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亚临床边缘性炎症对肾移植结局的影响。

Impact of Subclinical Borderline Inflammation on Kidney Transplant Outcomes.

作者信息

Seifert Michael E, Agarwal Gaurav, Bernard Miriam, Kasik Ellen, Raza S Sikandar, Fatima Huma, Gaston Robert S, Hauptfeld-Dolejsek Vera, Julian Bruce A, Kew Clifton E, Kumar Vineeta, Mehta Shikha, Ong Song, Rosenblum Frida, Towns Graham, Mannon Roslyn B

机构信息

Department of Pediatrics, University of Alabama School of Medicine, Birmingham, AL.

Department of Medicine, University of Alabama School of Medicine, Birmingham, AL.

出版信息

Transplant Direct. 2021 Jan 26;7(2):e663. doi: 10.1097/TXD.0000000000001119. eCollection 2021 Feb.

Abstract

BACKGROUND

Surveillance biopsies permit early detection of subclinical inflammation before clinical dysfunction, but the impact of detecting early subclinical phenotypes remains unclear.

METHODS

We conducted a single-center retrospective cohort study of 441 consecutive kidney transplant recipients between 2015 and 2018 with surveillance biopsies at 6 months post-transplant. We tested the hypothesis that early subclinical inflammation (subclinical borderline changes, T cell-mediated rejection, or microvascular injury) is associated with increased incidence of a composite endpoint including acute rejection and allograft failure.

RESULTS

Using contemporaneous Banff criteria, we detected subclinical inflammation in 31%, with the majority (75%) having a subclinical borderline phenotype (at least minimal inflammation with mild tubulitis [>i0t1]). Overall, subclinical inflammation was independently associated with the composite endpoint (adjusted hazard ratio, 2.88; 1.11-7.51;  = 0.03). The subgroup with subclinical borderline inflammation, predominantly those meeting the Banff 2019 i1t1 threshold, was independently associated with 5-fold increased hazard for the composite endpoint ( = 0.02). Those with concurrent subclinical inflammation and subclinical chronic allograft injury had worse outcomes. The effect of treating subclinical inflammation was difficult to ascertain in small heterogeneous subgroups.

CONCLUSIONS

Subclinical acute and chronic inflammation are common at 6 months post-transplant in kidney recipients with stable allograft function. The subclinical borderline phenotype with both tubulitis and interstitial inflammation was independently associated with poor long-term outcomes. Further studies are needed to elucidate the role of surveillance biopsies for management of allograft inflammation in kidney transplantation.

摘要

背景

监测性活检能够在临床功能出现障碍之前早期检测到亚临床炎症,但检测到早期亚临床表型的影响仍不明确。

方法

我们对2015年至2018年间连续的441例肾移植受者进行了一项单中心回顾性队列研究,这些受者在移植后6个月进行了监测性活检。我们检验了以下假设:早期亚临床炎症(亚临床临界改变、T细胞介导的排斥反应或微血管损伤)与包括急性排斥反应和移植失败在内的复合终点事件的发生率增加相关。

结果

根据同期的班夫标准,我们在31%的受者中检测到亚临床炎症,其中大多数(75%)具有亚临床临界表型(至少有轻度炎症伴轻度肾小管炎[>i0t1])。总体而言,亚临床炎症与复合终点事件独立相关(调整后的风险比为2.88;1.11 - 7.51;P = 0.03)。亚临床临界炎症亚组,主要是那些符合2019年班夫i1t1阈值的受者,与复合终点事件的风险增加5倍独立相关(P = 0.02)。同时存在亚临床炎症和亚临床慢性移植损伤的受者预后更差。在小的异质性亚组中,治疗亚临床炎症的效果难以确定。

结论

在移植肾功能稳定的肾移植受者中,移植后6个月亚临床急性和慢性炎症很常见。同时伴有肾小管炎和间质炎症的亚临床临界表型与不良的长期预后独立相关。需要进一步研究以阐明监测性活检在肾移植中管理移植炎症的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d750/7837932/bace9949d040/txd-7-e663-g001.jpg

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