高锰酸钾-甲醛-阿莫西林体系化学发光的研究及应用

在酸性介质中,高锰酸钾能氧化阿莫西林发生化学发光反应,而甲醛的存在可使发光强度增强。据此,采用流动注射技术,建立了一种测定阿莫西林的化学发光分析法。方法的检出限为3.0×10-8g/mL,相对标准偏差为1.52%(n=11,c=1.0×10-5g/mL),线性范围为5.0×10-8~2.0×10-5g/mL。该法已用于阿莫西林胶囊中阿莫西林含量的测定,结果满意。     

K3Fe(CN)6-钙黄绿素体系后化学发光反应测定盐酸氯丙嗪

发现了盐酸氯丙嗪在K3Fe(CN)6-钙黄绿素化学发光反应体系中的后化学发光反应,优化了反应条件,建立了一种利用后化学发光反应测定盐酸氯丙嗪的流动注射化学发光分析法.方法的检出限为3×10-8/mL,相对标准偏差为2.0%(2.0×10-6 g/mL盐酸氯丙嗪,n=11),线性范围为1.0×10-7～1.0×10-5 g/mL.此法已用于盐酸氯丙嗪片剂中盐酸氯丙嗪含量的测定,结果与药典方法测定值一致.     

流动注射化学发光分析法测定利福平

在酸性条件下,KMnO4能氧化利福平产生弱化学发光,并且,利福平能极大的增敏Na2SO3-KMnO4体系的化学发光信号。基于此,结合流动注射技术,建立了测定利福平的新方法。在优化的条件下,利福平在5.0×10-8g/mL~1.0×10-5g/mL范围内与化学发光强度呈良好的线性关系,检出限为3×10-8g/mL。对2.0×10-6g/mL的利福平进行11次平行测定,相对标准偏差为2.6%。该法用于胶囊和滴眼液中利福平的测定,并初步探讨了该化学发光反应机理。     

KMnO4-甲醛-茚三酮化学发光体系的研究

在甲醛存在下,KMnO4与茚三酮能够发生化学发光反应,产生很强的化学发光.据此采用流动注射技术,建立了一种利用KMnO4-甲醛-茚三酮化学发光体系测定茚三酮的方法.方法的检出限为3×10-8 g/mL;相对标准偏差为1.1%(4.0×10-6g/mL茚三酮,n=11);线性范围为1.0×10-7～2.0×10-4 g/mL.本法已用于样品中茚三酮的测定.     

流动注射-化学发光法测定富马酸依美斯汀

在酸性条件下,KMnO4与甲醛能够产生微弱的化学发光,而富马酸依美斯汀的存在能够大大增强该化学发光强度;结合流动注射技术,建立了测定富马酸依美斯汀的流动注射-化学发光新方法。该方法的线性范围分别为3.0×10-8～2.0×10-7g/mL,2.0×10-7～1.0×10-6g/mL和1.0×10-6～8.0×10-6g/mL。检出限为1.0×10-8g/mL,对2.0×10-6g/mL富马酸依美斯汀滴眼液平行测定11次,其相对标准偏差为1.3%。该方法已成功应用于滴眼液中富马酸依美斯汀的含量测定。     

二溴荧光素-N-氯代丁二酰亚胺化学发光体系测定片剂及人血浆中的氢溴酸右美沙芬

研究发现,碱性溶液中,二溴荧光素可吸收N-氯代丁二酰亚胺(NCS)氧化氢溴酸右美沙芬反应的化学能而产生化学发光,从而构建了二溴荧光素-NCS-氢溴酸右美沙芬化学发光体系.利用该体系建立了测定氢溴酸右美沙芬的流动注射化学发光新方法.方法线性范围是9.0×10-10～2.0×10-7 g/mL(r=0.9992),检出限为7.0×10-10 g/mL,对2.0×10-8 g/mL氢溴酸右美沙芬溶液进行11次平行测定的相对标准偏差(RSD)为1.6%.该法已用于片剂及人血浆中氢溴酸右美沙芬含量的测定,结果令人满意.在对有关反应的动力学性质、化学发光光谱及有关物质的紫外吸收光谱和荧光光谱研究的基础上,推断出可能的反应机理.     

高效液相色谱化学发光法测定血清中左羟丙哌嗪

在H2SO4介质中, KMnO4氧化左羟丙哌嗪产生化学发光, 甲醛可增敏上述化学发光, 在此基础上建立了反相高效液相色谱(RP-HPLC)分离, 柱后化学发光检测左羟丙哌嗪的新方法, 并成功应用于血清中左羟丙哌嗪的测定. 在优化的实验条件下, 该法测定左羟丙哌嗪的线性范围为1.0×10-7～1.0×10-5 g/mL, 检出限(3σ)为3×10-8 g/mL. 对2.0×10-6 g/mL的左羟丙哌嗪进行11次平行测定, 其相对标准偏差为2.3%.     

流动注射化学发光法测定阿莫西林

在碱性介质中 ,阿莫西林抗生素对鲁米诺 KMnO4化学发光反应有增敏作用 ,据此建立了微量快速测定阿莫西林的流动注射化学发光分析法。该法线性范围为 1 .0× 1 0 -7～ 5 .0× 1 0 -5g mL ,检出限为 3.0× 1 0 -8g mL ;对 1 .0× 1 0 -6g mL阿莫西林 1 1次平行测定 ,其相对标准偏差为 1 .7%。此法已用于阿莫西林胶囊中阿莫西林的测定。     

铁氰化钾-钙黄绿素体系后化学发光反应测定盐酸硫利达嗪

报道了盐酸硫利达嗪在铁氰化钾-钙黄绿素化学发光反应体系中的后化学发光反应。优化了反应条件,并建立了一种利用后化学发光反应测定盐酸硫利达嗪的流动注射化学发光分析法。方法的检出限为2.0×10-7g/mL,对2.0×10-6g/mL盐酸硫利达嗪测定的相对标准偏差为2.0%(n=11),线性范围为5.0×10-7～5.0×10-5g/mL。该法已用于盐酸硫利达嗪片剂中盐酸硫利达嗪含量的测定,结果与药典方法测定值一致。     

流动注射化学发光分析法测定利血平

研究发现在碱性介质中,利血平对Cr3 催化的Luminol-H2O2体系的化学发光有较强的抑制作用,据此建立了流动注射化学发光抑制法测定痕量利血平的新方法。该法线性范围宽,发光信号的降低值(ΔI)与利血平的质量浓度在1.0×10-8~2.0×10-5g/mL范围内呈良好的线性关系;检出限(3σ)为7.0×10-9g/mL;对于2.0~10-6g/mL利血平进行11次测定,相对标准偏差为1.8%。已用于针剂中利血平的测定。通过对化学发光光谱、紫外吸收光谱的研究,对机理进行了初步探讨。     

α-Amino acid derived enaminones and their application in the synthesis of N-protected methyl 5-substituted-4-hydroxypyrrole-3-carboxylates and other heterocycles

A new and simple synthesis of novel N-protected methyl 5-substituted-4-hydroxypyrrole-3-carboxylates, which exist in equilibrium with their 4-oxo tautomers, has been developed in two steps starting from N-protected α-amino acids. The key intermediates are enaminones, which can also be isolated, characterized, and used for the construction of other functionalized heterocycles, before they spontaneously decompose to pyrrole products. 4-Hydroxypyrroles are prone to partial aerial oxidation but can be efficiently alkylated or reduced to stable polysubstituted pyrrolidine derivatives.     

Specific intramolecular aromatic CH insertion of diazosulfonamides

The chemoselectivity in the intramolecular CH insertion of various diazosulfonamides has been experimentally studied. The results reveal that the aliphatic 1,4-, 1,5-, or 1,6-C(sp³)?H insertions of diazosulfonamides are not accessible, while the aromatic 1,5-C(sp²)?H insertion can be realized specifically by adjusting the diazo-adjacent group. In addition, the general chemoselectivities in the intramolecular CH insertions of diazosulfonyl compounds are summarized. Generally, diazosulfones undergo both aromatic 1,5-C(sp²)?H and aliphatic 1,5- and 1,6-C(sp³)?H insertions, while diazosulfonates undergo aliphatic 1,5- and 1,6-C(sp³)?H insertions. However, diazosulfonamides only undergo aromatic 1,5-C(sp²)?H insertion.     

N-Heterocyclic carbene-palladacyclic complexes: synthesis,characterization and their applications in the C-N coupling and α-arylation of ketones using aryl chlorides

N-Heterocyclic carbene-palladacyclic complexes 3 were successfully achieved in a one-pot procedure under mild conditions. The structure of 3a was unambiguously confirmed by X-ray single crystal diffraction and it was an active catalyst in the Buchwald-Hartwig amination and α-arylation of ketones even at very low catalyst loadings (0.01?mol%).     

Iodine-mediated oxidative Pictet-Spengler reaction using terminal alkyne as the 2-oxoaldehyde surrogate for the synthesis of 1-aroyl-β-carbolines and fused-nitrogen heterocycles

An efficient iodine-mediated oxidative Pictet-Spengler reaction in dimethyl sulphoxide (DMSO) using terminal alkynes as the 2-oxoaldehyde surrogate for the synthesis of aryl (9H-pyrido[3,4-b]indol-1-yl)methanones is described. The scope of the protocol includes the total synthesis of Fascaplysin, Eudistomins Y₁ and Y₂. The methodology is extended for preparing pyrrolo[1,2-a]-quinoxaline and indolo[1,5-a]quinoxaline derivatives. The utility of 1-aroyl-β-carbolines was demonstrated by performing palladium-catalyzed β-carboline directed ortho-C(sp2)-H functionalization of the phenyl ring with thiomethyl (SMe) group using DMSO as source and for accessing 4-aryl-canthin-6-ones.     

Facile synthesis of bicyclic 1-arylpyrazol-5-ones

In this Letter, we described a facile method for constructing fused bicyclic 1-arylpyrazol-5-one ring system. We employed various methylene-containing carboxylic acids as the substrates and proved that the pyrazolone ring closure requires activated methylene group in intermediate II. Accordingly, a series of structurally diversified, fused bicyclic 1-arylpyrazol-5-ones was prepared in moderate to high yields using the requisite substrates.     

A carbanion induced synthesis of highly congested pyrazole and imidazole containing heterocycles

An efficient approach to the synthesis of highly congested di, penta and hexacyclic pyrazoles as well as imidazole fragment containing novel heterocyclic molecule has been developed through a carbanion induced transformation of suitably functionalized 2H-pyran-2-ones, benzo[h]chromene and thiochromeno[4,3-b]pyrans. Due to the presence of fluorescence, we report their prime application metal sensor as off/on switching in ferric ions.     

Synthesis of pyrrolo[1,2-a]pyrazines and pyrazino[1,2-a]indoles by Curtius reaction in Morita-Baylis-Hillman derivatives

Synthesis of substituted pyrrolo[1,2-a]pyrazines and pyrazino[1,2-a]indoles from the Morita-Baylis-Hillman derivatives of acrylates via saponification followed by Curtius reaction is described.     

Cu0-catalysed 1,3-dipolar cycloadditions of α-amino acid derived N,N-cyclic azomethine imines to ynones

A series of 20 CuAIAC reactions between eight 4-acylamino substituted pyrazolidine-3-one-1-azomethine imines and four terminal ynones were performed using Cu⁰ as catalyst. The corresponding fluorescent cycloadducts were obtained in very high yields upon simple workup. Thus, Cu-metal turned out to be a better catalyst than Cu^I in terms of yield and ease of isolation. Availability of azomethine imines, mild reaction conditions, and simple workup enable a “click” access to libraries of densely substituted 2,3-dihydro-1H,5H-pyrazolo[1,2-a]pyrazol-1-ones. Reactivity of differently substituted dipoles was evaluated experimentally and by quantum chemical methods (DFT).     

Synthesis and antioxidative/anti-inflammatory activity of novel fullerene–polyamine conjugates

(E)-4-(Fullerenopyrrolidin-1-yl)-3-methylbut-2-enoic acid and its corresponding succinimidyl ester, readily obtained through Prato-type modification of C₆₀, were used for the selective N-acylation of polyamines. The thus obtained conjugates were evaluated for their antioxidative and anti-inflammatory activity and their cytotoxicity was determined. Members of this family of compounds showed interesting anti-lipid peroxidation, anti-lipoxygenase and anti-inflammatory activity and comparable cytocompatibility to spermidine.