Synthesis and characterization of the aqueous solution chemistry of the food-derived carcinogen model N-acetoxy-N-(1-methyl-5H-pyrido[4,5-b]indol-3-yl)acetamide and its N-pivaloyloxy analogue

We report the synthesis of N-acetoxy-N-(1-methyl-5H-pyrido[4,5-b]indol-3-yl)acetamide, 7, its N-pivaloyloxy analogue, 9, and improved synthesis of indole-2-acetonitrile, 3 (70% in five steps from indole-2-carboxylic acid), the carcinogenic amine Trp-P-2, 4 (40% from 3), and the nitro compound, 5 (40% from 4 by oxidation with H₂O₂ using Mo(CO)₆ catalyst). In aqueous solution at neutral pH, 7 primarily undergoes C-O bond cleavage to yield the hydroxamic acid, 8, but under the same conditions the sterically hindered 9 decomposes predominately by N-O bond cleavage with a pH independent rate constant that is 7.5-fold smaller than that for 7. In the pH range 0.5-7.0 three different processes for the decomposition of 9 were detected by kinetics. Only the process that dominates at neutral pH generates a nitrenium species that can be trapped by N₃⁻.     

Formation of Carcinogens in Processed Meat and Its Measurement with the Usage of Artificial Digestion—A Review

Meat is a rich source of various nutrients. However, it needs processing before consumption, what in turn generates formation of carcinogenic compounds, i.a., polycyclic aromatic hydrocarbons (PAH), nitrosamines (NOCs), and the most mutagenic heterocyclic aromatic amines (HAAs). It was widely found that many factors affect the content of carcinogens in processed meat. However, it has recently been discovered that after digestion free HAAs are released, which are not detectable before enzymatic treatment. It was established that the highest percentage of carcinogens is released in the small intestine and that its amount can be increased up to 6.6-fold. The change in free HAAs content in analyzed samples was dependent on many factors such as meat type, doneness, particle size of meat, and the enzyme concentration used for digestion. In turn, introduction of bacteria naturally occurring in the human digestive tract into the model significantly decreases total amount of HAAs. Contrary, the addition of food ingredients rich in polyphenols, fiber, and water (pepper powder, onions, apples) increases free HAAs’ release up to 56.06%. Results suggests that in vitro digestion should be an integral step of sample preparation. Artificial digestion introduced before chromatographic analysis will allow to estimate accurately the content of carcinogens in processed meat.     

Voltammetric Determination of Carcinogenic Derivatives of Pyrene Using a Boron-Doped Diamond Film Electrode

Based on the study of voltammetric behavior of carcinogenic 1-nitropyrene (1-NP), 1-aminopyrene (1-AP), and 1-hydroxypyrene (1-HP), optimum conditions have been found for the determination of these analytes by differential pulse voltammetry (DPV) at a boron-doped diamond film electrode. The optimum medium was methanol-Britton–Robinson buffer (BR buffer) pH 3.0 (70:30) for 1-NP and 1-AP, and methanol-BR buffer pH 5.0 (70:30) for 1-HP. Concentration dependences of the DPV response were measured in the range 1 · 10^?6–1 · 10^?4 mol dm^?3 (R = ?0.9998) with the limit of detection (LOD) 3 · 10^?7 mol dm^?3 for 1-NP, 1 · 10^?7–1 · 10^?5 mol dm^?3 (R = 0.9971) with LOD 6 · 10^?8 mol dm^?3 for 1-AP, and 1 · 10^?7–1 · 10^?5 mol dm^?3 (R = 0.9934) with LOD 1 · 10^?7 mol dm^?3 for 1-HP. Simultaneous determination of 1-NP and 1-AP in a mixture was tested in the methanol-BR buffer pH 3.0 (70:30) medium as well. The content of 1-AP in the concentration range from 1 · 10^?6 to 1 · 10^?4 mol dm^?3 had no effect on the sensitivity of the determination of 1-NP, and vice versa. Due to the close peak potentials of 1-AP and 1-HP, the direct determination of their mixture using voltammetric methods is impossible.     

Structure–activity relationship models for rat carcinogenesis and assessing the role mutagens play in model predictivity

We previously demonstrated that fragment based cat-SAR carcinogenesis models consisting solely of mutagenic or non-mutagenic carcinogens varied greatly in terms of their predictive accuracy. This led us to investigate how well the rat cancer cat-SAR model predicted mutagens and non-mutagens in their learning set. Four rat cancer cat-SAR models were developed: Complete Rat, Transgender Rat, Male Rat and Female Rat, with leave-one-out (LOO) validation concordance values of 69%, 74%, 67% and 73%, respectively. The mutagenic carcinogens produced concordance values in the range 69–76% compared with only 47–53% for non-mutagenic carcinogens. As a surrogate for mutagenicity, comparisons between single site and multiple site carcinogen SAR models were analysed. The LOO concordance values for models consisting of 1-site, 2-site and 4+-site carcinogens were 66%, 71% and 79%, respectively. As expected, the proportion of mutagens to non-mutagens also increased, rising from 54% for 1-site to 80% for 4+-site carcinogens. This study demonstrates that mutagenic chemicals, in both SAR learning sets and test sets, are influential in assessing model accuracy. This suggests that SAR models for carcinogens may require a two-step process in which mutagenicity is first determined before carcinogenicity can be accurately predicted.     

Theoretical study concerning the reactivity of imine derivatives of polycyclic aromatic hydrocarbons

The opening reaction of N-protonated polycyclic aromatic hydrocarbon imines has been computed by means of ab initio, density functional, and semiempirical methods of calculation. Imines are predicted to be more stable than the corresponding O-protonated derivatives, epoxides and diol epoxides. On the other hand, the activated N-methanesulfonylbenzene imine presented more favorable DeltaE( not equal ) and DeltaE(r) for ring opening due to the effect of hydrogen-bond interactions. Anti and syn trans-diol benzene imines did not show a different behavior from the unsubstituted imine. According to these calculations, bay-region, fjord-region, and bay-region methyl-substituted compounds opened more easily among the imine derivatives, following the same reactivity pattern as the oxygen analogs. The exothermicity of the opening process correlated with the charge delocalization in the resulting carbocation.     

Spatiotemporal Distribution and Analysis of Organophosphate Flame Retardants in the Environmental Systems: A Review

In recent times, there has been a cumulative apprehension regarding organophosphate flame retardants (OPFRs) owing to their high manufacturing and usage after brominated flame retardants were strictly regulated and banned from being distributed and used in many countries. OPFRs are known as the main organic pollutants in the terrestrial and aquatic environment. They are very dangerous to humans, plants and animals. They are also carcinogenic and some have been implicated in neurodevelopmental and fertility challenges. OPFRs are distributed into the environment through a number of processes, including the usage, improper disposal and production of materials. The solid phase extraction (SPE) method is suggested for the extraction of OPFRs from water samples since it provides high quality recoveries ranging from 67% to 105% and relative standard deviations (RSDs) below 20%. In the same vein, microwave-assisted extraction (MAE) is highly advocated for the extraction of OPFRs from sediment/soil. Recoveries in the range of 78% to 105% and RSDs ranging from 3% to 8% have been reported. Hence, it is a faster method of extraction for solid samples and only demands a reduced amount of solvent, unlike other methods. The extract of OPFRs from various matrices is then followed by a clean-up of the extract using a silica gel packed column followed by the quantification of compounds by gas chromatography coupled with a mass spectrometer (GC–MS) or a flame ionization detector (GC-FID). In this paper, different analytical methods for the evaluation of OPFRs in different environmental samples are reviewed. The effects and toxicities of these contaminants on humans and other organisms are also discussed.     

环境致癌物的计算机预测研究

环境致癌物可诱发人类或哺乳动物体内的肿瘤,建立环境致癌物的计算机预测模型对环境风险评价和生态安全具有重要的意义．通过构建了3780个化合物的数据集,随机选取其中3024个作为训练集,其余756个作为外部验证集;基于定量构-效关系（QSAR）方法,采用逐步判别分析和主成分分析建立数学模型．结果表明训练集非致癌物预测正确率为86．0％,可能致癌物的预测正确率为88．O％,而采用主成分建模时,非致癌物和可能致癌物的预测正确率分别为74．2％和73．1％．说明逐步判别分析法的结果优于主成分判别分析．同时确定了可能致癌物和非致癌物的分子结构参数,阐明了两者结构差异．以上结果为预测和评估环境致癌物提供参考依据．     

环境致癌物风险评价和生物标记物研究*

反映暴露水平与生物效应等重要信息的生物标记物研究是环境致癌物风险评价的核心内容。本文综述了环境化学致癌物风险性评价和生物标记物的研究现状与发展前景, 以及生物标记物在风险性优先顺序的战略规划过程中所起的重要作用。     

Electron Donor-Acceptor Complexing Reagents for the Detection of Pesticides on TLC

The formation of π-complexes to detect and identify a representative group of carbamate, anilide and urea pesticides was investigated. Results obtained with several electron-acceptor reagents used by previous workers are compared with those obtained with a group of nitro-substituted fluorene derivatives. The pesticides studied were chosen for their potential ability to act as electron donors. Detection limits after thin-layer chromatography ranged from 0.5 to 5.0 micrograms, depending upon the strength of the complex formed. Various chromatographic systems were studied and applications of in situ reflectance spectroscopy and mass spectrometry were investigated. The method combines a reasonable sensitivity with good selectivity and the pesticide may be recovered from the complex for further study. This non-destructive method of analysis should be of particular use in the separation and identification of these pesticides and their metabolites.     

Synthesis of 13C4-labelled oxidized metabolites of the carcinogenic polycyclic aromatic hydrocarbon benzo[a]pyrene

Polycyclic aromatic hydrocarbons (PAHs), such as benzo[a]pyrene (BaP), are ubiquitous environmental contaminants that are implicated in causing lung cancer. BaP is a component of tobacco smoke that is transformed enzymatically to active forms that interact with DNA. We reported previously development of a sensitive stable isotope dilution LC/MS method for analysis of BaP metabolites. We now report efficient syntheses of ¹³C₄-BaP and the complete set of its ¹³C₄-labelled oxidized metabolites needed as internal standards They include the metabolites not involved in carcinogenesis (Group A) and the metabolites implicated in initiation of cancer (Group B). The synthetic approach is novel, entailing use of Pd-catalyzed Suzuki, Sonogashira, and Hartwig cross-coupling reactions combined with PtCl₂-catalyzed cyclization of acetylenic compounds. This synthetic method requires fewer steps, employs milder conditions, and product isolation is simpler than conventional methods of PAH synthesis. The syntheses of ¹³C₄-BaP and ¹³C₄-BaP-8-ol each require only four steps, and the ¹³C-atoms are all introduced in a single step. ¹³C₄-BaP-8-ol serves as the synthetic precursor of all the oxidized metabolites of ¹³C-BaP implicated in initiation of cancer. The isotopic purities of the synthetic ¹³C₄-BaP metabolites were estimated to be ≥99.9%.