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小儿心肺移植

Pediatric heart and lung transplantation.

作者信息

Reddy Subash C, Webber Steven A

机构信息

Pediatric Heart and Heart-Lung Transplantation Program, Division of Cardiology, Children's Hospital of Pittsburgh, Pittsburgh, PA 15213, USA.

出版信息

Indian J Pediatr. 2003 Sep;70(9):723-9. doi: 10.1007/BF02724315.

Abstract

During the last two decades, several advances have resulted in marked improvement in medium-term survival with excellent quality of life in pediatric heart transplant recipients. These were possible due to better donor and recipient selection, increased surgical experience in transplantation for complex congenital heart disease, development of effective rejection surveillance, and wider choice of immunosuppressive medications. Despite all of these advances, recipients suffer from the adverse effects of non-specific immunosuppression including infections, post-transplant lymphoproliferative disorders and other malignancies, renal dysfunction and other important end-organ toxicities. Furthermore, newer immunosuppressive regimens appear (so far) to have had relatively little impact on the incidence of allograft coronary vasculopathy (chronic rejection). Progress in our understanding of the immunologic mechanisms of rejection and graft acceptance should lead to more targeted immunosuppressive therapy and avoidance of non-specific immunosuppression. The ultimate goal is to induce a state of tolerance, wherein the recipient will accept the allograft indefinitely without the need for long-term immunosuppression and yet remain immunocompetent to other antigens. This quest is currently being realized in many animal models of solid organ transplantation and offers great hope for the future.

摘要

在过去二十年中,多项进展使小儿心脏移植受者的中期生存率显著提高,生活质量良好。这些进展得益于更好的供体和受体选择、复杂先天性心脏病移植手术经验的增加、有效的排斥反应监测的发展以及免疫抑制药物选择范围的扩大。尽管取得了所有这些进展,但受者仍遭受非特异性免疫抑制的不良反应,包括感染、移植后淋巴细胞增生性疾病和其他恶性肿瘤、肾功能不全以及其他重要的终末器官毒性。此外,(迄今为止)新的免疫抑制方案对移植心脏冠状动脉病变(慢性排斥反应)的发生率影响相对较小。我们对排斥反应和移植物接受的免疫机制的理解取得进展,应能带来更具针对性的免疫抑制治疗,并避免非特异性免疫抑制。最终目标是诱导一种耐受状态,即受者无需长期免疫抑制就能无限期接受移植物,同时对其他抗原仍保持免疫活性。目前,这一探索在许多实体器官移植动物模型中正在实现,并为未来带来了巨大希望。

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