<i>In vitro</> effects of recombinant IFNα2B on the content of antigen-presenting CD66b<sup>+</sup>CD16<sup>+</sup>CD33<sup>+</sup>HLA<sup>-</sup>DR<sup>+</sup> subset of neutrophils in children with acute osteomyelitis

I. V. Nesterova, Galina A. Chudilova, Yu. V. Teterin, E. A. Chicherev, V. N. Chapurina, V. A. Tarakanov, N. K. Barova
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Abstract

Negative impact of S. aureus, seems to be a sufficient condition for the spread of the infectious process in the bone in acute osteomyelitis (AOM) due to its altered elimination caused by dysfunction of the immune system (IS), in particular, of neutrophilic granulocytes (NG). Correction of NG dysfunction in AOM under the influence of immunotropic substances and cytokines via modulation of the NG phenotypic subsets is of sufficient interest. Our aim was to evaluate the in vitro effects of recombinant IFN2b on the number and phenotype of CD66b+CD16+CD33+HLA-DR-, CD66b+CD16+CD33+HLA-DR+ subsets and on phagocytic function of neutrophilic granulocytes in acute osteomyelitis in children. The study of peripheral blood (PB) samples from children aged 8-15 years was carried out as follows: patients with АOM (n = 24) comprised study group 1 (SG1), healthy children (n = 13) were included into comparison group (CG). PB samples of children with AOM were incubated with recIFN2b (50 IU/L, 60 min, 37 C.) in the study group 1a (SG1a). Before and after incubation with recIFN2b, the number of NG subsets CD66b+CD16+CD33+HLA-DR-, CD66b+CD16+CD33+HLA-DR+ and the density values of receptor expression by fluorescence intensity (MFI) were also determined (FC 500, Beckman Coulter, США). Phagocytic activity of NCs was evaluated as the contents of actively phagocytic NCs (%PhAN), volume of the engulfed S. aureus (strain 209) by assessing their phagocytic number (PhN), phagocytic index (PhI). Bacterial killing was determined as the percentages of microbe digestion (%D), digestion index (DI). The cells from AOM patients revealed a subset expressing the HLA-DR receptor СD66b+CD16+CD33+HLA-DR+NG, which is absent in the PB of CG children. The cells with primed phenotype exhibited an increased expression density of activation receptors CD16 and CD66b. Incubation of PB in AOM with recIFN2b led to an increased proportion of CD66b+CD16+CD33+HLA-DR+ NG subset which showed active phagocytosis and improved digestion processes. The present study shows the emergence of activated subset of long-lived CD66b+CD16+CD33+HLA-DR+ NCs in children with AOM. This subpopulation has APC features, by presenting AG to T lymphocytes, with preserved effector properties. In an in vitro experimental system, a positive effect of recIFN2b was demonstrated, leading to an increased number of NGs of the CD66b+CD16+CD33+HLA-DR+ subset and recovery of S. aureus phagocytosis by NGs, thus being promising in the future for development of new approaches to optimization of complex therapy in the postoperative period of AOM treatment, prevention of complications and the opportunity to alleviate the disorders in the immune system.
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& lt; i> vitro< /比;重组IFNα2B对呈递抗原cd66 <sup>+</sup>CD16<sup>+</sup>CD33<sup>+</sup>HLA<sup>-</sup>DR<sup>+</sup>急性骨髓炎患儿中性粒细胞亚群
金黄色葡萄球菌的负面影响似乎是急性骨髓炎(AOM)中感染过程传播的充分条件,这是由于免疫系统(IS),特别是中性粒细胞(NG)的功能障碍导致其消除改变。在免疫亲性物质和细胞因子的影响下,通过调节NG表型亚群来纠正AOM中NG功能障碍是值得关注的。我们的目的是评估重组IFN2b在体外对急性骨髓炎儿童中CD66b+CD16+CD33+HLA-DR-、CD66b+CD16+CD33+HLA-DR+亚群数量和表型的影响,以及对中性粒细胞吞噬功能的影响。8-15岁儿童外周血(PB)样本的研究如下:研究1组(SG1)为АOM患者(n = 24),对照组(CG)为健康儿童(n = 13)。实验组1a (SG1a)中,AOM患儿PB样本与recIFN2b (50 IU/L, 60 min, 37℃)孵育。用recIFN2b孵化前后,测定NG亚群CD66b+CD16+CD33+HLA-DR-、CD66b+CD16+CD33+HLA-DR+的数量,荧光强度(MFI)测定受体表达密度值(FC 500, Beckman Coulter, США)。通过对吞噬数(PhN)、吞噬指数(PhI)的测定,以活性吞噬细胞的含量(%PhAN)、吞噬金黄色葡萄球菌(菌株209)的体积来评价吞噬细胞的吞噬活性。细菌杀灭测定为微生物消化百分比(%D)、消化指数(DI)。 AOM患者的细胞中有一个表达HLA-DR受体СD66b+CD16+CD33+HLA-DR+NG的亚群,而CG患儿的PB中不存在该亚群。激活受体CD16和CD66b的表达密度增加。用recIFN2b在AOM中培养PB,导致CD66b+CD16+CD33+HLA-DR+ NG亚群比例增加,表现出活跃的吞噬和改善的消化过程。目前的研究表明,AOM儿童中出现了活化的长寿命CD66b+CD16+CD33+HLA-DR+ nc亚群。该亚群具有APC特征,通过向T淋巴细胞呈递AG,保留了效应特性。在体外实验系统中,证实了recIFN2b的积极作用,导致CD66b+CD16+CD33+HLA-DR+亚群的ng数量增加,并恢复了金黄色葡萄球菌的吞噬作用,从而为AOM治疗术后优化复合治疗的新方法的开发,预防并发症和缓解免疫系统紊乱提供了机会。
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