铜—腺嘌呤络合物吸附波的研究

了在０．０８ｍｏｌ／ＬＮａＡｃ～０．０２ｍｏｌ／ＬＨＡｃ缓冲溶液铜与腺嘌呤（Ａｄｅ）络合物的极谱行为，结果表明，扫描电压为－０．２Ｖ～－０．７Ｖ时铜－腺嘌呤络合物在单扫示波极谱上有一络合物吸附波，其一阶导数峰电位主－０．４Ｖ（ｖｓ．ＳＣＥ），腺嘌呤浓度在１．０×１０＾－６～１．０×１０＾－５ｍｏｌ／Ｌ范围内与一阶导数波高呈良好的线性关系，检出限为１．０×１０＾－７ｍｏｌ／Ｌ，实验证明，该峰具有吸附     

The thermodynamics of proton dissociation of adenine

The thermodynamic quantities associated with ionization of the N₁ and N₉ protons of adenine have been calorimetrically determined as a function of temperature. The H values for proton dissociation of these groups, with pK values of 4.19 and 9.92, were found to be 5.1 and 9.1 kcal/mole, respectively, at 25°C, =0.025. The C _p values for proton dissociation of these groups were estimated to be –11 and –17 cal/mole-deg. These results indicate that the large heat capacity changes observed during conformational transitions of polynucleotides are not the result of ionization of the bases.     

Cu(phen)2+2和Cu(bpy)2+2与6-巯基嘌呤、腺嘌呤相互作用的研究

在ｐＨ为７．０的磷酸盐缓冲溶液中，用荧光光谱、紫外光谱、电化学及紫外光谱电化学等方法研究了铜配合物与６－巯基嘌呤、腺嘌呤的相互作用．结果表明，Ｃｕ（ｐｈｅｎ）２＋２和Ｃｕ（ｂｐｙ）２＋２与６－巯基嘌呤、腺嘌呤发生了相互作用，但作用程度不同．根据荧光光谱实验数据计算出Ｃｕ（ｐｈｅｎ）２＋２和Ｃｕ（ｂｐｙ）２＋２与６－巯基嘌呤、腺嘌呤的配位比均为１∶１；它们与６－巯基嘌呤作用的配位常数分别为２．２３×１０４Ｌ／ｍｏｌ和６．１１×１０４Ｌ／ｍｏｌ；与腺嘌呤作用的配位常数分别为１．９５×１０４Ｌ／ｍｏｌ和５．１２×１０４Ｌ／ｍｏｌ．电化学实验也获得了相近的结果．这为解释Ｃｕ（ｐｈｅｎ）２＋２和Ｃｕ（ｂｐｙ）２＋２与ＤＮＡ的作用机理及作用部位提供了有益的信息     

Heat-capacity measurements and thermodynamic functions of crystalline adenine; revised thermodynamic properties of aqueous adenine

The standard molar heat capacity C^°_p,m of adenine(cr) has been measured using adiabatic calorimetry over the range 6<(T/K)<310 and the results used to derive thermodynamic functions for adenine(cr) at smoothed temperatures. At T=298.15 K, C^°_p,m=(142.67±0.29) J · K⁻¹ · mol⁻¹ and the third law entropy S^°_m=(145.62±0.29) J · K⁻¹ · mol⁻¹. The standard molar Gibbs free energy of formation Δ_fG^°_m at T=298.15 K for crystalline adenine was calculated, using the standard molar enthalpy of formation for the compound and entropies of the elements from the literature, and found to be Δ_fG^°_m=(301.4±1.0) kJ · mol⁻¹. The results were combined with solution calorimetry and solubility measurements from the literature to yield revised values for the standard molar thermodynamic properties of aqueous adenine at T=298.15 K: Δ_fG^°_m=(313.4±1.0) kJ · mol⁻¹, Δ_fH^°_m=(129.5±1.4) kJ · mol⁻¹, and S_m^°=(217.68±0.44) J · K⁻¹ · mol⁻¹.     

Low-potential amperometric determination of purine derivatives through surface oxide regeneration method

This article described a novel amperometry which can be used for determination of purine derivatives including uric acid, xanthine, hypoxanthine, guanine, and adenine without surface contamination. By applying a constant potential of −0.125 V (vs. Ag/AgCl) in a flow injection system, the chelating capability of these purine derivatives converts the cuprous oxide layer into a soluble complex. This behavior would dissolve the passive oxide layer and expose the bottom copper layer to the solution, subsequently; an oxidation current which attributed to the regeneration of the original cuprous oxide layer is used to reflect the concentration of these purine derivatives. In a 50 mM phosphate buffer, pH 7.0, this approach provides a high sensitivity with LOQ of sub-micro molar level of five purines and high stability with a RSD of 2.5% for 10 μM xanthine (N = 12). This method does not suffer from most biological species including ascorbic acid, acetaminophen, creatine, dopamine, sarcosine, ammonium ion, chloride ion, and urea at equal or higher than its physiological concentration.     

The synthesis and crystal structure of a new diprotonated Schiff base cryptand

Abstract

The synthesis and crystal structure of the diprotonated cryptand derived from the reaction of tren and 2,6-diacetyl pyridine is reported. The imino nitrogens of the Schiff base linkages are directed so that the dicarbimine functions are in trans, trans geometry relative to the pyridine C-N bond. This configuration has not previously been reported in related pyridine-derived Schiff base macrocycles.     

Synthesis of novel 9-aryl and heteroarylpurine derivatives via copper mediated coupling reaction

A series of 9-(hetero)arylpurine derivatives has been prepared through N-arylation of 6-chloropurine with boronic acids in the presence of copper(II) acetate. Screening reaction conditions in terms of bases and solvents led to the successful coupling of a series of sterically demanding (hetero)arylboronic acids, never described so far. The coupling products were next readily converted into the target adenine derivatives. The described procedure provides easy access to original fragments for screening applications. Moreover these 9-aryl-6-chloropurine derivatives might be useful as intermediates for the preparation of purine derivatives with potential biological properties.     

酶荧光毛细分析法测定血清中微量丙酮酸

提出了一种用于血清微量丙酮酸（PA）测定的酶荧光毛细分析法（P-LE-FCA）。优选的测定条件为：乳酸脱氢酶和还原型辅酶Ⅰ的浓度分别为100U/L和60μmol/L,反应时间5min。测定PA的线性范围4—80μmol/L,检出限0.73μmol/L,RSD〈1.3%。血清共存物质对PA测定无明显干扰。使用该方法对血清PA进行测定,其回收率在93.0%—106.5%之间;结果与常规紫外分光光度法一致。本方法的样品预处理过程简单、省时,省试剂,灵敏度高,重现性好。     

On-line combination of single-drop liquid–liquid–liquid microextraction with capillary electrophoresis for sample cleanup and preconcentration: A simple and efficient approach to determining trace analyte in real matrices

In order to improve the sensitivity of capillary electrophoresis (CE) and overcome the deficiency of commercial CE instruments in handling complex matrices directly, we proposed a novel technique which combined single-drop liquid–liquid–liquid microextraction (SD-LLLME) with CE on-line. In this technique, SD-LLLME was realized using a commercial CE instrument and, to further concentrate the target analyte, large-volume sample stacking combined sweeping without polarity switching was utilized. Even though without agitating the donor phase in the extraction process, the model compound, adenine was enriched 550-fold in only 10 min. The enrichment factors were 760 and 1030 when the extraction time was extended to 30 and 60 min, respectively. The relative standard deviations (RSDs) of adenine were 5.24% and 2.29% for peak area and migration time, respectively, which indicated that this method was much more reproducible compared to the existing methods that combined sample-preparation strategies with CE. In addition, this approach was selective while cleaning up target analyte. These mentioned advantages allowed the developed method to be an attractive approach to determining trace target compounds in complex real samples.     

The ‘t‐Amino Effect’ of ortho‐Nitroso Amines. Synthesis of 2,6‐Diaminoadenine Derivatives from 6‐(Dialkylamino)‐5‐nitrosopyrimidines

The ‘t‐amino effect’ of amino‐nitroso compounds was documented by preparing the (dialkylamino)‐nitroso pyrimidines 4 – 18 , and cyclising them under thermal conditions in high yields to the purine derivatives 19 – 32 . The reactivity of the amino‐nitroso‐pyrimidines, particularly of 17 derived from diethyl iminodiacetate, and of 19 , derived from 1‐phenylimidazolidine, correlates with the stability of the intermediate azomethine ylide. Thermolysis of the amino‐nitroso‐pyrimidines 34 – 37 , possessing dialkylamino substituents at C(4) and C(6), proceeded by protiodenitrosation, leading to 38 – 41 .