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Pharmacokinetics of Hydroxyprogesterone Caproate and its Primary Metabolites during Pregnancy

机译:妊娠期己酸羟孕酮及其主要代谢产物的药代动力学

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Objective To measure pharmacokinetics of hydroxyprogesterone caproate (OHPC) and its major metabolites throughout pregnancy. Study Design Thirty women were prescribed OHPC for recurrent preterm birth prevention. Three cohorts of subjects had blood drawn for 7 consecutive days at one of three times: cohort 1 ( n =?6) after the first dose (weeks 16–20), cohort 2 ( n =?8) between weeks 24 and 28, and cohort 3 ( n =?16) between weeks 32 and 36. We measured serum trough levels after week 1 in cohort 1 or after two consecutive weekly doses in cohorts 2 and 3. In 10 subjects, we estimated OHPC terminal half-life at 28 days after their last dose. Results In cohorts 1, 2, and 3, the areas under curve (ng?×?h/mL) for OHPC were 571.4?±?195.2, 1,269.6?±?285.0, and 1,268.0?±?511.6, respectively. Maximum OHPC levels (ng/mL) were 5.0?±?1.5, 12.5?±?3.9, and 12.3?±?4.9, respectively. The areas under the curve for mono-hydroxylated metabolites were 208.5?±?92.4, 157.1?±?64.6, and 211.2?±?113.1, and maximum concentrations were 1.9?±?0.7, 1.5?±?0.7, and 1.8?±?1.0, respectively. Di-hydroxylated metabolite levels were significantly lower than mono-hydroxylated metabolites. Estimated terminal half-life of OHPC was 16.3?±?3.6 days and 19.7?±?6.2 days for the mono-hydroxylated metabolites. Conclusion After the first injection, OHPC maximum serum level was approximately half steady-state level. Measurable metabolites of unknown activity were detected.
机译:目的测定整个妊娠期间己酸羟孕酮(OHPC)及其主要代谢产物的药代动力学。研究设计为30名妇女开具OHPC预防复发性早产的处方。 3组受试者连续3天抽血3次,其中一次:第一次给药后(16-20周),组1(n =?6),第24周至28周之间,组2(n =?8),在第32周到第36周之间,以及第3组(n = 16)。我们在第1周的第1周后或在第2和3组的连续两次每周剂量后测量了血清谷水平。在10位受试者中,我们估计OHPC的终末半衰期为最后一次服药后28天。结果在队列1、2和3中,OHPC的曲线下面积(ng?×?h / mL)分别为571.4?±?195.2、1,269.6?±?285.0和1,268.0?±?511.6。最高OHPC水平(ng / mL)分别为5.0±1.5、12.5±3.9和12.3±4.9。单羟基化代谢物的曲线下面积为208.5±±92.4、157.1±±64.6和211.2±±113.1,最大浓度为1.9±±0.7、1.5±±0.7和1.8±±。分别为1.0。二羟基化代谢物水平显着低于单羟基化代谢物。 OHPC的终末半衰期估计为16.3±±3.6天,单羟基化代谢产物为19.7±±6.2天。结论首次注射后,OHPC最高血清水平约为稳态水平的一半。检测到未知活性的可测量代谢物。

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