利用捐献者来源的无细胞 DNA 为肾移植受者逐步减少免疫抑制疗法提供信息:一项观察性研究

IF 1.9 Q3 TRANSPLANTATION Transplantation Direct Pub Date : 2024-03-12 eCollection Date: 2024-04-01 DOI:10.1097/TXD.0000000000001610
George Osuchukwu, Alexa Trevino, Sarah McCormick, Navchetan Kaur, Brittany Prigmore, Nour Al Haj Baddar, Michelle S Bloom, Zachary Demko, Philippe Gauthier
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引用次数: 0

摘要

背景:免疫抑制疗法(IST)是异体移植物存活的必要条件,但会造成严重的不良影响。捐献者来源的无细胞 DNA(dd-cfDNA)是肾移植(KTx)活动性排斥反应的有效非侵入性生物标志物。支持在 IST 管理中使用 dd-cfDNA 检测的证据有限:在这项单中心观察性研究中,对 21 名被认为适合减用霉酚酸 (MPA) 的 KTx 患者进行了 dd-cfDNA 检测。患者的 dd-cfDNA 结果:在 21 位参与研究的患者中,17 位被认为是 dd-cfDNA 导致排斥反应的低风险患者,并接受了减少 MPA 的治疗;4 位被认为是 dd-cfDNA 导致排斥反应的高风险患者,并维持了最初的 MPA 剂量。在 4 名被认为是 dd-cfDNA 排斥高风险的患者中,1 人出现了慢性同种异体肾病和移植物丢失,另一人接受了指示性活组织检查,结果显示没有排斥迹象。dd-cfDNA被认为是排斥反应低风险的17名患者中,没有人出现同种异体移植排斥反应。在减少MPA后的6个月内,dd-cfDNA被用于监测;没有发现任何不良结果:这项概念验证研究报告了 dd-cfDNA 的使用情况,它可直接为 IST 管理提供信息,这些 KTx 都是 IST 减少的候选者。
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Use of Donor-derived Cell-free DNA to Inform Tapering of Immunosuppression Therapy in Kidney Transplant Recipients: An Observational Study.

Background: Immunosuppression therapy (IST) is required for allograft survival but can cause significant adverse effects. Donor-derived cell-free DNA (dd-cfDNA) is a validated noninvasive biomarker for active rejection in kidney transplant (KTx). Evidence supporting dd-cfDNA testing use in IST management is limited.

Methods: In this single-center observational study, dd-cfDNA testing was performed in 21 KTx patients considered good candidates for mycophenolic acid (MPA) reduction. Patients with dd-cfDNA <1% at the first visit (enrollment) had their MPA dosage reduced; those with dd-cfDNA ≥1% had their MPA dosage maintained. Patients were monitored with dd-cfDNA for 6 additional visits.

Results: Of 21 patients enrolled in the study, 17 were considered low risk for rejection by dd-cfDNA and underwent MPA reduction; 4 patients were considered high risk for rejection by dd-cfDNA and had their initial MPA dosage maintained. Of the 4 patients considered high risk for rejection by dd-cfDNA, 1 experienced chronic allograft nephropathy and graft loss, and another received an indication biopsy that showed no evidence of rejection. Of the 17 patients considered low risk for rejection by dd-cfDNA, none experienced allograft rejection. dd-cfDNA was used for surveillance in a 6-mo period following MPA reduction; no untoward results were noted.

Conclusions: This proof-of-concept study reports the use of dd-cfDNA to directly inform IST management in a cohort of KTx who were candidates for IST reduction.

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来源期刊
Transplantation Direct
Transplantation Direct TRANSPLANTATION-
CiteScore
3.40
自引率
4.30%
发文量
193
审稿时长
8 weeks
期刊最新文献
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