治疗药物监测可避免99mtc -二膦酸亚甲基(MDP)-庆大霉素相互作用引起的医源性改变。

W L Chen, M Y Perng, D Z Hwei, M D Yu
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引用次数: 0

摘要

庆大霉素是一种氨基糖苷类抗生素,用于治疗革兰氏阴性菌引起的各种感染,但它对肾脏有潜在毒性。由于其肾毒性,庆大霉素可引起99mTc-MDP骨显像上肾脏摄取异常。肾脏中放射性药物的存在,以及肾脏潴留的增加,往往会产生星图结果,错误地识别与肾血管或尿路阻塞等疾病相关的特征,甚至肾癌。生物分布的改变可能提供误导性信息,掩盖或模仿某些疾病症状。需要一种方法,使庆大霉素的治疗效益最大化,同时使肾毒性和显像上出现热肾的风险最小化。连续药代动力学给药是实现这一目标的一种方法。对22例患者进行庆大霉素治疗药物监测(TDM)和99mTc-MDP作为放射性药物的骨显像。本文提供的数据表明,通过连续给药庆大霉素,可以避免庆大霉素治疗引起的医源性改变。
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Therapeutic drug monitoring can avoid iatrogenic alterations caused by 99mTc-methylene diphosphonate (MDP)-gentamicin interaction.

Gentamicin is an aminoglycoside antibiotic used to treat a wide variety of infections caused by gram-negative organisms, but it is potentially toxic to the kidneys. Due to its nephrotoxicity, gentamicin may cause abnormal renal uptake to be seen on 99mTc-MDP bone scintigraphy. The presence of the radiopharmaceutical in the kidneys, along with an increase in renal retention, tend to produce scintigraphic results that falsely identify characteristics related to diseases such as renal vascular, or urinary tract obstruction, and even renal cancer. An altered biodistribution may provide misleading information that can either mask or mimic certain disease symptoms. A method to maximize the therapeutic benefit of gentamicin while minimizing the risk of nephrotoxicity and the appearance of a hot kidney on scintigraphy is desirable. Serial pharmacokinetic dosing has been proposed as a method to accomplish this goal. Therapeutic drug monitoring (TDM) of gentamicin therapy, and bone scintigraphy employing 99mTc-MDP as the radiopharmaceutical was carried out in 22 patients. The data presented here demonstrate that with serial pharmacokinetic dosing of gentamicin, the iatrogenic alteration caused by gentamicin therapy can be avoided.

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