微波辅助萃取-高效液相色谱法检测动物组织和牛奶中喹诺酮及非甾体类化合物

本文建立了一种快速的微薄辅助萃取-高效液相色谱法分离检测羊肝、牛肉和牛奶样品中三种喹诺酮类药物（氟罗沙星、洛美沙星和斯帕沙星）和两种非甾类化合物(酮洛芬和布洛芬)的方法。并对微波辅助萃取条件利用正交试验进行了优化：萃取温度为4℃、萃取时间为6min、萃取溶剂为乙腈、萃取溶剂体积为10mL。在浓度范围为0.25—0.75 μg•g－1时各待测物的三种不同水平的添加回收率在60.0%到107%之间,并获得较好的精确度（RSD＜11%）。     

超高效液相色谱-电喷雾串联四极杆质谱法检测牛奶中22种喹诺酮类抗菌素

应用液相色谱-电喷雾串联四极杆质谱仪,检测牛奶中的喹诺酮类(QNs)抗菌素.样品经柠檬酸磷酸盐缓冲液(Mcllvaine)超声提取,采用固相萃取(SPE)方法净化提取液并对目标物质进行富集,用UPLC-MS/MS检测.实验通过空白基质溶液稀释标准,建立校正的标准曲线,可以降低基质对离子化的干扰.结果表明:吡哌酸、依诺沙星、西诺沙星、奥索利酸在3～300 μg/kg,帕珠沙星在5～500 μg/kg,氧氟沙星、加替沙星、司帕沙星在0 5～50 μg/kg,其余14种喹诺酮类化合物在1～100 μg/kg的线性范围内均具有良好的线性关系,相关系数在0 9851～0 9997之间,定量限(LOQ)为0 008～0 339 μg/kg.除了氟甲喹、萘啶酸、那氟沙星的回收率小于60%外,其它喹诺酮的回收率均在63.1%～94.6%之间,相对标准偏差为0 86%～13.12%.     

四氯合钯(II)喹诺酮配合物的合成及与DNA的作用和抗增殖活性

在酸性条件下, 分别合成了四氯合钯(II)离子与2种喹诺酮(诺氟沙星, NFLX＝C16H18N3O3F; 环丙沙星, CPLX＝C17H18N3O3F)离子形成的配合物(NFLXH)2[PdCl4]•2H2O (1)和(CPLXH)2[PdCl4]•2H2O (2). 用元素分析、IR、UV以及摩尔电导测定等方法对其进行了表征. 配合物1的晶体结构经X射线单晶衍射确定, 结构参数: 三斜晶系, P-1空间群, a＝0.84561(17) nm, b＝0.94191(19) nm, c＝1.2832(3) nm; α＝111.26(3)°, β＝97.23(3)°, g＝96.38(3)°, V＝0.9312(4) nm3, Z＝1, 最后吻合因子R＝0.040, wR＝0.088. 利用紫外光谱法、荧光光谱法对配合物与小牛胸腺DNA (ct-DNA)的作用进行了研究, 研究表明, 配合物对DNA的作用模式为插入作用, 与DNA的结合常数Kb分别为: Kb(1)＝2.06×104, Kb(2)＝2.43×104. 其后测试了配合物对体外肿瘤细胞的抗增殖活性. 经采用四甲基偶氮唑蓝分析法(MTT法)测试后发现配合物1和2对人肺腺癌A549细胞、人原髓细胞白血病HL-60细胞的增殖抑制作用显著强于相应的喹诺酮分子本身, 其中配合物2对人肺腺癌A549细胞增殖有明显的抑制作用, 抑制率可高达(95.4±3.7)%, 半数抑制浓度(IC50, 72 h)为(124.5±10.3) μmol•L－1.     

An overview of analytical methodologies for the determination of antibiotics in environmental waters

The widespread occurrence of antibiotics as contaminants in the aquatic environment has increased attention in the last years. The concern over the release of antibiotics into the environment is related primarily to the potential for the development of antimicrobial resistance among microorganisms. This article presents an overview of analytical methodologies for the determination of quinolone (Qs) and fluoroquinolone (FQs), macrolide (MLs), tetracycline (TCs), sulfonamide (SAs) antibiotics and trimethoprim (TMP) in different environmental waters. The analysis of these antibiotics has usually been carried out by high-performance liquid chromatography (HPLC) coupled to mass spectrometry (MS) or tandem mass spectrometry (MS/MS) and to a lesser extent by ultraviolet (UV) or fluorescence detection (FD). A very important step before LC analysis is sample preparation and extraction leading to elimination of interferences and prevention of matrix effect and preconcentration of target analytes.     

三个喹啉氧基乙酰胺镧系(Eu、Gd、Er)配合物的合成、结构及Eu配合物的荧光性质

合成并通过单晶衍射表征了3个稀土配合物Ln(L)(NO₃)₃(H₂O)(L=N-苯基-2-(5-氯-8-喹啉氧基)乙酰胺,Ln=Eu(1),Gd(2),Er(3)),结构与拥有相同有机配体的Pr,Nd和Sm配合物同构。在每个配合物中,十配位的稀土离子采取扭曲的双帽四方反棱柱配位构型,分别与来自1个配体L的2个氧原子和1个氮原子,3个双齿配位硝酸根和1个水分子配位。配合物1能够发射Eu(Ⅲ)离子特征荧光,荧光寿命为437 μs。     

The synthesis and photolysis mechanisms of 8‐nitroquinoline‐based photolabile caging groups for carboxylic acid

Photolabile protecting groups have been extensively studied and applied for protection of small biological molecules, which make it convenient to detect the biological processes of the caged compounds. In this study, a series of 8‐nitroquinoline‐based photolabile caging groups for carboxylic acid were synthesized with improved photolysis efficiency. Among them, 6‐bromo‐8‐nitro‐1, 2‐dihydroquinolinyl chromophore was proven the best derivative on account of its longest absorption wavelength (345 nm), highest caging ability, and quantum yield (Φ = 0.003). Moreover, density functional theory calculations were performed in order to study the photolysis mechanisms. Theoretical calculations revealed that the reaction was kinetically inert under general mild condition with the high barrier height of 34.3 kcal/mol at carbonyl migration step, while under the photolysis condition, because of the large energy gap (64.5 kcal/mol) between S₀ and S₁ states, the reaction should be accessible in the triplet ground state (T₁) through successive excitation of S₀ → S₁ states, subsequent intersystem crossing of S₁ → T₁ states, and finally returned to the stable S₀ state for product via potential energy surface crossing between T₁ and S₀ states. Copyright © 2014 John Wiley & Sons, Ltd.     

高效液相色谱-串联质谱法测定蜂蜜中残留的19种喹诺酮类药物

建立了高效液相色谱-电喷雾串联质谱联用测定蜂蜜中恩诺沙星、环丙沙星、诺氟沙星、氧氟沙星、双氟沙星、恶喹酸、氟甲喹、沙拉沙星、司帕沙星、丹诺沙星、氟罗沙星、马波沙星、伊诺沙星、奥比沙星、吡哌酸、培氟沙星、洛美沙星、西诺沙星和萘啶酸等19种喹诺酮类药物残留的方法。比较酸性溶液阳离子固相萃取(PCX柱)、近中性缓冲溶液反相固相萃取（HLB柱）和碱性溶液阴离子固相萃取(PAX柱)3种不同提取净化方法的提取效果,最终选择使用碱性溶液溶解蜂蜜样品,强阴离子固相萃取柱一步富集净化。以甲醇和0.1%甲酸溶液作为流动相,C18作为分析色谱柱,采用梯度洗脱方式进行液相色谱分离,选择离子反应监测模式检测19种喹诺酮类药物,内标方法定量。在1～100 μg/L范围内,19种喹诺酮类药物的线性相关系数均大于0.991。通过实际样品的添加回收试验,方法的定量限（S/N=10）为1.0 μg/kg,3个添加水平的回收率为71%～118%,相对标准偏差为4.2%～6.7%。     

水溶性稠杂环均三唑并噻二唑体系的合成及生物活性(II): 环丙氟喹诺酮哌嗪衍生物

为发现3-位稠杂环取代喹诺酮衍生物新的生物活性, 以环丙氟氯喹诺酮羧酸(1)为起始原料, 经3步反应得到3-(4-氨基-5-巯基-均-三唑)氟氯喹酮(4). 在常温加热和微波辐射条件下, 4与异烟酸缩环合反应得到中间体3-[6-吡啶-3- 均三唑[3,4-b][1,3,4]噻二唑]氟氯喹诺酮(5). 喹诺酮环上的氯原子与取代哌嗪在聚乙二醇和无机碱催化作用下发生选择性亲核取代反应, 形成相应的3-(6-吡啶-3-均三唑[3,4-b][1,3,4]噻二唑)氟喹诺酮哌嗪游离碱, 与盐酸反应得相应水溶性盐酸盐6. 同时也发现, 用1的酯化物却不能得到中间体2, 而仅得到环丙氟氯吡唑并喹啉酮(3). 新化合物的结构经元素分析和光谱数据表征, 用MTT和二倍试管稀释方法评价了它们体外对CHO, HL60和L1210 3种癌细胞株及S. aureus和E.coli 2种菌株的抑制活性. 结果表明, 在合成的9个新化合物中, 化合物3和 6具有潜在的体外抑制癌细胞生长活性, 其中6的IC50均在50 mmol/L以下, 尤其是化合物6a和6d对L1210的IC50值达到8.0×10－6 mol/L以下, 显示良好的选择性和体外活性; 目标化合物体外抑菌试验有意义的发现, 虽然抑菌活性不及对照环丙沙性, 但对革兰阳性菌活性显著高于对阴性菌的活性, 这与喹诺酮药物的抗菌活性相反. 以上结果表明, 氟喹诺酮类抗菌剂的3位稠杂环取代衍生物作为新结构抗肿瘤或抗菌先导物具有进一步研究和开发的价值.     

Concise, enantiospecific synthesis of (3S,4R)-3-amino-4-ethylpiperidine as partner to a non-fluoroquinolone nucleus

An enantiospecific, eight-step synthesis of (3S,4R)-3-amino-4-ethylpiperidine 3 starting from readily available (S)-(−)-α-methyl-4-pyridinemethanol 6 has been achieved utilizing an Overman rearrangement of a chiral allylic trichloroacetimidate 13 as the key step. A diastereoselective hydrogenation of the resulting chiral allylic amine 15 afforded predominantly the desired trans-substituted piperidine. The conformation of the piperidine along with the directing nature of the amino function are implicated in the selectivity observed.     

A Novel Synthesis of Difloxacin Hydrochloride

Difloxacin, the third generation of new quinolone antibiotics, has broad-spectrum in vitro activity and excellent potency in vivo and has been found to be against gram-positive cocci, gram-negative bacteria, anaerobe, mycoplasm, chlamydia1,2. As described previously, high reaction temperature and hazardous reagents are the defects of the methods for preparation of difloxacin3,4. We have developed a new synthetic method as shown in the Scheme. 2,4-Dichloro-5-fluoro-acetophenone 1 was used as …