表征抗体对阿莫司林/谷胱甘肽病原体减少的红细胞的反应。

IF 2.5 3区医学 Q2 HEMATOLOGY

Transfusion Pub Date : 2024-12-25 DOI:10.1111/trf.18117

Christopher Karim, Anil Panigrahi, Ronald G Pearl, Neel R Sodha, Thomas M Beaver, J Peter R Pelletier, Gregory A Nuttall, T Brett Reece, Anna Erickson, Teresa Hedrick, Kathy Liu, Stanley Bentow, Laurence Corash, Nina Mufti, Jeanne Varrone, Richard J Benjamin

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引用次数: 0

摘要

背景：amustaline/谷胱甘肽病原体减少的红细胞（prrbc）特异性的天然抗体和治疗产生的抗体的临床意义尚不清楚。研究设计和方法：一项关于pr红细胞的3期随机临床试验比较了pr红细胞与常规红细胞在心脏或胸主动脉手术中的应用。在手术期间和术后7天内输血的受试者在基线、术后28天和75天进行prrbc特异性抗体筛查。检测治疗产生抗体的受试者是否存在溶血。冷冻保存的受试者红细胞样本使用吖啶特异性（2S197-2M1）单克隆抗体和人igg包被红细胞，通过流式细胞术检测循环prrbc。红细胞表面吖啶密度采用商业校准的藻红蛋白(PE)-头面板定量。结果：159名PRRBC受者中有5名（3.1%）和162名常规RBC受者中没有人出现治疗后出现的PRRBC特异性IgG，暴露于1-3个PRRBC单位后26-80天检测到低效价抗体，无临床溶血证据。1例患者DAT和elue呈弱（w+）阳性和prrbc特异性。单核细胞单层试验（MMA）在三个受试者中无反应，结果可解释。流式细胞术显示，与新鲜输入的prrbc（约7500 PE分子/RBC）相比，所有5名受试者的循环prrbc在检测极限下表达表面吖啶浓度（约150-301 PE分子/RBC）。在一些样品中，表面吖啶表达的缺失不能与pr红细胞的清除区分开来。讨论：在5例输注pr红细胞的受试者中检测到治疗中出现的pr红细胞特异性抗体，其特征是非临床显著的抗体。流式细胞术显示持续循环的pr红细胞具有极低的表面吖啶表达。（www.Clinicaltrials: gov标识符NCT03459287）。

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Characterizing the antibody response to amustaline/glutathione pathogen-reduced red blood cells.

Background: The clinical significance of natural and treatment-emergent antibodies specific for amustaline/glutathione pathogen-reduced red blood cells (PRRBCs) is not known.

Study design and methods: A Phase 3, randomized clinical trial of PRRBCs (ReCePI) compared PRRBCs with conventional RBCs in cardiac or thoracic-aorta surgery. Subjects transfused during and for 7 days after surgery were screened for PRRBC-specific antibodies at baseline, 28 and 75 days post-surgery. Subjects with treatment-emergent antibodies were assessed for evidence of hemolysis. Cryopreserved subject RBC samples were assayed by flow cytometry for circulating PRRBCs using an acridine-specific (2S197-2M1) monoclonal antibody, and for human IgG-coated RBCs. RBC-surface acridine density was quantitated using a commercial calibrated phycoerythrin (PE)-bead panel.

Results: Five of 159 (3.1%) PRRBC and zero of 162 conventional RBC recipients developed treatment-emergent PRRBC-specific IgG, low titer antibodies detected 26-80 days post-surgery after exposure to 1-3 PRRBC units, without clinical evidence of hemolysis. DAT and eluate were weak (w+) positive and PRRBC-specific in one subject. A monocyte monolayer assay (MMA) was non-reactive in the three subjects with an interpretable result. Flow cytometry demonstrated circulating PRRBCs in all five subjects expressing surface acridine concentrations at the limit of detection (approximately 150-301 PE molecules/RBC) compared with freshly transfused PRRBCs (approximately 7500 PE molecules/RBC). In some samples, loss of surface acridine expression could not be distinguished from clearance of the PRRBCs.

Discussion: Treatment-emergent PRRBC-specific antibodies with the characteristics of nonclinically significant antibodies were detected in five subjects transfused with PRRBCs. Flow cytometry demonstrated persistent circulating PRRBCs with minimal surface acridine expression. (www.

Clinicaltrials: gov Identifier NCT03459287).

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来源期刊

Transfusion 医学-血液学

CiteScore

4.70

自引率

20.70%

发文量

426

审稿时长

1 months

期刊介绍： TRANSFUSION is the foremost publication in the world for new information regarding transfusion medicine. Written by and for members of AABB and other health-care workers, TRANSFUSION reports on the latest technical advances, discusses opposing viewpoints regarding controversial issues, and presents key conference proceedings. In addition to blood banking and transfusion medicine topics, TRANSFUSION presents submissions concerning patient blood management, tissue transplantation and hematopoietic, cellular, and gene therapies.