Developmental toxicity of the emerging contaminant cyclophosphamide and the integrated biomarker response (IBRv2) in zebrafish

斑马鱼 发育毒性 氧化应激 毒性 生物标志物 生物 环磷酰胺 男科 细胞凋亡 孵化 毒理 内科学 内分泌学 基因 医学 生物化学 遗传学 化疗 动物科学 妊娠期 怀孕
作者
Tamilselvan Hema,Rama-Krishnan Poopal,Mathan Ramesh,Zongming Ren,Bin Li
出处
期刊:Environmental Science: Processes & Impacts [Royal Society of Chemistry]
卷期号:25 (8): 1391-1406 被引量:6
标识
DOI:10.1039/d3em00186e
摘要

The safety of cyclophosphamide (CP) in the early developmental stages is not studied yet; it is important to study the responses at these stages because they might have relevance to CP-administered humans. We studied the developmental toxicity of CP by analysing physiological, morphological, and oxidative stress, neurotransmission enzymes, gene expression and histological endpoints in zebrafish embryos/larvae. The study lasted for 120 hpf at environmentally relevant concentrations of CP. No visible alterations were noticed in the control group. Delayed hatching, slow heart rate, yolk sac oedema, pericardial oedema, morphological deformities, the incompetence of oxidative stress biomarkers, excessive generation of ROS, apoptosis, inhibition of neurotransmitters and histopathological anomalies were observed in CP-treated groups. These alterations were found to be concentration- and duration-dependent effects for physiological and morphological endpoints, whereas concentration-dependent effects were antioxidants, ROS, apoptosis and histological endpoints. Biomarkers and gene expression were standardised using the integrated biomarker response-IBRv2 index. The IBRv2 index showed a concentration-dependent behaviour. A non-lethal developmental and teratogenic effect was observed in CP-treated zebrafish embryos/larvae at the studied concentrations. The studied biomarkers are sensitive, and the responses are interrelated; thus, their responses are useful to assess veiled and unseen hazards of pharmaceuticals.
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