李佳琳, 王永, 金宇婷, 罗燃燃, 王彭彭, 张蕴晖, 蒋小红. 邻苯二甲酸二异壬酯胚胎期和哺乳期染毒对子代雄性大鼠生殖系统的影响[J]. 环境与职业医学, 2019, 36(4): 320-326. DOI: 10.13213/j.cnki.jeom.2019.18727
引用本文: 李佳琳, 王永, 金宇婷, 罗燃燃, 王彭彭, 张蕴晖, 蒋小红. 邻苯二甲酸二异壬酯胚胎期和哺乳期染毒对子代雄性大鼠生殖系统的影响[J]. 环境与职业医学, 2019, 36(4): 320-326. DOI: 10.13213/j.cnki.jeom.2019.18727
LI Jia-lin, WANG Yong, JIN Yu-ting, LUO Ran-ran, WANG Pengpeng, ZHANG Yun-hui, JIANG Xiao-hong. Effects of embryonic and lactatonal diisodecyl phthalate exposure on reproductve system of male offspring rats[J]. Journal of Environmental and Occupational Medicine, 2019, 36(4): 320-326. DOI: 10.13213/j.cnki.jeom.2019.18727
Citation: LI Jia-lin, WANG Yong, JIN Yu-ting, LUO Ran-ran, WANG Pengpeng, ZHANG Yun-hui, JIANG Xiao-hong. Effects of embryonic and lactatonal diisodecyl phthalate exposure on reproductve system of male offspring rats[J]. Journal of Environmental and Occupational Medicine, 2019, 36(4): 320-326. DOI: 10.13213/j.cnki.jeom.2019.18727

邻苯二甲酸二异壬酯胚胎期和哺乳期染毒对子代雄性大鼠生殖系统的影响

Effects of embryonic and lactatonal diisodecyl phthalate exposure on reproductve system of male offspring rats

  • 摘要: 目的 作为环境内分泌干扰物邻苯二甲酸二乙基己脂(DEHP)的替代物,邻苯二甲酸二异壬酯(DINP)已逐渐成为用量最大的增塑剂之一。本研究旨在探索DINP胚胎期及哺乳期染毒对雄性子代生殖系统的影响及其可能机制。

    方法 采用两代繁殖实验设计,在Wistar雌性受孕大鼠的GD7(受孕第8天)至PND21(产后第21天),每天经口灌胃DINP,染毒剂量为5、50、500、1 000 mg/kg(体重),玉米油为溶剂对照组,每组由5~6只孕鼠组成。PND2时,测量子代仔鼠的肛殖距(AGD),并计算其AGD指数。在PND4时通过窝标准化操作保持每窝8只仔鼠(4只雌鼠,4只雄鼠)。分别于PND21和PND49,从各剂量组随机抽取10只雄性仔鼠,用ELISA法测定其血清睾酮水平,并解剖观察其睾丸病理变化;计算PND21时睾丸和附睾系数,并用实时定量PCR方法测定睾酮合成途径关键基因的mRNA表达情况。

    结果 与溶剂对照组相比较,DINP染毒组新生仔鼠的围生期损失数和雌雄性别比差异无统计学意义(P>0.05),但雄性仔鼠的AGD缩短,分别为(5.15±0.37)、(5.17±0.33)、(4.57±0.38)、(5.16±0.32)mm,500、1000mg/kg染毒组雄性仔鼠的AGD指数(2.48±0.19、2.51±0.13)降低。与对照组相比:PND21时,50mg/kg及以上的DINP处理组中Star基因mRNA表达量增高,500及1 000 mg/kg处理组中Scarb1的mRNA表达量降低,Lhcgr基因mRNA表达量也在1 000 mg/kg剂量组降低(均P < 0.05)。PND49 DINP染毒组大鼠生精细胞和精子减少,间质细胞出现聚集现象,但PND21和PND49雄性仔鼠血清睾酮浓度未发现降低(P>0.05)。

    结论 胚胎期及哺乳期DINP暴露对雄性F1代大鼠的生殖系统存在影响,睾酮合成过程中关键基因Scarb1StarLhcgr可能在其作用机制中发挥一定作用。

     

    Abstract: Objectve As an alternatve to environmental endocrine disruptor diethylhexyl phthalate (DEHP), diisodecyl phthalate (DINP) has gradually become one of the most widely used plastcizers. This study aims to explore the effects of embryonic and lactatonal DINP exposure on the reproductve system of male offspring and its possible mechanisms.

    Methods In a two-generaton reproducton toxicity study, pregnant Wistar rats were treated with 5, 50, 500, and 1 000 mg/kg (body weight) DINP or corn oil (solvent control) by gavage once a day from gestatonal day 7 (GD7) to postnatal day 21 (PND21), with 5-6 pregnant rats in each group. On PND2, the anogenital distance (AGD) of the pups was measured and the AGD Index was calculated. On PND4, the liters were culled to 8 pups per liter (4 females and 4 males). On PND21 and PND49, 10 male pups randomly selected from each dose group were measured for serum testosterone levels by ELISA and observed for testcular pathological changes. The testis and epididymis coefficients were calculated on PND21, and the mRNA expressions of key genes in testosterone synthesis pathway were determined by real-tme quanttatve PCR.

    Results Compared with the solvent control group, the perinatal loss and male-female sex rato of the newborn rats in the designed DINP groups were not statstcally different (P>0.05), but the AGDs of male pups were signifcantly shortened to (5.15±0.37), (5.17±0.33), (4.57±0.38), and (5.16±0.32) mm in the order of low to high DINP exposure level, respectvely, and the AGD indices of the 500 and 1 000mg/kg dose groups were signifcantly reduced to (2.48±0.19) and (2.51±0.13), respectvely. Compared with the control group, on PND21, the mRNA expression levels of Star were signifcantly increased in the DINP-treated groups at 50 mg/kg and above, the levels of Scarb1 were signifcantly decreased in the DINP-treated groups at 500 and 1 000 mg/kg, and the levels of Lhcgr was signifcantly reduced in the 1 000 mg/kg DINP-treated group (P < 0.05). The spermatogenic cells and spermatozoa decreased and aggregaton appeared in the intersttal cells afer the DINP treatment on PND49; but there was no signifcant decrease in serum testosterone concentratons in the male rats on PND21 and PND49 (P>0.05).

    Conclusion Embryonic and lactatonal DINP exposure affects the reproductve system of male F1 rats. Scarb1, Star and Lhcgr, key genes of testosterone synthesis, may play a role in the male reproductve toxicity of DINP.

     

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