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造血干细胞移植物中TCRαβ+和CD45RA+ T细胞的选择性清除:影响清除效果的因素分析

Selective TCRαβ+ and CD45RA+ T-cell depletion of hematopoietic stem cell graft: An analysis on factors that affect depletion performance.

作者信息

Ang Chieh Hwee, Gan Gina, Ho Ren How, Heng Kee Khiang, Linn Yeh Ching

机构信息

Department of Hematology, Singapore General Hospital, Singapore.

出版信息

Cell Transplant. 2025 Jan-Dec;34:9636897251336965. doi: 10.1177/09636897251336965. Epub 2025 May 8.

Abstract

Selective depletion of TCRαβ+ and CD45RA+ subsets of apheresed hematopoietic progenitor cells, HPC(A), enables haploidentical hematopoietic stem cell transplant (haplo-HSCT) by circumventing risks of graft-versus-host disease. Here, we analyze our institution's large series of T-cell depletion processes to review procedure performance and explore factors that affect depletion efficiency and graft composition. Over 6 years, 91 haploidentical donors underwent peripheral blood CD34+ stem cell mobilization with granulocyte-colony stimulating factor, with 12 (13%) receiving additional pre-emptive plerixafor. HPC(A) was split into two fractions for TCRαβ and CD45RA depletion with the CliniMACS PLUS device. TCRαβ depletion resulted in a median 4.3 (interquartile range, 4.1-4.5) log reduction, with CD34 recovery at 98% (94%-103%) and TCRγδ+ cell recovery at 89% (74%-98%). CD45RA depletion resulted in a median 4.8 (4.3-5.2) log reduction, with CD3+/CD45RO+ cell recovery at 41% (34%-47%) and CD34 recovery at 58% (51%-68%). TCRαβ depletion efficiency was maintained even when total nucleated cell counts exceeded the maximal specified number, provided the target fraction was within capacity of the depletion kit. Platelet contamination did not affect depletion efficacy or CD34 recovery. Age increases the proportion of CD45RO+ memory cells and TCRαβ subset in HPC(A), while plerixafor increases the latter. Although statistically significant correlation exists between pre-depletion cell composition and depletion performance for some cell subsets, the post-depletion product still met pre-specified threshold without being affected to a clinically relevant extent, over a wide range of input cell numbers. Such robustness of the depletion systems is critical for successful performance of haplo-HSCT.

摘要

选择性去除采集的造血祖细胞(HPC(A))中的TCRαβ+和CD45RA+亚群,可通过规避移植物抗宿主病风险实现单倍型造血干细胞移植(haplo-HSCT)。在此,我们分析了本机构大量的T细胞去除过程,以评估操作流程并探索影响去除效率和移植物组成的因素。在6年多的时间里,91名单倍型供者接受了粒细胞集落刺激因子动员外周血CD34+干细胞,其中12名(13%)接受了额外的预先使用的普乐沙福。HPC(A)被分为两部分,使用CliniMACS PLUS设备进行TCRαβ和CD45RA去除。TCRαβ去除导致中位数4.3(四分位间距,4.1 - 4.5)对数减少,CD34回收率为98%(94% - 103%),TCRγδ+细胞回收率为89%(74% - 98%)。CD45RA去除导致中位数4.8(4.3 - 5.2)对数减少,CD3+/CD45RO+细胞回收率为41%(34% - 47%),CD34回收率为58%(51% - 68%)。即使总核细胞计数超过最大指定数量,只要目标部分在去除试剂盒的容量范围内,TCRαβ去除效率仍能维持。血小板污染不影响去除效果或CD34回收率。年龄增加了HPC(A)中CD45RO+记忆细胞和TCRαβ亚群的比例,而普乐沙福增加了后者。尽管某些细胞亚群的去除前细胞组成与去除性能之间存在统计学上的显著相关性,但在广泛的输入细胞数量范围内,去除后产物仍达到预先指定的阈值,且未受到临床相关程度的影响。这种去除系统的稳健性对于haplo-HSCT的成功实施至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ce72/12062598/78d03fd4c560/10.1177_09636897251336965-img2.jpg

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