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供体来源的游离DNA在肾移植中的临床应用。

Clinical use of donor-derived cell-free DNA in kidney transplantation.

作者信息

Jaikaransingh Vishal, Makadia Bhaktidevi, Khan Hafiz S, Hasan Irtiza

机构信息

Department of Medicine, Divison of Nephrology, University of Florida College of Medicine-Jacksonville, Jacksonville, FL 32209, United States.

出版信息

World J Transplant. 2024 Dec 18;14(4):97219. doi: 10.5500/wjt.v14.i4.97219.

Abstract

Traditional monitoring of kidney transplant recipients for allograft dysfunction caused by rejection involves serial checks of serum creatinine with biopsy of the renal allograft if dysfunction is suspected. This approach is labor-intensive, invasive and costly. In addition, because this approach relies on a rise in serum creatinine above historical baselines, injury to the allograft can be extensive before this rise occurs. In an effort to address this, donor-derived cell-free DNA (dd-cf DNA) is being used with increasing frequency in the clinical setting as a means of diagnosing a rejection of the renal allograft early in the course. This can potentially allow for early intervention to minimize not only injury, but the intensity of antirejection therapy needed and the avoidance of side effects. Here, we will review the available methodology for the determination and quantification of dd-cf DNA, the data supporting its use in clinical practice and the limitations of this technology.

摘要

传统上,对肾移植受者因排斥反应导致的移植物功能障碍进行监测,包括定期检测血清肌酐,若怀疑功能障碍则对肾移植物进行活检。这种方法劳动强度大、具有侵入性且成本高昂。此外,由于这种方法依赖于血清肌酐高于历史基线水平的升高,在这种升高发生之前,移植物可能已经受到广泛损伤。为了解决这个问题,供体来源的游离DNA(dd-cf DNA)在临床环境中的使用频率越来越高,作为一种在病程早期诊断肾移植物排斥反应的手段。这有可能实现早期干预,不仅将损伤降至最低,还能减少所需抗排斥治疗的强度并避免副作用。在此,我们将综述用于测定和定量dd-cf DNA的现有方法、支持其在临床实践中应用的数据以及该技术的局限性。

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Donor-Derived Cell-Free DNA and Active Rejection in Renal Allografts.供体来源的游离DNA与肾移植中的急性排斥反应
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Emerging role of cell-free DNA in kidney transplantation.游离DNA在肾移植中的新作用
World J Exp Med. 2021 Nov 20;11(5):55-65. doi: 10.5493/wjem.v11.i5.55.

本文引用的文献

2
Donor-Derived Cell Free DNA: Is It All the Same?供体细胞游离 DNA:都一样吗?
Kidney360. 2020 Jun 19;1(10):1118-1123. doi: 10.34067/KID.0003512020. eCollection 2020 Oct 29.

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