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Individual sensitivity to cytogenetic effects of benzo[alpha]pyrene in cultured human lymphocytes: influence of glutathione S-transferase M1 genotype

机译:对培养的人淋巴细胞中苯并αpy的细胞遗传学效应的个体敏感性:谷胱甘肽S-转移酶M1基因型的影响

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Sister chromatid exchange (SCE) and chromosome aberrations (CA) in peripheral lymphocytes has been widely used in assessing exposure to mutagens and carcinogens. One of the extensively studied genotoxins is benzo[alpha]pyrene (BaP). We studied the ability of BaP to induce SCE and CA in 16 glutathione S-transferase M1 (GSTM1)-positive and 15 GSTM1-null individuals by analyzing 72-h whole-blood lymphocyte cultures, either BaP-untreated (controls) or treated with 5 μM of BaP for 24 or 48 h. There was no differences in the level of BaP-induced chromosomal aberrations between GSTM1-positive or null individuals when the cells were BaP-exposed for 24 h (0.083 ± 0.059 vs. 0.090 ± 0.058) or 48 h (0.092 ± 0.057 vs. 0.096 ± 0.050. The frequency of SCE in controls was GSTM1-positive = 2.96 ± 0.35 and GSTM1-null = 3.23 ± 0.56 while that for BaP-treated lymphocytes was GSTM1-positive = 5.56 ± 0.83 and GSTM1-null = 6.09 ± 1.11 and were not statistically significant. The rates of BaP-induced in vitro chromatid and chromosome-type gaps and breaks were similar in all groups, although GSTM1-null genotype chromatid-type breaks were more frequent (0.064 ± 0.039 per metaphase) than chromosome-type breaks (0.032 ± 0.027 per metaphase) after 48 h treatment with BaP (p < 0.001). These findings suggest that BaP-induced in vitro SCE and CA are not influenced by the GSTM1 genotype.
机译:周围淋巴细胞中的姐妹染色单体交换(SCE)和染色体畸变(CA)已广泛用于评估对诱变剂和致癌物的暴露。广泛研究的基因毒素之一是苯并[(BaP)。我们通过分析未经BaP处理(对照)或用BaP处理的72小时全血淋巴细胞培养物,研究了BaP在16个谷胱甘肽S-转移酶M1(GSTM1)阳性和15个GSTM1 null个体中诱导SCE和CA的能力。 5μM的BaP持续24或48 h。当细胞暴露于BaP 24小时(0.083±0.059 vs.0.090±0.058)或48 h(0.092±0.057 vs.0.096)时,GSTM1阳性或无效个体之间BaP诱导的染色体畸变水平没有差异。 ±0.050。对照组中SCE的频率为GSTM1阳性= 2.96±0.35和GSTM1-null = 3.23±0.56,而BaP处理的淋巴细胞的SCE频率为GSTM1阳性= 5.56±0.83和GSTM1-null = 6.09±1.11,分别为所有组中BaP诱导的体外染色单体和染色体型缺口和断裂的发生率均相似,尽管GSTM1空基因型染色单体型断裂比染色体断裂更频繁(每个中期0.064±0.039)。 BaP治疗48 h后(每个中期0.032±0.027)(p <0.001),这些发现表明BaP诱导的体外SCE和CA不受GSTM1基因型的影响。

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