3,4-环氧丁烷-1,2-二醇对不同GSTT1和GSTM1基因型人淋巴细胞姊妹染色单体交换的诱导作用

Sabrina Bernardini , Katarina Pelin , Kimmo Peltonen , Hilkka Järventaus , Ari Hirvonen , Constantin Neagu , Marja Sorsa , Hannu Norppa
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引用次数: 29

摘要

研究了用1,3-丁二烯的代谢产物3,4-环氧丁烷-1,2-二醇(EBD)处理48小时对22名具有两种多态性谷胱甘肽S-转移酶(GSTT1和GSTM1)基因型的人类供体全血淋巴细胞培养物中姐妹染色单体交换(SCEs)的诱导作用。对于这两个基因,包括代表缺乏相应GST基因和同工酶的纯合“无效”基因型和至少有一个完整基因和GST活性的“阳性”基因型的供体。SCE/细胞的平均频率在所有基因型组中相似:GSTT1无效(n=10)(250μM EBD平均22.0,250 500μM EBD平均32.9)、GSTT1阳性(n=14)(分别为21.3和34.6)、GSTM1无效(n=10)(20.3和33.5)和GSTM1阳性供体(n=15)(20.6和34.8),所有供体的淋巴细胞培养均显示复制指数显著降低。EDB诱导的SCE或复制指数的差异可能与GSTM1和GSTT1基因型单独或组合无关。当将EBD诱导SCEs与其他两种已知的丁二烯环氧化物代谢产物进行比较时,1,2:3,4-二环氧丁烷(DEB)在比EBD或1,2-环氧-3-丁烯(MEB)低两个数量级以上的浓度下是有效的。结果表明,EBD在培养的人淋巴细胞中是SCE的有效诱导剂,尽管不如MEB有效,而且明显不如DEB有效。与先前对DEB和MEB的研究结果相反,多态性GSTM1和GSTT1似乎不参与人类淋巴细胞中EBD的解毒。
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Induction of sister chromatid exchange by 3,4-epoxybutane- 1,2-diol in cultured human lymphocytes of different GSTT1 and GSTM1 genotypes

The induction of sister chromatid exchanges (SCEs) by a 48-h treatment with 3,4-epoxybutane-1,2-diol (EBD), a metabolite of 1,3-butadiene, was studied in whole-blood lymphocyte cultures of 22 human donors with known genotypes of two polymorphic glutathione S-transferases (GSTs), GSTT1 and GSTM1. For both genes, donors representing a homozygous ‘null’ genotype lacking the respective GST gene and isozyme and a ‘positive’ genotype with at least one intact gene and GST activity were included. The mean frequencies of SCE/cell were similar in all genotype groups: GSTT1 null (n = 10) (mean 22.0 for 250 μM and 32.9 for 250 500 μM of EBD), GSTT1 positive (n = 14) (21.3 and 34.6, respectively), GSTM1 null (n = 10) (20.3 and 33.5) and GSTM1 positive donors (n = 15) (20.6 and 34.8). At 500 μM concentration of EBD, the lymphocyte cultures of all donors showed a significantly decreased replication index. No differences in EDB-induced SCEs or in replication index could be associated with the GSTM1 and GSTT1 genotypes either separately or in combination. When SCEs induction by EBD was compared to that of two other known epoxide metabolites of butadiene, 1,2:3,4-diepoxybutane (DEB) was effective at concentrations over two orders of magnitude lower than EBD or 1,2-epoxy-3-butene (MEB). It is concluded that EBD is an efficient inducer of SCE in cultured human lymphocytes, although not quite as effective as MEB and clearly less effective than DEB. Contrary to previous findings with DEB and MEB, the polymorphic GSTM1 and GSTT1 do not appear to be involved in the detoxification of EBD in human lymphocytes.

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