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实体器官移植中的痛风:一个具有挑战性的临床问题。

Gout in solid organ transplantation: a challenging clinical problem.

作者信息

Stamp Lisa, Searle Martin, O'Donnell John, Chapman Peter

机构信息

Department of Medicine, Christchurch School of Medicine and Health Sciences, University of Otago, Christchurch, New Zealand.

出版信息

Drugs. 2005;65(18):2593-611. doi: 10.2165/00003495-200565180-00004.

Abstract

Hyperuricaemia occurs in 5-84% and gout in 1.7-28% of recipients of solid organ transplants. Gout may be severe and crippling, and may hinder the improved quality of life gained through organ transplantation. Risk factors for gout in the general population include hyperuricaemia, obesity, weight gain, hypertension and diuretic use. In transplant recipients, therapy with ciclosporin (cyclosporin) is an additional risk factor. Hyperuricaemia is recognised as an independent risk factor for cardiovascular disease; however, whether anti-hyperuricaemic therapy reduces cardiovascular events remains to be determined. Dietary advice is important in the management of gout and patients should be educated to partake in a low-calorie diet with moderate carbohydrate restriction and increased proportional intake of protein and unsaturated fat. While gout is curable, its pharmacological management in transplant recipients is complicated by the risk of adverse effects and potentially severe interactions between immunosuppressive and hypouricaemic drugs. NSAIDs, colchicine and corticosteroids may be used to treat acute gouty attacks. NSAIDs have effects on renal haemodynamics, and must be used with caution and with close monitoring of renal function. Colchicine myotoxicty is of particular concern in transplant recipients with renal impairment or when used in combination with ciclosporin. Long-term urate-lowering therapy is required to promote dissolution of uric acid crystals, thereby preventing recurrent attacks of gout. Allopurinol should be used with caution because of its interaction with azathioprine, which results in bone marrow suppression. Substitution of mycophenylate mofetil for azathioprine avoids this interaction. Uricosuric agents, such as probenecid, are ineffective in patients with renal impairment. The exception is benzbromarone, which is effective in those with a creatinine clearance >25 mL/min. Benzbromarone is indicated in allopurinol-intolerant patients with renal failure, solid organ transplant or tophaceous/polyarticular gout. Monitoring for hepatotoxicty is essential for patients taking benzbromarone. Physicians should carefully consider therapeutic options for the management of hypertension and hyperlipidaemia, which are common in transplant recipients. While loop and thiazide diuretics increase serum urate, amlodipine and losartan have the same antihypertensive effect with the additional benefit of lowering serum urate. Atorvastatin, but not simvastatin, may lower uric acid, and while fenofibrate may reduce serum urate it has been associated with a decline in renal function. Gout in solid organ transplantation is an increasing and challenging clinical problem; it impacts adversely on patients' quality of life. Recognition and, if possible, alleviation of risk factors, prompt treatment of acute attacks and early introduction of hypouricaemic therapy with careful monitoring are the keys to successful management.

摘要

实体器官移植受者中高尿酸血症的发生率为5%-84%,痛风的发生率为1.7%-28%。痛风可能很严重且会导致残疾,可能会阻碍通过器官移植获得的生活质量改善。普通人群中痛风的危险因素包括高尿酸血症、肥胖、体重增加、高血压和使用利尿剂。在移植受者中,环孢素治疗是另一个危险因素。高尿酸血症被认为是心血管疾病的独立危险因素;然而,抗高尿酸血症治疗是否能减少心血管事件仍有待确定。饮食建议对痛风的管理很重要,应教育患者采用低热量饮食,适度限制碳水化合物摄入,增加蛋白质和不饱和脂肪的比例摄入量。虽然痛风是可治愈的,但其在移植受者中的药物管理因不良反应风险以及免疫抑制药物和降尿酸药物之间潜在的严重相互作用而变得复杂。非甾体抗炎药、秋水仙碱和皮质类固醇可用于治疗急性痛风发作。非甾体抗炎药对肾血流动力学有影响,必须谨慎使用并密切监测肾功能。秋水仙碱的肌毒性在肾功能受损的移植受者中或与环孢素联合使用时尤其值得关注。需要长期降尿酸治疗以促进尿酸结晶溶解,从而预防痛风复发。由于别嘌醇与硫唑嘌呤相互作用会导致骨髓抑制,应谨慎使用。用霉酚酸酯替代硫唑嘌呤可避免这种相互作用。促尿酸排泄药,如丙磺舒,对肾功能受损的患者无效。例外的是苯溴马隆,它对肌酐清除率>25 mL/min的患者有效。苯溴马隆适用于不耐受别嘌醇的肾衰竭、实体器官移植或有痛风石/多关节痛风的患者。服用苯溴马隆的患者必须监测肝毒性。医生应仔细考虑移植受者中常见的高血压和高脂血症的治疗选择。虽然袢利尿剂和噻嗪类利尿剂会升高血清尿酸,但氨氯地平和氯沙坦具有相同的降压作用,还有降低血清尿酸的额外益处。阿托伐他汀可降低尿酸,但辛伐他汀不行,非诺贝特虽然可能降低血清尿酸,但与肾功能下降有关。实体器官移植中的痛风是一个日益严重且具有挑战性的临床问题;它对患者的生活质量有不利影响。识别并尽可能减轻危险因素、及时治疗急性发作以及在仔细监测下尽早开始降尿酸治疗是成功管理的关键。

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