Bourget P, Roulot C, Fernandez H
Department of Clinical Pharmacy, Hôpital Necker-Enfants Malades, Paris, France.
Clin Pharmacokinet. 1995 Feb;28(2):161-80. doi: 10.2165/00003088-199528020-00006.
Pregnancy is a specific dynamic state, and the potential usefulness of caring for a disorder in the fetus or the mother is now well established. Previously, pregnant women have been excluded from clinical trials, therefore only a few studies concerning evaluation of the pregestational metabolism or transplacental transfer (TPT) of drugs exist. Questions regarding the TPT of drugs are extensive and complex. For example, does TPT occur at a given gestational age, in the context of a particular type of pathology or when a drug is administered by a certain dosage regimen? If this is the case, what is the rapidity of penetration of the products of conception by the drug (bearing in mind its physicochemical characteristics)? Need harmful adverse effects on the child be feared? Is such penetration desirable, of no consequence, or dangerous? Does the possibility exist of accumulation in the placenta, fetal tissue or amniotic fluid? Should such findings modify the therapeutic regimens of drugs given to expectant mothers? Exchange mechanisms are complicated and models developed in vitro only partially reflect the actual equilibria that exist between mother and fetus. These include: (i) the perfused cotyledon model, which while simple, elegant and inexpensive, offers only a localised, restricted and fixed view of pregnancy; (ii) isolated anatomical fractions that are informative, but which straddle the border between physiology and pharmacology; and (iii) the necessary study, using microsomes, of placental metabolic capacity (enzyme cartography). In vivo study of TPT is based upon various multicompartmental pharmacokinetic models, some of which have been relatively validated in animals. The simplest indicator for the in vivo evaluation of TPT of a drug in the human species is determination of a feto-maternal blood concentration ratio (usually performed at the time of placental separation). However, the usefulness and limitations of this parameter are controversial, and it would seem preferable to associate it with a pharmacokinetic profile of variations in blood concentrations established in the mother. Furthermore, any extrapolation of a single result to fetal and adjacent tissues must be done with the greatest caution. Although, no drug should be used in pregnancy unless there is a clear therapeutic indication, study of the TPT of therapeutically useful agents is essential to the understanding of their metabolism and is a prerequisite to the safe use of medications during pregnancy.
妊娠是一种特殊的动态状态,现在已经充分证实了关注胎儿或母亲疾病的潜在益处。以前,孕妇被排除在临床试验之外,因此关于孕前药物代谢或经胎盘转运(TPT)的研究很少。关于药物经胎盘转运的问题广泛而复杂。例如,在特定的胎龄、特定类型的病理情况下或采用特定的给药方案时,药物是否会发生经胎盘转运?如果是这样,考虑到药物的理化特性,药物穿透妊娠产物的速度有多快?是否需要担心对胎儿产生有害的不良反应?这种穿透是可取的、无影响的还是危险的?药物是否有可能在胎盘、胎儿组织或羊水中蓄积?这些发现是否应该改变给准妈妈用药的治疗方案?交换机制很复杂,体外建立的模型只能部分反映母体和胎儿之间实际存在的平衡。这些模型包括:(i)灌注叶状绒毛膜模型,虽然简单、精巧且成本低廉,但只能提供局部、有限且固定的妊娠视图;(ii)孤立的解剖部分,虽然有参考价值,但跨越了生理学和药理学的边界;(iii)使用微粒体对胎盘代谢能力(酶谱)进行必要的研究。药物经胎盘转运的体内研究基于各种多室药代动力学模型,其中一些模型已在动物身上得到了相对验证。在人体中对药物经胎盘转运进行体内评估的最简单指标是测定胎儿-母体血药浓度比(通常在胎盘分离时进行)。然而,这个参数的实用性和局限性存在争议,似乎最好将其与母体中建立的血药浓度变化的药代动力学曲线相关联。此外,将单一结果外推至胎儿及邻近组织时必须极其谨慎。尽管除非有明确的治疗指征,否则孕期不应使用任何药物,但对治疗有用药物的经胎盘转运进行研究对于了解其代谢至关重要,并且是孕期安全用药的先决条件。
