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首页> 外文期刊>Pediatric transplantation. >Renal function and histology in children after small bowel transplantation.
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Renal function and histology in children after small bowel transplantation.

机译:小肠移植后儿童的肾功能和组织学。

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摘要

CKD is a frequent long-term complication after SBTx. CNIs are a well-known factor, but probably not the only cause. We assessed the incidence, risk factors, and severity of CKD in 27 children with SBTx (15 combined liver/SBTx) and prednisone/TAC-based maintenance immunosuppression. Median follow-up was seven yr (3-21). A renal biopsy was performed in 14 patients, 1-18 yr post-SBTx. A reduced GFR was observed in 17 children (63%) during the follow-up with none requiring dialysis. CNI toxicity was observed in 11/14 biopsies, as early as two yr post-transplant, and could occur with a normal mGFR. The dose of TAC was reduced by 50% in 13 patients with CKD and/or significant kidney histological lesions, and six were also given MMF. This led to a significant improvement in renal function: mGFR normalized in eight patients and improved or stabilized in five. No rejection occurred. At last follow-up, 37% had CKD stage 2 and 15% had CKD stage 3. In conclusion, CKD is frequent in children after SBTx and probably multifactorial. Less nephrotoxic immunosuppressive protocols may improve mGFR and should be further considered. The kidney histology helps in designing personalized immunosuppression strategies for patients.
机译:CKD是SBTx术后的一种频繁的长期并发症。 CNI是一个众所周知的因素,但可能不是唯一的原因。我们评估了27例SBTx(15例合并肝/ SBTx)和基于泼尼松/ TAC维持免疫抑制的儿童的CKD发生率,危险因素和严重性。中位随访时间为7年(3-21)。 SBTx后1-18年对14例患者进行了肾脏活检。随访期间,有17名儿童(63%)的GFR降低,而无需透析。早在移植后两年,就在11/14活检中观察到CNI毒性,而正常mGFR可能会发生CNI毒性。在13例患有CKD和/或明显肾脏组织学病变的患者中,TAC的剂量减少了50%,并且有6名患者接受了MMF。这导致肾功能显着改善:mGFR在8例患者中恢复正常,在5例中改善或稳定。没有拒绝发生。在最后一次随访中,有37%的儿童患有CKD 2期,有15%的儿童具有CKD 3期。总而言之,SBTx患儿的CKD很常见,可能是多因素的。肾毒性较小的免疫抑制方案可改善mGFR,应进一步考虑。肾脏组织学有助于设计针对患者的个性化免疫抑制策略。

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