体外生成的人多形核中性粒细胞表型

Q4 Medicine
Fernando Marcos Rodríguez, C. Carabajal-Miotti, Susana Graciela Ruiz de Frattari, Adriana Haydee Vargas, N. E. González-Silva, I. Novak
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引用次数: 1

摘要

背景:在不同的物种和健康或疾病情况下,有各种各样的多形核中性粒细胞表型。目的:研究体外培养的人中性粒细胞表型。方法:在征得伦理同意的情况下采集人肝素化血样。进行多形核中性粒细胞纯化和自体培养。用LPS、fMLP或OVA刺激中性粒细胞。采用免疫荧光法。结果:体外生成了表达CD80、CD86和HLA-DR分子的“多形核中性粒细胞-抗原提呈细胞”谱。免疫荧光分析显示:CD80的表达,CTFT对照与CTFT fMLP、CTFT对照与CTFT OVA之间差异有统计学意义(p<0.05)。CD86表达量,CTFT对照组与CTFT fMLP、CTFT对照组与CTFT LPS、CTFT对照组与CTFT OVA之间差异均有统计学意义(p<0.05)。HLA-DR表达,CTFT对照与CTFT LPS比较差异有统计学意义(p<0.05)。关于“多态核中性粒细胞-CD4- cd45ro”谱,分析显示:CD4表达,CTFT对照组与CTFT fMLP之间差异有统计学意义(p<0.05)。CD45RO表达差异无统计学意义。“多形核中性粒细胞-抗原提呈细胞”表型,在30分钟释放含有CD80、CD86的NETs:配对对照样品(7.4%),LPS(12.69%)、fMLP(16.67%)和OVA(18.47%)刺激。30分钟时,配对对照样品(0%)中NETs中HLA-DR表达,LPS刺激(16.17%)。在17小时,配对对照样本(0%),卵细胞刺激(4.54%)。“多形核中性粒细胞-CD4- cd45ro”表型,释放表达CD4和C45RO分子的NETs。在30分钟,配对对照样本(0%),LPS (7.67%), fMLP(6.38%)和OVA(0%)刺激。结论:表型表达的分子可通过影响细胞微环境发挥相关作用,可作为可能的治疗靶点加以考虑。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Human Polymorphonuclear Neutrophil Phenotypes Generated in vitro
Background: There are a variety of polymorphonuclear neutrophil phenotypes described in different species and health or disease situations.  Objective: Study human neutrophil phenotypes generated in vitro. Methods: Heparinized human blood samples were collected with ethical consent. Polymorphonuclear neutrophils purification and autologous cultures was performed. Neutrophil stimulation was performed with LPS, fMLP or OVA. Immunofluorescence was applied.  Results: “Polymorphonuclear neutrophil-antigen presenting cell” profile was generated in vitro, expressing CD80, CD86 and HLA-DR molecules. Immunofluorescence analysis show: CD80 expression, significant differences between CTFT control and CTFT fMLP (p<0.05), CTFT control and CTFT OVA (p<0.0001). CD86 expression, significant differences between CTFT control and CTFT fMLP (p<0.05), CTFT control and CTFT LPS (p<0.05), CTFT control and CTFT OVA (p<0.0001). HLA-DR expression, significant differences between CTFT control and CTFT LPS (p<0.05). About “Polymorphonuclear neutrophil-CD4-CD45RO” profile, analysis show: CD4 expression, significant differences between CTFT control and CTFT fMLP (p<0.05). CD45RO expression, no significant differences. “Polymorphonuclear neutrophil-antigen presenting cell” phenotype, released NETs with CD80, CD86 at 30 minutes: paired control samples (7.4%), stimulated with LPS (12.69%), fMLP (16.67%) and OVA (18.47%). HLA-DR expression in NETs, at 30 minutes, in paired control samples (0%), stimulated with LPS (16.17%). At 17 hs, in paired control samples (0%), with OVA stimulation (4.54%). “Polymorphonuclear neutrophil-CD4-CD45RO” phenotype, released NETs expressing CD4 and C45RO molecules. At 30 minutes, in paired control samples (0%), stimulated with LPS (7.67%), fMLP (6.38%) and OVA (0%). Conclusions: Molecules expressed by phenotypes can play a relevant role by influencing cellular microenvironment and can be taken into account as possible therapeutic targets.
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CiteScore
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