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吲哚美辛和花生四烯酸对苯乙烯及苯乙烯-7,8-氧化物诱导姐妹染色单体交换的影响。

Effects of indomethacin and arachidonic acid on sister chromatid exchange induction by styrene and styrene-7,8-oxide.

作者信息

Lee S H, Norppa H

机构信息

Department of Preventive Medicine, Catholic University Medical College, Seoul, South Korea.

出版信息

Mutat Res. 1995 Dec;348(4):175-81. doi: 10.1016/0165-7992(95)90006-3.

Abstract

Styrene is converted into styrene-7,8-oxide in human lymphocyte cultures, in a reaction probably mediated by oxyhemoglobin. As a consequence, styrene induces sister-chromatid exchanges (SCEs) in whole-blood lymphocyte cultures without exogenous metabolic activation systems. Another metabolic pathway that could be involved in the metabolism of styrene is cooxidation by prostaglandin-endoperoxide synthase (PES). To study the role of PES in the metabolism of styrene, human whole-blood lymphocyte cultures were treated for the entire culture time of 72 h with styrene (0.5 and 1 mM) or styrene-7,8-oxide (50 and 100 microM), in the presence and absence of 75 or 150 microM indomethacin (an inhibitor of PES) and arachidonic acid (substrate of PES). Indomethacin potentiated SCE induction by both styrene and styrene-7,8-oxide; a slight but statistically significant enhancement (16-32%; p < 0.05-0p < 0.001) was observed in all treatments with styrene and at 150 microM indomethacin in the case of styrene-7,8-oxide. At 150 microM, arachidonic acid induced a 15-20% suppression (p < 0.01) in SCE induction by both styrene (1 mM only) and styrene-7,8-oxide (100 microM only). Indomethacin or arachidonic acid did not alone influence the frequency of SCEs. The results suggest that PES acts as an inactivation route for styrene and styrene-7,8-oxide in human whole-blood lymphocyte cultures, possibly through PES-mediated binding to glutathione.

摘要

在人类淋巴细胞培养物中,苯乙烯可转化为7,8 - 环氧苯乙烯,此反应可能由氧合血红蛋白介导。因此,在没有外源性代谢激活系统的情况下,苯乙烯可在全血淋巴细胞培养物中诱导姐妹染色单体交换(SCEs)。另一条可能参与苯乙烯代谢的途径是由前列腺素内过氧化物合酶(PES)进行的共氧化作用。为研究PES在苯乙烯代谢中的作用,在存在和不存在75或150微摩尔吲哚美辛(一种PES抑制剂)及花生四烯酸(PES的底物)的情况下,用苯乙烯(0.5和1毫摩尔)或7,8 - 环氧苯乙烯(50和100微摩尔)对人类全血淋巴细胞培养物进行72小时的整个培养时间处理。吲哚美辛增强了苯乙烯和7,8 - 环氧苯乙烯对SCE的诱导作用;在所有苯乙烯处理组以及150微摩尔吲哚美辛处理7,8 - 环氧苯乙烯的情况下,均观察到轻微但具有统计学意义的增强(16 - 32%;p < 0.05 - p < 0.001)。在150微摩尔时,花生四烯酸在苯乙烯(仅1毫摩尔)和7,8 - 环氧苯乙烯(仅100微摩尔)诱导SCE方面均诱导了15 - 20%的抑制(p < 0.01)。吲哚美辛或花生四烯酸单独均不影响SCE的频率。结果表明,在人类全血淋巴细胞培养物中,PES可能通过介导与谷胱甘肽的结合,作为苯乙烯和7,8 - 环氧苯乙烯的失活途径。

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