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Dimethylarsinic acid may promote prostate carcinogenesis inrats

机译:二甲基亚砷酸可能促进前列腺癌的发生老鼠

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摘要

Arsenic is a known human carcinogen, inducing tumors of the lung, urinary bladder, skin, liver and prostate. However, there are no reports of prostate tumors induced by arsenicals in in vivo animal models. In a previous study, we found that HMGB2 expression was a predictive marker for prostate carcinogens in the rat 4-week repeated dose test. In this study, six-week-old male F344 rats were orally treated with a total of six chemicals (2-acetylaminofluorene (2-AAF), p-cresidine, dimethylarsinic acid (DMA), glycidol, N-nitrosodiethylamine and acrylamide) for four weeks. Animals were sacrificed at the end of the study, and HMGB2 and Ki-67 immunohistochemistry was performed. The numbers of HMGB2- and Ki-67- positive cells in all prostate lobes were significantly increased by DMA, one of the arsenicals, compared with the controls. Meanwhile, the number of Ki-67-positive cells in lateral and dorsal prostate lobes was significantly decreased by 2-AAF with the reduction of body weight, but HMGB2 expression was not. The other chemicals did not change HMGB2 and Ki-67 expression. These data indicate that DMA may have an ability to enhance prostate carcinogenesis.
机译:砷是一种已知的人类致癌物,会诱发肺,膀胱,皮肤,肝脏和前列腺的肿瘤。但是,尚无体内动物模型中由砷引起的前列腺肿瘤的报道。在先前的研究中,我们发现HMGB2表达是大鼠4周重复剂量测试中前列腺致癌物的预测标记。在这项研究中,对六周大的F344大鼠进行了口服六种化学药品的治疗(2-乙酰氨基芴(2-AAF),对甲酚丁啶,二甲基s啶酸(DMA),缩水甘油,N-亚硝基二乙胺和丙烯酰胺)四周。在研究结束时处死动物,并进行HMGB2和Ki-67免疫组织化学。与对照相比,砷中的一种是DMA,所有前列腺叶中HMGB2-和Ki-67-阳性细胞的数量均显着增加。同时,随着体重的减少,2-AAF明显减少了外侧和背侧前列腺叶中Ki-67阳性细胞的数量,但HMGB2表达并未降低。其他化学物质未改变HMGB2和Ki-67表达。这些数据表明DMA可能具有增强前列腺癌发生的能力。

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