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首页> 外文期刊>Frontiers in Immunology >Age Distribution of Multiple Functionally Relevant Subsets of CD4+ T Cells in Human Blood Using a Standardized and Validated 14-Color EuroFlow Immune Monitoring Tube
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Age Distribution of Multiple Functionally Relevant Subsets of CD4+ T Cells in Human Blood Using a Standardized and Validated 14-Color EuroFlow Immune Monitoring Tube

机译:使用标准化和经过验证的14色EUROFLOW免疫监测管,人血液中CD4 + T细胞多功能相关子集的年龄分布

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CD4+ T cells comprise multiple functionally distinct cell populations that play a key role in immunity. Despite blood monitoring of CD4+ T-cell subsets is of potential clinical utility, no standardized and validated approaches have been proposed so far. The aim of this study was to design and validate a single 14-color antibody combination for sensitive and reproducible flow cytometry monitoring of CD4+ T-cell populations in human blood to establish normal age-related reference values and evaluate the presence of potentially altered profiles in three distinct disease models—monoclonal B-cell lymphocytosis (MBL), systemic mastocytosis (SM), and common variable immunodeficiency (CVID). Overall, 145 blood samples from healthy donors were used to design and validate a 14-color antibody combination based on extensive reagent testing in multiple cycles of design–testing–evaluation–redesign, combined with in vitro functional studies, gene expression profiling, and multicentric evaluation of manual vs. automated gating. Fifteen cord blood and 98 blood samples from healthy donors (aged 0–89 years) were used to establish reference values, and another 25 blood samples were evaluated for detecting potentially altered CD4 T-cell subset profiles in MBL ( n = 8), SM ( n = 7), and CVID ( n = 10). The 14-color tube can identify ≥89 different CD4+ T-cell populations in blood, as validated with high multicenter reproducibility, particularly when software-guided automated (vs. manual expert-based) gating was used. Furthermore, age-related reference values were established, which reflect different kinetics for distinct subsets: progressive increase of na?ve T cells, T-helper (Th)1, Th17, follicular helper T (TFH) cells, and regulatory T cells (Tregs) from birth until 2 years, followed by a decrease of na?ve T cells, Th2, and Tregs in older children and a subsequent increase in multiple Th-cell subsets toward late adulthood. Altered and unique CD4+ T-cell subset profiles were detected in two of the three disease models evaluated (SM and CVID). In summary, the EuroFlow immune monitoring TCD4 tube allows fast, automated, and reproducible identification of ≥89 subsets of CD4+ blood T cells, with different kinetics throughout life. These results set the basis for in-depth T-cell monitoring in different disease and therapeutic conditions.
机译:CD4 + T细胞包含多种功能性不同的细胞群,其在免疫中起关键作用。尽管对CD4 + T细胞亚群的血液监测是潜在的临床实用,但到目前为止没有提出标准化和验证的方法。本研究的目的是设计和验证单一的14色抗体组合,用于敏感和可再现的流式细胞术监测人血液中的CD4 + T细胞群,以建立正常年龄相关的参考值,并评估潜在改变的曲线的存在三种不同的疾病模型 - 单克隆B细胞淋巴细胞症(MBL),全身性乳细胞症(SM)和常见的可变免疫缺陷(CVID)。总体而言,来自健康供体的145个血液样本基于在设计测试评估重新设计的多个循环中的广泛试剂测试中设计和验证14色抗体组合,结合体外功能研究,基因表达分析和多中心对手册与自动化门控的评估。来自健康供体的十五个脐带血和98粒血液样品用于建立参考值,并评估另一种25个血样,用于检测MBL(n = 8),SM中的潜在改变的CD4 T细胞子集谱(n = 7),CVID(n = 10)。 14色管可以鉴定血液中的≥89种不同的CD4 + T细胞群,如多中心再现性验证,特别是当使用软件引导的自动化(基于手动专家的)门控时。此外,建立了年龄相关的参考值,其反映了不同子集的不同动力学:Na ve T细胞,T-辅助(Th)1,Th17,卵泡辅助T(TFH)细胞和调节性T细胞的逐渐增加(从出生之前到2年,然后在年龄较大的儿童中减少Na?Ve T细胞,Th2和Tregs,随后对已婚后期的多个Th-Cell子集增加。在评估的三种疾病模型中检测到改变和独特的CD4 + T细胞子集谱(SM和CVID)中的两种。总之,EuroFlow免疫监测TCD4管允许快速,自动化,可再现的CD4 +血液T细胞≥89亚群,在整个生命中具有不同的动力学。这些结果设定了不同疾病和治疗条件的深入T细胞监测的基础。

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