Umbilical cord blood as a promising source of NK cells for immunotherapy

R. Velichinskii, J. Vavilova, A. Boyko, O. A. Shustova, A. Palamarchuk, G. Yusubalieva, O. N. Kucherova, M. Streltsova, E. Kovalenko
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Abstract

Currently, a large number of studies on genetic modification of cord blood NK cells (UCB-NK) are carried out at both clinical and preclinical levels. Immunotherapy based on UCB-NK cells has great potential for antitumor therapy. However, despite having known several advantages over peripheral blood NK cells (PB- NK), including a high concentration in cord blood and low virulence rate, UCB-NK cells are predominantly characterized in the scientific literature as immature and low-functioning NK cells. In this work, we studied the phenotypic characteristics of UCB-NK cells and the possibility of stimulatory compensation of the decreased functional activity of UCB-NK cells. Our studies revealed UCB-NK cells can be characterized as poorly differentiated and weakly activated cells with high level of inhibitory receptor NKG2A and low level of activating receptor NKG2C and HLA-DR, accordingly with the literature data. Two types of stimuli were chosen to stimulate freshly isolated UCB-NK cells: 1) 100 units of IL-2; 2) combinations of 100 units IL-2 and K-562 feeder cells expressing membrane-bound IL-21 (K562-mbIL21). It was shown the degranulation (LAMP-1) and proliferative activity was higher than for parallel cultured ex vivo PB-NK cells under the same conditions for UCB-NK cells stimulated for 7 days with IL-2 + K562-mbIL21. Moreover, stimulation in the way of IL-2 + K562-mbIL21 seemed to be a more perspective way to obtain a large number of proliferatively active UCB-NK cells compared to stimulation with IL-2 only. Since genetic modification of NK cells is a promising way to improve the antitumor properties of NK cells, retroviral transduction procedure was performed to study of the stimulated UCB-NK cells. UCB-NK cells stimulated with IL-2 + K562-mbIL21 were transduced on day 8 of cultivation. In this study, we used targeted overexpression of the adaptor molecule DAP12, which is involved in the signaling of activating NK cell receptors. PB-NK cells and UCB-NK cells were transduced under the equal experimental conditions in same volume of viral particles. As a result, the transduction efficiency was found to be more than 4-fold higher for UCB-NK cells compared to PB-NK cells. Thus, UCB-NK cells appear to be a promising tool for further research in cancer immunotherapy.
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脐带血作为一种有前途的免疫治疗NK细胞来源
目前,大量关于脐带血NK细胞(UCB-NK)基因修饰的研究在临床和临床前水平均有开展。基于UCB-NK细胞的免疫治疗在抗肿瘤治疗中具有很大的潜力。然而,尽管已知与外周血NK细胞(PB- NK)相比有一些优势,包括脐带血中的高浓度和低毒力率,但在科学文献中,UCB-NK细胞主要以不成熟和低功能NK细胞为特征。在这项工作中,我们研究了UCB-NK细胞的表型特征以及UCB-NK细胞功能活性下降的刺激补偿的可能性。我们的研究表明,UCB-NK细胞具有低分化弱活化的特点,具有高水平的抑制性受体NKG2A,低水平的活化受体NKG2C和HLA-DR。选择两种类型的刺激刺激新分离的UCB-NK细胞:1)100单位的IL-2;2) 100个单位IL-2与表达膜结合IL-21 (K562-mbIL21)的K-562饲养细胞联合。结果表明,在相同条件下,IL-2 + K562-mbIL21刺激UCB-NK细胞7天后,其脱颗粒(LAMP-1)和增殖活性高于体外平行培养的PB-NK细胞。此外,与仅IL-2刺激相比,IL-2 + K562-mbIL21的刺激方式似乎是获得大量增殖活性UCB-NK细胞的更有前景的方式。由于NK细胞的遗传修饰是提高NK细胞抗肿瘤特性的一种有希望的方法,因此采用逆转录病毒转导程序来研究受刺激的UCB-NK细胞。IL-2 + K562-mbIL21刺激的UCB-NK细胞在培养第8天转导。在本研究中,我们使用靶向过表达adaptor分子DAP12,该分子参与激活NK细胞受体的信号传导。PB-NK细胞和UCB-NK细胞在相同的实验条件下,在相同体积的病毒颗粒中转导。结果,发现UCB-NK细胞的转导效率比PB-NK细胞高4倍以上。因此,UCB-NK细胞似乎是癌症免疫治疗进一步研究的一个有前途的工具。
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来源期刊
Medical Immunology (Russia)
Medical Immunology (Russia) Medicine-Immunology and Allergy
CiteScore
0.70
自引率
0.00%
发文量
88
审稿时长
12 weeks
期刊介绍: The journal mission is to promote scientific achievements in fundamental and applied immunology to various medical fields, the publication of reviews, lectures, essays by leading domestic and foreign experts in the field of fundamental and experimental immunology, clinical immunology, allergology, immunodiagnostics and immunotherapy of infectious, allergy, autoimmune diseases and cancer.
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