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1.
在生理酸度(pH 7.4)下,采用荧光光谱、紫外光谱法并结合溴化乙锭(EB)荧光探针、I-效应、离子强度及DNA热变性效应等实验手段研究了自制的β-二酮Ti(Ⅳ)新型抗肿瘤前药与DNA之间的相互作用。前药能极大地猝灭溴化乙锭(EB)-DNA体系的荧光,其电子吸收光谱在280 nm处的最大吸收峰在加入DNA后产生明显红移和减色效应。实验还发现KI对前药-DNA体系的荧光猝灭效率明显小于自由形式存在的前药的荧光猝灭效率;这些实验结果说明前药以嵌插方式作用于DNA的亲核位点。  相似文献   

2.
在pH=7.4的Tris-HCl介质中,利用荧光光谱和紫外吸收光谱法,研究了一种新型蒽环类抗癌药物柔红霉素衍生物(4′-O-(α-L-夹竹桃糖基)柔红霉素,ODNR)与小牛胸腺DNA(ctDNA)的相互作用。 通过离子强度的影响、KI荧光猝灭实验和单双链ctDNA作用的比较实验,分析了ODNR与ctDNA的相互作用模式。 结果表明,ODNR通过嵌插方式与ctDNA发生作用。 ctDNA对ODNR的荧光有明显的猝灭作用,其机理属于静态猝灭。 通过Scatchard方程求得不同温度下的结合常数和结合位点数,由热力学参数确定分子间作用力为疏水作用,也可能存在静电作用。  相似文献   

3.
采用荧光光谱和吸收光谱法研究了叶酸(FA)与鲱鱼精DNA(DNA)的相互作用。研究了DNA热变性、离子强度、阴离子猝灭剂KI及金属离子对FA-DNA体系的影响,分析了FA与DNA的相互作用模式,获得了不同温度下的结合常数、结合位点数及热力学参数。结果表明,DNA对FA的荧光有明显的猝灭作用,作用过程为静态猝灭,FA通过沟槽模式和静电作用力与DNA结合。  相似文献   

4.
在模拟人体生理条件下,采用紫外光谱法、荧光光谱法、DNA热变性及黏度法研究欧前胡素及同分异构体异欧前胡素与DNA的作用机制,并探讨其构效关系.紫外光谱表明,加入DNA后,欧前胡素和异欧前胡素的紫外光谱均呈现减色效应;荧光光谱显示,随着欧前胡素或异欧前胡素浓度的增大,DNA-BR的荧光被猝灭,表明欧前胡素和异欧前胡素对BR与DNA的结合存在竞争性抑制;盐效应、DNA热变性温度、黏度法等实验进一步证明欧前胡素和异欧前胡素与DNA的作用模式均为嵌插与静电混合作用模式.研究表明,欧前胡素和异欧前胡素均与DNA发生作用,且欧前胡素与DNA作用强于异欧前胡素.  相似文献   

5.
烷基酚与DNA相互作用的荧光光谱法研究   总被引:2,自引:0,他引:2  
用荧光光谱法研究了环境激素辛基酚(OP)、壬基酚(NP)与小牛胸腺DNA(ctDNA)的相互作用.实验发现,随着ctDNA的加入,辛基酚、壬基酚的荧光光谱产生了有规律地猝灭,且最大发射峰红移.其中荧光猝灭是由于形成了烷基酚-DNA加合物而引起的静态猝灭.辛基酚、壬基酚与ctDNA均以插嵌模式相互作用,其结合常数分别为5.1×105 L·mol-1 和1.4×106 L·mol-1 ,结合位点分别为1.31和1.45.热力学参数确定了辛基酚及壬基酚与ctDNA的作用力类型主要是疏水作用力.  相似文献   

6.
塑化剂邻苯二甲酸二丁酯与小牛胸腺DNA的沟槽结合   总被引:1,自引:0,他引:1  
运用多种光谱学方法,结合化学计量学多元曲线分辨-交替最小二乘法(MCRALS),以及分子模拟技术,在人体生理酸度(pH=7.4)条件下研究了邻苯二甲酸二丁酯(DBP)与小牛胸腺DNA(ctDNA)的相互作用。采用MCR-ALS法分析了DBP与ctDNA作用的紫外光谱数据矩阵,结果表明DBP与ctDNA作用形成了DBP-ctDNA复合物。荧光猝灭实验显示,ctDNA对DBP的荧光猝灭属于形成复合物的单一静态猝灭,其主要驱动力为疏水作用和氢键。通过单双链、熔点和粘度等实验证明DBP与ctDNA发生了沟槽结合,结合区域为A、T碱基富集区。圆二色谱和琼脂糖凝胶电泳分析表明,DBP与ctDNA结合导致ctDNA结构变得更为松散,但未造成质粒DNA损伤。分子模拟形象直观地展现了两者的结合姿态,预测结果与实验结果吻合。  相似文献   

7.
在生理酸度条件下(pH7.4),运用紫外–可见吸收光谱、荧光光谱、圆二色谱(CD)和傅立叶红外光谱(FT–IR)并结合分子模拟、DNA熔点及粘度测定,研究了沙丁胺醇(Sal)与小牛胸腺DNA(ctDNA)的相互作用。结果表明,ctDNA以静态方法猝灭Sal的内源荧光,25℃时ctDNA与Sal的结合常数为1.26×104L·mol,氢键和范德华力是两者结合的主要驱动力。Sal存在下,ctDNA的熔点无明显变化,KI荧光猝灭效应和盐效应不明显,证实Sal与ctDNA主要通过沟槽模式结合。FT-IR与分子模拟结果显示,Sal倾向于与ctDNA的胸腺嘧啶(T碱基)结合。CD和凝胶电泳分析表明,Sal与ctDNA结合没有对DNA产生明显损伤,DNA仍维持B型构象。  相似文献   

8.
吡蚜酮与牛血清白蛋白的相互作用   总被引:2,自引:0,他引:2  
利用紫外吸收、荧光、同步荧光光谱及圆二色谱研究了吡蚜酮与牛血清白蛋白(BSA)的相互作用. 结果发现, 吡蚜酮使BSA的紫外吸收峰强度降低, 峰位红移; BSA的特征荧光峰猝灭, 荧光猝灭常数KSV随着温度的升高而降低, 表明吡蚜酮与BSA发生了较强的相互作用, 且吡蚜酮对BSA的荧光猝灭机制属于静态猝灭. 计算了不同温度下的结合常数和结合位点数; 由van′t Hoff方程计算出体系的ΔH和ΔS值, 得出二者之间的作用力主要为氢键和范德华力; 根据非辐射能量转移理论确定了给体-受体间的结合距离r=2.4 nm. 采用同步荧光光谱和圆二色谱考察了吡蚜酮对牛血清白蛋白构象的影响.  相似文献   

9.
红景天苷与DNA的结合作用研究   总被引:1,自引:0,他引:1  
在pH=7.4的生理酸度条件下,采用荧光光谱和紫外-可见光谱法,并结合I-效应、离子强度的影响、DNA熔点及粘度测定等实验手段,研究了红景天苷与小牛胸腺DNA的相互作用.结果表明,DNA对红景天苷的内源荧光有明显的猝灭作用,猝灭过程为静态猝灭.由荧光猝灭实验数据,计算出不同温度下红景天苷与DNA之间作用的结合常数和热力...  相似文献   

10.
本文采用紫外吸收光谱、荧光光谱、荧光偏振等方法研究了硫酸奎宁(QN)与小牛胸腺DNA(ctDNA)的相互作用,考察了影响其相互作用的各种因素,探讨了作用机理和作用方式。DNA存在时,QN的荧光被显著猝灭,吸收光谱出现减色现象。荧光偏振和阴离子猝灭等实验证实QN通过嵌插方式与ctDNA作用。测得QN与DNA的本征键合常数为1.51(±0.13)×104 L/mol,结合位点数为0.997,一分子的QN可以和大约1个碱基对作用。  相似文献   

11.
光谱法研究盐酸小檗碱与DNA的相互作用   总被引:4,自引:1,他引:3  
采用荧光和紫外(UV)光谱等手段,研究了中药有效成分小檗碱(Ber)与脱氧核糖核酸(DNA)的键合作用。结果发现,小檗碱能插入到DNA双螺旋碱基对之间的空腔中,使小檗碱在eλm=530 nm处较弱的荧光强度显著提高;酸度显著影响其相互之间的作用;随着DNA浓度的增大,Ber的荧光强度增大,显示了很好的光敏性能。偏振、荧光猝灭实验等也进一步表明:Ber与DNA的作用方式主要是嵌插结合;离子强度的大小会影响Ber与DNA之间的作用。在pH=3.0适宜酸度条件下,建立了以Ber为探针定量测定DNA的分析方法。方法线性范围为0~5.2×10-5mol/L,精密度(RSD)为2.7%(n=7),检出限为1.43×10-7mol/L。  相似文献   

12.
The binding of pyrene-1-carboxaldehyde (1-PyCHO) with ctDNA was investigated through absorption, intrinsic and induced circular dichroism, viscosity measurements and steady-state fluorescence. The binding and the number of monomer units of the polymer involved in the binding of one dye molecule (site size) have been quantified. The results indicated that the 1-PyCHO molecule binds to the ctDNA in an intercalative mode. The spectroscopic evidence of this intercalation process is also corroborated by the effect of urea, iodide-induced fluorescence quenching of pyrene-1-carboxaldehyde and competitive binding using a fluorescent intercalator, SYBR Green I (SG). The induced circular dichroism (ICD) spectra of pyrene-1-carboxaldehyde complexed with ctDNA show that pyrene-1-carboxaldehyde intercalates into ctDNA and that the intercalation orientation of pyrene to the DNA base-pairs long axis is heterogeneous. On the other hand, the intrinsic circular dichroism (CD) spectra show a stabilization of the right-handed B form of ctDNA, due to the intercalation process.  相似文献   

13.
本文以稳态荧光光谱、紫外-可见吸收光谱、荧光偏振、热变性、阴离子猝灭等手段,研究了一种具有强电荷转移能力的化合物2,7-二[(N-乙基咔唑-3-基)丙烯-1-酮基]芴与DNA的相互作用。研究结果表明,2,7-二[(N-乙基咔唑-3-基)丙烯-1-酮基)芴与DNA的作用方式是混合模式,以嵌插作用为主,同时存在沟槽相互作用,其咔唑基团可能插入到DNA的碱基对之间,结合常数K为8 123.48mol/L,结合位点n为0.71。该发光探针灵敏度高,结合稳定。  相似文献   

14.
Hu Z  Tong C 《Analytica chimica acta》2007,587(2):187-193
The fluorescence intensity of methylene blue (MB) quenched by DNA in the pH range of 6.5-8.0 was studied with synchronous fluorescence technology. A novel method for detecting single-stranded and double-stranded DNA was developed. The decreased fluorescence intensity at 664 nm is in proportion to the concentration of DNA in the range of 0.28-11.0 μmol L−1 for ctDNA, 0.14-8.25 μmol L−1 for thermally denatured ctDNA and 0.28-8.25 μmol L−1 for hsDNA. The detection limits (S/N = 3) are 0.11, 0.04 and 0.04 μmol L−1, respectively. The method is rapid, selective, and the reagents are lower toxic. It has been used for the determination of DNA in synthetic samples with good satisfaction. In addition, the interaction modes between MB and ctDNA and the mechanism of the fluorescence quenching were also discussed in detail. The experimental results from absorption spectra and fluorescence polarization indicate that the possible interaction modes between MB and DNA are the electrostatic binding and the intercalation binding.  相似文献   

15.
利用模板法在氧化铟锡(ITO)电极表面制备了三维有序多孔结构的金掺杂纳米Ti O2薄膜修饰电极(3DOM GTD/ITO),并在此修饰电极上成功固定小牛胸腺DNA(ct DNA),从而构建了一种新型的DNA生物传感器(DNA/3DOM GTD/ITO),并通过透射电镜(TEM)、扫描电镜(SEM)对修饰电极的表面形貌进行表征。采用电化学交流阻抗(EIS)法研究了ct DNA在3DOM GTD/ITO修饰电极表面的固定情况,结果表明,ct DNA已被成功地固定在3DOM GTD/ITO修饰电极表面。采用循环伏安法、微分脉冲伏安法等电化学方法研究了抗肿瘤药物槲皮素(Qu)在3DOM GTD/ITO修饰电极表面的电化学性质及与ct DNA的相互作用。结果表明,Qu在3DOM GTD/ITO修饰电极表面有1对准可逆的氧化还原峰,其氧化还原反应为2电子和2质子的转移过程。Qu可与固定在修饰电极上的ct DNA发生较强的结合作用,其结合常数(K)为3.61×106L/mol。循环伏安实验、紫外-可见吸收光谱、分子荧光光谱、圆二色性光谱均表明Qu与ct DNA之间的相互作用模式为嵌插作用。Qu与ct DNA的碱基结合具有序列选择性,对Qu与聚(d G-d C)及聚(d A-d T)的结合常数进行计算,得到结合常数比K(d G-d C)/K(d A-d T)=3.5,表明Qu与ct DNA发生嵌插作用时更倾向于结合在GC富集区域。  相似文献   

16.
The DNA-binding behaviors of the fluorescein?Cporphyrinatozinc(II) complex Zn(Fl-PPTPP) (Fl-PPTPP?=?5-(4-fluoresceinpropyloxy)phenyl-10,15,20-triphenylporphyrin) and fluorescein?Cporphyrinatocopper(II) complex Cu(Fl-PPTPP) with calf thymus DNA (CT-DNA) were investigated by UV?CVis absorption titrations, fluorescence spectra, viscosity measurements, thermal denaturation and circular dichroism. The results suggest that both complexes interact with CT-DNA by intercalation. In addition, their photocleavage reactions with pBR322 supercoiled plasmid DNA were investigated. Both complexes exhibit significant DNA cleavage activity, and singlet oxygen may play an important role in these reactions.  相似文献   

17.
This study was designed to examine the interaction of an anthracycline disaccharide, 4′-O-(β-L-oleandrosyl) daunorubicin (DNR–D2), with calf thymus deoxyribonucleic acid (ctDNA) by UV–vis in combination with fluorescence spectroscopy and molecular modeling techniques under physiological conditions (Britton–Robinson buffer solutions, pH 7.4). By the analysis of UV–vis and fluorescence spectrum, it was observed that the binding mode between DNR–D2 and ctDNA might be intercalation, and fluorescence quenching mechanism of DNR–D2 by ctDNA was a static quenching type. Upon binding to ctDNA, the anthraquinone chromophore of DNR–D2 could slide into the C–G rich region of ctDNA. Hydrogen bonding forces may play an essential role in the binding of DNR–D2 to ctDNA. Furthermore, the results obtained from computational modeling corroborated the experimental results obtained from spectroscopic investigations. These studies are valuable for a better understanding the datailed mode of DNR–D2–DNA interaction, which should be important in deeper insight into the therapeutic efficiency of DNR–D2.  相似文献   

18.
It is noteworthy to understand the details of interactions between antitumor drugs and DNA because the binding modes and affinities affect their antitumor activities. Here, The interaction of toluidine blue (TB), a potential antitumor drug for photodynamic therapy of tumor, with calf thymus DNA (ctDNA) was explored by UV–vis, fluorescence, circular dichroism (CD) spectroscopy, UV-melting method and surface-enhance Raman spectroscopy (SERS). The experimental results suggest that TB could bind to ctDNA via both electrostatic interaction and partial intercalation. The fluorescence quenching of TB by ctDNA was static and due to electron transfer from bases to the excited singlet state of TB. At low [TB]/[DNA] ratio, TB mainly partially intercalated into ctDNA resulting in the slight increase of base stacking degree; at high [TB]/[DNA] ratio, excessive TB externally stacked along the helix surface via coupling with partially intercalated ones, thereby inducing B-A transition of ctDNA. The conformational transition of DNA was confirmed by the obvious improvement of the thermal stability of ctDNA. The SERS spectra suggest that TB could partially intercalate into DNA basepairs with its ring C1NC1′ side buried.  相似文献   

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