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采用新的诱导耐受方案并联合低剂量免疫抑制进行肠道移植后完全无排斥反应。

Complete freedom from rejection after intestinal transplantation using a new tolerogenic protocol combined with low immunosuppression.

作者信息

Pirenne Jacques, Koshiba Takaaki, Geboes Karel, Emonds Marie Paule, Ferdinande Patrick, Hiele Martin, Nevens Frederik, Waer Mark

机构信息

Catholic University Hospitals Leuven, Herestraat 49, B-3000 Leuven, Belgium. Jacques.Pirenne@ uz.kuleuven.ac.be.

出版信息

Transplantation. 2002 Mar 27;73(6):966-8. doi: 10.1097/00007890-200203270-00024.

Abstract

BACKGROUND

Intestinal transplantation (Itx) remains the most difficult form of transplantation. This is due to the high immunogenicity of the bowel that currently obligates Itx patients to heavy immunosuppression, which causes infection, posttransplant lymphoproliferative disease (PTLD), and drug toxicity. Wider application of Itx depends on the development of tolerogenic strategies to promote engraftment while reducing the need for immunosuppression. We applied a strategy to clinical Itx that combines intraportal donor-specific blood transfusion with a deliberately low immunosuppression protocol (no high-dose steroids; lower tacrolimus level).

METHODS

A 55-year-old patient received a combined liver/Itx. Donor-specific whole blood was taken from the donor during procurement and transfused in the recipient portal vein after graft reperfusion. For induction immunosuppression, no intravenous bolus of steroids was given; only two doses of anti-interleukin 2 receptor antibody were administered. The patient received posttransplantation maintenance immunosuppression with lower tacrolimus levels than average (15 ng/ml first month; 5-10 ng/ml thereafter), low-dose azathioprine (1 mg/kg first to third months; 0.5 mg/kg thereafter), and low-dose steroids (Medrol 8 mg twice daily first and second months; 4 mg twice thereafter). The patient was monitored for rejection, graft-versus-host disease, infection, and PTLD. Protocol biopsy specimens were taken from the distal ileum (2 per week).

RESULTS

Clinical, endoscopic, and histologic signs of rejection did not develop. Chimerism was identified at day 28. Graft-versus-host disease was absent clinically. Chimerism was self-limiting and disappeared without modifying baseline immunosuppression and without observing a change in graft function. The patient remained free of systemic opportunistic infections, PTLD, and drug toxicity. Total parenteral nutrition was stopped at 7 weeks after transplantation. The patient remains free of total parenteral nutrition and free of rejection at 14 months after transplantation.

CONCLUSIONS

We describe an Itx patient who remained rejection free despite receiving significantly lower immunosuppression than average. We hypothesize that intraoperative immunomodulation via intraportal donor-specific blood transfusion in the absence of nonspecific overimmunosuppression promoted Itx acceptance.

摘要

背景

肠道移植(Itx)仍然是最难的移植形式。这是由于肠道具有高免疫原性,目前这使得Itx患者必须接受强效免疫抑制,从而导致感染、移植后淋巴细胞增生性疾病(PTLD)和药物毒性。Itx的更广泛应用取决于开发诱导免疫耐受的策略,以促进植入,同时减少对免疫抑制的需求。我们将一种门静脉内输注供体特异性血液与刻意采用低免疫抑制方案(不使用高剂量类固醇;较低的他克莫司水平)相结合的策略应用于临床肠道移植。

方法

一名55岁患者接受了肝脏/肠道联合移植。在获取供体器官期间采集供体特异性全血,并在移植器官再灌注后输注到受体门静脉。诱导免疫抑制时,未给予静脉推注类固醇;仅给予两剂抗白细胞介素2受体抗体。该患者接受的移植后维持免疫抑制中,他克莫司水平低于平均水平(第一个月为15 ng/ml;此后为5 - 10 ng/ml),低剂量硫唑嘌呤(第一个月至第三个月为1 mg/kg;此后为0.5 mg/kg),以及低剂量类固醇(第一个月和第二个月为美卓乐8 mg,每日两次;此后为4 mg,每日两次)。对患者进行排斥反应、移植物抗宿主病、感染和PTLD的监测。定期从回肠末端取活检标本(每周2次)。

结果

未出现排斥反应的临床、内镜和组织学征象。在第28天检测到嵌合体。临床上未出现移植物抗宿主病。嵌合体具有自限性,在未改变基线免疫抑制且未观察到移植器官功能变化的情况下消失。患者未发生全身性机会性感染、PTLD和药物毒性。移植后7周停止了全胃肠外营养。移植后14个月,患者无需全胃肠外营养且未发生排斥反应。

结论

我们描述了一名肠道移植患者,尽管其接受的免疫抑制明显低于平均水平,但仍未发生排斥反应。我们推测,在不存在非特异性过度免疫抑制的情况下,通过门静脉内输注供体特异性血液进行术中免疫调节促进了肠道移植的接受。

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