Smith Judith A, Donepudi Roopali V, Argoti Pedro S, Giezentanner Anita L, Jain Ranu, Boring Noemi, Garcia Elisa, Moise Kenneth J
Department of Obstetrics, Gynecology and Reproductive Medicine, UTHealth McGovern Medical SchoolHouston, TX, USA; Department of Pharmacy, Memorial Hermann Hospital-Texas Medical Centre (TMC)Houston, TX, USA.
Department of Obstetrics, Gynecology and Reproductive Medicine, UTHealth McGovern Medical School Houston, TX, USA.
Front Pharmacol. 2017 Jan 24;8:11. doi: 10.3389/fphar.2017.00011. eCollection 2017.
Indications for surgery during pregnancy have increased. Specifically fetal interventions have increased from conditions that were considered lethal like twin-twin transfusion syndrome and severe fetal anemia to non-lethal conditions like myelomeningocele. The optimal anesthetic agent for surgery is yet to be determined. Success of the procedure is often dictated by the efficacy of the anesthetic to immobilize the fetus without over-sedating mom. Remifentanil is used as preferred agent due to its short half-life however pharmacokinetics in pregnancy is unknown. To determine the pharmacokinetic parameters of remifentanil in a mid-trimester pregnant patient population undergoing fetal intervention. A validated liquid chromatography assay with ultraviolet absorbance was employed to estimate maternal serum remifentanil levels. Blood samples were obtained at baseline and at selected time points: 5, 15, 30, 45, 60 min after the beginning of the remifentanil infusion and at 15, 30, and 60 min post end of infusion. Ten pregnant patients were enrolled in the study however only eight patients had sampling obtained at all time points. The mean gestational age was 22.2 (±2.7) weeks, maternal age was 27.8 (±5.1) years and body mass index was 29.6 (±6.3). After receiving a continuous infusion of remifentanil, mean total dose was 975.3 μg, C was 2.0 ng/mL and C was 8.4 ng/mL. A two-compartment model best described the plasma remifentanil data. Mean pharmacokinetic parameters were: volume of distribution (Vd) = 124.6 L (16.2-530.8 L), maternal remifentanil total clearance (Cl) = 170.7 L/h (17.7-486.9 L/h), and half-life (t) = 0.6 h (0.2-0.9 h). The maternal remifentanil area under the curve (AUC) ranged from 2.7 to 21.7 μg/Lh. The mean alpha-acidic glycoprotein was 124.8 mg/dL (81.3-149.8). The pharmacokinetic profile of remifentanil in pregnant women is similar to previously reported general population profiles. This data did provide potential rationale for the clinical observations why when remifentanil is dosed based on non-pregnant guidelines, it did not uniformly provide adequate fetal immobilization as per anecdotal perception of operating fetal surgeons. These findings are important for the development of further clinical studies to optimize dosing for surgery during pregnancy including the estimation of placental transfer and total fetal exposure.
孕期手术的指征有所增加。具体而言,胎儿干预已从诸如双胎输血综合征和严重胎儿贫血等被认为致命的情况,扩展到如脊髓脊膜膨出等非致命情况。手术的最佳麻醉剂尚未确定。手术的成功通常取决于麻醉剂使胎儿不动且不过度镇静母亲的效果。瑞芬太尼因其半衰期短而被用作首选药物,然而其在孕期的药代动力学尚不清楚。为了确定瑞芬太尼在接受胎儿干预的孕中期孕妇群体中的药代动力学参数。采用经过验证的具有紫外吸收的液相色谱分析法来估计母体血清瑞芬太尼水平。在基线以及选定的时间点采集血样:瑞芬太尼输注开始后5、15、30、45、60分钟以及输注结束后15、30和60分钟。该研究纳入了10名孕妇,但只有8名患者在所有时间点都进行了采样。平均孕周为22.2(±2.7)周,产妇年龄为27.8(±5.1)岁,体重指数为29.6(±6.3)。接受瑞芬太尼持续输注后,平均总剂量为975.3μg,C为2.0ng/mL,C为8.4ng/mL。二室模型最能描述血浆瑞芬太尼数据。平均药代动力学参数为:分布容积(Vd)=124.6L(16.2 - 530.8L),母体瑞芬太尼总清除率(Cl)=170.7L/h(17.7 - 486.9L/h),半衰期(t)=0.6h(0.2 - 0.9h)。母体瑞芬太尼曲线下面积(AUC)范围为2.7至21.7μg/Lh。平均α-酸性糖蛋白为124.8mg/dL(81.3 - 149.8)。瑞芬太尼在孕妇中的药代动力学特征与先前报道的一般人群特征相似。这些数据确实为临床观察提供了潜在的理论依据,即为何当按照非孕期指南给予瑞芬太尼时,根据胎儿外科手术医生的经验感受,它并不能始终如一地提供足够的胎儿制动效果。这些发现对于开展进一步的临床研究以优化孕期手术的给药方案,包括估计胎盘转运和胎儿总暴露量而言非常重要。
Zotero 插件