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Immune response genes in the post-Q-fever fatigue syndrome, Q fever endocarditis and uncomplicated acute primary Q fever

机译:Q发热后疲劳综合征,Q发热心内膜炎和单纯性急性Q发热的免疫反应基因

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Background: The influence of immune response gene variations on the development of chronic complications of Q fever is presently unclear. Aim: To compare the frequencies of allelic polymorphisms in immune response genes in different Q fever patient groups. Design: Genetic association study. Methods: We measured the frequencies of immune response gene variants in: (ⅰ) an expanded group of 31 post-Q-fever fatigue patients (QFS); (ⅱ) 22 Q fever endocarditis patients (QFE); and (ⅲ) 22 patients who made an uncomplicated recovery from their initial attack of primary acute Q fever, comparing them with various standard control panels from the general population. Results: There were significant differences between the three Q fever groups. QFS patients differed from both QFE and uncomplicated patients and controls in the frequency of carriage of HLA-DRB1~*11 and of the 2/2 genotype of the interferon-γ intron1 microsatellite. Carriage of the HLA DRB1~*11 allele was associated with reduced interferon-γ and IL-2 responses from PBMC stimulated with ligand in short-term culture. QFE showed differences in the IL-10 promoter micro-satellites R and G and had higher frequencies of the TNF-α receptor Ⅱ 196R polymorphism. Q fever patients who had made an uncomplicated recovery differed from those with QFS or QFE, but were not significantly different in allelic frequencies to the control panels. Discussion: These immunogenetic differences support the concept of different immune states in chronic Q fever, determined by genetic variations in host immune responses, rather than by solely properties of Coxiella burnetii.
机译:背景:目前尚不清楚免疫应答基因变异对Q发热慢性并发症发展的影响。目的:比较不同Q热病患者免疫应答基因中等位基因多态性的频率。设计:遗传关联研究。方法:我们在以下人群中测量了免疫应答基因变异的频率:(ⅰ)扩大了一组31名Q发热后疲劳患者(QFS); (ⅱ)22例Q型发烧心内膜炎患者(QFE); (ⅲ)22例患者,他们从最初的急性Q发热初期发作中获得了简单的康复,并将其与普通人群的各种标准对照组进行了比较。结果:三个Q发热组之间存在显着差异。 QFS患者不同于QFE患者和单纯患者,其HLA-DRB1〜* 11携带频率和干扰素-γintron1微卫星的2/2基因型的携带频率有所不同。 HLA DRB1〜* 11等位基因的携带与短期培养中配体刺激的PBMC的干扰素-γ和IL-2反应降低有关。 QFE在IL-10启动子微卫星R和G上显示出差异,并且TNF-α受体Ⅱ196R多态性的频率更高。恢复简单的Q型发热患者与QFS或QFE患者不同,但与对照组的等位基因频率无明显差异。讨论:这些免疫遗传学差异支持慢性Q发烧中不同免疫状态的概念,这是由宿主免疫反应的遗传变异决定的,而不是由柯氏杆菌的特性决定的。

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