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Is prenatal glucocorticoid administration another origin of adult disease?

机译:产前糖皮质激素治疗是成人疾病的另一个来源吗?

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1. The intra-uterine environment is now believed to play a major role in the origin of many adult diseases. Illnesses in which there is significant 'programming' before the time of birth include hypertension, diabetes, coronary heart disease and stroke. Acting on a genetic predisposition, intra-uterine triggers appear to programme the individual's metabolism and endocrine milieu and, after birth, these risk factors are then either amplified or minimized by environmental influences. The triggers operative during fetal life that have been studied most extensively are undernutrition and glucocorticoid exposure. 2. Over the past decade, a series of studies in sheep have focused on the perinatal and life-long consequences of glucocorticoid exposure in mid- to late-pregnancy. These studies in the sheep model have shown that maternal injections with glucocorticoids, in a manner similar to clinical treatment for women at risk of preterm birth, enhance fetal lung maturation, but were also associated with developmental and other functional alterations that are of concern. With weekly doses to the mother, there is restricted fetal growth, delayed myelination of the central nervous system, altered blood pressure soon after birth and increased insulin response to glucose challenge in early adulthood. If the glucocorticoids are given to the fetus by ultrasound-guided intramuscular injection, rather than to the mother, the effects on lung maturation are similar, but growth is spared and blood pressure after birth is unaltered. Increased insulin response to glucose challenge occurs in early adulthood with glucocorticoid by either route and is independent of growth restriction. 3. The findings in experimental animals are supported by studies of children in the Western Australian Preterm Infant Follow-up Study. Multivariate analyses have shown that increasing the number of glucocorticoid exposures, for the purpose of enhancing lung maturation prior to preterm birth, is associated with reduced birthweight and behavioural disorders at 3 years of age. 4. The results of these animal and clinical studies provide further support for a role of prenatal glucocorticoid exposure in triggering predisposition to adult disease. Further exploration of these models is expected to uncover the mechanisms and lead to effective strategies that may underpin clinical interventions.
机译:1.人们现在认为,子宫内环境在许多成人疾病的起源中起着重要作用。出生前有明显“编程”的疾病包括高血压,糖尿病,冠心病和中风。根据遗传易感性,宫内触发似乎可以控制个体的新陈代谢和内分泌环境,出生后,这些危险因素会因环境影响而扩大或最小化。营养不良和糖皮质激素暴露是胎儿生命中最有效的触发因素。 2.在过去的十年中,对绵羊的一系列研究集中于在妊娠中晚期妊娠糖皮质激素的暴露对围产期和终生的影响。这些在绵羊模型中的研究表明,母体注射糖皮质激素的方式类似于对有早产风险的妇女进行临床治疗的方式,可增强胎儿的肺成熟度,但也与令人关注的发育和其他功能改变有关。每周给母亲服用一次,会限制胎儿的生长,延缓中枢神经系统的髓鞘形成,出生后不久便会改变血压,成年初期对葡萄糖激发的胰岛素反应也会增加。如果将糖皮质激素通过超声引导的肌内注射而不是母亲给予胎儿,对肺成熟的影响是相似的,但可以避免生长,并且出生后的血压不会改变。在成年早期使用糖皮质激素通过任一途径发生的胰岛素对葡萄糖激发的反应增加,并且与生长限制无关。 3.实验动物的发现得到了西澳大利亚州早产儿随访研究中儿童研究的支持。多变量分析表明,为了增强早产前肺成熟的目的,增加糖皮质激素暴露的次数与3岁以下的体重减轻和行为障碍有关。 4.这些动物和临床研究的结果为产前糖皮质激素暴露在诱发成人疾病易感性中的作用提供了进一步的支持。预期对这些模型的进一步探索将揭示其机制,并导致可能为临床干预提供基础的有效策略。

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