产前曲前列尼尔可减轻先天性膈疝大鼠模型的肺动脉高压表型。
Prenatal treprostinil reduces the pulmonary hypertension phenotype in the rat model of congenital diaphragmatic hernia.
机构信息
Center for Fetal Research, Children's Hospital of Philadelphia, Philadelphia, United States; Department of Development and Regeneration, Cluster Woman and Child, KU Leuven, Leuven, Belgium.
Center for Fetal Research, Children's Hospital of Philadelphia, Philadelphia, United States.
出版信息
EBioMedicine. 2022 Jul;81:104106. doi: 10.1016/j.ebiom.2022.104106. Epub 2022 Jun 29.
BACKGROUND
Persistent pulmonary hypertension (PH) causes significant mortality and morbidity in infants with congenital diaphragmatic hernia (CDH). Since pulmonary vascular abnormalities in CDH develop early during foetal development, we hypothesized that prenatal maternal administration of treprostinil, through its anti-remodelling effect, would improve the PH-phenotype in the nitrofen rat model of CDH.
METHODS
In a dose-finding study in normal, healthy pregnant rats, we demonstrated target-range foetal plasma treprostinil concentrations without signs of toxicity. Next, an efficacy study was performed assessing the effects of treprostinil administration at 900 and 1500ng/kg/min from gestational day (GD) 16 until term (GD 21) in CDH and control pups. Pulmonary vascular and airway morphometry, lung mechanics, and expression patterns of genes implicated in the prostaglandin vasoactive pathway were studied.
FINDINGS
In rats maternal administration of 1500ng/kg/min treprostinil reached target foetal concentrations, with no detrimental maternal or foetal side-effects. Prenatal exposure to 900 and 1500 ng/kg/min treprostinil reduced the medial wall thickness (%MWT) (CDH·900, 38.5± 8·4%; CDH.1500, 40·2±9·7%; CDH, 46·6±8·2%; both p < 0·0001) in rat pups with CDH, however increased the %MWT in normal foetuses (C.T.900, 36·6±11·1%; C.T.1500, 36·9±9·3%; C.P., 26·9±6·2%; both p < 0·001). Pulmonary airway development, lung hypoplasia and pulmonary function were unaffected by drug exposure.
INTERPRETATION
In pregnant rats maternally administered treprostinil crosses the placenta, attains foetal target concentrations, and is well tolerated by both mother and foetuses. This report shows a significant reduction of pulmonary arteriole muscularization with prenatal treprostinil in a nitrofen rat model, supporting the promise of this treatment approach for PH of CDH.
FUNDING
United Therapeutics Corporation provided treprostinil and financial support (ISS-2020-10879).
背景
持续性肺动脉高压(PH)会导致先天性膈疝(CDH)婴儿出现显著的死亡率和发病率。由于 CDH 中的肺血管异常在胎儿发育早期就已经发生,我们假设通过其抗重塑作用,在 nitrofen 大鼠 CDH 模型中,产前给予曲前列尼尔可改善 PH 表型。
方法
在正常健康的妊娠大鼠的剂量发现研究中,我们证明了胎盘中曲前列尼尔的靶浓度范围,而没有毒性迹象。接下来,进行了一项疗效研究,评估了从妊娠第 16 天(GD 16)至妊娠第 21 天(GD 21),以 900 和 1500ng/kg/min 的剂量给予曲前列尼尔对 CDH 和对照幼仔的影响。研究了肺血管和气道形态计量学、肺力学以及参与前列腺素血管活性途径的基因的表达模式。
结果
在给予 1500ng/kg/min 曲前列尼尔的大鼠中,母鼠达到了靶胎浓度,且没有母鼠或胎鼠的不良副作用。产前暴露于 900 和 1500ng/kg/min 曲前列尼尔可降低 CDH 幼仔的中膜厚度(%MWT)(CDH·900,38.5±8.4%;CDH.1500,40.2±9.7%;CDH,46.6±8.2%;均 p<0.0001),但增加了正常胎儿的%MWT(C.T.900,36.6±11.1%;C.T.1500,36.9±9.3%;C.P.,26.9±6.2%;均 p<0.001)。药物暴露对肺气道发育、肺发育不全和肺功能没有影响。
结论
在妊娠大鼠中,母体给予曲前列尼尔可穿过胎盘,达到胎仔的靶浓度,且母鼠和胎鼠均能耐受。本报告显示,在 nitrofen 大鼠模型中,产前给予曲前列尼尔可显著减少肺小动脉肌化,这支持了这种治疗方法对 CDH 肺动脉高压的应用前景。
资金
联合治疗公司提供了曲前列尼尔并提供了资金支持(ISS-2020-10879)。
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