Crystal structure, magnetic and photoelectric properties of coordination polymer[ Co2（C3H4N2）4（ C10H2O8） ]n

The coordination polymer is designed and synthe-sized through the choice of organic ligand and coordina-tion geometry of metal ion as well as the control over theinfinite network topology structure, which usually con-tains both the characteristic of the organic molecules andmetal ions. So, it exhibits more singular function and haspotential application in optics, electrics, information, ca-talysis, medicament, metallurgy, novel material and lifesciences fields. And it has been the confluence m…     

N-叔丁基(4aS,8aS)-十氢异喹啉-3(S)-甲酰胺的合成及结构表征

以L-苯丙氨酸为原料制备N-叔丁基-1,2,3,4四-氢异喹啉-3(S)甲-酰胺(T ICC),后者经铑/氧化铝催化加氢制备N-叔丁基(4aS,8aS)十-氢异喹啉-3(S)甲-酰胺(DH IQ)。1H-NMR、M S确定产物的化学结构;GC-M S分析产物中的异构体;单晶X射线衍射确定DH IQ的绝对构型;旋光度的测定表明DH IQ产物的光学纯度达到了98%。     

P(3-co-4)HB解聚酶的分离纯化及酶学性质研究

聚(3-羟基丁酸酯-co-4-羟基丁酸酯)(P(3-co-4)HB)解聚酶是由微生物所分泌的一种胞外酶,可以将P(3-co-4)HB降解为水溶性小分子物质,为了阐明P(3-co-4)HB材料的生物降解机理并建立其生物循环系统,P(3-co-4)HB降解菌和降解酶的研究越来越受到关注。本论文以Penicillium sp.DS-04菌株为材料,对其产生的P(3-co-4)HB解聚酶进行了分离纯化,发酵液经过冻干和分子筛层析得到了P(3-co-4)HB解聚酶的纯酶组分,纯化倍数和回收率分别为3.15和10.44%,SDS-PAGE显示该酶分子量为44.0kDa。本文还对P(3-co-4)HB解聚酶的酶学性质进行了测定,并初步探讨了解聚酶的作用模式。     

2-乙基-3-羟基-6-苯硫基-4(1H)-吡啶酮对动物实验性急性肝损伤的保护作用

目的 :研究 2 -乙基 - 3-羟基 - 6-苯硫基 - 4 ( 1H) -吡啶酮 (HPP)对四氯化碳 (CCl4 )、硫代乙酰胺 (TAA)及D -氨基半乳糖 (D -GalN)引发的小鼠急性肝损伤的影响 .方法 :用CCl4 、TAA、D -GalN引发动物急性肝损伤 ,HPP通过口服给药 ,测定动物血清中谷丙转氨酶 (GPT)、谷草转氨酶 (GOT)、谷胱甘肽过氧化物酶 (GSH -Px)、超氧化物歧化酶 (SOD)的活性 ,用硫代巴比妥酸法测定肝组织中丙二醛 (MDA)含量 .结果 :HPP 1.6mg·kg- 1、6.4mg·kg- 1显著抑制动物血清中GPT、GOT活性的升高 ,显著抑制GSH -Px ,SOD活性的降低且能降低肝组织中脂质过氧化产物MDA含量的升高 ,同时HPP对CCl4 所致大鼠急性肝损伤也有一定的抑制作用 ,实验表明HPP对正常小鼠血清及肝脏GPT活力无明显影响 .结论 :HPP对动物急性肝损伤有明显的抑制作用     

Theoretical study on the lithium bond interaction of furan homologues C4H4Y （Y=O,S） with LiCH3 via DFT and MP2

The optimizations geometries and interaction energy corrected by BSSE of the complexes between C4H4Y （Y=O, S） and CHiLi have been calculated at the B3LYP/6-311＋＋G^＊＊ and MP2/6-311＋＋G^＊＊ levels. Three complexes were obtained. Abnormally, the calculations showed that all the C10--Li14 bond lengths increased obviously but the blue-shift of C10-Li14 stretching frequency occurred after formed complexes. The calculated binding energy with basis set super-position error （BSSE） and zero-point vibrational energy corrections of complexes I-III is -45.757, -35.700 and -39.107 kJ·mol^-1, respectively. The analyses on the combining interaction with the atom-in-molecules theory （AIM） also showed that a relatively strong lithium bond interaction presented in furan homologues C4H4Y-LiCH3 systems. Natural bond orbital theory （NBO） analysis has been performed, and the results revealed that the complex I is formed with n-σ type lithium bond interaction between C4H40 and LiCH3, complex II is formed with TT-s type lithium bond interaction between C4H4O and LiCH3, and complex III is formed with TT-s and n-s type lithium bond interactions between C4H4S and LiCH3, respectively.     

ADTIQ导致SH-SY5Y细胞凋亡和多巴胺转运体表达降低

新内源性神经毒素1-乙酰基-6,7-二羟基-1,2,3,4-四氢异喹啉(ADTIQ)生成与糖代谢密切相关,可能成为糖尿病并发PD的一个关键因素,但是其神经毒性还不清楚.针对ADTIQ的神经毒性,该研究采用SH-SY5Y细胞为模型,MTT法,Annexin V/PI双染法,Caspase 3/7活性检测细胞存活率和细胞凋亡,Western-blot检测多巴胺转运体(DAT)的表达量.结果表明,随着ADTIQ浓度增大,细胞的存活率逐渐下降,凋亡率增加,同时ADTIQ导致DAT表达降低.研究提示ADTIQ导致多巴胺神经元的凋亡与PD的发生息息相关,糖尿病引起ADTIQ增加,可能成为高糖损伤多巴胺神经元的一个重要原因.