混合溶剂中酶促合成维生素A乳酸酯

研究了混合溶剂中脂肪酶催化合成维生素A乳酸酯.首先对催化合成维生素A乳酸酯反应的脂肪酶和反应介质进行了研究,其次对影响合成维生素A乳酸酯反应的因素(温度、底物摩尔比、反应时间和酶量等)进行了探讨,优化了反应条件:在5 mL混合溶剂(叔丁醇/正己烷(v/v)=3:2)中,0.167 g维生素A醋酸酯和0.150g乳酸在25 mg脂肪酶Novozym 435催化下,在35℃、150 r/m in下反应6 h,产率可以达到52.19%,固定化酶可连续使用5次以上,产率仍达45%以上.     

固定化脂肪酶催化高酸废油脂酯交换生产生物柴油

 探讨了固定化脂肪酶Novozym 435催化高酸废油脂与乙酸甲酯酯交换生产生物柴油. Novozym 435能催化高酸废油脂与乙酸甲酯的酯交换反应,反应24 h后甲酯产率为77.5%,但该值大大低于以精制玉米油为原料时的甲酯产率(86.2%). 系统研究了反应体系中的水、游离脂肪酸和乙酸对反应的影响. 当反应体系中的水含量低于0.05%时,水对酶反应速率和甲酯产率影响甚小,而水含量高于0.05%时,酶反应速率和甲酯产率随着水含量的增加而降低. 游离脂肪酸对反应有较大影响,甲酯产率随着游离脂肪酸含量的增加而急剧下降. 乙酸甲酯与游离脂肪酸反应产生的副产物乙酸是导致甲酯产率显著下降的原因. 在反应体系中添加适量(油重的10%)的有机碱三羟甲基氨基甲烷或三乙胺可有效提高酶促高酸废油脂的酯交换反应速率和甲酯产率,使反应12 h后的甲酯产率分别达到85.9%和80.8%; 碱的加入还提高了酶的操作稳定性,添加有机碱三羟甲基氨基甲烷或三乙胺可使反应10批次后Novozym 435的相对酶活力分别由对照值86%提高到97%和93%.     

有机相酶催化氨解反应拆分制备(R)-4-氯-3-羟基丁酸乙酯

通过脂肪酶催化的氨解反应拆分4-氯-3-羟基丁酸乙酯. 经过对脂肪酶及反应溶剂的筛选, 确定最佳脂肪酶及溶剂分别为Novozym435和二氧六环; 并在该反应体系中考察了温度、底物浓度、酶浓度与摇床转速对反应的影响. 综合考虑反应的反应速度和对映体选择率, 确定较佳的反应条件为: 温度30 ℃、底物浓度0.5 mol/L、酶量10 mg/mL、摇床转速200 n/min. 反应35 h后, ee可以达到99%以上, 此时转化率为57.7%.     

离子液体中扁桃酸乙酯的酶促不对称水解

对脂肪酶在离子液体中不对称水解扁桃酸乙酯制备R-扁桃酸进行了研究,发现脂肪酶N435在离子液体[BMIM]Br中的活性和立体选择性最高.研究了离子液体浓度、底物浓度、反应时间、反应温度、缓冲液pH值和摇床转速等因素对反应的影响,适宜反应条件为:1.39mol/LDL-扁桃酸乙酯、1.71mol/L[BMIM]Br、Tris-HCl缓冲液pH7.5、10mgN435酶、30℃、150r/min反应6h,该条件下产物对映体过量值(ee)可达58.78%,产率为65.23%,并对离子液体进行了重复利用.     

脂肪酶催化扁桃酸乙酯酯交换反应的研究

利用脂肪酶Novozym 435在正丁醇体系中催化酯交换反应,对(R,S)-扁桃酸乙酯进行了动力学拆分,考察了系统初始加水量,反应温度,振荡速度,底物浓度等因素对脂肪酶催化活性和对映体选择性的影响.研究结果表明,最适初始加水量为0.4%;在20℃~60℃范围内,酶催化活性随温度升高而增加,酶选择性随温度先升高后下降,最适温度45℃;底物扁桃酸乙酯浓度达5000 mmol/L时,未观察到底物抑制现象,反应初速度为2.78mmol.L-1.m in-1.     

新型酰基供体用于酶法动力学拆分制备(R)-1-(2-萘基)乙胺的研究

首次成功实现了光学纯(R)-1-(2-萘基)乙胺的高效酶法动力学拆分制备,考察了脂肪酶种类、溶剂、酰基供体、底物浓度、反应温度等对拆分效果的影响,发现新型酰基供体——正戊酸对氯苯酯能够很好地抑制非酶促自催化酰胺化效应.在甲苯溶剂中,底物浓度300 mmol/L,40℃条件下,采用该供体在脂肪酶Novozym 435催化下,动力学拆分反应8 h转化率达到理论最佳值50%,eep>99%.     

柴油溶剂中脂肪酶催化高酸值废油脂酯化制备生物柴油

采用0＃柴油作为反应溶剂,利用固定化脂肪酶催化高酸值废油脂与甲醇酯化反应制备生物柴油。来源于Candida antarctica的固定化脂肪酶Novozym435在0＃柴油溶剂中具有极高的催化活性。以酸价高达157×10-3的废油脂为原料,废油脂质量比10%的Novozym435,甲醇与废油脂初始摩尔比2∶1,0＃柴油与废油脂质量比5∶1,摇床摇速170r/min,50℃下反应2h甲酯化率可达95.10%。0＃柴油作为反应溶剂有效地溶解了高酸值废油脂和甲醇,降低了反应体系的黏度和消除了甲醇对Novozym435的负面影响,提高了Novozym435的稳定性。同时,0＃柴油溶剂对未脱胶废油脂中残留的对脂肪酶有害的磷脂等胶类物质具有一定的稀释作用。该工艺省却了溶剂蒸馏的繁琐工序,直接得到脂肪酸甲酯和石化柴油的混合燃料。     

微波辅助酶促月桂酸淀粉酯的合成

以天然玉米淀粉和月桂酸为原料,脂肪酶Novozym 435为催化剂,研究了微波辐照下月桂酸淀粉酯的酶促合成.通过对淀粉进行预处理活化来提高淀粉的酯化反应活性,并主要考察了微波功率、月桂酸用量、脂肪酶Novozym 435用量及反应时间等参数对酶促月桂酸淀粉酯合成的影响.采用气相色谱法进行取代度的测定,并以取代度为考察指标,确定了最佳的反应条件.结果表明,淀粉的最佳预处理方法为NaOH/尿素混合溶液法,经该法处理后淀粉的酯化反应活性大大提高;微波辐照技术的应用大大缩短了反应时间,并提高了月桂酸淀粉酯的取代度.适宜的工艺条件为:微波功率为240 W,月桂酸用量为30%,酶加入量为7%,反应时间26 min.     

脂肪酶催化缩聚法合成可完全降解的聚羟基丙酸酯(英文)

以3-羟基丙酸甲酯为聚合单体,建立了以固定化脂肪酶Novozym 435为催化剂的酶催化缩聚反应体系,合成可完全降解的高分子聚酯聚羟基丙酸酯,考察了反应条件和介质对反应性能的影响,结果表明,纯度大于95%的单体即可在温和条件下合成聚羟基羧酸酯;降低反应压力可有效提升产物产率和分子量.通过选择合适的有机溶剂介质和表面活性剂,可使产物分子量提升至13000(Mw)以上.脂肪酶催化剂重复利用能力优异,经6批次反应后,其相对活性保持在95%以上.     

脂肪酶催化二次动力学拆分制备高光学纯度(S)-萘普生

设计了一种利用立体选择性相反的两种脂肪酶催化二次动力学拆分,由外消旋萘普生甲酯制备高光学纯度(S)-萘普生的方法。理论曲线预测,与简单的酶促动力学拆分反应相比,二次动力学拆分可以明显提高高光学纯度产物的产率.根据几种脂肪酶在微水/异辛烷双液相反应体系中不对称水解萘普生甲酯的立体选择性和对映体比率(E),首先选用R选择性的固定化南极假丝酵母脂肪酶(Novozym 435)对外消旋萘普生甲酯进行第一次拆分,然后选用S选择性的柱状假丝酵母脂肪酶(CRL)对S过量的剩余底物萘普生甲酯在同样的反应体系中进行第二次拆分.该二次拆分反应对映体过量值为96.8%的(S)-萘普生产率达19.9%.     

Toward new camptothecins. Part 6: Synthesis of crucial ketones and their use in Friedländer reaction

In the context of the preparation of camptothecin and luotonin A analogs, the synthesis of some key keto-precursors and their use in Friedländer condensation are described. This paper also focuses on the stability of these keto intermediates and emphasizes the major differences between indolizinones and pyrroloquinazolinones series. Noteworthy is also the report of some original structures isolated as by-products of some experiments.     

KMnO4-mediated oxidative CN bond cleavage of tertiary amines: Synthesis of amides and sulfonamides

KMnO₄-mediated oxidative CN bond cleavage of tertiary amines producing secondary amine was introduced, which was trapped by electrophiles (acyl chloride and sulfonyl chloride) to form amides and sulfonamides. The reaction could take place at mild condition, tolerating a wide range of function groups and affording products in moderate to excellent yields.     

Chemistry of heterocyclic compounds at the A. E. Favorsky Irkutsk Institute of Chemistry, Siberian Branch of the Russian Academy of Sciences, over 50 years (Review)

The review contains a concise historical account and information on the most significant researches undertaken by the staff at the A. E. Favorsky Irkutsk Institute of Chemistry, Siberian Branch of the Russian Academy of Sciences on the Chemistry of Heterocyclic Compounds. Dedicated to Academician of the Russian Academy of Sciences B. A. Trofimov on his 70th jubilee. Translated from Khimiya Geterotsiklicheskikh Soedinenii, No. 10, pp. 1443–1502, October, 2008.     

关于"对‘燃料电池物理及化学性能的有限时间热力学分析方法'的讨论”答复

把有限时间热力学理论用于化学过程的研究,将会得到一系列新的结论,开展这方面的研究是很有意义的.文献[1]以燃料电池为例,在同时考虑化学反应及传热不可逆性的情况下,研究了燃料电池的性能界限,文献[2]指出了文献[1]计算化学反应及传热不可逆性而引起系统与有关环境的总熵产生率的错误以及由此而导致的结论所存在的问题,并进行了富有启发性的分析与讨论.但文献[2]对于系统与有关环境的总熵产生率的计算也是不正确的,由此得到的其它结论自然不能成立.本文将就此情况下系统与有关环境的总熵产生率的计算再次进行讨论,并给出电池功率和效率的有限时间热力学性能界限.     

Regiospecific synthesis of quercetin O-β-d-glucosylated and O-β-d-glucuronidated isomers

Quercetin, the polyphenolic compound, which has the highest daily intake, is well known for its protective effects against aging diseases and has received a lot of attention for this reason. Both quercetin 3-O-β-d-glucuronide and quercetin 3′-O-β-d-glucuronide are human metabolites, which, together with their regioisomers, are required for biological as well as physical chemistry studies. We present here a novel synthetic route based on the sequential and selective protections of the hydroxyl functions of quercetin allowing selective glycosylation, followed by TEMPO-mediated oxidation to the glucuronide. This methodology enabled us to synthesize the five O-β-d-glucosides and four O-β-d-glucuronides of quercetin, including the major human metabolite, quercetin 3-O-β-d-glucuronide.     

Cl+F2→ClF+F和F+ClF′→ClF+F′反应机理的密度泛函理论研究

用密度泛函理论(DFT)B3LYP方法, 在6-311G基组下,计算研究了反应Cl+F2→ClF+F和对称反应F+ClF′→ClF+F′的机理。求得前者的过渡态为三角形,活化能为15.57 kJ*mol-1;后者的过渡态为线形和三角形,活化能分别为11.52和196.25 kJ*mol-1。结果均经过振动分析和IRC计算验证。     

丙三醇浓溶液玻璃化转变与结构松弛参数DSC分析

In order to examine the effects of water contents and heating/cooling rates on the glass transition and the structure relaxation parameters of glycerol/water mixtures, five aqueous solutions (60%, 70%, 80%, 90% and 100%) were investigated using the differential scanning calorimetry. Four scanning rates (10, 15, 20, 25 K/min) were used to obtain the glass transition parameters. The fitting results of plasticization constants indicated that Gordon-Taylor relationship could not be used effectively without considering scanning rates and that point on calorimetric step was chosen as the glass transition temperature. The specific heat changes during glass transition processes were relative not only to water content but also to heating rates. With the increasing of water contents in glycerol aqueous solutions, the structure relaxation activation energies and dynamic fragilities were decreased. Since the thermodynamic fragilities were increased with the increasing of water content, so the dynamic fragility and thermodynamic fragility were changed inversely if the water contents were changed in glycerol/water mixtures.     

Deuterodehalogenation—a mild method for synthesising deuterated heterocycles

We report a mild and efficient method for introducing deuterium into a range of heterocycles by reacting readily available halide analogues in a deuterodehalogenation reaction using D₈-IPA or Et₃SiD under palladium-catalysed conditions.     

The conversion of 2-cyano cyanothioformanilides into 3-aminoindole-2-carbonitriles using triphenylphosphine

2-Cyano cyanothioformanilide 3a reacts with triphenylphosphine in the presence of water to give 2-(cyanomethyleneamino)benzonitrile 4a, 2-(cyanomethylamino)benzonitrile 5, 3-aminoindole-2-carbonitrile 2a and (2-cyanoindol-3-yl)iminotriphenylphosphorane 6a. In the presence of p-toluenesulfonic acid in MeOH the reaction between 2-cyano cyanothioformanilide 3a and triphenylphosphine (2 equiv) gives 3-aminoindole-2-carbonitrile 2a in 90% yield. Under the same conditions 2-(cyanomethyleneamino)benzonitrile 4a gives anthranilonitrile 8a, 3-aminoindole-2-carbonitrile 2a and N-(2-cyanophenyl)formamide 9. In addition, substituted 2-cyano cyanothioformanilides 3b-f react with triphenylphosphine and p-toluenesulfonic acid in MeOH to give 3-aminoindole-2-carbonitriles 2b-f in 63-75% yields. Under analogous conditions 2-cyano-4,5-dimethoxyphenyl cyanothioformanilide 2g gives only 4,5-dimethoxyanthranilonitrile 8g and 4,6,7-trimethoxyquinazoline-2-carbonitrile 14g, but in refluxing dry PhMe in the absence of p-toluenesulfonic acid 2-cyano-4,5-dimethoxyphenyl cyanothioformanilide 3g, (2-cyano-5,6-dimethoxyindol-3-yl)iminotriphenylphosphorane 6g and 2-(cyanomethyleneamino)-4,5-dimethoxybenzonitrile 4g are obtained. The structure of 2-(cyanomethyleneamino)-4,5-dimethoxybenzonitrile 4g is supported unambiguously via independent synthesis and comparison to the isomeric 6,7-dimethoxyquinazoline-2-carbonitrile 15. All new compounds are fully characterised and a tentative mechanism for the transformation of 2-cyano cyanothioformanilides to indoles is proposed.