مشخصات پژوهش

خانه /CRISPRi-mediated knock-down ...
عنوان
CRISPRi-mediated knock-down of PRDM1/BLIMP1 programs central memory differentiation in ex vivo-expanded human T cells
نوع پژوهش مقالات در نشریات
کلیدواژه‌ها
T cell, PRDM1, BLIMP1, CRISPR interference, Memory T cell
چکیده
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.
پژوهشگران محمد آزادبخت (نفر اول)، علی صیاد منش (نفر دوم)، نغمه ناظر (نفر سوم)، امیرحسین احمدی (نفر چهارم)، سارا همتی (نفر پنجم)، هدی محمدزاده (نفر ششم به بعد)، مرضیه ابراهیمی (نفر ششم به بعد)، حسین بهاروند (نفر ششم به بعد)، بابک خلج (نفر ششم به بعد)، محمود رضا آقامعالی (نفر ششم به بعد)، محسن بصیری (نفر ششم به بعد)