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苯并(a)芘通过破坏细胞周期动力学并激活多种人类细胞系中Caspase-3介导的凋亡来引发细胞毒性。

Benzo(a)pyrene triggers cytotoxicity by disrupting cell cycle dynamics and activating Caspase-3-mediated apoptosis in multiple human cell lines.

作者信息

Kim Chul-Hong, Shin Geun-Seup, Park Sehwan, Kim Ji-Young, An Mi-Jin, Lee Hyun-Min, Jo Ah-Ra, Park Yuna, Hong Tae Kyung, Kim Jinho, Hwangbo Yujeong, Kim Jung-Woong

机构信息

Department of Life Science, Chung-Ang University, Heukseok-ro 84, Seoul 06974, Republic of Korea.

出版信息

Toxicol Res (Camb). 2025 Apr 14;14(2):tfaf053. doi: 10.1093/toxres/tfaf053. eCollection 2025 Apr.

Abstract

Benzo(a)pyrene (B(a)P), a polycyclic aromatic hydrocarbon (PAH), is a known endocrine disruptor linked to various environmentally induced diseases. While recent studies have explored its role in short- and long-term disease development, there is limited research on B(a)P's cytotoxic effects across different cell types. This study aims to evaluate the cytotoxicity of B(a)P exposure in several human cell lines under controlled conditions. We employed flow cytometry (FACS) for quantitative cytotoxicity analysis at the single-cell level. Our findings revealed that B(a)P exhibited minimal cytotoxicity in lung and liver cells, but potent toxicity in breast cells. Notably, B(a)P-induced cytotoxicity in breast cells was associated with increased cleaved caspase-3 expression, leading to cell death. This process was further linked to cell cycle arrest, as indicated by altered cyclin B1 expression in a B(a)P-dependent manner, resulting in reduced cell viability. In summary, these results suggest that breast cells are particularly sensitive to B(a)P-induced cytotoxicity, which is driven by apoptosis and cell cycle disruption.

摘要

苯并(a)芘(B(a)P)是一种多环芳烃(PAH),是一种已知的与多种环境诱导疾病相关的内分泌干扰物。虽然最近的研究探讨了其在短期和长期疾病发展中的作用,但关于B(a)P对不同细胞类型的细胞毒性作用的研究有限。本研究旨在评估在受控条件下B(a)P暴露对几种人类细胞系的细胞毒性。我们采用流式细胞术(FACS)在单细胞水平进行定量细胞毒性分析。我们的研究结果表明,B(a)P在肺细胞和肝细胞中表现出最小的细胞毒性,但在乳腺细胞中具有强烈的毒性。值得注意的是,B(a)P诱导的乳腺细胞毒性与裂解的半胱天冬酶-3表达增加有关,导致细胞死亡。这一过程进一步与细胞周期停滞有关,如细胞周期蛋白B1表达以B(a)P依赖的方式改变所示,导致细胞活力降低。总之,这些结果表明乳腺细胞对B(a)P诱导的细胞毒性特别敏感,这是由凋亡和细胞周期破坏驱动的。

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