首页> 外文期刊>South African medical journal: Suid-Afrikaanse tydskrif vir geneeskunde >Nevirapine plasma concentrations in premature infants exposed to single-dose nevirapine for prevention of mother-to-child transmission of HIV-1.
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Nevirapine plasma concentrations in premature infants exposed to single-dose nevirapine for prevention of mother-to-child transmission of HIV-1.

机译:暴露于单剂量奈韦拉平的早产儿奈韦拉平血浆浓度可预防HIV-1的母婴传播。

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BACKGROUND: No pharmacokinetic data exist for premature infants receiving single-dose nevirapine (sd NVP) for prevention of mother-to-child transmission (MTCT) of HIV. AIM: To describe NVP decay pharmacokinetics in two groups of premature infants - those whose mothers either received or did not receive NVP during labour. METHODS: Infants less than 37 weeks' gestation were prospectively enrolled. Mothers received sd NVP during labour. Infants received sd NVP and zidovudine. Blood was collected on specified days after birth and NVP concentrations were determined by liquid chromatography-mass spectrometry. RESULTS: Data were obtained from 81 infants, 58 born to mothers who received sd NVP during labour (group I) and 23 to mothers who did not receive NVP (group II). Of the infants 29.6% were small for gestational age (SGA). Median (range) maximum concentration (Cmax), time to reach maximum concentration (Tmax), area under the plasma concentration-time curve (AUC) and half-life (T(1/2)) were 1 438 (350 - 3 832) ng/ml, 25h50 (9h40 - 83h45), 174 134 (22 308 - 546 408) ng/h/ml and 59.0 (15.4 - 532.6) hours for group I and 1 535 (635 - 4 218) ng/ml, 17h35 (7h40 - 29h), 168 576 (20 268 - 476 712) ng/h/ml and 69.0 (22.12 - 172.3) hours for group II. For group II, the median (range) volume of distribution (Vd) and body clearance (Cl) were 1 702.6 (623.7 - 6 189.8) ml and 34.9 (6.2 - 163.8) ml/h. The AUC was higher (p=0.006) and Cl lower (p<0.0001) in SGA infants. Plasma concentrations exceeding 100ng/ml were achieved over 8 days in 78% infants in group I and 70.0% in group II. The MTCT rate was 4.8%. CONCLUSION: Women in preterm labour often deliver with little advance warning. Our study suggests that NVP dosing of preterm infants as soon as possible after birth without maternal intrapartum dosing may be as effective as combined maternal and infant dosing.
机译:背景:尚无接受单剂量奈韦拉平(sd NVP)预防HIV母婴传播(MTCT)的早产儿的药代动力学数据。目的:描述两组早产儿的NVP衰减药代动力学-那些母亲在分娩期间接受或不接受NVP的婴儿。方法:前瞻性纳入小于37周的婴儿。母亲在分娩期间接受了sd NVP。婴儿接受sd NVP和齐多夫定治疗。在出生后的特定日期收集血液,并通过液相色谱-质谱法测定NVP浓度。结果:数据来自81例婴儿,其中58例分娩时接受sd NVP的母亲(第一组)和23例未接受NVP的母亲(第二组)。在这些婴儿中,有29.6%的人小于胎龄(SGA)。中位数(范围)最大浓度(Cmax),达到最大浓度的时间(Tmax),血浆浓度-时间曲线下的面积(AUC)和半衰期(T(1/2))为1 438(350-3 832) )ng / ml,I组的25h50(9h40-83h45),174134(22308-546408)ng / h / ml和59.0(15.4-532.6)小时,以及1535(635-4218)ng / ml, II组的17h35(7h40-29h),168576(20 268-476712)ng / h / ml和69.0(22.12-172.3)小时。对于第二组,中位数(范围)分布量(Vd)和身体清除率(Cl)为1 702.6(623.7-6 189.8)ml和34.9(6.2-163.8)ml / h。 SGA婴儿的AUC较高(p = 0.006),Cl较低(p <0.0001)。 I组中78%的婴儿和II组中70.0%的婴儿在8天内血浆浓度超过100ng / ml。 MTCT率为4.8%。结论:早产妇女通常很少提供预警。我们的研究表明,不经母体分娩的早产儿在出生后尽快进行NVP给药可能与母体和婴儿联合给药一样有效。

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