CRISPRi-mediated knock-down of PRDM1/BLIMP1 programs central memory differentiation in ex vivo-expanded human T cells.

IF 2.2 4区 工程技术 Q3 PHARMACOLOGY & PHARMACY
Bioimpacts Pub Date : 2022-01-01 Epub Date: 2021-12-07 DOI:10.34172/bi.2021.23522
Mohammad Azadbakht, Ali Sayadmanesh, Naghme Nazer, Amirhossein Ahmadi, Sara Hemmati, Hoda Mohammadzade, Marzieh Ebrahimi, Hossein Baharvand, Babak Khalaj, Mahmoud Reza Aghamaali, Mohsen Basiri
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引用次数: 0

Abstract

Introduction: B lymphocyte-induced maturation protein 1 (BLIMP1) encoded by the positive regulatory domain 1 gene (PRDM1), is a key regulator in T cell differentiation in mouse models. BLIMP1-deficiency results in a lower effector phenotype and a higher memory phenotype. Methods: In this study, we aimed to determine the role of transcription factor BLIMP1 in human T cell differentiation. Specifically, we investigated the role of BLIMP1 in memory differentiation and exhaustion of human T cells. We used CRISPR interference (CRISPRi) to knock-down BLIMP1 and investigated the differential expressions of T cell memory and exhaustion markers in BLIMP1-deficient T cells in comparison with BLIMP1-sufficient ex vivo expanded human T cells. Results: BLIMP1-deficiency caused an increase in central memory (CM) T cells and a decrease in effector memory (EM) T cells. There was a decrease in the amount of TIM3 exhaustion marker expression in BLIMP1-deficient T cells; however, there was an increase in PD1 exhaustion marker expression in BLIMP1-deficient T cells compared with BLIMP1-sufficient T cells. Conclusion: Our study provides the first functional evidence of the impact of BLIMP1 on the regulation of human T cell memory and exhaustion phenotype. These findings suggest that BLIMP1 may be a promising target to improve the immune response in adoptive T cell therapy settings.

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在体外扩增的人T细胞中,crispr介导的PRDM1/BLIMP1敲除可编程中央记忆分化。
B淋巴细胞诱导成熟蛋白1 (BLIMP1)由正调控结构域1基因(PRDM1)编码,是小鼠模型中T细胞分化的关键调控因子。blimp1缺陷导致较低的效应表型和较高的记忆表型。方法:本研究旨在确定转录因子BLIMP1在人T细胞分化中的作用。具体来说,我们研究了BLIMP1在人类T细胞记忆分化和衰竭中的作用。我们使用CRISPR干扰(CRISPRi)敲除BLIMP1,并研究了与BLIMP1充足的体外扩增人T细胞相比,缺乏BLIMP1的T细胞中T细胞记忆和衰竭标志物的差异表达。结果:blimp1缺失导致中枢记忆(CM) T细胞增加,效应记忆(EM) T细胞减少。blimp1缺陷T细胞中TIM3耗竭标志物的表达量降低;然而,与blimp1充足的T细胞相比,缺乏blimp1的T细胞中PD1衰竭标志物的表达增加。结论:本研究首次提供了BLIMP1调控人类T细胞记忆和衰竭表型的功能证据。这些发现表明,在过继性T细胞治疗中,BLIMP1可能是一个有希望改善免疫反应的靶点。
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来源期刊
Bioimpacts
Bioimpacts Pharmacology, Toxicology and Pharmaceutics-Pharmaceutical Science
CiteScore
4.80
自引率
7.70%
发文量
36
审稿时长
5 weeks
期刊介绍: BioImpacts (BI) is a peer-reviewed multidisciplinary international journal, covering original research articles, reviews, commentaries, hypotheses, methodologies, and visions/reflections dealing with all aspects of biological and biomedical researches at molecular, cellular, functional and translational dimensions.
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