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生物重要芳香胺的气相色谱/质谱分析。在人体剂量测定中的应用。

GC/MS analysis of biologically important aromatic amines. Application to human dosimetry.

作者信息

Stillwell W G, Bryant M S, Wishnok J S

出版信息

Biomed Environ Mass Spectrom. 1987 May;14(5):221-7. doi: 10.1002/bms.1200140505.

Abstract

Human exposure to aromatic amines may be monitored by measuring the amount of sulfinamide adduct bound to hemoglobin. In order to develop a sensitive and selective method for measuring aromatic amines present in low concentrations the mass spectra of the pentafluoropropionamide derivatives of a series of aromatic amines were determined under various ionization conditions. With electron ionization the aromatic amine derivatives typically yield intense molecular ions with fragmentation leading to elimination of C2F5 and COC2F5. Higher molecular weight polycyclic aromatic amines, e.g., 6-aminochrysene, give prominent molecular ions as well as intense ions corresponding to M - 174 (loss of CNHCOC2F5). With positive chemical ionization using methane as reagent gas the derivatives give protonated molecular ions as the base peaks, as well as the associated ions at M + 29 and M + 41. Negative ion chemical ionization yields, primarily, peaks corresponding to the loss of HF from the molecular anions. Negative ion chemical ionization with selected ion monitoring is generally more suitable than positive chemical ionization or electron ionization for the quantitative analysis of aromatic amines present in biological samples in the mid femtomolar range. Exposure of human subjects to aromatic amines was determined via basic hydrolysis of the isolated sulfinic acid amide hemoglobin adducts. Analysis of the derivatized extracts by gas chromatography/negative ion chemical ionization/mass spectrometry demonstrated the presence of aniline, ortho-, meta-, and para-toluidine, 2-naphthylamine, and 4-aminobiphenyl. The hemoglobin adduct levels of these amines in both cigarette smokers and nonsmokers were determined.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

人体接触芳香胺的情况可通过测量与血红蛋白结合的亚磺酰胺加合物的量来监测。为了开发一种灵敏且选择性的方法来测量低浓度存在的芳香胺,在各种电离条件下测定了一系列芳香胺的五氟丙酰胺衍生物的质谱。在电子电离下,芳香胺衍生物通常会产生强烈的分子离子,并伴随碎片化,导致消除C2F5和COC2F5。分子量较高的多环芳香胺,如6-氨基 Chrysene,会产生显著的分子离子以及对应于M - 174(失去CNHCOC2F5)的强离子。使用甲烷作为反应气进行正化学电离时,衍生物会产生质子化分子离子作为基峰,以及M + 29和M + 41处的相关离子。负离子化学电离主要产生对应于分子阴离子失去HF的峰。对于定量分析中飞摩尔范围内生物样品中存在的芳香胺,负离子化学电离结合选择离子监测通常比正化学电离或电子电离更合适。通过对分离出的亚磺酸酰胺血红蛋白加合物进行碱性水解来确定人体受试者对芳香胺的接触情况。通过气相色谱/负离子化学电离/质谱对衍生化提取物进行分析,证明了苯胺、邻甲苯胺、间甲苯胺、对甲苯胺、2-萘胺和4-氨基联苯的存在。测定了吸烟者和非吸烟者中这些胺的血红蛋白加合物水平。(摘要截取自250字)

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