Using targeted fetal rat testis genomic and endocrine alterations to predict the effects of a phthalate mixture on the male reproductive tract

IF 2.9 Q2 TOXICOLOGY Current Research in Toxicology Pub Date : 2024-01-01 DOI:10.1016/j.crtox.2024.100180
L. Earl Gray Jr , Christy S. Lambright , Nicola Evans , Jermaine Ford , Justin M. Conley
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Abstract

Administration of phthalates in utero disrupts gene expression and hormone levels in the fetal rat testis, which are key events in an Adverse Outcome Pathway (AOP) for the Phthalate Syndrome. These measures can be used to predict the postnatal adverse effects of phthalate esters (PEs) on male rat sexual differentiation. Here, pregnant rats were exposed to dibutyl (DBP)- and diisononyl (DINP) phthalate on gestational days 14 to 18 individually and as a mixture (DBP,250 mg/kg/d; DINP, 750 mg/kg/d; and DBP 250 mg/kg/d plus DINP 750 mg/kg/d). We found that each PE reduced testosterone production (T Prod) and related gene transcripts by about 50 % and that they acted in a dose additive manner, reducing T Prod and gene expression by 75 % as a mixture. Based upon effects on T Prod, DINP was 0.33 times as potent as DBP and thus the DBP + DINP mixture was predicted to be equivalent to 500 mg DBP/kg/d.

Logistic regression models of T Prod predicted that the adverse effects of the DBP + DINP mixture group versus the DBP and DINP individual treatments would reduce anogenital distance (AGD) by 27 % versus 10 %, increase hypospadias in 18 % versus < 1 %, induce epididymal agenesis in 46 % versus 10 %, and increase areolae/nipples in 4.8 % versus < 0.1 % of the, respectively. These predictions were highly consistent with effects from previously published dose response studies on the male reproductive effects of DBP. In summary, these results support the use of this New Approach Method to predict the detrimental effects of PEs and PE mixtures, replacing or reducing the need to run long-term, resource and animal use intensive extended one-generation reproduction studies for this class of chemicals.

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利用目标胎鼠睾丸基因组和内分泌的改变来预测邻苯二甲酸酯混合物对雄性生殖道的影响
子宫内施用邻苯二甲酸酯会破坏胎鼠睾丸中的基因表达和激素水平,这是邻苯二甲酸酯综合征不良后果途径(AOP)中的关键事件。这些指标可用于预测邻苯二甲酸酯(PE)对雄性大鼠性分化的产后不良影响。在这里,怀孕大鼠在妊娠第 14 到 18 天分别接触了邻苯二甲酸二丁酯 (DBP) 和邻苯二甲酸二异壬酯 (DINP) 以及它们的混合物(DBP,250 毫克/千克/天;DINP,750 毫克/千克/天;以及 DBP 250 毫克/千克/天加 DINP 750 毫克/千克/天)。我们发现,每种聚乙烯都能使睾酮产量(T Prod)和相关基因转录物减少约 50%,而且它们以剂量相加的方式发挥作用,混合物能使 T Prod 和基因表达量减少 75%。根据对 T Prod 的影响,DINP 的效力是 DBP 的 0.33 倍,因此预测 DBP + DINP 混合物相当于 500 毫克 DBP/千克/天。根据 T Prod 的逻辑回归模型预测,DBP + DINP 混合物组与 DBP 和 DINP 单个处理组相比,其不利影响分别是:肛距(AGD)减少 27% 对 10%,尿道下裂增加 18% 对 1%,诱发附睾发育不全 46% 对 10%,乳晕/乳头增大 4.8% 对 0.1%。这些预测与之前公布的 DBP 对男性生殖影响的剂量反应研究结果高度一致。总之,这些结果支持使用这种新方法来预测聚乙烯和聚乙烯混合物的有害影响,从而取代或减少对这一类化学品进行长期、资源和动物使用密集型延长一代生殖研究的需要。
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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
期刊最新文献
Editorial Board Contents Evaluation of the diphenyl herbicide, oxyfluorfen, for effects on thyroid hormones in the juvenile rat Ethylene dimethanesulfonate effects on gene promoter activities related to the endocrine function of immortalized Leydig cell lines R2C and MA-10 Placental transfer of tofacitinib in the ex vivo dual-side human placenta perfusion model
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