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肝移植排斥反应的诊断、预防及管理进展

Advances in diagnosis, prevention, and management of hepatic allograft rejection.

作者信息

Wiesner R H

机构信息

Liver Transplantation Unit, Mayo Clinic, Rochester, MN 55905.

出版信息

Clin Chem. 1994 Nov;40(11 Pt 2):2174-85.

PMID:7955405
Abstract

Despite recent improvements in immunosuppressive therapy, hepatic allograft rejection remains a major cause of morbidity and late graft loss in patients undergoing liver transplantation. Although some biochemical tests suggest hepatic allograft damage, the gold standard for defining rejection remains based on morphologic findings. Acute cellular rejection usually occurs within the first 3 weeks posttransplantation and the incidence varies between 40% and 70%. Ductopenic rejection occurs in 5-10% of patients undergoing initial liver transplantation and usually occurs between 6 weeks and 6 months after the procedure. Induction and maintenance of immunosuppression with triple-drug therapy (cyclosporine, prednisone, and azathioprine) and other combinations that include anti-lymphocyte preparations have led to an overall decrease in the incidence of both cellular and ductopenic rejection. In addition, the availability of FK506 as a rescue therapy has saved grafts in some patients experiencing chronic (ductopenic) rejection. Overall, the correlation between the degree of biochemical liver dysfunction and the presence and severity of histologic rejection remains poor. Histologic severity of rejection, however, suggests which patients will require more immunosuppressive therapy and which patients may need antilymphocyte therapy to control the rejection episode. Some rejection episodes remain resistant to all known therapy and eventually lead to graft loss. New immunosuppressive agents and regimens are needed to improve graft and patient survival, decrease the incidence of cellular and ductopenic rejection, minimize drug-related side effects and complications, and reduce the high cost of immunosuppressive therapy.

摘要

尽管免疫抑制治疗近来有所改进,但肝移植受者的肝移植排斥反应仍然是发病和晚期移植物丢失的主要原因。虽然一些生化检查提示肝移植物受损,但定义排斥反应的金标准仍基于形态学表现。急性细胞性排斥反应通常发生在移植后的头3周内,发生率在40%至70%之间。胆管减少性排斥反应发生在5%至10%的初次肝移植受者中,通常在手术后6周和6个月之间出现。采用三联药物疗法(环孢素、泼尼松和硫唑嘌呤)以及包括抗淋巴细胞制剂在内的其他联合方案进行免疫抑制诱导和维持治疗,已使细胞性和胆管减少性排斥反应的发生率总体下降。此外,FK506作为挽救治疗药物的应用,已使一些发生慢性(胆管减少性)排斥反应的患者的移植物得以挽救。总体而言,肝脏生化功能障碍的程度与组织学排斥反应的存在及严重程度之间的相关性仍然较差。然而,排斥反应的组织学严重程度提示哪些患者需要更强的免疫抑制治疗,哪些患者可能需要抗淋巴细胞治疗来控制排斥反应发作。一些排斥反应发作对所有已知治疗均耐药,最终导致移植物丢失。需要新的免疫抑制药物和方案来提高移植物和患者的存活率,降低细胞性和胆管减少性排斥反应的发生率,将药物相关的副作用和并发症降至最低,并降低免疫抑制治疗的高昂费用。

相似文献

1
Advances in diagnosis, prevention, and management of hepatic allograft rejection.肝移植排斥反应的诊断、预防及管理进展
Clin Chem. 1994 Nov;40(11 Pt 2):2174-85.
2
Hepatic allograft rejection: new developments in terminology, diagnosis, prevention, and treatment.肝移植排斥反应:术语、诊断、预防及治疗方面的新进展
Mayo Clin Proc. 1993 Jan;68(1):69-79. doi: 10.1016/s0025-6196(12)60022-6.
3
A multicenter analysis of the first experience with FK506 for induction and rescue therapy after pancreas transplantation.FK506用于胰腺移植后诱导和挽救治疗的首次经验的多中心分析。
Transplantation. 1996 Jan 27;61(2):261-73. doi: 10.1097/00007890-199601270-00018.
4
FK 506 therapy for refractory renal allograft rejection: lessons from liver transplantation.FK506治疗难治性肾移植排斥反应:来自肝移植的经验教训。
Clin Transplant. 1996 Aug;10(4):323-32.
5
Clinical aspects of sensitization.致敏作用的临床方面。
Clin Transpl. 1997:285-96.
6
Determinants of late allograft nephrectomy.移植肾晚期切除的决定因素。
Clin Nephrol. 1995 Nov;44(5):284-9.
7
Steroid withdrawal from long-term immunosuppression in liver allograft recipients.
Transplantation. 1993 Apr;55(4):789-94. doi: 10.1097/00007890-199304000-00020.
8
Late acute liver allograft rejection; a study of its natural history and graft survival in the current era.晚期急性肝移植排斥反应;当前时代其自然史和移植物存活的研究。
Transplantation. 2013 Apr 15;95(7):955-9. doi: 10.1097/TP.0b013e3182845f6c.
9
[Diagnosis of rejection in a transplanted liver].[移植肝排斥反应的诊断]
Cesk Patol. 2015;51(4):166-8.
10
Induction immunosuppressive therapy is associated with a low rejection rate after liver transplantation.诱导免疫抑制治疗与肝移植后低排斥率相关。
Clin Transplant. 1997 Aug;11(4):328-33.

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Am J Transl Res. 2024 Apr 15;16(4):1353-1365. doi: 10.62347/GHKH4280. eCollection 2024.
2
Variations in Practice to Therapeutic Monitoring of Tacrolimus following Primary Adult Liver Transplantation.成人原发性肝移植后他克莫司治疗监测的实践差异
Int J Organ Transplant Med. 2016;7(1):1-8. Epub 2016 Feb 1.