Preparation and Characterization of Olaquindox Polyclonal Antibody

本研究先将喹乙醇琥珀酸单酯化,使其转变为带有羧基的衍生物。合成产物经重结晶纯化,得率为52.47%。合成产物进行结构鉴定,合成了具有喹乙醇分子结构特征的喹乙醇半抗原。采用活化酯法将半抗原与牛血清白蛋白（BSA）进行偶联,采用混合酸酐法将半抗原与卵清蛋白（OVA）进行偶联,分别制备免疫原和包被抗原。紫外扫描与红外图谱分析结果表明,半抗原与载体蛋白偶联成功,与BSA、OVA的结合比分别为3.8:1和5.0:1。以OLA-BSA作为免疫原免疫4只新西兰大白兔,获得了较高效价的抗血清,以OLA-OVA作为包被抗原,间接ELISA法测定各兔的效价,分别为1:6400;1:1600;1:12800;1:6400。间接ELISA法喹乙醇的抑制中浓度IC50为743.3 ng/mL,最低检测限IC20为5.71 ng/mL。从电泳图谱分析可以看出,经纯化得到了纯度较高的喹乙醇多克隆抗体,为喹乙醇免疫分析方法的进一步研制和开发奠定基础。     

Glycation sites in neoglycoglycoconjugates from the terminal monosaccharide antigen of the O‐PS of Vibrio cholerae O1, serotype Ogawa,and BSA revealed by matrix‐assisted laser desorption–ionization tandem mass spectrometry

We present the MALDI‐TOF/TOF‐MS analyses of various hapten–bovine serum albumin (BSA) neoglycoconjugates obtained by squaric acid chemistry coupling of the spacer‐equipped, terminal monosaccharide of the O‐specific polysaccharide of Vibrio cholerae O1, serotype Ogawa, to BSA. These analyses allowed not only to calculate the molecular masses of the hapten–BSA neoglycoconjugates with different hapten–BSA ratios (4.3, 6.6 and 13.2) but, more importantly, also to localize the covalent linkages (conjugation sites) between the hapten and the carrier protein. Determination of the site of glycation was based on comparison of the MALDI‐TOF/TOF‐MS analysis of the peptides resulting from the digestion of BSA with similar data resulting from the digestion of BSA glycoconjugates, followed by sequencing by MALDI‐TOF/TOF‐MS/MS of the glycated peptides. The product‐ion scans of the protonated molecules were carried out with a MALDI‐TOF/TOF‐MS/MS tandem mass spectrometer equipped with a high‐collision energy cell. The high‐energy collision‐induced dissociation (CID) spectra afforded product ions formed by fragmentation of the carbohydrate hapten and amino acid sequences conjugated with fragments of the carbohydrate hapten. We were able to identify three conjugation sites on lysine residues (Lys235, Lys437 and Lys455). It was shown that these lysine residues are very reactive and bind lysine specific reagents. We presume that these Lys residues belong to those that are considered to be sterically more accessible on the surface of the tridimensional structure. The identification of the y‐series product ions was very useful for the sequencing of various peptides. The series of a‐ and b‐product ions confirmed the sequence of the conjugated peptides. Copyright © 2010 John Wiley & Sons, Ltd.     

Facile and Sensitive Spectrophotometric Determination of Propoxur in Formulations and Environmental Samples

A facile, rapid, and sensitive spectrophotometric method for the determination of propoxur in insecticidal formulations, fortified water, vegetables, agricultural wastewater, and agricultural soil samples has been elaborated. The proposed method is based on the hydrolysis of propoxur under basic conditions, followed by instantaneous azo coupling of the resulting 2‐isopropoxyphenol with the anilines 2a – c . This yielded the orange‐red chromophore 3a (λ_max=at 470 nm), the pale‐red coupling product 3b (490 nm), or the red derivative 3c (478 nm), which are stable for 46 h, 38 h, and 24 h, respectively, and could be readily analyzed spectrophotometrically.     

Quasiphosphonium intermediates—IV: Isolation and identification of intermediates in the arbuzov and perkow reactions of neopentyl esters of phosphorus(III) acids with α-halogenoacetophenones

Crystalline ketophosphonium bromides have been isolated as intermediates in the reactions of trineopentyl phosphite, dineopentyl phenylphosphonite, and neopentyl diphenylphosphinite with α-bromoacetophenone. Thermal decomposition in solution occurs in each case to yield neopentyl bromide and the corresponding Arbuzov product only. Rearrangement to the Perkow intermediate or product does not occur. An identifiable Perkow intermediate was separated from the reaction of neopentyl diphenylphosphinite with α-chloroacetophenone at O° and was shown to yield neopentyl chloride and the corresponding Perkow product by a first-order process in chloroform (t1/2 ca 40min at 33°). It is suggested that the betaine formed by initial attack of phosphorus at the carbonyl carbon atom may be a common first intermediate in reactions that yield both Arbuzov and Perkow products     

Stability studies of propoxur herbicide in environmental water samples by liquid chromatography-atmospheric pressure chemical ionization ion-trap mass spectrometry

Liquid chromatography-atmospheric pressure ionization ion-trap mass spectrometry has been investigated for the analysis of polar pesticides in water. The degradation behavior of propoxur, selected as a model pesticide belonging to the N-methylcarbamate group, in various aqueous matrices (Milli-Q water, drinking water, rain water, seawater and river water) was investigated. Two interfaces of atmospheric pressure ionization, atmospheric pressure chemical ionization (APCI) and electrospray ionization (ESI), were compared during the study. Propoxur and its transformation product (N-methylformamide) were best ionized as positive ions with both APCI and ESI, while another transformation product (2-isopropoxyphenol) yielded stronger signals as negative ions only with APCI. In addition, the effects of various pH, matrix type and irradiation sources (sunlight, darkness, indoor lighting and artificial UV lamp) on the chemical degradation (hydrolysis) were also assessed. From the kinetic studies of degradation, it was found that the half-life of propoxur was reduced from 327 to 161 h in Milli-Q water with variation of irradiation conditions from dark to sunlight exposure. Degradation rates largely increased with increasing pH. The half-life of the target compound dissolved in Milli-Q water under darkness decreased from 407 to 3 h when the pH of Milli-Q water was increased from 5 to 8.5. These suggest that hydrolysis of propoxur is light-intensity and pH-dependent. In order to mimic contaminated natural environmental waters, propoxur was spiked into real water samples at 30 microg/l. The degradation of propoxur in such water samples under various conditions were studied in detail and compared. With the ion trap run in a time-scheduled single ion monitoring mode, typical limits of detection of the instrument were in the range of 1-10 microg/l.     

Sensitive determination of propoxur by spectrophotometry using 3-aminopyridine.

A simple spectrophotometric method for the determination of propoxur, a widely used insecticide, in various environmental samples and pesticide formulations is described. The method is based on the coupling of the hydrolysis product of propoxur with diazotized 3-aminopyridine in an alkaline medium, to form an azo-dye which has a maximum absorbance at 463 nm. Beer's law is obeyed over the concentration range of 0.05 to 1.2 microg ml(-1) of propoxur. The molar absorptivity and Sandell's sensitivity are found to be 3.10 x 10(4) l mol(-1) cm(-1) and 0.007 microg cm(-2), respectively. The important analytical parameters and optimum reaction conditions were evaluated. The method is free from the interference of other commonly used pesticides and inorganic metal ions.     

二氟亚烷基卡宾与甲醛环加成反应机理的理论研究

用二阶微扰理论研究单重态二氟亚烷基卡宾与甲醛发生的环加成反应机理,采用MP2/6-31G^*方法计算了势能面上各驻点的构型参数、振动频率和能量.结果表明,单重态二氟亚烷基卡宾与甲醛的环加成反应主要有两种反应通道,通道1中,两个反应物经a,b和c三条反应途径生成三元环构型的产物P1,其中途径c是主反应途径,该途径有两步组成:(Ⅰ)二氟亚烷基卡宾与甲醛生成了1个富能中间体(INT1c),是无势垒放热反应,放出能量为219.18kJ/mol;(Ⅱ)中间体(INT1c)异构化为产物二氟亚烷基环氧乙烷,其势垒为134.71kJ/mol.通道2的反应途径由三步组成:(Ⅰ)反应物首先生成了1个富能中间体(INT1b),为无势垒的放热反应,放出的能量142.77kJ/mol;(Ⅱ)中间体(INT1b)异构化成另一中间体(INT2),其势垒为22.31kJ/mol;(Ⅲ)中间体(INT2)异构化成四元环构型产物P2,其势垒为11.98kJ/mol.     

Determination of Triazines and N-Methylcarbamate Pesticides in Water by High-Performance Liquid Chromatography-Diode Array Detection

A rapid and selective method for the simultaneous determination of triazine herbicides (atrazine, its degradation product desethylatrazine, simazine, prometryn, terbutryn) and N-methylcarbamate insecticides (propoxur, carbaryl and methiocarb) in surface water has been developed. A 0.5 L of the water sample was preconcentrated by passage through a 1 g C₁₈ solid-phase extraction cartridge. The retained compounds were eluted with 5 mL of methanol from the cartridge. The pesticides were separated and quantified by reversed-phase high-performance liquid chromatography with UV diode-array detection. Analytical separation was performed using a concave gradient elution with acetonitrile and water on a C₁₈ column. Prometryn and terbutryn were determined at 240 nm; propoxur, methiocarb at 204 nm and the others at 220 nm. Recoveries varied from 85 to 102% over concentrations at 0.025 and 0.2 µg L^?1. The limits of detection for the compounds investigated are in the range of 0.005-0.012 µg L^?1.     

分光光度法测定果蔬中残杀威残留量

在碱性条件下残杀威水解生成酚盐,在盐酸介质中对氨基苯磺酸与亚硝酸根发生重氮化反应,上述所得酚盐和重氮化产物在氨性溶液中偶联生成偶氮染料,此偶联产物的最大吸收波长为427nm,据此提出了分光光度法测定果蔬中残杀威含量的方法。残杀威的质量浓度在0.17～2.04mg·L-1范围内与其吸光度呈线性关系,检出限(3s/k)为0.03mg·L-1。方法用于测定果蔬中残杀威的含量,相对标准偏差(n=5)在0.3%～0.7%之间,加标平均回收率为96%。     

Synthesis of a novel diarylphosphinic acid: a distorted ground state mimic and transition state analogue for amide hydrolysis

We describe herein the synthesis of a new unsymmetrical diarylphosphinic acid, a hapten aimed to produce catalytic antibodies for the hydrolysis of heterocyclic amides. The phosphinate functionality was selected as a mimic both of the tetrahedral intermediate and the transition state of higher energy along the reaction profile. The phenyl and 2,4,6-(trimethyl)-phenyl groups flanking the phosphinate were chosen in order to impose rotation around the P–C bond, a choice supported by ab initio calculations. This new hapten should elicit catalytic antibodies whose binding site could affect the distortion at nitrogen as well as the twist along the N–C(O) bond for heterocyclic amides. This hapten along with a series of new sterically hindered unsymmetrical phosphinic acid derivatives was prepared by a key palladium-catalysed step.     

Rapid and Sensitive Screening Method for the Determination of Carbaryl and Propoxur Using p-Nitroaniline

Abstract

A rapid screening method for the determination of carbaryl and propoxur using p-nitroaniline is described. Carbaryl and propoxur are determined spectrophotometrically: carbaryl forms a stable blue coloured species with diazotized p-nitroaniline in a fairly alkaline medium while propoxur forms a purple coloured species with the same reagent under similar conditions. The blue and purple coloured species are extracted into 3-methyl-1-butanol showing absorbance maxima at 605 and 540 nm, respectively. The relationship between absorbance and concentration is linear in the range of 0.12 - 0.96 ppm and 0.19–1.5 ppm, respectively for carbaryl and propoxur. The method can successfully be applied for the determination of carbaryl and propoxur to levels as low as 0.04 and 0.06 and 0.12 and 0.19 ppm in water and grain samples, respectively.     

Solid-Phase Synthesis of a Biotin Derivative and its Application to the Development of Anti-Biotin Antibodies

A biotin derivative, namely biotin–aminocaproic acid–lysine (BAL), was synthesized with solid-phase chemistry, conjugated to a carrier-protein, and used for rabbit immunization. The aminocaproic acid–lysine “long-arm” was used in order to project the biotin-hapten above the carrier-protein surface. Lysine was selected due to its N^ε-amino group, through which BAL was conjugated to the carrier-protein. BAL was synthesized on a commercially available resin with the Fmoc-solid-phase strategy; this has simplified the experimental procedure, overcome the need for intermediate purification steps, and led to a final product of high purity, with high yield. The anti-BAL antibodies recognized free biotin, as shown with an in-house-developed ELISA, in which biotin conjugated to a synthetic “lysine–dendrimer” was used to coat the ELISA microwells. In immunocytology and Western-blot experiments, the anti-BAL antibodies led to similar results with those obtained with streptavidin. Synthetic derivatives of hapten molecules that can be easily prepared with solid-phase chemistry, such as BAL, may be used for the development of specific antibodies for the corresponding hapten.     

去甲氯胺酮半抗原及其全抗原的合成与鉴定

在低温条件下,去甲氯胺酮与琥珀醛酸反应,合成了半抗原羧基-去甲氯胺酮,电喷雾质谱鉴定结果表明,目标半抗原合成成功;通过碳二亚胺法将半抗原与载体蛋白偶联制备人工抗原,红外光谱法鉴定结果表明,人工抗原合成成功,基质辅助激光解析电离飞行时间质谱鉴定表明去甲氯胺酮半抗原与牛血清白蛋白的偶联比为11:1。经动物免疫,获得高效价特异性多克隆抗体,抗血清效价可达5.12×104。     

Steric strain and reactivity: electrophilic bromination of trans-(1-methyl-2-adamantylidene)-1-methyladamantane

trans-(1-Methyl-2-adamantylidene)-1-methyladamantane (DMAD, 1b) reacts with Br(2) in chlorinated hydrocarbon solvents to give either a bromonium polybromide ion pair or a substitution product, depending on bromine concentration. The first intermediate is a 1:1 pi-complex having K(f) = 1.85(0.19) x 10(3) M(-)(1) at 25 degrees C, which rapidly evolves to the bromonium tribromide ion pair. At high bromine concentration, which shifts all equilibria involving the counteranion of the ion pair intermediate toward the pentabromide species, this bromonium ion is stable and unable to further evolve into products. Temperature-dependent NMR spectra indicate chemical exchange of Br(+) between the sides of the plane containing the two carbons of the bromonium ion. At very low bromine concentration, no ionic intermediate is detected and the reaction rapidly yields a rearranged substitution product, identified as 10. Under these conditions the disappearance of the pi-complex follows a first-order rate law, and the observed rate constant increases with increasing olefin concentration, showing that product formation implies Br(-) as counteranion of the ionic intermediate, whose formation is a reversible process. A comparison of the results reported here for the bromination of 1b with those previously found for the parent olefin, adamantylideneadamantane (1a), shows that steric strain markedly affects the reactivity of the double bond.     

Direct detection of a transient oxenium ion in water generated by laser flash photolysis

Laser flash photolysis of the quinol ester 2b in O2-saturated aqueous phosphate buffer at pH 7.1 with excitation at 266 nm generates a transient intermediate with lambda(max) 460 nm that decays in a first-order manner with an aqueous solution lifetime of (170 +/- 10) ns at 22 degrees C. This intermediate is not affected by O2, but reacts rapidly with N3- with an apparently diffusion-limited rate constant of (6.6 +/- 0.2) x 10(9) M-1 s-1. Steady state photolysis of 2b yields the quinol 3b as a major reaction product with a yield of ca. 30-35% after correction for photolytic decomposition of 3b. This is the same product that is quantitatively produced by hydrolysis of 2b in the dark. Photolysis of 2b in the presence of 40 mM N3- completely suppresses the yield of 3b The photolytic intermediate is identified as the aryloxenium ion 1b, that was previously indirectly detected by N3--trapping during the hydrolysis of 2b, based on the chemical behavior of the transient and the quantitative agreement of the N3-/solvent selectivity ratio, kaz/ks, measured directly during the flash photolysis experiment, and indirectly by the azide clock procedure during the hydrolysis reaction. Other, as of yet unidentified, transients are produced during the photolysis reaction. A strong transient absorbance band observed at 360 nm decays in a biphasic manner with two first-order rate constants, neither of which are affected by O2 or N3-. The lifetimes of the two intermediates of ca. 12 and 75 mus are considerably longer than that of 1b. Another very short-lived species can be detected at early reaction times (相似文献   

Efficient synthesis of 4,4'-bi-1H-imidazol-2-ones from 5-amino-alpha-imino-1H-imidazole-4-acetonitriles and isocyanates

Reactions of 5-amino-alpha-imino-1H-imidazole-4-acetonitriles 1 with alkyl and aryl isocyanates led to efficient syntheses of 5'-amino-5-imino-4,4'-bi-1H-imidazol-2-ones 3 formed by intramolecular cyclization of the corresponding 5-amino-alpha-(N-alkyl/arylcarbamoyl)imino-1H-imidazole-4-acetonitriles 2. The cyclization occurs only slowly in solution but is considerably accelerated by the addition of a catalytic amount of DBU (1,8-diazabicyclo[5.4.0]undec-7-ene). The reaction of the N-arylamidine 6b, the synthetic precursor of the imidazole 1b, with benzyl isocyanate also led to the formation of 4,4'-bi-1H-imidazol-2-one 3b in quantitative yield. The imidazole intermediate 2b has been isolated and found to be identical with the compound obtained by reaction of the imidazole 1b and benzyl isocyanate. The N-arylamidine 6c (R = 4-NCC(6)H(4)) reacted with benzyl isocyanate in a similar way, but the electrophilicity of the amidine carbon atom resulted in rapid hydrolysis of the intermediate 7c leading ultimately to the isolation of the urea 9. The N-alkylamidines 6a and 6d behaved differently in their reaction with benzyl isocyanate, and the major product isolated in these reactions is again the urea 9.     

Reactivity of a phosphoranyl radical generated by photoreaction of phenyl diphenylphosphinite with 10-methylacridinium iodide. α-Scission vs. single electron transfer

Photoreaction of phenyl diphenylphosphinite ( 1b ) with 10-methylacridinium iodide ( 2 ) in aqueous acetonitrile under an argon atmosphere gives 10-methylacridan, the reduction product from 2 , in a quantitative yield and phenyl diphenylphosphinate, the oxidation product from 1b , in a low yield, as well as a large amount of diphenylphosphinic acid and a moderate amount of phenol. The product distribution observed here is interpreted well in terms of decomposition of a phosphoranyl intermediate through both α-scission and single electron transfer (SET) pathways.     

An efficient route for the preparation of a 21-fluoro progestin-16 alpha,17 alpha-dioxolane,a high-affinity ligand for PET imaging of the progesterone receptor

Two different synthetic routes were explored for the synthesis of fluoro furanyl norprogesterone (FFNP) 1, a high-affinity ligand for the progesterone receptor (PgR) that is being developed as a PET imaging agent for PgR-positive breast cancer. Both approaches proceed through a key intermediate, triol 5. The first approach, starting from keto-ketal 2, employed a dioxenyl group as a synthon for installing a corticosteroid side chain in keto-alcohol 4. The second approach, starting from propargylic acetate 12b, involved the application of a two-step method, a Pd(II)-catalyzed oxidative rearrangement followed by a base-catalyzed acetate rearrangement of the intermediate unsaturated acetate 13b, to generate the requisite corticosteroid side chain in keto-acetate 14b. This intermediate was further elaborated to the final product 1 via efficient dihydroxylation with potassium permangnate, furan acetalization with scandium triflate, and mesylation and fluorination reactions. The palladium-catalyzed route is considerably more efficient than the dioxene approach for the synthesis of key intermediate triol 5, and the scandium triflate-catalyzed acetalization, in particular, led to a considerable improvement in the overall yield of the endo furan acetal alcohol 16a. This route provides a major improvement in the overall yield of the final progestin target, FFNP 1.     

Analysis of carbofuran residues in soil by the stopped-flow technique

A simple method for the determination of carbofuran by the stopped-flow technique and which is suitable for its routine analysis in soil samples is reported. The method was based on the coupling reaction between carbofuran phenol (the hydrolysis product of carbofuran) and diazotised sulphanilic acid to form a coloured compound, the rate of formation of which was monitored spectrophotometrically. The calibration graph was linear in the range 1-40 micrograms ml-1 (RSD, 2%) and the method was highly selective. The average recovery of carbofuran was 96.5% from soil, and less than 0.5 micrograms g-1 could be detected. A procedure for the resolution of propoxur - carbofuran mixtures of mass ratios in the range 5:1-1:10 with a precision of ca 3% is also described.     

Rearrangements of the Diels-Alder cycloadducts obtained from acetylenic sulfones and 1,3-diphenylisobenzofuran

1,3-Diphenylisobenzofuran afforded Diels-Alder cycloadducts 4a,b with n-butyl- and phenyl-substituted acetylenic sulfones 3a,b, respectively. The products underwent various types of rearrangements under pyrolytic, acid-catalyzed, and photochemical conditions. In the presence of acid, or upon heating in xylenes, they afforded the ketones 5a,b. In addition, the dehydration product 7a was produced from the pyrolysis of 4a, and the unexpected transposed ketone 6b was generated under acid-catalyzed or pyrolytic conditions from 4b via a postulated epoxide intermediate. The photolysis of 4a afforded ketone 5a as the sole isolated product, whereas 5b afforded oxepin 8b and indenyl phenyl ketone 9b. The formation of the latter two products can be rationalized by a series of pericyclic reactions. These include an intramolecular [2+2] cycloaddition, followed by a 1,3-dipolar cycloreversion, for the transformation of 4b to 8b and a series of electrocyclic and [1,3]sigmatropic reactions to convert 8b into 9b.