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Therapeutic drug monitoring of antiretroviral agents.

机译:抗逆转录病毒药物的治疗药物监测。

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HIV+ patients fail antiretroviral therapy due to inadequate drug concentrations reaching the site of viral replication and/or the development of viral resistance to the antiretroviral agents. Adequate drug concentrations may not be reaching the virus due to poor compliance, poor absorption, or other pharmacokinetic factors such as metabolism, elimination, and drug interactions. The most important and most common pharmacokinetic drug interactions involve inhibition of metabolism, induction of metabolism, altered drug absorption, inhibition of renal excretion, and displacement from plasma protein binding sites. If a patient is failing antiretroviral therapy, TDM of antiretroviral agents could help in determining both adequacy of drug concentrations and patients' adherence. Ongoing studies will determine whether total drug concentration or free drug concentration of the protease inhibitors is the best predictor of response. Trough concentrations could prove to be the most important predictor of response, but additional studies are needed to compare trough, peak, and AUC concentrations with response to treatment. Finally, if some patients fail therapy due to inadequate drug concentrations, then increasing the dose could benefit patients' outcome and increase longevity. Clinical trials are needed that compare patients who receive a fixed-dosage regimen with patients who have adjusted dose regimens. Such a study is the best way to determine the true value of TDM of the antiretrovirals.
机译:由于药物浓度不足到达病毒复制位点和/或对抗逆转录病毒药物产生了病毒抗性,HIV +患者未能通过抗逆转录病毒治疗。由于依从性差,吸收差或其他药代动力学因素(例如代谢,消除和药物相互作用),可能无法使足够的药物浓度到达病毒。最重要和最常见的药代动力学药物相互作用包括抑制代谢,诱导代谢,改变药物吸收,抑制肾排泄以及从血浆蛋白结合位点置换。如果患者未接受抗逆转录病毒治疗,则抗逆转录病毒药物的TDM可以帮助确定药物浓度和患者依从性。正在进行的研究将确定蛋白酶抑制剂的总药物浓度还是游离药物浓度是反应的最佳预测因子。谷浓度可能被证明是最重要的反应预测因子,但是还需要进一步的研究来比较谷,峰和AUC浓度与对治疗的反应。最后,如果某些患者由于药物浓度不足而使治疗失败,那么增加剂量可以使患者受益并延长寿命。需要进行临床试验,以比较接受固定剂量方案的患者和已调整剂量方案的患者。这项研究是确定抗逆转录病毒药物TDM真正价值的最佳方法。

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