Esposito Raffaela, Giammarino Anna, De Blasio Antonietta, Martinelli Vincenzo, Cirillo Ferdinando, Scopacasa Francesco, Federico Stefano, Russo Domenico
Department of Nephrology, School of Medicine, University of Naples Federico II, Naples - Italy.
J Nephrol. 2007 Jan-Feb;20(1):57-62.
Posttransplant erythrocytosis (PTE; i.e., hematocrit [Ht] >=51%) may be responsible for cardiovascular events. Angiotensin-converting enzyme inhibitors (ACEIs) are increasingly employed in PTE treatment. Diverse ACEIs have been administered at variable doses and with erratic follow-up. In addition, guidelines recommend the administration of ACEIs as first-line therapy for PTE but do not give information on dosage. In this study the dose-response of a single ACEI was assessed, and patients were followed up for 1 year. The role of ACE gene polymorphism in both prevalence of PTE and successful response to ACEI therapy was also tested.
At study entry, blood chemistry and ACE-gene polymorphism were measured. ACEI (ramipril) was initiated at 1.25 mg/day; if Ht was still >=51%, ramipril was increased every 6 weeks to ensuing greater dosages. Scheduled dosages were 1.25, 2.5, 5.0, 7.5 and 10 mg/day. Blood chemistry was repeated every 6 weeks. Serum erythropoietin (EPO) concentration was assayed at the start and end of the study. Follow-up was extended for 1 year.
PTE developed 12.6 +/- 16.0 months after transplantation in 40 out of 400 patients; 27 patients completed the study. Initial Ht was not correlated with any variable. Final Ht appeared normalized in 26 out of 27 patients. Mean dose (+/- SD) of ramipril was 4.6 +/- 3.6 mg. Mean time for correction of PTE was 135 days, and was not dependent on baseline Ht, hemoglobin or EPO. PTE relapsed in 4 patients. Prevalence of PTE and successful response to ramipril was not dependent on ACE-gene polymorphism.
Ramipril was effective in PTE; low doses normalized Ht in most patients. No clinical characteristics or biochemical variables predicted the response to ramipril. PTE may relapse; thus long-term follow-up is mandatory.
移植后红细胞增多症(PTE,即血细胞比容[Ht]≥51%)可能是心血管事件的病因。血管紧张素转换酶抑制剂(ACEI)越来越多地用于PTE的治疗。不同的ACEI以不同剂量给药,随访情况也不稳定。此外,指南推荐将ACEI作为PTE的一线治疗药物,但未提供剂量信息。在本研究中,评估了单一ACEI的剂量反应,并对患者进行了1年的随访。还测试了ACE基因多态性在PTE患病率和对ACEI治疗的成功反应中的作用。
在研究开始时,测量血液生化指标和ACE基因多态性。ACEI(雷米普利)起始剂量为1.25毫克/天;如果Ht仍≥51%,雷米普利每6周增加剂量以达到更高剂量。预定剂量为1.25、2.5、5.0、7.5和10毫克/天。每6周重复检测血液生化指标。在研究开始和结束时测定血清促红细胞生成素(EPO)浓度。随访延长至1年。
400例患者中有40例在移植后12.6±16.0个月发生PTE;27例患者完成了研究。初始Ht与任何变量均无相关性。27例患者中有26例的最终Ht似乎恢复正常。雷米普利的平均剂量(±标准差)为4.6±3.6毫克。纠正PTE的平均时间为135天,且不依赖于基线Ht、血红蛋白或EPO。4例患者PTE复发。PTE的患病率和对雷米普利的成功反应不依赖于ACE基因多态性。
雷米普利对PTE有效;低剂量可使大多数患者的Ht恢复正常。没有临床特征或生化变量可预测对雷米普利的反应。PTE可能复发;因此必须进行长期随访。
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