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计算性 panel reactive antigen 升高与肺移植等待时间延长和死亡率升高相关。

Increased Calculated Panel Reactive Antigen Is Associated With Increased Waitlist Time and Mortality in Lung Transplantation.

机构信息

Division of Cardiovascular and Thoracic Surgery, Duke University Medical Center, Durham, North Carolina.

Division of Cardiovascular and Thoracic Surgery, Duke University Medical Center, Durham, North Carolina.

出版信息

Ann Thorac Surg. 2020 Aug;110(2):414-423. doi: 10.1016/j.athoracsur.2020.02.061. Epub 2020 Apr 3.

Abstract

BACKGROUND

Sensitized candidates with unacceptable antigens are a group that demands special attention in organ transplantation. Calculated panel reactive antigen (cPRA) is not used to modify allocation priorities in lung transplantation. The impact of cPRA on waiting list time and mortality is unknown.

METHODS

We performed a retrospective review of candidates for lung transplantation listed from May 2005 to 2018. Data from the Organ Procurement and Transplantation Network/United Network for Organ Sharing STAR (Standard Analysis and Research) dataset was paired with additional unacceptable human leukocyte antigen (UA-HLA) data, which were used to calculate the listing cPRA. Candidates were stratified based on the lack of UA-HLAs or cPRA level for candidates with unacceptable antigens reported. Unadjusted competing risks and adjusted subdistribution hazard models were fit.

RESULTS

A total of 29,085 candidates met inclusion criteria for analysis. Of these, 23,562 (81%) with no UA-HLAs, 3472 (11.9%) with a cPRA less than 50, and 2051 with a cPRA greater than or equal to 50 (7.1%). On adjusted analysis, a cPRA greater than or equal to 50 was independently associated with increased waitlist mortality at 1 year (hazard ratio, 1.71; 95% confidence interval, 1.55-1.88; P < .001) and decreased rate of transplantation (71.9% vs 69.5% vs 44.4%; P < .001). Furthermore, patients with a cPRA greater than or equal to 50 had a longer waitlist time compared with a cPRA less than 50 and no UA-HLA candidates (mean 293.69 days vs 162.38 days and 143.26 days, respectively; P < .001). However, once transplanted, posttransplant survival among the cohorts was similar.

CONCLUSIONS

Further evaluation of organ allocation with consideration of a candidate's cPRA may be warranted in order to optimize equity in access to transplants.

摘要

背景

在器官移植中,具有不可接受抗原的致敏候选者是一个需要特别关注的群体。计算的群体反应性抗原(cPRA)并未用于修改肺移植的分配优先级。cPRA 对候补名单时间和死亡率的影响尚不清楚。

方法

我们对 2005 年 5 月至 2018 年期间列出的肺移植候选者进行了回顾性审查。从器官采购与移植网络/联合器官共享网络 STAR(标准分析与研究)数据集获得的数据与额外的不可接受的人类白细胞抗原(UA-HLA)数据进行了配对,这些数据用于计算列出的 cPRA。根据候选者是否具有不可接受的抗原报告缺乏 UA-HLA 或 cPRA 水平对候选者进行分层。拟合了未经调整的竞争风险和调整后的亚分布风险模型。

结果

共有 29085 名候选者符合分析纳入标准。其中,23562 名(81%)候选者无 UA-HLA,3472 名(11.9%)cPRA 小于 50,2051 名 cPRA 大于或等于 50(7.1%)。在调整后的分析中,cPRA 大于或等于 50 与 1 年时等待名单死亡率增加独立相关(危险比,1.71;95%置信区间,1.55-1.88;P<.001),并且移植率降低(71.9%比 69.5%比 44.4%;P<.001)。此外,与 cPRA 小于 50 和无 UA-HLA 候选者相比,cPRA 大于或等于 50 的患者等待名单时间更长(分别为 293.69 天、162.38 天和 143.26 天;P<.001)。但是,一旦移植,各队列的移植后生存率相似。

结论

为了优化移植机会的公平性,可能需要进一步评估候选者的 cPRA 对器官分配的影响。

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