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癌症患者中部分纯化的γ干扰素的药代动力学研究。

Pharmacokinetic study of partially pure gamma-interferon in cancer patients.

作者信息

Gutterman J U, Rosenblum M G, Rios A, Fritsche H A, Quesada J R

出版信息

Cancer Res. 1984 Sep;44(9):4164-71.

PMID:6430557
Abstract

A pharmacokinetic study was performed with partially pure immune (gamma) interferon (IFN-gamma) in patients with metastatic cancer. Nine patients were given IFN-gamma by the i.m. route in doses ranging from 1.5 X 10(5) to 9.6 X 10(6) antiviral units. There was no detectable antiviral activity in patients' serum, and only minimal side effects were observed. Fifteen patients were given IFN-gamma by i.v. bolus infusion in doses ranging from 1.5 X 10(5) to 54 X 10(6) units. Serum clearance of antiviral activity was described by a monoexponential disappearance curve. The serum half-life was dose dependent (3 min at the lower doses and 34 min at the highest doses). There were few consistent biological effects observed in the patients. Based on these pharmacokinetic data, eight patients were treated by a 6-hr continuous infusion consisting of 3 X 10(6) units by i.v. bolus followed by 4 X 10(6) units/hr for 6 hr. This regimen resulted in consistent serum levels of IFN-gamma ranging from 40 to 60 units over the 6-hr period. Marked granulocytopenia occurred within 24 hr and was sustained during the 10-day infusion period. There was marked increase in serum beta 2-microglobulin. We conclude that, in order to induce consistent serum antiviral activity, partially pure IFN-gamma, because of its rapid serum disappearance curve, must be administered by continuous i.v. infusion.

摘要

在转移性癌症患者中进行了部分纯化的免疫(γ)干扰素(IFN-γ)的药代动力学研究。9名患者通过肌肉注射途径给予IFN-γ,剂量范围为1.5×10⁵至9.6×10⁶抗病毒单位。患者血清中未检测到抗病毒活性,仅观察到轻微的副作用。15名患者通过静脉推注输注给予IFN-γ,剂量范围为1.5×10⁵至54×10⁶单位。抗病毒活性的血清清除率由单指数消失曲线描述。血清半衰期呈剂量依赖性(低剂量时为3分钟,高剂量时为34分钟)。在患者中观察到的一致生物学效应很少。基于这些药代动力学数据,8名患者接受了6小时持续输注治疗,包括静脉推注3×10⁶单位,随后以4×10⁶单位/小时的速度持续输注6小时。该方案导致在6小时内IFN-γ的血清水平持续保持在40至60单位之间。24小时内出现明显的粒细胞减少,并在10天的输注期内持续存在。血清β2-微球蛋白显著增加。我们得出结论,为了诱导一致的血清抗病毒活性,由于其血清消失曲线迅速,部分纯化的IFN-γ必须通过静脉持续输注给药。

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