When a pregnant or breast feeding woman requires treatment for a disease condition during the perinatal period, a major concern is whether drug therapy will result in a potentially harmful drug exposure to her offspring. To obtain approval to legally market a drug, a drug manufacturer must prove to the Food and Drug Administration that the drug is safe and effective for its intended use. Proof of safety for use in pregnant or breast feeding mothers is currently not required. Therefore, information on drug transfer and offspring exposure needed to evaluate the potential risk associated with a therapeutic option is generally not available. The pregnant Holstein cow and her newborn calf was tested as an animal model that may be used to study in utero and lactational drug transfer and offspring exposure. Two drugs used in human medicine and veterinary medicine, phenylbutazone and ivermectin were tested in the model. Prior to parturition, pregnant cows were dosed orally to steady-state with phenylbutazone at 5 mg/kg/day or given a single subcutaneous injection of 200 mcg ivermectin/kg bw. The level of drug transfer to calves exposed in utero, in utero combined with lactational exposure, and lactational exposure only, were measured from days 1 through 7 postpartum. At birth the plasma level in phenylbutazone-exposed calves was approximately half the dam's steady-state level. For ivermectin-exposed calves plasma levels were at or below the limit of quantitation (0.5 ng/ml) at birth suggesting that placental transfer of ivermectin is limited. For both drugs, rapid accumulation of the drug in calf plasma occurred with lactational exposure during the first week of life to a mean daily dose of 2 mcg ivermectin/kg bw or 0.09 mg phenylbutazone/kg bw/day. The accumulation observed in the newborn calf is attributed to the lipid solubility and long elimination half-lives of these drugs. Thus the results showed that drug transfer and offspring exposure could be studied in the cow-calf model. The results highlight the importance of considering not only the dose but also physicochemical characteristics and pharmacokinetics when evaluating the safety of a newborn's exposure to a drug in breast milk.
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机译:当孕妇或哺乳期妇女在围产期需要治疗某种疾病时,主要关注的问题是药物治疗是否会导致对她的后代的潜在有害药物暴露。为了获得合法销售药品的批准,药品制造商必须向食品药品监督管理局证明该药品对于其预期用途是安全有效的。目前不需要孕妇或哺乳期母亲的安全性证明。因此,通常无法获得评估与治疗选择相关的潜在风险所需的有关药物转移和后代暴露的信息。测试了荷斯坦奶牛和她的新生小牛的动物模型,该动物模型可用于研究子宫内和哺乳类药物的转移以及后代的暴露。在模型中测试了用于人类医学和兽医学的两种药物,苯基丁a和伊维菌素。在分娩前,给怀孕的母牛口服苯丁a 5毫克/千克/天至稳态,或单次皮下注射200 mcg伊维菌素/千克体重。从产后第1天到第7天,测量在子宫内暴露于,在子宫内暴露于与仅泌乳接触的犊牛的药物转移水平。出生时,暴露于苯丁氮酮的小牛的血浆水平约为大坝稳态水平的一半。对于伊维菌素接触的小牛,出生时血浆水平等于或低于定量限(0.5 ng / ml),表明伊维菌素的胎盘转移受到限制。对于这两种药物,在生命的第一周内随着泌乳接触,药物在小牛血浆中迅速积累,每日平均剂量为2 mcg伊维菌素/ kg bw或0.09 mg苯基丁a / kg bw /天。在新生小牛中观察到的积累归因于这些药物的脂溶性和长消除半衰期。因此,结果表明可以在牛犊模型中研究药物转移和后代暴露。结果突出了评估新生儿暴露于母乳中药物的安全性时,不仅要考虑剂量,还应考虑其理化特性和药代动力学的重要性。
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