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Developmental programming: prenatal BPA treatment disrupts timing of LH surge and ovarian follicular wave dynamics in adult sheep.发育编程:产前 BPA 处理破坏成年绵羊 LH 峰和卵巢卵泡波动力学的时间。
Toxicol Appl Pharmacol. 2014 Sep 1;279(2):119-28. doi: 10.1016/j.taap.2014.05.016. Epub 2014 Jun 9.

本文引用的文献

1
Developmental programming: Impact of prenatal testosterone treatment and postnatal obesity on ovarian follicular dynamics.发育编程:产前睾酮治疗和产后肥胖对卵巢卵泡动力学的影响。
J Dev Orig Health Dis. 2012 Aug;3(4):276-86. doi: 10.1017/S2040174412000128.
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Developmental programming: impact of prenatal testosterone excess on ovarian cell proliferation and apoptotic factors in sheep.发育编程:胎儿睾丸酮过多对绵羊卵巢细胞增殖和凋亡因子的影响。
Biol Reprod. 2012 Jul 26;87(1):22, 1-10. doi: 10.1095/biolreprod.112.100024. Print 2012 Jul.
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The primordial follicle reserve is not renewed after chemical or γ-irradiation mediated depletion.原始卵泡储备在化学或γ辐射介导耗竭后不会得到更新。
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Developmental programming: gestational testosterone treatment alters fetal ovarian gene expression.发育编程:孕期睾酮处理改变胎儿卵巢基因表达。
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Ultrasound characteristics of experimentally induced luteinized unruptured follicles (LUF) and naturally occurring hemorrhagic anovulatory follicles (HAF) in the mare.马的实验性黄体化未破裂卵泡(LUF)和自然发生的出血性无排卵卵泡(HAF)的超声特征。
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Endocrine disrupting chemicals and disease susceptibility.内分泌干扰化学物质与疾病易感性。
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Neonatal exposure to bisphenol A or diethylstilbestrol alters the ovarian follicular dynamics in the lamb.新生期暴露于双酚 A 或己烯雌酚会改变羔羊的卵巢卵泡动态。
Reprod Toxicol. 2011 Nov;32(3):304-12. doi: 10.1016/j.reprotox.2011.06.118. Epub 2011 Jun 21.
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Developmental origin of reproductive and metabolic dysfunctions: androgenic versus estrogenic reprogramming.生殖和代谢功能障碍的发育起源:雄激素与雌激素的重编程。
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Neonatal exposure to bisphenol A reduces the pool of primordial follicles in the rat ovary.新生儿期接触双酚 A 会减少大鼠卵巢中原始卵泡的数量。
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发育编程:产后雌二醇会加剧绵羊胎儿期暴露于过量睾酮和双氢睾酮所诱导的卵巢卵泡缺陷。

Developmental programming: postnatal estradiol amplifies ovarian follicular defects induced by fetal exposure to excess testosterone and dihydrotestosterone in sheep.

作者信息

Veiga-Lopez A, Wurst A K, Steckler T L, Ye W, Padmanabhan V

机构信息

1Department of Pediatrics, University of Michigan, Ann Arbor, MI, USA.

出版信息

Reprod Sci. 2014 Apr;21(4):444-55. doi: 10.1177/1933719113503412. Epub 2013 Sep 27.

DOI:10.1177/1933719113503412
PMID:24077439
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3960842/
Abstract

Excess of prenatal testosterone (T) induces reproductive defects including follicular persistence. Comparative studies with T and dihydrotestosterone (DHT) have suggested that follicular persistence is programmed via estrogenic actions of T. This study addresses the androgenic and estrogenic contributions in programming follicular persistence. Because humans are exposed to estrogenic environmental steroids from various sources throughout their life span and postnatal insults may also induce organizational and/or activational changes, we tested whether continuous postnatal exposure to estradiol (E) will amplify effects of prenatal steroids on ovarian function. Pregnant sheep were treated with T, DHT, E, or ED (E and DHT) from days 30 to 90 of gestation. Postnatally, a subset of the vehicle (C), T, and DHT females received an E implant. Transrectal ultrasonography was performed in the first breeding season during a synchronized cycle to monitor ovarian follicular dynamics. As expected, number of ≥8 mm follicles was higher in the T versus C group. Postnatal E reduced the number of 4 to 8 mm follicles in the DHT group. Percentage of females bearing luteinized follicles and the number of luteinized follicles differed among prenatal groups. Postnatal E increased the incidence of subluteal cycles in the prenatal T-treated females. Findings from this study confirm previous findings of divergences in programming effects of prenatal androgens and estrogens. They also indicate that some aspects of follicular dynamics are subject to postnatal modulation as well as support the existence of an extended organizational period or the need for a second insult to uncover the previously programmed event.

摘要

产前睾酮(T)过量会导致包括卵泡持续存在在内的生殖缺陷。对T和双氢睾酮(DHT)的比较研究表明,卵泡持续存在是由T的雌激素作用所编程的。本研究探讨了雄激素和雌激素在卵泡持续存在编程中的作用。由于人类在其整个生命周期中会从各种来源接触到具有雌激素活性的环境类固醇,并且出生后的损伤也可能诱导组织和/或激活变化,因此我们测试了出生后持续暴露于雌二醇(E)是否会放大产前类固醇对卵巢功能的影响。在妊娠第30至90天,对怀孕的绵羊给予T、DHT、E或ED(E和DHT)处理。出生后,对一部分接受载体处理(C)、T和DHT处理的雌性绵羊植入E。在第一个繁殖季节的同步周期中进行经直肠超声检查,以监测卵巢卵泡动态。正如预期的那样,T组中直径≥8 mm的卵泡数量高于C组。出生后给予E可减少DHT组中直径4至8 mm的卵泡数量。产前处理组中出现黄素化卵泡的雌性比例和黄素化卵泡数量存在差异。出生后给予E增加了产前接受T处理的雌性绵羊亚黄体期的发生率。本研究结果证实了先前关于产前雄激素和雌激素编程效应存在差异的研究结果。它们还表明,卵泡动态的某些方面会受到出生后调节,同时也支持存在一个延长的组织期或需要第二次损伤才能揭示先前编程事件的观点。