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首页> 外文期刊>Food and Chemical Toxicology: An International Journal Published for the British Industrial Biological Research >Diallyl trisulfide as an inhibitor of benzo(a)pyrene-induced precancerous carcinogenesis in MCF-10A cells
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Diallyl trisulfide as an inhibitor of benzo(a)pyrene-induced precancerous carcinogenesis in MCF-10A cells

机译:二烯丙基三硫化物作为苯并(a)re诱导的MCF-10A细胞癌前癌变的抑制剂

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摘要

Diallyl trisulfide (DATS) is a garlic organosulfide that is toxic to cancer cells, however, little is known about its effect in the initiation phase of carcinogenesis. We sought to determine whether DATS could inhibit the carcinogen, benzo(a)pyrene (BaP), from inducing precancerous activity, in vitro. MCF-10A cells were either pre-treated (PreTx) or concurrently treated (CoTx) with 1 μM BaP, and 6 or 60 μM DATS for up to 24. h. The DATS 6 and 60 μM CoTx inhibited BaP-induced cell proliferation by an average of 71.1% and 120.8%, respectively, at 6. h. The 60 μM DATS pretreatment decreased BaP-induced G2/M cell cycle transition by 127%, and reduced the increase in cells in the S-phase by 42%; whereas 60 μM DATS CoTx induced a 177% increase in cells in G1. DATS effectively inhibited (P< 0.001) BaP-induced peroxide formation by at least 54%, which may have prevented the formation of BaP-induced DNA strand breaks. In this study, we reveal mechanisms involved in DATS inhibition of BaP-induced carcinogenesis, including inhibition of cell proliferation, regulation of cell cycle, attenuation of ROS formation, and inhibition of DNA damage. At the doses evaluated, DATS appears to be an effective attenuator of BaP-induced breast carcinogenesis, in vitro.
机译:二烯丙基三硫化物(DATS)是一种对癌细胞有毒的大蒜有机硫化物,但是,其在致癌作用起始阶段的作用鲜为人知。我们试图确定DATS是否可以在体外抑制致癌物苯并(a)re(BaP)诱导癌前活动。将MCF-10A细胞用1μMBaP和6或60μMDATS预处理(PreTx)或同时处理(CoTx)长达24小时。在6 h,DATS 6和60μMCoTx分别平均抑制BaP诱导的细胞增殖71.1%和120.8%。 60μMDATS预处理使BaP诱导的G2 / M细胞周期转变降低了127%,并使S期细胞的增加减少了42%;而60μMDATS CoTx诱导G1细胞增加了177%。 DATS有效抑制(P <0.001)BaP诱导的过氧化物形成至少54%,这可能已经阻止了BaP诱导的DNA链断裂的形成。在这项研究中,我们揭示了DATS抑制BaP诱导的癌变的机制,包括抑制细胞增殖,调节细胞周期,减弱ROS形成和抑制DNA损伤。在评估的剂量下,DATS在体外似乎是BaP诱导的乳腺癌致癌作用的有效衰减剂。

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