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对 SMFM 声明的警示性回应:妊娠期糖尿病的药物治疗。

A cautionary response to SMFM statement: pharmacological treatment of gestational diabetes.

机构信息

Divisions of Endocrinology and Maternal-Fetal Medicine, Departments of Medicine and Obstetrics and Gynecology, University of Colorado, Anschutz Medical Campus, Aurora, CO.

Division of Maternal-Fetal Medicine, Department of Obstetrics and Gynecology, University of Oklahoma Health Sciences Center, Oklahoma City, OK.

出版信息

Am J Obstet Gynecol. 2018 Oct;219(4):367.e1-367.e7. doi: 10.1016/j.ajog.2018.06.013. Epub 2018 Jun 28.

Abstract

Use of oral agents to treat gestational diabetes mellitus remains controversial. Recent recommendations from the Society for Maternal-Fetal Medicine assert that metformin may be a safe first-line alternative to insulin for gestational diabetes mellitus treatment and preferable to glyburide. However, several issues should give pause to the widespread adoption of metformin use during pregnancy. Fetal concentrations of metformin are equal to maternal, and metformin can inhibit growth, suppress mitochondrial respiration, have epigenetic modifications on gene expression, mimic fetal nutrient restriction, and alter postnatal gluconeogenic responses. Because both the placenta and fetus express metformin transporters and exhibit high mitochondrial activity, these properties raise important questions about developmental programming of metabolic disease in offspring. Animal studies have demonstrated that prenatal metformin exposure results in adverse long-term outcomes on body weight and metabolism. Two recent clinical randomized controlled trials in women with gestational diabetes mellitus or polycystic ovary syndrome provide evidence that metformin exposure in utero may produce a metabolic phenotype that increases childhood weight or obesity. These developmental programming effects challenge the conclusion that metformin is equivalent to insulin. Although the Society for Maternal-Fetal Medicine statement endorsed metformin over glyburide if oral agents are used, there are few studies directly comparing the 2 agents and it is not clear that metformin alone is superior to glyburide. Moreover, it should be noted that prior clinical studies have dosed glyburide in a manner inconsistent with its pharmacokinetic properties, resulting in poor glycemic control and high rates of maternal hypoglycemia. We concur with the American Diabetes Association and American Congress of Obstetricians and Gynecologists, which recommend insulin as the preferred agent, but we believe that it is premature to embrace metformin as equivalent to insulin or superior to glyburide. Due to the uncertainty of the long-term metabolic risks of either metformin or glyburide, we call for carefully controlled studies that optimize oral medication dosing according to their pharmacodynamic and pharmacokinetic properties in pregnancy, appropriately target medications based on individual patterns of hyperglycemia, and follow the offspring long-term for metabolic risk.

摘要

使用口服药物治疗妊娠期糖尿病仍然存在争议。最近,母胎医学学会提出,二甲双胍可能是治疗妊娠期糖尿病的安全一线替代胰岛素药物,优于格列本脲。然而,有几个问题应该让人们对在怀孕期间广泛使用二甲双胍持谨慎态度。胎儿的二甲双胍浓度与母体相同,而且二甲双胍可以抑制生长、抑制线粒体呼吸、对基因表达产生表观遗传修饰、模拟胎儿营养限制,并改变产后糖异生反应。由于胎盘和胎儿都表达二甲双胍转运体,并表现出高线粒体活性,这些特性提出了关于后代代谢疾病发育编程的重要问题。动物研究表明,产前暴露于二甲双胍会导致体重和代谢的长期不良后果。最近两项关于患有妊娠期糖尿病或多囊卵巢综合征的女性的临床随机对照试验提供了证据,证明宫内暴露于二甲双胍可能会产生一种代谢表型,增加儿童的体重或肥胖。这些发育编程效应挑战了二甲双胍等同于胰岛素的结论。尽管母胎医学学会的声明支持在使用口服药物时将二甲双胍优于格列本脲,但很少有研究直接比较这两种药物,也不清楚二甲双胍是否单独优于格列本脲。此外,应该注意的是,之前的临床研究以不符合其药代动力学特性的方式给格列本脲给药,导致血糖控制不佳和母体低血糖发生率高。我们同意美国糖尿病协会和美国妇产科医师学会的建议,即胰岛素是首选药物,但我们认为,将二甲双胍视为等同于胰岛素或优于格列本脲还为时过早。由于二甲双胍或格列本脲的长期代谢风险不确定,我们呼吁进行精心控制的研究,根据其在妊娠期间的药效学和药代动力学特性优化口服药物剂量,根据个体高血糖模式适当靶向药物,并对后代进行长期代谢风险随访。

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