肺移植后5年以上血浆供体来源无细胞DNA水平的变化:试点数据

Q4 Medicine
Deborah Jo Levine , Zachary P. Demko , David J. Ross
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引用次数: 2

摘要

慢性同种异体肺移植功能障碍(chronic lung allograft dysfunction, CLAD)是肺移植(LT)中一种非常普遍且具有破坏性的并发症,最终导致同种异体肺移植失败、发病率和死亡率增加。血浆供体来源无细胞DNA (dd-cfDNA)的测定已成为肝移植后一种有价值的无创监测工具;然而,感染和其他炎症引起的宿主cfDNA变异增加会使该方法复杂化。方法在一项回顾性的初步研究中,研究人员分析了合并合并疾病(胃食管反流、抗体介导的排斥反应或慢性感染)的肝移植后5年以上的患者中dd-cfDNA的百分比(%dd-cfDNA)和dd-cfDNA的绝对数量(cp/mL),并将其分为复杂(C-CLAD)和非复杂(U-CLAD)两组。术后中位时间为2149天(1899 - 2920)。C-CLAD (N=5)队列的dd-cfDNA中位数为1.79% (IQR: 1.04-2.29),显著高于U-CLAD队列(N=7, 0.49%;0.28 - -0.88) (p = 0.018)。绝对dd-cfDNA在C-CLAD中也显著升高(43.2 cp/mL;27.9-89.3)高于U-CLAD队列(19.6 cp/mL;8.1 - -27.9) (p = 0.048)。结论:我们报道了迄今为止未被描述的ld -cfDNA水平的分化,与异体移植物数量的增加有关,而不是与宿主血浆cfDNA的改变有关。此外,dd-cfDNA分析与C-CLAD共病条件的关联可能为潜在的治疗和减轻分子损伤提供见解。dd-cfDNA纵向绝对数量的测量可能为未来病理生物学的临床研究设计和治疗算法提供额外的价值。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Variability in plasma donor-derived cell-free DNA levels with CLAD more than 5-years after Lung Transplantation: Pilot data

Background

Chronic lung allograft dysfunction (CLAD) is a highly prevalent and devastating complication in lung transplant (LT), culminating in increased allograft failure, morbidity, and mortality. Determination of the fraction of plasma donor-derived cell-free DNA (dd-cfDNA) has emerged as a valuable noninvasive monitoring tool after LT; however, the increased variance of host cfDNA caused by infection and other inflammation can complicate the approach.

Methods

In a retrospective pilot study, we analyzed both the fraction of dd-cfDNA (%dd-cfDNA) and absolute quantity of dd-cfDNA (cp/mL) in recipients with CLAD ≥ 5-year post-LT with co-morbid conditions (gastro-esophageal reflux, antibody-mediated rejection, or chronic infection) designated as complicated (C-CLAD) and uncomplicated (U-CLAD) cohorts.

Results

Median time post-LT was 2,149 days (1,899-2,920). The median %dd-cfDNA for the C-CLAD (N=5) cohort was 1.79% (IQR: 1.04-2.29) and significantly elevated compared to the U-CLAD cohort (N=7, 0.49%; 0.28-0.88) (p=0.018). Absolute dd-cfDNA was also significantly higher in C-CLAD (43.2 cp/mL; 27.9-89.3) than the in U-CLAD cohort (19.6 cp/mL; 8.1-27.9) (p=0.048).

Conclusions

We report a heretofore undescribed dichotomy of dd-cfDNA levels with CLAD ≥ 5-years, related specifically to elevation in allograft quantity as opposed to alteration in host plasma cfDNA. Further, dd-cfDNA analysis in association with co-morbid conditions in C-CLAD may offer insights for potential treatment and alleviation of molecular injury. Measurement of longitudinal absolute quantity dd-cfDNA may provide additional value for future clinical study design of pathobiology and CLAD treatment algorithms.

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来源期刊
Transplantation Reports
Transplantation Reports Medicine-Transplantation
CiteScore
0.60
自引率
0.00%
发文量
24
审稿时长
101 days
期刊介绍: To provide to national and regional audiences experiences unique to them or confirming of broader concepts originating in large controlled trials. All aspects of organ, tissue and cell transplantation clinically and experimentally. Transplantation Reports will provide in-depth representation of emerging preclinical, impactful and clinical experiences. -Original basic or clinical science articles that represent initial limited experiences as preliminary reports. -Clinical trials of therapies previously well documented in large trials but now tested in limited, special, ethnic or clinically unique patient populations. -Case studies that confirm prior reports but have occurred in patients displaying unique clinical characteristics such as ethnicities or rarely associated co-morbidities. Transplantation Reports offers these benefits: -Fast and fair peer review -Rapid, article-based publication -Unrivalled visibility and exposure for your research -Immediate, free and permanent access to your paper on Science Direct -Immediately citable using the article DOI
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