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通过高效液相色谱法测定肝、心和肾移植患者的环孢素药代动力学特征。

Cyclosporine pharmacokinetic profiles in liver, heart, and kidney transplant patients as determined by high-performance liquid chromatography.

作者信息

Burckart G J, Venkataramanan R, Ptachcinski R J, Starzl T E, Griffith B P, Hakala T R, Rosenthal J T, Hardesty R L, Iwatsuki S, Brady J

出版信息

Transplant Proc. 1986 Dec;18(6 Suppl 5):129-36.

Abstract

Cs pharmacokinetic profiles using HPLC have aided in predicting necessary dosage alterations for specific groups of transplant patients. Additional information has been gained by HPLC profiles in nontransplant subjects who are healthy or have a stable disease state. The clinician now knows that liver disease not only impairs Cs elimination but may also have a pronounced effect upon drug absorption. While the cardiac failure patient may have reversible inhibition of Cs clearance, other factors may affect the distribution of the drug to lower dosage requirements. Impaired renal function is not an impediment to Cs elimination, but malabsorption similar to that observed in liver and bone marrow transplant patients may still occasionally complicate therapy. Pharmacokinetic information on Cs must be integrated into the complex care plan of a transplant patient to optimally utilize and monitor this pharmacologic agent.

摘要

使用高效液相色谱法(HPLC)得到的环孢素(Cs)药代动力学特征有助于预测特定移植患者群体所需的剂量调整。通过HPLC分析,在健康或疾病状态稳定的非移植受试者中也获得了更多信息。临床医生现在知道,肝脏疾病不仅会损害Cs的清除,还可能对药物吸收产生显著影响。虽然心力衰竭患者可能会出现Cs清除的可逆性抑制,但其他因素可能会影响药物分布,从而降低剂量需求。肾功能受损并非Cs清除的障碍,但与肝移植和骨髓移植患者中观察到的情况类似的吸收不良,仍可能偶尔使治疗复杂化。关于Cs的药代动力学信息必须纳入移植患者的综合护理计划中,以最佳地使用和监测这种药物。

相似文献

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Cyclosporine concentration determinations for monitoring and pharmacokinetic studies.
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Cyclosporine kinetics in renal transplantation.肾移植中环孢素的动力学
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本文引用的文献

4
High-performance liquid chromatographic determination of cyclosporin A in human plasma and urine.
J Chromatogr. 1980 Jun 13;182(3-4):454-8. doi: 10.1016/s0378-4347(00)81500-5.
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High pressure liquid chromatographic determination of cyclosporin A in plasma.
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High pressure liquid chromatographic determination of cyclosporin-A in human plasma.
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