Toxicokinetics of a developmental toxicity test in zebrafish embryos and larvae: Relationship with drug exposure in humans and other mammals

IF 2.9 Q2 TOXICOLOGY Current Research in Toxicology Pub Date : 2024-01-01 DOI:10.1016/j.crtox.2024.100187
Tasuku Nawaji , Naohiro Mizoguchi , Ryuta Adachi , Hiroki Teraoka
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Abstract

To study the effects of drugs on embryo/fetal development (EFD), developmental and reproductive toxicity studies in zebrafish (Danio rerio) embryos is expected to be an accepted alternative method to animal studies using mammals. However, there is a lack of clarity in the relationship between the concentration of developmental toxicity agents in whole embryos or larvae (Ce) and that in aqueous solution (Cw), and also between the amount of drug exposure required to cause developmental toxicity in zebrafish embryos or larvae and that required in mammals. Here, we measured Ce for developmental toxicity agents every 24 h starting at 24 h post fertilization (hpf). We found a high correlation (R2: 0.87–0.96) between log [Ce/Cw] and the n-octanol–water distribution coefficient at pH 7 (logD) of each drug at all time points up to 120 hpf. We used this relationship to estimate the Ce values of the 21 positive-control reference drugs listed in ICH guidelines on reproductive and developmental toxicity studies (ICH S5). We then calculated the area under the Ce–time curve in zebrafish (zAUC) for each drug from the regression equation between log [Ce/Cw] and logD and compared it with the AUC at the no-observed-adverse-effect level in rats and rabbits and at the effective dose in humans described in ICH S5. The log of the calculated zAUC for the 14 drugs identified as positive in the zebrafish developmental toxicity test was relatively highly positively correlated with the log [AUC] for rats, rabbits, and humans. These findings provide important and positive information on the applicability of the zebrafish embryo developmental toxicity test as an alternative method of EFD testing. (267 words)

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斑马鱼胚胎和幼体发育毒性试验的毒物动力学:与人类和其他哺乳动物药物暴露的关系
为了研究药物对胚胎/胎儿发育(EFD)的影响,在斑马鱼(Danio rerio)胚胎中进行发育和生殖毒性研究有望成为使用哺乳动物进行动物研究的公认替代方法。然而,发育毒性药物在整个胚胎或幼体中的浓度(Ce)与在水溶液中的浓度(Cw)之间的关系,以及在斑马鱼胚胎或幼体中引起发育毒性所需的药物暴露量与哺乳动物所需的药物暴露量之间的关系尚不明确。在这里,我们从受精后 24 小时(hpf)开始,每 24 小时测量一次发育毒性药物的 Ce。我们发现,在 120 hpf 之前的所有时间点,每种药物的对数[Ce/Cw]与 pH 值为 7 的正辛醇-水分配系数(logD)之间存在高度相关性(R2:0.87-0.96)。我们利用这一关系估算了 ICH 生殖与发育毒性研究指南(ICH S5)中列出的 21 种阳性对照参比药物的 Ce 值。然后,我们根据 log [Ce/Cw] 与 logD 之间的回归方程计算出每种药物在斑马鱼体内的 Ce 时间曲线下面积(zAUC),并将其与 ICH S5 中所述的大鼠和兔子无不良反应水平以及人类有效剂量下的 AUC 进行比较。在斑马鱼发育毒性试验中确定为阳性的 14 种药物的计算 zAUC 的对数与大鼠、兔子和人类的对数[AUC]呈相对高度正相关。这些发现为斑马鱼胚胎发育毒性试验作为 EFD 试验替代方法的适用性提供了重要而积极的信息。(267字)
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来源期刊
Current Research in Toxicology
Current Research in Toxicology Environmental Science-Health, Toxicology and Mutagenesis
CiteScore
4.70
自引率
3.00%
发文量
33
审稿时长
82 days
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