In vivo evidence for the existence of a threshold for hyperglycemia-induced major fetal malformations: relevance to the etiology of diabetic teratogenesis.

A Torchinsky, V Toder, H Carp, H Orenstein, A Fein
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Abstract

The present study was carried out to evaluate whether hyperglycemia-induced major fetal anomalies are thresholded phenomena. Streptozotocin (STZ)-treated female ICR mice were examined on day 19 of pregnancy by methods routinely used in Segment II teratological studies. Simultaneously, the glucose and hemoglobin A1c (HbA1c) levels in maternal-blood were measured and mice with glucose levels > 9.5 mmol/l (mean + 3 SD) were considered to be diabetic. The occurrence of litters with fetuses having gross structural anomalies was clearly associated with glucose levels > 27.8 mmol/l. A wide range of HbA1c levels (between 6 and 18 SD above the mean) were observed, within which only single malformed fetuses were found in the litters of diabetic females. A decreased pregnancy rate in diabetic ICR mice was associated with glucose levels > 16.7 mmol/l and with HBA1c levels > 6 SD above the mean. The results of this study suggest that there is a threshold glucose level associated with a clear increase of the number of litters with severely malformed fetuses in diabetic ICR mice. Results of this study also suggest the existence of HbA1c-associated factors determining, along with glucose, the teratogenic response of ICR mice to diabetes. The interpretation of results obtained in terms of the multifactorial/threshold model leads to the hypothesis that the teratogenic potential of diabetes may consist of two components; one associated with 'direct' teratogens perturbing developmental processes in embryos at a 'critical moment' in organogenesis, and a second component, associated with a direct or indirect influence of the diabetic environment on developmental processes in the preimplantation embryos.

体内存在高血糖诱导的主要胎儿畸形阈值的证据:与糖尿病致畸的病因学相关。
本研究旨在评估高血糖引起的重大胎儿异常是否为阈值现象。在妊娠第19天,用常规II节致畸研究方法对经STZ处理的雌性ICR小鼠进行检查。同时测定母血葡萄糖和血红蛋白A1c (HbA1c)水平,葡萄糖水平> 9.5 mmol/l(平均+ 3 SD)的小鼠为糖尿病。出现大体结构异常的窝鼠与血糖水平> 27.8 mmol/l明显相关。观察到的HbA1c水平范围很广(高于平均值6至18 SD),在该范围内,仅在糖尿病母鼠窝中发现单个畸形胎儿。糖尿病ICR小鼠妊娠率降低与血糖水平> 16.7 mmol/l和HBA1c水平> 6 SD相关。本研究结果表明,糖尿病ICR小鼠严重畸形胎仔数明显增加与阈值葡萄糖水平相关。本研究结果还表明,hba1c相关因子的存在与葡萄糖一起决定了ICR小鼠对糖尿病的致畸反应。根据多因子/阈值模型获得的结果的解释导致了糖尿病致畸潜力可能由两个组成部分组成的假设;其中一个因素与在器官发生的“关键时刻”干扰胚胎发育过程的“直接”致畸物有关,第二个因素与糖尿病环境对着床前胚胎发育过程的直接或间接影响有关。
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