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Prepubertal di-n-butyl phthalate exposure alters Sertoli and Leydig cell function and lowers bone density in adult male mice

机译:青春期前邻苯二甲酸二正丁酯暴露会改变成年雄性小鼠的Sertoli和Leydig细胞功能并降低骨密度

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摘要

Phthalate exposure impairs testis development and function, however whether phthalates affect non-reproductive functions is not well understood. To investigate this, C57Bl/6J mice were fed 1-500 mg di-n-butyl phthalate (DBP) in corn oil, or vehicle only, daily from 4-14 days, after which tissues were collected (prepubertal study). Another group was fed 1-500 mg DBP/kg/day from 4-21 days then maintained untreated until 8 weeks for determination of adult consequences of prepubertal exposure. Bones were assessed by micro-computed tomography and dual energy X-ray absorptiometry, and testosterone by radioimmunoassay. DBP exposure decreased prepubertal femur length, marrow volume and mean moment of inertia. Adult animals exposed prepubertally to low DBP doses had lower bone mineral content (BMC) and bone mineral density (BMD) and less lean tissue mass than vehicle-treated animals. Altered dynamics of the emerging Leydig population were found in 14 day old animals fed 100-500 mg DBP/kg/day. Adult mice had variable testicular testosterone and serum testosterone and luteinizing hormone concentrations following prepubertal exposure, and dose-dependent reduction in CYP11A1. INSL3 was detected in Sertoli cells of adult mice administered the highest dose of 500 mg DBP/kg/day prepubertally, a finding supported by the induction of INSL3 expression in TM4 cells exposed to 50 μ M, but not 5 μ M, DBP. We propose that low dose DBP exposure is detrimental to bone but that normal BMD/BMC following high dose DBP exposure reflects changes in testicular somatic cells that confer protection to bones. These findings will fuel concerns that low dose DBP exposure impacts health beyond the reproductive axis.
机译:邻苯二甲酸酯的暴露会损害睾丸的发育和功能,但是人们对邻苯二甲酸酯是否会影响非生殖功能的认识尚不清楚。为了对此进行研究,每天从4-14天开始,向C57Bl / 6J小鼠饲喂玉米油中的1-500 mg邻苯二甲酸二正丁酯(DBP)或仅添加媒介物,然后收集组织(青春期前)。另一组从4-21天开始喂1-500 mg DBP / kg /天,然后保持不治疗直到8周,以测定青春期前成人暴露的后果。通过微计算机断层扫描和双能X线吸收法评估骨骼,通过放射免疫法评估睾丸激素。 DBP暴露可减少青春期前股骨长度,骨髓体积和平均转动惯量。与媒介物处理的动物相比,青春期前暴露于低DBP剂量的成年动物的骨矿物质含量(BMC)和骨矿物质密度(BMD)较低,并且瘦肉组织质量较小。在饲喂100-500 mg DBP / kg /天的14日龄动物中发现了新兴的Leydig种群的动态变化。成年小鼠的青春期前暴露后,其睾丸睾丸激素和血清睾丸激素及黄体生成激素的浓度发生变化,CYP11A1的剂量依赖性降低。在成年前最高剂量为500 mg DBP / kg / day的成年小鼠的支持细胞中检测到INSL3,这一发现得到了在暴露于50μM,但未暴露于5μM DBP的TM4细胞中诱导INSL3表达的支持。我们建议低剂量DBP暴露对骨骼有害,但是高剂量DBP暴露后正常的BMD / BMC反映了睾丸体细胞的变化,从而赋予骨骼保护。这些发现将加剧人们对低剂量DBP暴露会影响生殖轴以外的健康的担忧。

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