Role of the Pharmacist in Managing Antidepressant Drug Interactions in the Solid Organ Transplant Population

Suzanne C Harris, C. Hyatt
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Abstract

In transplant patients, Major Depressive Disorder (MDD) is the most prevalent psychiatric disorder and is associated with reduced quality of life, with prevalence rates of MDD in up to 25% of solid organ transplant (SOT) patients [1]. MDD can lead to medication nonadherence, which can cause rejection of the transplant organ. Additionally, antidepressant medications have a range of unique side effects and potential for pharmacokinetic and pharmacodynamic interactions. Many of the transplant medications are metabolized by cytochrome P450 3A4 enzymes, putting them at risk for pharmacokinetic drug interactions. In addition, these medications can have pharmacodynamic interactions with antidepressants. Corticosteroids can cause weight gain, leading to diabetes and obesity. Cyclosporine causes hypertension in 50% of kidney transplant patients. Tacrolimus and cyclosporine have been reported to have central nervous toxicity in one-third of patients. Corticosteroids, sirolimus, and cyclosporine have been associated with hyperlipidemia [2]. Hence, these interactions with antidepressants can result in altered concentrations of immunosuppressants or additive untoward side effects (Table 1).
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在实体器官移植人群中,药剂师在抗抑郁药物相互作用管理中的作用
在移植患者中,重度抑郁症(MDD)是最常见的精神障碍,与生活质量下降有关,在实体器官移植(SOT)患者中,重度抑郁症的患病率高达25%[1]。重度抑郁症会导致药物不依从,从而引起移植器官的排斥反应。此外,抗抑郁药物有一系列独特的副作用和潜在的药代动力学和药效学相互作用。许多移植药物是由细胞色素P450 3A4酶代谢的,这使它们面临药代动力学药物相互作用的风险。此外,这些药物可能与抗抑郁药有药效学上的相互作用。皮质类固醇会导致体重增加,导致糖尿病和肥胖。环孢素导致50%的肾移植患者高血压。据报道,他克莫司和环孢素对三分之一的患者有中枢神经毒性。皮质类固醇、西罗莫司和环孢素与高脂血症有关[2]。因此,这些与抗抑郁药的相互作用可能导致免疫抑制剂浓度的改变或副作用的增加(表1)。
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