Detection of DNA strand breaks, DNA-protein crosslinks, and telomerase activity in nickel-transformed BALB/c-3T3 cells.

Y. Lei, J. K. Chen, Z. L. Wu
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引用次数: 7

Abstract

Although nickel compounds are known carcinogens, the underlying carcinogenic mechanisms are not fully understood. The objective of this research was to determine if the genotoxic lesions of DNA strand breaks and DNA-protein crosslinks are present in nickel-transformed BALB/c-3T3 cells, and to further elucidate the potential carcinogenesis of insoluble and soluble nickel compounds through telomerase activity in nickel-transformed BALB/c-3T3 cell lines. DNA strand breaks, DNA-protein crosslinks and telomerase activity were investigated by single cell gel electrophoresis (comet assay), (125)I-postlabelling techniques, and the TRAP-silver staining assay, respectively. Results showed that both DNA strand breaks and DNA-protein crosslinks were present in nickel-transformed BALB/c-3T3 cells. However, the highest levels of DNA strand breaks and DNA-protein crosslinks were found in insoluble crystalline NiS-transformed cells and high levels of DNA strand breaks and DNA-protein crosslinks were also found in the transformed cells induced by two water-soluble NiCl(2) and NiSO(4) at moderate concentrations of cytotoxicity. These data suggest that these two genetic endpoints are useful biomarkers and are associated with cell transformation and carcinogensis of insoluble and soluble nickel compounds. Also, we found that the crystalline NiS- and NiCl(2)-transformed cells possessed a high telomerase activity. A weak telomerase was found in NiSO(4)-transformed cells. The results seem to indicate that in addition to crystalline NiS, some water-soluble nickel compounds such as NiCl(2) are also highly carcinogenic. These results may partly explain the cell transformation and relative carcinogenic potency of insoluble crystalline NiS, soluble NiCl(2), and NiSO(4).
镍转化BALB/c-3T3细胞中DNA链断裂、DNA-蛋白交联和端粒酶活性的检测。
虽然镍化合物是已知的致癌物,但其潜在的致癌机制尚不完全清楚。本研究的目的是确定镍转化的BALB/c-3T3细胞中是否存在DNA链断裂和DNA-蛋白交联的遗传毒性病变,并通过镍转化的BALB/c-3T3细胞系的端粒酶活性进一步阐明不溶性和可溶性镍化合物的潜在致癌作用。DNA链断裂、DNA-蛋白交联和端粒酶活性分别通过单细胞凝胶电泳(彗星法)、(125)i后标记技术和trap银染色法进行研究。结果表明,在镍转化的BALB/c-3T3细胞中存在DNA链断裂和DNA-蛋白交联。然而,在不溶性结晶nis转化细胞中发现了最高水平的DNA链断裂和DNA-蛋白质交联,在中等浓度的细胞毒性下,两种水溶性NiCl(2)和NiSO(4)诱导的转化细胞中也发现了高水平的DNA链断裂和DNA-蛋白质交联。这些数据表明,这两个遗传终点是有用的生物标志物,与不溶性和可溶性镍化合物的细胞转化和致癌作用有关。此外,我们发现结晶的NiS和NiCl(2)转化细胞具有较高的端粒酶活性。在NiSO(4)转化细胞中发现弱端粒酶。结果似乎表明,除了晶体镍外,一些水溶性镍化合物如NiCl(2)也具有高度致癌性。这些结果可以部分解释不溶性晶体NiS、可溶性NiCl(2)和NiSO(4)的细胞转化和相对致癌效力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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