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优化外周血单个核细胞冷冻保存及用于抗原特异性记忆B细胞的免疫斑点分析

Optimizing PBMC Cryopreservation and Utilization for ImmunoSpot Analysis of Antigen-Specific Memory B Cells.

作者信息

Becza Noémi, Yao Lingling, Lehmann Paul V, Kirchenbaum Greg A

机构信息

Research and Development, Cellular Technology Ltd. (CTL), Shaker Heights, OH 44122, USA.

出版信息

Vaccines (Basel). 2025 Jul 19;13(7):765. doi: 10.3390/vaccines13070765.

Abstract

Measuring frequencies of antigen-specific memory B cells (B), their immunoglobulin (Ig) class and subclass usage, cross-reactivity, and affinity can provide insights into the efficacy of future antibody responses in case of antigen re-encounter. B cell ImmunoSpot assays can provide such information; however, like most cell-based tests, they require considerable amounts of blood to be drawn from the donor and this has hindered their inclusion in clinical trials and routine immune diagnostics. : We introduce strategies for reducing the cell numbers required to 2-3 million peripheral blood mononuclear cells (PBMCs) per antigen, obtainable from 2-3 mL of blood from healthy adult donors. : Except when B frequencies were very low, we found that testing PBMCs in singlet wells, but in serial dilution, enables as reliable B frequency assessments as when testing replicate wells at a single fixed cell number. Additionally, B cell ImmunoSpot assays can be multiplexed for detecting four Ig classes, or IgG subclasses, simultaneously and without loss of sensitivity. The requirement for low cell numbers and the retention of B cell functionality by cryopreserved PBMCs equivalent to freshly isolated material implies that fewer than the standard 10 million PBMCs per vial can be frozen. This would reduce the number of individuals who could not be tested for B due to insufficient availability of PBMCs, a common problem with such assays. : The predictable need for and recovery of cryopreserved PBMCs facilitates planning of and optimal cell utilization in B cell ImmunoSpot assays and increases the practical feasibility of extensive B characterization in larger cohorts.

摘要

测量抗原特异性记忆B细胞(B细胞)的频率、其免疫球蛋白(Ig)的类别和亚类使用情况、交叉反应性及亲和力,可深入了解再次接触抗原时未来抗体反应的效力。B细胞免疫斑点检测可提供此类信息;然而,与大多数基于细胞的检测一样,它们需要从供体抽取大量血液,这阻碍了它们纳入临床试验和常规免疫诊断。:我们介绍了将每个抗原所需细胞数量减少至200 - 300万个外周血单个核细胞(PBMC)的策略,这些细胞可从健康成年供体的2 - 3毫升血液中获得。:除了B细胞频率非常低的情况外,我们发现将PBMC在单孔中进行检测,但采用连续稀释的方式,与在单个固定细胞数量下检测重复孔相比,能够进行同样可靠的B细胞频率评估。此外,B细胞免疫斑点检测可以进行多重检测,同时检测四种Ig类别或IgG亚类,且不会损失灵敏度。对低细胞数量的要求以及冷冻保存的PBMC与新鲜分离材料相当的B细胞功能保留意味着每个冻存管中可冷冻的PBMC数量少于标准的1000万个。这将减少因PBMC可用性不足而无法进行B细胞检测的个体数量,这是此类检测中常见的问题。:对冷冻保存的PBMC的可预测需求和回收便于B细胞免疫斑点检测的规划和最佳细胞利用,并增加了在更大队列中进行广泛B细胞特征分析的实际可行性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/783e/12299797/c6c9a11f486d/vaccines-13-00765-g001.jpg

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