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二醋吗啡透过早产新生儿皮肤的体外研究。

An in vitro study of diamorphine permeation through premature human neonatal skin.

作者信息

Barrett D A, Rutter N, Davis S S

机构信息

Department of Pharmaceutical Sciences, University Park, Nottingham University, UK.

出版信息

Pharm Res. 1993 Apr;10(4):583-7. doi: 10.1023/a:1018958305002.

Abstract

The permeation kinetics of diamorphine through human premature neonatal cadaver skin over a range of gestational ages between 24 and 36 weeks was investigated using small diffusion cells. A strong inverse correlation was noted between the apparent permeability coefficient and the gestational age of the skin (P < 0.01; n = 26). The calculated apparent permeability coefficients decreased with gestational age from 6.0 x 10(-2) cm.hr-1 at 24 weeks' gestation to 5.2 x 10(-6) cm.hr-1 at 36 weeks' gestation. The amount of diamorphine remaining bound within the skin at the end of the in vitro experiments did not change significantly with gestational age of the skin. Diamorphine was subject to degradation over the course of the in vitro experiments to produce significant amounts of 6-monoacetylmorphine and evidence is presented to suggest that this was due to residual skin esterase activity. It is calculated that the steady-state flux rate of diamorphine through neonatal skin observed in these experiments would be sufficient to obtain a therapeutic plasma concentration of morphine assuming a 2-cm2 area for application and a delivery rate of 15 micrograms hr-1 kg-1. However, the prolonged half-life of morphine in the premature neonate would result in a delay of some hours before the attainment of this level.

摘要

使用小型扩散池研究了二醋吗啡在24至36周不同胎龄的人类早产新生儿尸体皮肤上的渗透动力学。观察到表观渗透系数与皮肤胎龄之间存在强烈的负相关(P < 0.01;n = 26)。计算得到的表观渗透系数随胎龄增加而降低,从妊娠24周时的6.0×10⁻² cm·hr⁻¹降至妊娠36周时的5.2×10⁻⁶ cm·hr⁻¹。体外实验结束时,皮肤内残留的二醋吗啡量并未随皮肤胎龄发生显著变化。在体外实验过程中,二醋吗啡会发生降解,产生大量6-单乙酰吗啡,有证据表明这是由于皮肤中残留的酯酶活性所致。据计算,在这些实验中观察到的二醋吗啡透过新生儿皮肤的稳态通量率,假设应用面积为2 cm²且给药速率为15 μg·hr⁻¹·kg⁻¹,将足以使血浆中吗啡达到治疗浓度。然而,吗啡在早产新生儿体内的半衰期延长,会导致在达到该水平之前延迟数小时。

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