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100例肝移植后原发性胆汁性肝硬化复发患者的长期随访

Long-term follow-up after recurrence of primary biliary cirrhosis after liver transplantation in 100 patients.

作者信息

Jacob Dietmar A, Neumann Ulf P, Bahra Marcus, Klupp Jochen, Puhl Gero, Neuhaus Ruth, Langrehr Jan M

机构信息

Department of General, Visceral and Transplantation Surgery, Humboldt University of Berlin, Charité Virchow Clinic, Berlin, Germany.

出版信息

Clin Transplant. 2006 Mar-Apr;20(2):211-20. doi: 10.1111/j.1399-0012.2005.00471.x.

Abstract

Orthotopic liver transplantation (OLT) is the only effective curative therapy for end-stage primary biliary cirrhosis (PBC). Survival after OLT is excellent, although recent data have shown a recurrence rate of PBC of up to 32% after transplantation. The aim of this study is to investigate the course after disease recurrence, particularly with regard to liver function and survival in a long-term follow-up. Between April 1989 and April 2003, 1,553 liver transplantations were performed in 1,415 patients at the Charité, Virchow Clinic. Protocol liver biopsies were taken after one, three, five, seven, 10 and 13 yr. One hundred (7%) patients suffered from histologically proven PBC. Primary immunosuppression consisted of cyclosporine (n = 54) or tacrolimus (Tac) (n = 46). Immediately after OLT, all patients received ursodeoxycholic acid. Corticosteroids were withdrawn three to six months after OLT. The median age of the 85 women and 15 men was 55 yr (range 25-66 yr). The median follow-up after liver transplantation was 118 months (range 16-187 months) and after recurrence 30 months (range 4-79 months). Actuarial patient survival after five, 10 and 15 yr was 87, 84 and 82% respectively. Ten patients (10%) died after a median survival time of 32 months. Two of these patients developed organ dysfunction owing to recurrence of PBC. Histological recurrence was found in 14 patients (14%) after a median time of 61 months (range 36-122 months). Patients with Tac immunosuppression developed PBC recurrence more often (p < 0.05) and also earlier (p < 0.05). Fifty-seven patients developed an acute rejection and two patients a chronic rejection episode. Liver function did not alter within the first five yr after histologically proven PBC recurrence. Multivariate analysis of the investigated patients showed that the recipient's age and Tac immunosuppression were significant risk factors for PBC recurrence. Long-term follow-up of up to 15 yr after liver transplantation, owing to PBC, in addition to maintenance of liver function, shows excellent organ and patient survival rates. Although protocol liver biopsies revealed histological recurrence in 14 (14%) patients, only two patients developed graft dysfunction. Tac-treated patients showed more frequently and also earlier histologically proven PBC recurrence; however, in our population we could not observe an impact on graft dysfunction and patient's survival.

摘要

原位肝移植(OLT)是终末期原发性胆汁性肝硬化(PBC)唯一有效的治愈性疗法。OLT后的生存率很高,尽管最近的数据显示移植后PBC的复发率高达32%。本研究的目的是调查疾病复发后的病程,特别是在长期随访中肝功能和生存率方面。1989年4月至2003年4月期间,在夏里特维肖诊所对1415例患者进行了1553例肝移植。在1年、3年、5年、7年、10年和13年后进行了常规肝脏活检。100例(7%)患者经组织学证实患有PBC。初始免疫抑制包括环孢素(n = 54)或他克莫司(Tac)(n = 46)。OLT后,所有患者立即接受熊去氧胆酸治疗。OLT后3至6个月停用皮质类固醇。85名女性和15名男性的中位年龄为55岁(范围25 - 66岁)。肝移植后的中位随访时间为118个月(范围16 - 187个月),复发后的中位随访时间为30个月(范围4 - 79个月)。5年、10年和15年的患者精算生存率分别为87%、84%和82%。10例患者(10%)在中位生存时间32个月后死亡。其中2例患者因PBC复发出现器官功能障碍。14例患者(14%)在中位时间61个月(范围36 - 122个月)后出现组织学复发。接受Tac免疫抑制的患者PBC复发更频繁(p < 0.05)且更早(p < 0.05)。57例患者发生急性排斥反应,2例患者发生慢性排斥反应。在组织学证实PBC复发后的前5年,肝功能没有改变。对研究患者的多因素分析表明,受者年龄和Tac免疫抑制是PBC复发的重要危险因素。因PBC进行肝移植后长达15年的长期随访显示,除了维持肝功能外,器官和患者的生存率很高。尽管常规肝脏活检显示14例(14%)患者有组织学复发,但只有2例患者出现移植功能障碍。接受Tac治疗的患者组织学证实的PBC复发更频繁且更早;然而,在我们的研究人群中,我们未观察到对移植功能障碍和患者生存的影响。

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