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淋巴途径——II. 以白蛋白作为阻滞剂在兔体内注射人重组干扰素-α 2 的药代动力学

The lymphatic route--II. Pharmacokinetics of human recombinant interferon-alpha 2 injected with albumin as a retarder in rabbits.

作者信息

Bocci V, Muscettola M, Naldini A, Bianchi E, Segre G

出版信息

Gen Pharmacol. 1986;17(1):93-6. doi: 10.1016/0306-3623(86)90017-0.

Abstract

The aim of the present investigation was to define whether multisite subcutaneous (s.c.) administration in unanesthetized, unrestrained rabbits of human recombinant interferon-alpha 2 (rec. IFN-alpha 2) either in saline, human albumin (ALB) solution (4, 7 and 10% final concentrations), or in a solution containing 75 U of hyaluronidase, modified the pharmacokinetic parameters calculated from the IFN plasma levels. Plasma disappearance rates of rec. IFN-alpha 2 were measured in rabbits after intravenous (i.v.) administration and the kinetic was adequately represented by a three-pools mammillary model. This model was the basis for evaluating the absorption and distribution of rec. IFN-alpha 2 after s.c. administration. The increase of ALB concentration (from 4 to 10%) caused a significant reduction of the plasma IFN Cmax while both the mean residence time and the release time of IFN increased linearly with the ALB concentration. The data support the postulation that s.c. administration of albumin acts as an interstitial fluid expander and may favour absorption of IFN via lymphatics rather than blood capillaries. Improvement of therapeutic index of IFN by using this route remains to be shown in clinical trials.

摘要

本研究的目的是确定在未麻醉、未束缚的兔体内,将重组人α-2干扰素(rec. IFN-α2)多点皮下注射于生理盐水、人白蛋白(ALB)溶液(终浓度分别为4%、7%和10%)或含75 U透明质酸酶的溶液中,是否会改变根据血浆IFN水平计算出的药代动力学参数。静脉注射(i.v.)后,在兔体内测定rec. IFN-α2的血浆清除率,其动力学可用三室乳突模型充分描述。该模型是评估rec. IFN-α2皮下注射后的吸收和分布的基础。ALB浓度的增加(从4%到10%)导致血浆IFN Cmax显著降低,而IFN的平均驻留时间和释放时间均随ALB浓度呈线性增加。这些数据支持以下假设:皮下注射白蛋白可作为组织间液扩容剂,可能有利于IFN通过淋巴管而非毛细血管吸收。通过该途径提高IFN治疗指数仍有待临床试验证实。

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