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用于鉴定内源性亲电试剂的加合蛋白质。

Adducted proteins for identification of endogenous electrophiles.

作者信息

Törnqvist M, Kautiainen A

机构信息

Department of Radiobiology, Stockholm University, Sweden.

出版信息

Environ Health Perspect. 1993 Mar;99:39-44. doi: 10.1289/ehp.99-1567046.

Abstract

Chemically reactive compounds in tissues can be monitored through their products of reaction with biomacromolecules. For the purpose of in vivo dose monitoring, hemoglobin (Hb) has been preferred to DNA because of its well-defined life span and more facile chemical identification of adducts. Through the N-alkyl Edman method, adducts to the N-terminals (valines) of the globin chains are measured mass spectrometrically with high sensitivity. In studies of low molecular weight adducts from occupational exposures or tobacco smoke, background levels were found in nonexposed control persons. In some cases the origin of these adducts could be determined. For instance, the 2-hydroxyethyl adduct has been shown to originate from ethylene oxide, a metabolite of endogenously produced ethene. The measured level, about 20 pmole/g globin, agrees well with the ethylene oxide dose calculated from expired ethene. Animal studies indicate contributions from the intestinal flora and dietary factors. An average background level of about 200 pmole/g globin of methylvaline has been observed in unexposed humans. From reaction-kinetic studies of S-adenosylmethionine (SAM), it has been shown that the background mainly originates from SAM. In twin studies, a genetic influence on the level has been shown. Furthermore, a contribution from tobacco smoking to the level was demonstrated in these studies. Certain aldehydes, e.g., malonaldehyde, have been shown to be related to dietary factors and lipid peroxidation. These studies show the usefulness of the method in a search for reactive compounds in the body, with the ultimate goal of assessing the total genotoxic load.

摘要

组织中的化学反应性化合物可通过其与生物大分子的反应产物进行监测。出于体内剂量监测的目的,由于血红蛋白(Hb)的寿命明确且其加合物的化学鉴定更为简便,因此相较于DNA,它更受青睐。通过N - 烷基埃德曼法,可利用质谱高灵敏度地测定球蛋白链N末端(缬氨酸)的加合物。在对职业暴露或烟草烟雾产生的低分子量加合物的研究中,未暴露的对照人群中也发现了背景水平。在某些情况下,可以确定这些加合物的来源。例如,已证明2 - 羟乙基加合物源自环氧乙烷,环氧乙烷是内源性产生的乙烯的代谢产物。测得的水平约为20皮摩尔/克球蛋白,与根据呼出乙烯计算出的环氧乙烷剂量非常吻合。动物研究表明肠道菌群和饮食因素也有影响。在未暴露的人群中,已观察到甲基缬氨酸的平均背景水平约为200皮摩尔/克球蛋白。通过对S - 腺苷甲硫氨酸(SAM)的反应动力学研究表明,背景主要源自SAM。在双胞胎研究中,已表明该水平受遗传影响。此外,这些研究还证明了吸烟对该水平有影响。某些醛类,如丙二醛,已被证明与饮食因素和脂质过氧化有关。这些研究表明该方法在寻找体内反应性化合物方面的有用性,其最终目标是评估总的遗传毒性负荷。

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