分散固相萃取-高效液相色谱-串联质谱法同时测定畜禽肉中63种兽药残留

建立了分散固相萃取-高效液相色谱-串联质谱(dispersive-SPE-HPLC-MS/MS)同时测定畜禽肉中 β-内酰胺类、喹诺酮类、磺胺类、磺胺类增效剂和抗寄生虫类共5类63种兽药残留的新方法。样品经0.1 mol/L Na₂EDTA溶液及含1% (体积分数)乙酸的乙腈溶液涡旋提取,提取液经C18分散固相萃取净化后,用Poroshell EC-C18色谱柱(100 mm×2.1 mm, 2.4 μm)分离,在电喷雾离子源正离子模式下以动态多反应监测(DMRM)方式采集数据并做定性筛查和定量分析。63种药物在相应的浓度范围内线性关系良好,相关系数均大于0.99;不同畜禽肉(猪肉、牛肉及鸡肉)在3个不同添加水平下的平均回收率为62.2%~112.0%,相对标准偏差(RSD)为3.1%~16.3%,检出限(LOD, S/N≥3)和定量限(LOQ, S/N≥10)分别为0.1~3.0 μg/kg和0.5~10.0 μg/kg。该方法简便快速、灵敏可靠,适用于畜禽产品中兽药多残留的同时快速定性筛查和定量分析。     

对甲苯磺酰胺基乙酰腙类化合物的生物活性及其量子化学计算

以对甲苯磺酰氯为原料, 通过与氨基乙酸反应得到中间体对甲苯磺酰氨基乙酸, 再经酯化、肼解得到对甲苯磺酰氨基乙酰肼, 然后与相应的醛缩合得一系列对甲苯磺酰胺基乙酰腙类化合物. 其结构经元素分析, IR, 1H NMR和13C NMR确证. 采用量子化学方法, 在DFT-B3LYP/6-31G*水平上计算了标题化合物4a～4g的反应热、电荷分布和前线轨道能级. 初步生物活性试验结果表明该系列部分化合物在不同浓度下对植物的生长调节表现出一定的规律性.     

Degradation of Perfluorooctane Sulfonamide by Acinetobacter Sp. M and Its Extracellular Enzymes

The Acinetobacter sp. strain M isolated from a contaminated soil sample in Jiangsu Province of China was found to be able to degrade perfluorooctane sulfonamide (PFOSA) effectively. Fluoride anion (F^?) released from PFOSA degradation was detected by ion chromatography, and showed positive correlation to the growth curve of Acinetobacter sp. strain M. The PFOSA degradation efficiency of strain M was approximately 27 %, as assessed by GC analysis. It was shown that enzymes localized outside of cells of Acinetobacter sp. strain M catalyzed the degradation of PFOSA. This further indicates a possibly new (multi‐step/pathway) mechanism for PFOSA degradation. It revealed that the extracellular enzyme of the Acinetobacter strain M preferentially cleaves carbon‐carbon and carbon‐fluorine bonds instead of destroying the carbon‐sulfur bond. The growth condition for Acinetobacter sp. strain M was optimized at 30 °C and pH 7.0 in the presence of 2000 mg L^?1 of PFOSA and 0.5 % (v/v) of Tween‐20. The optimal PFOSA degradation time was found to be 12 h, with a degradation efficiency of 76 % by extracellular enzymes in strain M as determined by GC analysis. The result may provide potential applications for biodegradition of perfluoro organic compounds, such as derivatives of perfluorooctane (C8).     

Dynamic Ligand Reactivity in a Rhodium Pincer Complex

Ligand cooperativity provides (transition) metal complexes with new reactivities in substrate activation and catalytic reactions, but usually the ligand acts as an internal (Brønsted) base, while the metal acts as a (Lewis) acid. We describe the synthesis and stepwise activation of a new phosphane‐pyridine‐amide ligand PNN^H2 in combination with Rh^I. The ligand is susceptible to stepwise proton and hydride loss from the nitrogen arm (imine formation) and deprotonation at the pyridylphosphine arm (dearomatization), giving rise to amine complex 1 , amido species 2 , imine complex 3 and dearomatized compound 4 . Complex 4 bears a dual‐mode cooperative PNN′ ligand containing both a (nucleophilic) basic methine fragment and a reactive (electrophilic) imine moiety. The basic ligand arm enables substrate deprotonation while the imine ligand arm enables reversible “storage” of the activated (nucleophilic) form of a sulfonamide substrate at the ligand. In combination with metal‐based reactivity, this allows for the mono‐alkylation of o‐toluenesulfonamide with iodomethane. Compounds 1 , 3 and 4 are structurally characterized. We also report the first structurally characterized example of an aminal in the coordination sphere of rhodium, complex 5 , [Rh(CO)( PNN′′ )], formed by sequential N?H activation of sulfonamide by the dearomatized ligand PNN′ and follow‐up nucleophilic attack of anionic sulfonamide onto the imine fragment.     

磁性多壁碳纳米管固相萃取/高效液相色谱-串联质谱法测定蜂蜜中多组分兽药残留

建立了以磁性多壁碳纳米管为吸附剂的分散固相萃取/高效液相色谱-串联质谱检测方法,对蜂蜜中3大类44种兽药残留进行测定。样品经pH 4.0的Na2EDTA-Mcllvaine缓冲液提取,加入自制磁性多壁碳纳米管吸附目标物。目标物经10%氨水-甲醇洗脱后,液相色谱-串联质谱MRM模式进行定性定量分析。44种药物在1~40 ng/m L浓度范围内线性关系良好,相关系数均大于0.99;在3个不同浓度添加水平下,回收率为78.0%~105.1%,相对标准偏差(RSD)为1.2%~8.9%,检出限为0.2~2.0μg/kg。结果表明,该方法简单方便,易于操作,为蜂蜜中磺胺类、喹诺酮类以及硝基咪唑类兽药残留的测定提供了新途径。     

固相萃取–高效液相色谱法测定蔬菜中8种磺胺类抗生素

建立固相萃取–高效液相色谱同时测定蔬菜中8种磺胺类抗生素(SAs)的分析方法。蔬菜样品经10 m L乙腈(添加2 g Na_2SO_4+0.1 g CH_3COONa+0.1 g Na_2EDTA)超声提取,提取液用正己烷液–液萃取去脂,经C18–OH固相萃取小柱净化后用高效液相色谱法紫外检测器测定。检测波长为270 nm,柱温为25℃,以乙腈–0.01 mol/L磷酸水溶液为流动相,采用梯度洗脱程序,8种SAs可以较好分离,质量浓度在0.10~100.00 mg/L范围内与色谱峰面积均成良好的线性关系,相关系数为0.999 7~0.999 9,方法检出限为25~75μg/kg,定量限为54~140μg/kg。8种SAs的加标平均回收率为68.70%~122.7%,测定结果的相对标准偏差为1.8%~4.5%(n=5)。该法具有灵敏度高、样品处理简单等优点,可用于蔬菜中磺胺类抗生素的检测。     

Primary sulfonamide as a coupling partner: Copper(I)-catalyzed regioselective cross-coupling of 2-nitro benzenesulfonamides with thiol through the cleavage of Ar–SO2NH2 bonds

In this article, we have presented a novel and efficient method for the direct synthesis of unsymmetrical sulfides through the copper(I)-catalyzed cross-coupling of 2-nitro benzenesulfonamides with thiols in the presence of catalytic amount of CuI in DMF as solvent at 100?°C. In addition, the products were obtained in high to excellent yields. More importantly, the novel system showed the primary 2-nitro benzenesulfonamides as a new coupling partner and regioselectively promoted C–S bond-forming transformations through the cleavage of Ar–SO₂NH₂ bonds.     

CATALYSIS OF POLYSTYRENE N-HYDROXYL SULFONAMIDE FOR ESTERIFICATION OF BUTANOL WITH ACETIC ANHYDRIDE

Polystyrene N-hydroxyl sulfonamide resin l was prepared and used to catalyze the esterification of n-butanol and acetic anhydride. The mechanism of catalytic esterification proved by IR spectra of the resins was found that O-H and N-H of the N-lrydroxyl sulfonamide resin reacted with the acetic anhydride respectively to form the active intermediate polystyrene N.O-diaceyl sulfonamate which was cleaved by n-butanol to produce butyl acetate. The catalytic esterification by resin I was in good agreement with the kinetic model of “bi-bi-ping-pong“ mechanism.     

Solvent extraction studies of newbis-sulfonamide group-containing podands

A number of new open chainbis-sulfonamides with 2, 3 and 4 ether oxygen atoms were synthesized and their Na⁺ and K⁺ extractability was tested. For these types of ligands, both sulfonamide protons are ionized and two aqueous phase cations are complexed in the extraction. The ligand-cation complexes are composed of the ligand in a dianion form, a metal cation and tetramethylammonium hydroxide (TMA) as the co-cation in a ratio of 1 : 1 : 1 when TMA is present, or of ligand and metal cation in a ratio of 1 : 2 when only metal hydroxide is present in the aqueous solution. The influence of different substituents on the phenyl amide group on extractability and extraction selectivity was investigated. An X-ray crystal structure was obtained for the podand containing four ether oxygen atoms. The properties of open-chain ligands were compared with the analogous macrocyclic compounds.     

p-TSA-catalyzed one-pot synthesis and docking studies of some 5H-indeno[1,2-b]quinoline-9,11(6H,10H)-dione derivatives as anticonvulsant agents

The present work describes a facile, one-pot three component environment friendly, green synthesis of a series of 5-(4-methoxyphenyl)-7,7-dimethyl-10-phenyl-7,8-dihydro-5H-indeno[1,2-b]quinoline-9,11(6H,10H)-dione derivatives 8(a-n). 1,3-indanedione, aryl-aldehyde and enaminone was thoroughly ground in the presence of catalytic amount of p-toluene sulfonic acid (p-TSA) to give the titled compounds in good yields. All the synthesized derivatives were evaluated for their anticonvulsant activity using the maximal electroshock (MES) method with phenytoin as a standard drug along with their neurotoxicity effect. Derivatives 8b, 8e and 8k exhibited significant anticonvulsant activity (P<0.001). The neurotoxicity study clearly revealed that all the tested compounds are non-toxic at a dose of 40 mg/kg. The molecular modeling studies also predicted good binding interactions of most active molecules with the serotonin 5-HT_2A receptor. Therefore, it can be safely concluded that synthesized derivatives 8(a-n) would represent useful leads for further investigation in the development of a new class of anticonvulsant agents.