Immature and activated phenotype of blood NK cells is associated with acute rejection in adult liver transplant

CD16 免疫学 医学 外周血单个核细胞 人口 免疫系统 自然杀伤细胞 移植 内科学 细胞毒性T细胞 CD8型 CD3型 生物 体外 生物化学 环境卫生
作者
Shifei Song,Zhi Yao,Guangyao Tian,Xiangle Sun,Yuguo Chen,Wei Qiu,Wenyu Jiao,Heyu Huang,Ying Yu,Mingqian Li,Guoyue Lv
出处
期刊:Liver Transplantation [Wiley]
卷期号:29 (8): 836-848 被引量:1
标识
DOI:10.1097/lvt.0000000000000139
摘要

Natural killer (NK) cells contribute to liver transplant (LTx) rejection. However, the blood-circulating NK-cell dynamics of patients who experience acute rejection (AR) are unclear. Herein, we longitudinally profiled the total NK cells and their subsets, along with the expression of activating and inhibitory receptors in sequential peripheral blood mononuclear cell samples, spanning from before LTx to the first year after LTx of 32 patients with AR and 30 patients under a steady immune status. Before transplantation, patients with AR (rejectors) contained a significantly higher proportion of the immature CD56 bright CD16 - subset and a lower cytolytic CD56 dim CD16 + in the total blood-circulating NK cells than patients with steady immunity. Both subsets contained a high NKp30-positive population, and CD56 dim CD16 + additionally exhibited a high NKp46-positive ratio. The NKp30-positive ratio in CD56 dim CD16 + subset showed the most prominent AR predictive ability before LTx and was an independent risk factor of LTx AR. After transplantation, the blood-circulating NK cells in rejectors maintained a higher CD56 bright CD16 - and lower CD56 dim CD16 + composition than the controls throughout the first year after LTx. Moreover, both subsets maintained a high NKp30-positive ratio, and CD56 dim CD16 + retained a high NKp46-positive ratio. The blood-circulating NK cell subset composition was consistent during AR, while the expressions of NKp30 and NKp46 were augmented. Collectively, a more immature CD56 bright CD16 - subset composition and an activated phenotype of high NKp30 expression were the general properties of blood-circulating NK cells in rejected LTx recipients, and the NKp30-positive ratio in CD56 dim CD16 + NK subset before LTx possessed AR predictive potential.
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