A Highly Sensitive Spectrophotometric Assay of Bleomycins Based on the Fading Reaction of Some Halofluorescein Dyes

In weak acidic medium, anticancer antibiotics bleomycin A5 （BLMA5） and bleomycin A2 （BLMA2） can react with halofluorescein dyes such as erythrosin （Ery）, eosin Y （EY）, eosin B （EB） and rose bengal （RB） by virtue of electrostatic attraction and hydrophobic force to form the ion-association complexes, which can result in the fading reactions of four halofluorescein dyes. The maximum fading wavelengths of these four dyes were located at 527 nm for Ery, 515 nm for EY, 517 nm for EB and 546 nm for RB, respectively. The decrements of absorbance （AA） were directly proportional to the concentrations of bleomycin in a certain range. A new method for the determination of bleomycins anticancer drugs based on fading reactions of halofluorescein dyes has been developed. The method was not only highly sensitive but also simple and rapid. The molar absorptivities （ε） ranged from 1.5 × 10^5 to 7.5 × 10^5 L·mol^-1·cm^-1. It was applied to determination of the bleomycins in human serum, urine and rabbit serum samples. In this work, the spectral properties and the optimum reaction conditions were investigated. The structure of ion-association complexes and the reaction mechanism were discussed.     

Theoretical Study of the Low-Lying Excited States of Butoxy Radicals and Non-Radiative Decay Routes

The potential energy surfaces for the butoxy radical dissociation into R·＋O on the six low-lying electronic states have been determined with the combined CASSCF and MR-CI methods. The isomerization reactions between the different conformers of 1- and 2-butoxy radicals at the X and B states have been also investigated with the MP2, B3LYP, and CASSCF methods. The non-radiative decay mechanisms of butoxy radicals at the B state have been characterized with the computed potential energy surfaces and intersections. Supported by recent LIF experimental results, it was predicted that the t-butoxy radical would predissociate via the B/C intersection. As to 1- and 2-butoxy radicals, the relative energies of the transition states for the isomerization reactions between conformers at the B state are much lower than those of the B/C intersections, resulting in the predominance of the isomerization in the decay of the B state for 1- and 2-butoxy radicals.     

Cyclin A-Cdk2 Phosphorylates BH3 only Protein Bad in vitro and in vivo

Increasing evidence suggests that Cyclin A-Cdk2 activity is required in the apoptosis process induced by various stimuli. To determine a specific substrate of Cyclin A-Cdk2 for apoptosis, in this study, we carried out anin vitro kinase assay using immunoprecipitated complex Cyclin A-Cdk2 as an enzyme source, and recombinant protein GST-Bad as a substrate. Our study showed that Bad was clearly phosphorylated by Cyclin A-Cdk2 in vitro. To examine whether protein Bad can also be phosphorylated by Cyclin A-Cdk2 kinase in vivo, we transiently overexpressed protein Bad with Cyclin A or Cdk2-dn, a dominant negative version of Cdk2, in Hela cells and determined the phosphorylation status of protein Bad. The test showed that protein Bad was clearly phosphorylated in Cyclin A overexpressed cells,but not in Cdk2-dn or mock transfectent. Moreover, etoposide also caused the phosphorylation of endogenetic Bad. In conclusion, here we provide first time evidence that protein Bad can be a substrate of Cyclin A-Cdk2 apoptosis for in vitro and in vivo.     

硫代樟脑光化学反应的理论研究

运用量子化学方法优化了硫代樟脑的最低5个电子态(S₀, T₁, S₁, T₂和S₂)的结构, 并计算了它们的相对能量. 计算结果表明: S₁, T₁和T₂态的能量非常接近, 而S₂的能量远远高于T₂态, 这与之前对几种小的硫代羰基化合物的研究结论一致. 确定了硫代樟脑分子在T₁态发生β-插入反应和类Norrish II型反应的机理, 计算的势垒相对于S₀的振动零点分别为314.1和332.6 kJ/mol. 在400 nm波长的光的照射下, 分子被激发到S₁态, 此时分子没有足够的能量发生反应, 只能通过内转换回到基态. 当激发光波长在254 nm时, 硫代樟脑分子被激发到S₂态, 这时候体系有了足够的内部能量使反应发生. 实验上已经观察到此激发光波长下, 气态硫代樟脑可以发生β-插入反应和类Norrish II型反应.     

桑蚕丝素蛋白初始结构对其矿化作用的影响

以碱金属离子诱导桑蚕丝素蛋白溶液发生构象转变, 研究了蛋白质初始结构对其矿化作用的影响. FT-IR, XRD和SEM等测试结果显示, 未经任何处理的桑蚕丝素蛋白溶液矿化后形成片状复合物, 其无机相以二水磷酸氢钙(DCPD)为主; 而经过K^＋和Na^＋金属离子处理后, 桑蚕丝素溶液的结构由无规线团/螺旋构象向β-折叠发生转变, 矿化后成纤维状, 并相互结合呈现纳米级的三维多孔结构, 其无机相以热力学稳定的羟基磷灰石(HA)为主. 可以认为, 丝素蛋白结构转化为较伸展的β-折叠后, 使得更多的亲水基团暴露在外面, 在丝素蛋白分子不断凝聚成纤过程中, HA结晶快速生长并附着在这些微纤上, 最终形成纤维状的丝素蛋白/HA复合物. 该结果为阐明蛋白质的生物矿化过程及其调控机理提供了理论依据, 同时可以从矿化复合物的形成来反映这些微量元素可能对骨组织形成的影响, 为临床骨组织的修复提供一定的参考.     

采用多光程长建模方法检测血液成分含量

为了提高近红外光谱血液成分含量分析模型的预测精度,利用多个光程长(optical path length,OPL)共同参与建模的方法进行血糖等6种血液成分的定量分析。通过微米位移机构实现不同光程长血液光谱的测量,由全自动生化分析仪给出生化成分分析结果,并出具化验单。采用偏最小二乘法(PLS2)进行血液的近红外光谱建模及预测。由于血液光谱存在显著的非线性特征,不同光程长的血液样本的等效吸收系数不同,同一波长不同光程长(0.20~1.25 mm)测得的血液光谱互不相关。主动把非线性特性作为一种测量手段引入,不再利用单个的最佳光程长建模,而是用各个血液组分对应的多个最佳光程长的近红外光谱同时参与建立校正模型,进行血液成分的分析预测。研究结果表明,多光程长建模方法用于血液成分含量分析,可提高血液成分校正模型的预测精度。     

杂多酸催化H2O/THF或乙醚中三组分一锅煮合成α-胺基膦酸酯

发现杂多酸是在水/四氢呋喃或乙醚中三组分一锅煮高产率合成α-胺基膦酸酯的有效催化剂.研究了催化剂用量、反应溶剂、醛和胺的结构对反应的影响.     

联苯甲酰双缩氨基脲硫氰酸根硝酸根混合阴离子配位钕(Ⅲ)配合物的合成与结构

合成了联苯甲酰双缩氨基脲硫氰酸根、硝酸根混合配位的钕(Ⅲ)配合物。在此配合物中只有1个链状配体,另有2个硫氰酸根、1个硝酸根和1个水分子参与配位。总配位数是9。晶体结构分析表明,该配合物晶体属三斜晶系,P空间群。晶胞参数a=10。866(2),b=13.687(3),c=15.433(3),α=98.75(4)°,β=107.64(5)°,γ=112.14(5)°。最终偏差因子R=0.075。用INDO方法计算结果表明:NCS对Nd(Ⅲ)的配位比=C基对Nd(Ⅲ)的配位强。     

稀土离子在多孔阳离子交换剂内的扩散动力学

研究了稀土离子在Amberlyst15、D001、XN1010多孔树脂内的自扩散。结果表明,扩散过程遵循二级分散扩散机制。用粒内扩散方程求算了有效粒内扩散系数e,将e分解为树脂孔道扩散系数p及树脂固相扩散系数s,p与该离子在外部溶液中的自扩散系数相近,而s接近于与实验用的多孔树脂交联度相同的凝胶树脂内的自扩散系数值。