Division of Obstetrics and Gynecology, The University of Western Australia, Perth, Western Australia, Australia.
Centre for Perinatal and Neonatal Medicine, Tohoku University Hospital, Sendai, Japan.
PLoS One. 2021 Sep 24;16(9):e0257847. doi: 10.1371/journal.pone.0257847. eCollection 2021.
Intraamniotic inflammation is associated with up to 40% of preterm births, most notably in deliveries occurring prior to 32 weeks' gestation. Despite this, there are few treatment options allowing the prevention of preterm birth and associated fetal injury. Recent studies have shown that the small, non-competitive allosteric interleukin (IL)-1 receptor inhibitor, rytvela, may be of use in resolving inflammation associated with preterm birth (PTB) and fetal injury. We aimed to use an extremely preterm sheep model of chorioamnionitis to investigate the anti-inflammatory efficacy of rytvela in response to established intra-amniotic (IA) lipopolysaccharide (LPS) exposure. We hypothesized that rytvela would reduce LPS-induced IA inflammation in amniotic fluid (AF) and fetal tissues.
Sheep with a single fetus at 95 days gestation (estimated fetal weight 1.0 kg) had surgery to place fetal jugular and IA catheters. Animals were recovered for 48 hours before being randomized to either: i) IA administration of 2 ml saline 24 hours before 2 ml IA and 2 ml fetal intravenous (IV) administration of saline (Saline Group, n = 7); ii) IA administration of 10 mg LPS in 2 ml saline 24 hours before 2 ml IA and 2 ml fetal IV saline (LPS Group, n = 10); 3) IA administration of 10 mg LPS in 2 ml saline 24 hours before 0.3 mg/fetal kg IA and 1 mg/fetal kg fetal IV rytvela in 2 ml saline, respectively (LPS + rytvela Group, n = 7). Serial AF samples were collected for 120 h. Inflammatory responses were characterized by quantitative polymerase chain reaction (qPCR), histology, fluorescent immunohistochemistry, enzyme-linked inmmunosorbent assay (ELISA), fluorescent western blotting and blood chemistry analysis.
LPS-treated animals had endotoxin and AF monocyte chemoattractant protein (MCP)-1 concentrations that were significantly higher at 24 hours (immediately prior to rytvela administration) relative to values from Saline Group animals. Following rytvela administration, the average MCP-1 concentrations in the AF were significantly lower in the LPS + rytvela Group relative to in the LPS Group. In delivery samples, the expression of IL-1β in fetal skin was significantly lower in the LPS + rytvela Group compared to the LPS Group.
A single dose of rytvela was associated with partial, modest inhibition in the expression of a panel of cytokines/chemokines in fetal tissues undergoing an active inflammatory response.
羊膜腔内炎症与高达 40%的早产有关,尤其是在 32 周前分娩的情况下。尽管如此,仍几乎没有治疗方法可以预防早产和相关的胎儿损伤。最近的研究表明,小的、非竞争性的白细胞介素(IL)-1 受体抑制剂 rytvela 可能有助于解决与早产(PTB)和胎儿损伤相关的炎症。我们旨在使用极早产羊的绒毛膜羊膜炎模型来研究 rytvela 在应对已建立的羊膜内(IA)脂多糖(LPS)暴露时的抗炎疗效。我们假设 rytvela 将减少 LPS 诱导的羊水中(AF)和胎儿组织中的 IA 炎症。
怀孕 95 天(估计胎儿体重 1.0 公斤)的单胎绵羊进行手术,放置胎儿颈静脉和 IA 导管。动物恢复 48 小时后,随机分为以下三组:i)IA 给予 2 ml 生理盐水,24 小时前 IA 和 2 ml 胎儿静脉内(IV)给予生理盐水(生理盐水组,n = 7);ii)IA 给予 2 ml 生理盐水中的 10 mg LPS,24 小时前 IA 和 2 ml 胎儿 IV 生理盐水(LPS 组,n = 10);iii)IA 给予 2 ml 生理盐水中的 10 mg LPS,24 小时前 IA 和 1 mg/fetal kg IV 分别给予 2 ml 生理盐水的 0.3 mg/fetal kg rytvela(LPS+rytvela 组,n = 7)。连续采集 120 小时的 AF 样本。通过定量聚合酶链反应(qPCR)、组织学、荧光免疫组织化学、酶联免疫吸附测定(ELISA)、荧光 Western 印迹和血液化学分析来描述炎症反应。
与生理盐水组动物相比,LPS 处理的动物在 24 小时(在给予 rytvela 之前)时的内毒素和 AF 单核细胞趋化蛋白 1(MCP-1)浓度明显更高。给予 rytvela 后,LPS+rytvela 组的 AF 中 MCP-1 浓度明显低于 LPS 组。在分娩样本中,与 LPS 组相比,LPS+rytvela 组胎儿皮肤中 IL-1β 的表达明显降低。
单次给予 rytvela 与胎儿组织中一组细胞因子/趋化因子的表达部分适度抑制有关,这些胎儿组织正在经历活跃的炎症反应。
