基因33/Mig6/ERRFI1对六价铬诱导人支气管上皮细胞转化的影响与暴露时间长短有关。

IF 1.2 4区 环境科学与生态学 Q4 ENVIRONMENTAL SCIENCES
Cen Li, Dina Edeni, Sarah Platkin, Raymond Liu, Jiangwei Li, Maheen Hossain, Mozibur Rahman, Humayun Islam, John L Phillips, Dazhong Xu
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引用次数: 0

摘要

六价铬(Cr(VI))化合物是环境致癌物和职业性致癌物。本研究追踪了Cr(VI)对BEAS-2B肺支气管上皮细胞肿瘤转化的慢性影响,无论是否缺失基因33 (Mig6, EFFRI1),这是一种多功能接头蛋白。我们发现,与对照细胞相比,基因33缺失细胞在暴露于Cr(VI) 8周而非24周转化后,表现出更强的非锚定依赖性生长。基因33缺失的细胞在暴露于Cr(VI) 8周而不是24周后转化后,与对照细胞相比,细胞增殖水平更高,对急性Cr(VI)毒性的抵抗力更强,尽管24周转化的细胞对急性Cr(VI)毒性的抵抗力增强。然而,基因33缺失的细胞在暴露于Cr(VI) 8周和24周后均表现出迁移增加。此外,只有暴露于Cr(VI) 24周后转化的细胞才能在裸鼠体内形成皮下肿瘤。虽然两种细胞类型形成的肿瘤大小没有明显差异,但基因33缺失的细胞在肿瘤的组织学表现和MMP3表达上有明显差异。我们的研究结果表明,在慢性暴露于Cr(VI)时,BEAS-2B细胞发生了进行性肿瘤转化,并且这些细胞对基因33缺失具有适应性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Effect of Gene 33/Mig6/ERRFI1 on hexavalent chromium-induced transformation of human bronchial epithelial cells depends on the length of exposure.

Hexavalent chromium (Cr(VI)) compounds are environmental and occupational lung carcinogens. The present study followed the chronic effect of Cr(VI) on the neoplastic transformation of BEAS-2B lung bronchial epithelial cells with or without deletion of Gene 33 (Mig6, EFFRI1), a multifunctional adaptor protein. We find that Gene 33-deleted cells exhibit increased anchorage-independent growth compared to control cells after transformed by 8-week but not 24-week Cr(VI) exposure. Gene 33-deleted cells show a higher level of cell proliferation and are more resistant to acute Cr(VI) toxicity compared to control cells after transformed by 8-week but not 24-week Cr(VI) exposure, despite that 24-week-transformed cells have increased resistance to acute Cr(VI) toxicity. However, Gene 33-deleted cells show increased migration after transformed by both 8-week and 24-week Cr(VI) exposures. Furthermore, only cells transformed by 24 weeks of Cr(VI) exposure can form subcutaneous tumors in nude mice. Although no significant difference in the size of tumors formed by the two cell types, there is a marked difference in the histological manifestation and more MMP3 expression in tumors from Gene 33-deleted cells. Our results demonstrate progressive neoplastic transformation of BEAS-2B cells and the adaptation of these cells to Gene 33 deletion during chronic exposure to Cr(VI).

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CiteScore
4.60
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