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产前类固醇治疗临床剂量的1%直接给予早产绵羊胎儿时,足以诱导肺成熟。

One percent of the clinical dose used for antenatal steroid therapy is sufficient to induce lung maturation when administered directly to the preterm ovine fetus.

作者信息

Fee Erin L, Takahashi Tsukasa, Takahashi Yuki, Carter Sean, Furfaro Lucy, Clarke Michael W, Milad Mark A, Usuda Haruo, Newnham John P, Saito Masatoshi, Jobe Alan H, Kemp Matthew W

机构信息

Division of Obstetrics and Gynecology, Medical School, The University of Western Australia, Perth, Western Australia, Australia.

Centre for Perinatal and Neonatal Medicine, Tohoku University Hospital, Sendai, Japan.

出版信息

Am J Physiol Lung Cell Mol Physiol. 2022 Jun 1;322(6):L853-L865. doi: 10.1152/ajplung.00058.2022. Epub 2022 Apr 19.

Abstract

Antenatal steroids (ANSs) are routinely administered to women judged to be at imminent risk of preterm delivery. Their principal benefit is precocious functional maturation of the preterm fetal lung. Current dosing regimens expose the mother and fetus to high steroid levels that may be unnecessary, increasing the potential risks of disruption to the maternal and fetal hypothalamic-pituitary-adrenal (HPA) axis and glucose regulation, alterations in placental function, and reduced fetal growth. Using a sheep model of pregnancy, we tested the hypothesis that direct fetal administration of an ultra-low dose course of betamethasone phosphate (∼0.33 mg) would be sufficient to elicit functional maturation of the fetal lung. A jugular catheter was installed in singleton ovine fetuses at 122-day gestation under general anesthesia. Animals were randomized to receive either: ) fetal intravenous betamethasone phosphate to target fetal plasma betamethasone mean levels of 2 ng/mL for 26 h (fetal treatment group; = 16); ) fetal intravenous saline for 26 h and two maternal intramuscular injections of 0.25 mg/kg betamethasone phosphate + betamethasone acetate, simulating a standard clinical treatment (maternal treatment group; = 12); or ) fetal intravenous saline only for 26 h (negative control group; = 10). Fetuses were delivered 48 h after surgery, ventilated for 30 min to allow the collection of lung function and physiological data, and euthanized. Quantitative PCR and Western blots were used to assess markers of lung maturation. The average total betamethasone phosphate dose for the fetal treatment group was 1% (0.3 mg) of the maternal treatment group (31-mg betamethasone phosphate + betamethasone acetate). At 30 min of ventilation, arterial [Formula: see text], pH, heart rate, and ventilation efficacy index (VEI) were significantly ( < 0.05) and equivalently improved in both the fetal treatment group and maternal treatment group, relative to the negative control group. Similarly, SP-A, SP-C, and AQ-5 mRNA expression was significantly higher in both the fetal treatment group and maternal treatment group, relative to negative control. Maternal steroid administration was not required to generate preterm fetal lung maturation in sheep. Using a low dose and targeting steroid treatments directly to the fetus has the potential to significantly reduce maternal exposures, while simultaneously reducing the potential risk of adverse outcomes associated with current clinical dosing regimens.

摘要

产前类固醇(ANSs)通常用于被判定有早产风险的孕妇。其主要益处是促进早产胎儿肺的功能早熟。目前的给药方案会使母亲和胎儿暴露于可能不必要的高类固醇水平,增加了扰乱母婴下丘脑 - 垂体 - 肾上腺(HPA)轴和葡萄糖调节、改变胎盘功能以及降低胎儿生长的潜在风险。我们使用绵羊妊娠模型,测试了直接给胎儿超低剂量(约0.33毫克)磷酸倍他米松疗程足以引发胎儿肺功能成熟的假设。在全身麻醉下,于妊娠122天时为单胎绵羊胎儿植入颈静脉导管。将动物随机分为三组:)胎儿静脉注射磷酸倍他米松,使胎儿血浆倍他米松平均水平达到2纳克/毫升,持续26小时(胎儿治疗组;n = 16);)胎儿静脉注射生理盐水26小时,并对母亲进行两次肌肉注射0.25毫克/千克磷酸倍他米松 + 醋酸倍他米松,模拟标准临床治疗(母亲治疗组;n = 12);或)仅给胎儿静脉注射生理盐水26小时(阴性对照组;n = 10)。术后48小时分娩胎儿,通气30分钟以收集肺功能和生理数据,然后实施安乐死。使用定量PCR和蛋白质免疫印迹法评估肺成熟标志物。胎儿治疗组的磷酸倍他米松总剂量平均为母亲治疗组(31毫克磷酸倍他米松 + 醋酸倍他米松)的1%(0.3毫克)。通气30分钟时,相对于阴性对照组,胎儿治疗组和母亲治疗组的动脉[公式:见原文]、pH值、心率和通气效能指数(VEI)均显著(P < 0.05)且同等程度地得到改善。同样,相对于阴性对照组,胎儿治疗组和母亲治疗组中表面活性蛋白A(SP - A)、表面活性蛋白C(SP - C)和水通道蛋白5(AQ - 5)的mRNA表达均显著更高。在绵羊中,无需母体给予类固醇即可实现早产胎儿肺成熟。采用低剂量并将类固醇治疗直接靶向胎儿有潜力显著减少母体暴露,同时降低与当前临床给药方案相关的不良结局的潜在风险。

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