nk细胞表型病毒基因型驱动的慢性病毒性丙型肝炎的特点

A. Savchenko, E. P. Tikhonova, A. Anisimova, I. Kudryavtsev, Vasilij Belenjuk, A. Borisov
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摘要

由于直接抗病毒药物(DAD)作用而消除丙型肝炎病毒(HCV)会影响病毒表型的改变,从而影响NK细胞的功能活性。然而,公布的数据非常矛盾。的目标。研究DAD治疗HCV基因型依赖性慢性丙型肝炎(CVHC)患者后NK细胞亚群表型的改变材料:对111例CVHC患者和21名健康志愿者进行了检查。诊断依据流行病学、临床和实验室资料。所有111例CVHC患者均直接接受抗病毒药物索非布韦和维帕他韦治疗12周。采用多色流式细胞术分析NK细胞表型的变化。结果。在DAD治疗前,不同HCV基因型的CVHC患者血液样本中发现细胞因子产生计数减少,细胞毒性NK细胞频率增加。无论HCV基因型如何,在CVHC患者中也发现了具有高水平功能活性的细胞毒性细胞的不平衡。HCV基因型1和基因型3患者免疫调节性NK细胞水平明显升高。此外,在HCV基因型1和3的患者中,表达糖水解酶(CD38)和外链5-核苷酸酶(CD73)的NK细胞数量增加。因此,CVHC患者NK细胞表型的这种改变表现为持续的高病毒载量,在HCV基因型1携带者中达到峰值,而在HCV基因型2患者中最低。DAD治疗后NK细胞变化最显著的是HCV基因型为2的CVHC患者(表达cd8的NK细胞亚群组成和计数的正常化)。只有HCV基因型为2的患者在治疗后外周血双阴性CD38CD73 NK细胞的频率增加。HCV基因型1和3的患者在DAD治疗后NK细胞亚群组成也有轻微改善。结论。评估由HCV基因型驱动的CVHC患者DAD治疗过程中NK细胞表型的特异性变化无疑具有重要意义和高度相关性。获得的结果是新颖的,并补充了对CVHC免疫发病机制的见解。分析CVHC患者NK细胞表型和功能活性可能促进HCV感染治疗新方法的发展。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
FEATURES OF NK CELL PHENOTYPE VIRUS GENOTYPE-DRIVEN CHRONIC VIRAL HEPATITIS C
Elimination of the hepatitis C virus (HCV) due to direct antiviral drug (DAD) action affects alteration in virus phenotype and, accordingly, NK cell functional activity. However, the published data are very contradictory. Aim. Investigating alterations in NK cell subset phenotype after DAD treatment of HCV genotype-dependent chronic viral hepatitis C (CVHC) patients. Material. 111 CVHC patients and 21 healthy volunteers were examined. The diagnosis was established on epidemiological, clinical and laboratory data. All 111 subjects with CVHC received direct antiviral drugs Sofosbuvir and Velpatasvir for 12 weeks. The study of the NK cell phenotypes wwas analyzed by multicolor flow cytometry. Results. A decreased count of cytokine-producing along with increased frequency of cytotoxic NK cells were found in CVHC patients blood samples with various HCV genotypes prior to DAD treatment. The imbalance of cytotoxic cells with a high level of functional activity was also found in CVHC patients regardless of HCV genotype. The patients with HCV genotypes 1 and 3 showed significantly increased level of immunoregulatory NK cells. In addition, increased count of glycohydrolase (CD38) and ecto-5-nucleotidase (CD73)-expressing NK cells were found in patients with HCV genotypes 1 and 3. Hence, such alterations in NK cell phenotype in CVHC patients were presented as sustained high viral load which peaking at carriers of HCV genotype 1 that was minimal in patients with HCV genotype 2. The most prominent change in NK cells after DAD treatment was found in CVHC patients with HCV genotype 2 (normalization of CD8-expressing NK cell subset composition and count). Only patients with HCV genotype 2 after treatment had increased frequencies of peripheral blood double-negative CD38CD73 NK cells. Patients with HCV genotypes 1 and 3 also showed minimally improved in NK cell subset composition after DAD treatment. Conclusions. Evaluation of specific changes in NK cell phenotype during DAD treatment of CVHC patients driven by HCV genotype undoubtedly is of importance and high relevance. The results obtained are novel and complement the insights into CVHC immunopathogenesis. Analysis of NK cell phenotypes and functional activity in patients with CVHC may promote development of new methods for treating HCV infection.
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