were calculated. The ionic strength of the Tris‐HCl buffer had a great influence on the wavelength of maximum emission of BSA. Under low ionic strength, the emission spectra of BSA influenced by A‐Zn(II) had a small blue shift. Compared to A‐Zn(II), the emission spectra of BSA in the presence of the Schiff base ligand A and A‐Cu(II) had no significant λ_em shift. At high ionic strength, the emission spectra of BSA upon addition of the Schiff base A, A‐Fe(II), and A‐Zn(II) all had a red shift, but the emission spectra of BSA had λ_em shift neither at low ionic strength, nor at high ionic strength in the presence of A‐Cu(II). Furthermore, the temperature did not affect the λ_em shift of BSA emission spectra.     

Spectral and thermal studies of alloxan complexes

The complexes of alloxan with Cr(III), Mn(II), Fe(III), Co(II), Ni(II), Cu(II), Zn(II) Cd(II), Hg(II), Ti(IV) and Zr(II) have been isolated and characterized on the basis of elemental analysis, molar conductivity, spectral studies (mid infrared, ¹H-NMR and UV/vis spectra), X-ray powder diffraction (XRD) and scanning electron microscopy (SEM). The thermal decomposition of the metal complexes was studied by thermogravimetric analysis (TGA) and differential thermal analysis (DTA). The kinetic thermodynamic parameters, E*, ΔH*, ΔS* and ΔG*, were calculated using Coats and Redfern and Horowitz and Metzger equations. The ligand and its complexes have been studied for possible biological activity including antibacterial and antifungal activity.     

Investigations of preferential solvation on 1,4-dimethoxy-3-methyl anthracene-9,10-dione

Synthesis, spectroscopic and thermal studies of some complexes of a new N(2)-Schiff base ligand of N(1),N(2)-bis((E)-2-methyl-3-phenylallylidene)ethane-1,2-diamine (L) with a general formula of MLX(2) (M = Zn(II), Cd(II) and Hg(II); X = Cl(-), Br(-), I(-), SCN(-) and N(3)(-)) are described. The ligand and its complexes were characterized by elemental analysis, molar conductance, UV-vis spectra, FT-IR spectra, MS, (1)H NMR and (13)C NMR spectra. The conductivity measurement as well as spectral data indicated that the complexes are non-electrolyte. (1)H and (13)C NMR spectra have been studied in DMSO-d(6) and/or CDCl(3). The thermal behavior of the complexes shows weight loss by decomposition of the anions and ligand segments in the subsequent steps. Activation thermodynamic parameters of decomposition such as E*, ΔH*, ΔS* and ΔG* were calculated from TG curves.     

Comparison of chemical and thermal protein denaturation by combination of computational and experimental approaches. II

Chemical and thermal denaturation methods have been widely used to investigate folding processes of proteins in vitro. However, a molecular understanding of the relationship between these two perturbation methods is lacking. Here, we combined computational and experimental approaches to investigate denaturing effects on three structurally different proteins. We derived a linear relationship between thermal denaturation at temperature T(b) and chemical denaturation at another temperature T(u) using the stability change of a protein (ΔG). For this, we related the dependence of ΔG on temperature, in the Gibbs-Helmholtz equation, to that of ΔG on urea concentration in the linear extrapolation method, assuming that there is a temperature pair from the urea (T(u)) and the aqueous (T(b)) ensembles that produces the same protein structures. We tested this relationship on apoazurin, cytochrome c, and apoflavodoxin using coarse-grained molecular simulations. We found a linear correlation between the temperature for a particular structural ensemble in the absence of urea, T(b), and the temperature of the same structural ensemble at a specific urea concentration, T(u). The in silico results agreed with in vitro far-UV circular dichroism data on apoazurin and cytochrome c. We conclude that chemical and thermal unfolding processes correlate in terms of thermodynamics and structural ensembles at most conditions; however, deviations were found at high concentrations of denaturant.     

S-异丙甲草胺与小牛胸腺DNA的相互作用

应用紫外光谱、荧光光谱、DNA热变性法以及黏度法研究了S-异丙甲草胺与小牛胸腺DNA(ctDNA)的相互作用. 结果表明, S-异丙甲草胺使ctDNA在200 nm处的吸收峰发生明显改变, 表现出红移和减色效应, 而对260 nm处的吸收峰产生影响较小, 排除了嵌插作用的可能; ctDNA对S-异丙甲草胺内源性荧光表现出很强的猝灭作用, 且随温度的升高, 其猝灭程度有所下降, 表明S-异丙甲草胺是以形成加合物的方式与ctDNA结合的, 并求得了它们在不同温度下的结合常数; 将不同离子强度条件下S-异丙甲草胺与ctDNA作用以及不同S-异丙甲草胺浓度下ctDNA的热变性温度和黏度变化的研究结果与紫外光谱和荧光光谱相结合, 可以判断S-异丙甲草胺是以沟槽作用的方式与ctDNA结合的.     

Phosphorus Schiff base ligand and its complexes: Experimental and theoretical investigations

A phosphorus-containing Schiff base was prepared from bis{3-[2-(4-amino-1,5-dimethyl-2-phenylpyrazol-3-ylideneamino)ethyl]indol-1-ylmethyl}phosphinic acid and paraformaldehyde as a novel antibacterial compound. The reaction of the Schiff base ligand with VO(IV), Ni(II), Co(II), Cu(II), Zn(II), Cd(II), Hg(II), Pd(II) and Pt(IV) led to binuclear species of metal complexes, depending on the ratio of metal ion and ligand. The ligand and its complexes were investigated using elemental analysis, Fourier transform infrared, ¹H NMR, ¹³C NMR, UV–visible and mass spectra, thermogravimetric analysis, conductivity measurements and thermal analysis. The results showed that the Schiff base behaves as a tetradentate ligand; moreover, on the basis of conductance results, of all the prepared complexes are non-electrolytes, excepting the Pt(IV) complex. The metal complexes were found to be formed with a metal-to-ligand ratio of 2:1, except for the Pt(IV) complex with a ratio of 1:1. The activation thermodynamic parameters (ΔE*, ΔH*, ΔS*, ΔG* and K) and the activation energy of thermal decomposition were determined from thermogravimetric analysis using the Coats–Redfern method. The biological activities of the metal complexes were screened against the growth of bacteria and fungi in vitro to assess the antimicrobial potential and study the toxicity of the compounds. The prepared compounds have noteworthy antimicrobial properties.     

FTIR studies of collagen model peptides: complementary experimental and simulation approaches to conformation and unfolding

X-ray crystallography of collagen model peptides has provided high-resolution structures of the basic triple-helical conformation and its water-mediated hydration network. Vibrational spectroscopy provides a useful bridge for transferring the structural information from X-ray diffraction to collagen in its native environment. The vibrational mode most useful for this purpose is the amide I mode (mostly peptide bond C=O stretch) near 1650 cm-1. The current study refines and extends the range of utility of a novel simulation method that accurately predicts the infrared (IR) amide I spectral contour from the three-dimensional structure of a protein or peptide. The approach is demonstrated through accurate simulation of the experimental amide I contour in solution for both a standard triple helix, (Pro-Pro-Gly)10, and a second peptide with a Gly --> Ala substitution in the middle of the chain that models the effect of a mutation in the native collagen sequence. Monitoring the major amide I peak as a function of temperature gives sharp thermal transitions for both peptides, similar to those obtained by circular dichroism spectroscopy, and the Fourier transform infrared (FTIR) spectra of the unfolded states were compared with polyproline II. The simulation studies were extended to model early stages of thermal denaturation of (Pro-Pro-Gly)10. Dihedral angle changes suggested by molecular dynamics simulations were made in a stepwise fashion to generate peptide unwinding from each end, which emulates the effect of increasing temperature. Simulated bands from these new structures were then compared to the experimental bands obtained as temperature was increased. The similarity between the simulated and experimental IR spectra lends credence to the simulation method and paves the way for a variety of applications.