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Assessing variation in the potential susceptibility of fish to pharmaceuticals considering evolutionary differences in their physiology and ecology

机译:考虑鱼类生理和生态方面的进化差异评估鱼类对药物的潜在敏感性变化

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摘要

Fish represent the planet's most diverse group of vertebrates and they can be exposed to a wide range of pharmaceuticals. For practical reasons, extrapolation of pharmaceutical effects from ‘model’ species to other fish species is adopted in risk assessment. Here, we critically assess this approach. First, we show that between 65% and 86% of human drug targets are evolutionarily conserved in 12 diverse fish species. Focusing on nuclear steroid hormone receptors, we further show that the sequence of the ligand binding domain that plays a key role in drug potency is highly conserved, but there is variation between species. This variation for the oestrogen receptor, however, does not obviously account for observed differences in receptor activation. Taking the synthetic oestrogen ethinyloestradiol as a test case, and using life-table-response experiments, we demonstrate significant reductions in population growth in fathead minnow and medaka, but not zebrafish, for environmentally relevant exposures. This finding contrasts with zebrafish being ranked as more ecologically susceptible, according to two independent life-history analyses. We conclude that while most drug targets are conserved in fish, evolutionary divergence in drug-target activation, physiology, behaviour and ecological life history make it difficult to predict population-level effects. This justifies the conventional use of at least a 10× assessment factor in pharmaceutical risk assessment, to account for differences in species susceptibility.
机译:鱼代表着地球上最多样化的脊椎动物,它们可以接触多种药物。出于实际原因,在风险评估中采用了从“模型”物种到其他鱼类物种的药物作用推断。在这里,我们严格评估这种方法。首先,我们表明在12种不同的鱼类中,有65%至86%的人类药物目标在进化上得到了保护。着眼于核甾体激素受体,我们进一步表明,在药物效力中起关键作用的配体结合域的序列是高度保守的,但物种之间存在差异。然而,雌激素受体的这种变化显然不能解释受体活化的差异。以合成雌激素乙炔雌二醇为测试案例,并使用生命表响应实验,我们证明了与环境相关的暴露,fat鱼,now鱼和青aka(而不是斑马鱼)的种群增长显着减少。根据两项独立的生命历史分析,这一发现与斑马鱼被列为对生态更敏感的物种形成鲜明对比。我们得出的结论是,尽管大多数药物靶标在鱼类中均得到保存,但药物靶标激活,生理学,行为和生态生活史的进化差异使得难以预测种群水平的影响。这证明了在药物风险评估中常规使用至少10倍评估因子来解释物种敏感性的差异是合理的。

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