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首页> 外文期刊>American journal of cardiovascular drugs: drugs, devices, and other interventions >Calcineurin inhibitor-associated early renal insufficiency in cardiac transplant recipients: risk factors and strategies for prevention and treatment.
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Calcineurin inhibitor-associated early renal insufficiency in cardiac transplant recipients: risk factors and strategies for prevention and treatment.

机译:钙调神经磷酸酶抑制剂相关的心脏移植受者早期肾功能不全:危险因素和预防和治疗策略。

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Cardiac transplantation is the definitive treatment for eligible patients with end-stage cardiac failure. Techniques have evolved to reduce surgical mortality to under 5%. Immediate and subsequent long-term survival is more dependent on acute and chronic rejection and the complications of immunosuppressive therapy. Ten-year survival is greater than 50%.The success of transplantation over the last 20 years has been largely due to the advances in immunosuppression. The most notable and dramatic milestone was the introduction of cyclosporine in the early 1980s, which resulted in a significant improvement in allograft and patient survival. Cyclosporine is a peptide that inhibits the immune system by suppressing T-helper cell activation via inhibition of calcineurin, a critical intracellular enzyme. Tacrolimus has a similar (but not identical) mechanism of action, and was introduced in the 1990s. Drugs such as cyclosporine and tacrolimus, generically referred to as calcineurin inhibitors, have become the cornerstones of immunosuppressive protocols.As a group, calcineurin inhibitors have adverse effects, including neurotoxicity, hypertension, and nephrotoxicity, which complicate their use. Early renal insufficiency manifests as postoperative oliguria (<50 mL/h urine output) or rising serum creatinine levels. There are a variety of postulated causes for calcineurin inhibitor-associated early renal insufficiency including direct calcineurin inhibitor-mediated renal arteriolar vasoconstriction, increased levels of endothelin-1 (a potent vasoconstrictor), as well as decreased nitric oxide production and alterations in the kidney's ability to adjust to changes in serum tonicity.Once early renal insufficiency occurs, no single treatment has been shown to be effective. Approaches discussed in this paper include reduction in calcineurin inhibitor dosages, as well as various drugs to promote increased renal perfusion such as misoprostol and dopamine. In addition, the paper emphasizes the importance of ruling out other causes of renal insufficiency in the early postoperative period, including volume depletion, depressed cardiac output, and mechanical obstruction to urine flow.Given that there is no highly efficacious treatment for this syndrome, ways to avoid its occurrence are desirable. One paper is referenced that suggests that avoidance of rapid changes in tacrolimus level during the first three days of therapy is associated with a low occurrence of early renal insufficiency.
机译:心脏移植是针对合格的终末期心力衰竭患者的最终治疗方法。技术已经发展到可以将手术死亡率降低到5%以下。立即和随后的长期生存更多地取决于急性和慢性排斥反应以及免疫抑制疗法的并发症。十年生存率超过50%。过去20年中移植的成功很大程度上归功于免疫抑制的发展。最显着,最引人注目的里程碑是在1980年代初引入了环孢菌素,这导致了同种异体移植和患者存活率的显着提高。环孢菌素是一种通过抑制钙调磷酸酶(一种重要的细胞内酶)抑制T辅助细胞活化来抑制免疫系统的一种肽。他克莫司具有相似(但不完全相同)的作用机理,并于1990年代引入。环孢素和他克莫司等药物通常被称为钙调神经磷酸酶抑制剂,已成为免疫抑制方案的基石。钙调神经磷酸酶抑制剂作为一个整体具有不利影响,包括神经毒性,高血压和肾毒性,使它们的使用复杂化。早期肾功能不全表现为术后少尿(<50 mL / h尿量)或血清肌酐水平升高。与钙调神经磷酸酶抑制剂相关的早期肾功能不全有多种推测的原因,包括直接的钙调神经磷酸酶抑制剂介导的肾小动脉血管收缩,内皮素-1(有效血管收缩剂)水平升高,一氧化氮生成减少和肾脏能力改变一旦发生早期肾功能不全,就没有单一疗法被证明是有效的。本文讨论的方法包括降低钙调神经磷酸酶抑制剂的剂量,以及各种促进肾灌注增加的药物,如米索前列醇和多巴胺。此外,本文强调必须排除术后早期肾功能不全的其他原因,包括容量减少,心输出量降低和尿流机械性阻塞。鉴于此综合征尚无有效的治疗方法,避免其发生是可取的。有一篇论文被引用,表明在治疗的前三天内避免他克莫司水平的快速变化与早期肾功能不全的发生率低有关。

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