Maternal Fetal Medicine Fellowship Program, Department of Obstetrics and Gynecology, University of Mississippi Medical Center, Jackson, MS 39216.
Hypertension. 2013 Dec;62(6):1068-73. doi: 10.1161/HYPERTENSIONAHA.113.01514. Epub 2013 Sep 23.
Preeclampsia, new onset hypertension with proteinuria during pregnancy, is associated with chronic inflammation and placental oxidative stress (ROS). Chronic interleukin-17 (IL-17) increases blood pressure, autoantibodies (angiotensin II type I receptor [AT1-AA]), and ROS during pregnancy. The objective of this study was to determine whether T-helper 17 (TH17) suppression via IL-17 recombinant receptor C (IL-17RC) decreases pathophysiology associated with placental ischemia (reduced uterine perfusion pressure [RUPP]). On gestation day 14, miniosmotic pumps infusing 100 pg of IL-17RC per day were implanted into pregnant rats undergoing RUPP. On gestation day 18, carotid catheters were inserted. On gestation day 19, mean arterial pressure was recorded and TH17 cells, oxidative stress, and AT1-AA were measured and analyzed via 1-way ANOVA. Mean arterial pressure increased from 101 ± 2 mm Hg in normal pregnant rats (n = 19) to 120 ± 1 mm Hg in RUPP rats (n = 17) but decreased to 110 ± 2 mm Hg in RUPP+IL-17RC rats (n = 22). Pup weight decreased from 2.28 ± 0.2 g in normal pregnant rats to 1.96 ± 0.3 g in RUPP rats but was significantly increased to 2.01 ± 0.1 in RUPP+IL-17RC rats. TH17 cells were 1.77% in RUPP rats but decreased to 0.65% in RUPP+IL-17RC rats. Urinary isoprostanes were normalized in RUPP+IL-17RC rats (52 pg/µg) compared with 89 pg/µg in RUPP controls. Placental ROS was 652 relative light units in RUPP rats but decreased to 337 relative light units in RUPP+IL-17RC rats. AT1-AA was 17.27 ± 0.7 bpm in RUPP rats but decreased to 5.00 ± 0.5 bpm in RUPP+IL-17RC rats. With this study, we show that infusion of IL-17RC blunts TH17s, oxidative stress, AT1-AA, and hypertension in the RUPP model of preeclampsia, indicating that TH17 cells may play an important role in disease pathophysiology.
子痫前期是一种妊娠期间新发生的高血压合并蛋白尿的疾病,与慢性炎症和胎盘氧化应激(ROS)有关。慢性白细胞介素 17(IL-17)在妊娠期间增加血压、自身抗体(血管紧张素 II 型受体 [AT1-AA])和 ROS。本研究的目的是确定通过白细胞介素 17 重组受体 C(IL-17RC)抑制辅助性 T 细胞 17(TH17)是否可以减轻与胎盘缺血(降低子宫灌注压 [RUPP])相关的病理生理学变化。在妊娠第 14 天,将每天输注 100pg IL-17RC 的微型渗透泵植入正在接受 RUPP 的妊娠大鼠体内。在妊娠第 18 天,插入颈动脉导管。在妊娠第 19 天,记录平均动脉压,并通过单向方差分析测量和分析 TH17 细胞、氧化应激和 AT1-AA。正常妊娠大鼠(n=19)的平均动脉压从 101±2mmHg 升高至 RUPP 大鼠(n=17)的 120±1mmHg,但降至 RUPP+IL-17RC 大鼠(n=22)的 110±2mmHg。正常妊娠大鼠的幼仔体重从 2.28±0.2g 降至 RUPP 大鼠的 1.96±0.3g,但在 RUPP+IL-17RC 大鼠中显著增加至 2.01±0.1g。TH17 细胞在 RUPP 大鼠中占 1.77%,但在 RUPP+IL-17RC 大鼠中降至 0.65%。与 RUPP 对照组的 89pg/μg 相比,RUPP+IL-17RC 大鼠的尿异前列腺素恢复正常(52pg/μg)。RUPP 大鼠的胎盘 ROS 为 652 相对光单位,但在 RUPP+IL-17RC 大鼠中降至 337 相对光单位。AT1-AA 在 RUPP 大鼠中为 17.27±0.7bpm,但在 RUPP+IL-17RC 大鼠中降至 5.00±0.5bpm。通过这项研究,我们表明,在子痫前期的 RUPP 模型中,输注 IL-17RC 可抑制 TH17s、氧化应激、AT1-AA 和高血压,表明 TH17 细胞可能在疾病的病理生理学中发挥重要作用。
