首页> 外文期刊>Sleep & breathing =: Schlaf & Atmung >Decrease of perforin positive CD3 + γδ-T cells in patients with obstructive sleep disordered breathing
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Decrease of perforin positive CD3 + γδ-T cells in patients with obstructive sleep disordered breathing

机译:阻塞性睡眠无序呼吸患者的穿孔素阳性CD3 +γδ-T细胞降低

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Abstract Introduction Sleep related breathing disorders (SRBD) cause sleep fragmentation, intermittent hypoxia or a combination of both leading to homeostasis perturbations, including in the immune system. We investigated whether SRBD patients with or without intermittent hypoxia show substantial differences in perforin and granzyme-B positive peripheral blood lymphocytes. Methods A total of 87 subjects were included and distributed as follows: 24 controls (C), 19 patients with respiratory effort related arousals due to increased upper airway resistance (UAR) without hypoxic events, 24 obese patients with obstructive sleep apnea (OSA) (oOSA), and 20 without obesity (noOSA). After polysomnographic recording, we analyzed in fasting blood samples routine hematologic and biochemical parameters and the percentage of lymphocytes containing the proteins perforin and granzyme-B (GrB). Kruskal-Wallis tests and a posteriori multiple comparisons were applied for statistical analysis of results. Results Perforin-positive γδ-cells revealed significant differences between groups ( p ?=?0.017), especially between the Control group and the oOSA ( p -value?=?0.04); the remaining SRBD groups also showed differences from the control (C vs UAR: p ?=?0.08; C vs noOSA?=?0.09), but they did not raise to statistical significance. There were no differences among the SRBD groups. Granzyme-B cells were decreased in SRBD patients, but the differences were not statistically significant. No additional statistical significant result was found in the other investigated lymphocyte subsets. Conclusions Obstructive sleep-disordered breathing is associated with a decrease in perforin-positive CD3 + γδ-T cells. Although this finding was detected in lean patients without intermittent hypoxia, the reduction was only statistically significant in obese patients with severe OSA. Because CD3 + γδ-T cells play an important role in the control of tumor cells, our findings are directly relevant for the study of the association of OSA and cancer.
机译:摘要睡眠睡眠相关呼吸障碍(SRBD)引起睡眠碎片,间歇性缺氧或导致稳态扰动的组合,包括免疫系统。我们调查了是否有或没有间歇性缺氧的SRBD患者显示出对穿孔素和Granzyme-B阳性外周血淋巴细胞的显着差异。方法总共包括87个受试者并分发如下:24例对照(C),19例呼吸努力患者相关的唤醒患者由于上气道阻力增加(UAR)没有缺氧事件,24例肥急睡眠呼吸暂停症(OSA)( OOSA)和20没有肥胖(Noosa)。在多面体摄影记录之后,我们在空腹血液样本中分析常规血液学和生化参数以及含有蛋白质穿孔素和Granzyme-B(GRB)的淋巴细胞的百分比。 Kruskal-Wallis测试和后验多重比较用于结果统计分析。结果Perforin阳性γδ细胞揭示了组之间的显着差异(P?= 0.017),尤其是对照组和OOSA(P-value?= 0.04);剩余的SRBD组还显示出与对照的差异(C VS UAR:P?= 0.08; C vs noosa?= 0.09),但它们没有提高统计显着性。 SRBD组之间没有差异。 SRBD患者中颗粒酶-B细胞减少,但差异没有统计学意义。在其他研究的淋巴细胞亚群中没有发现额外的统计显着结果。结论阻塞性睡眠无序呼吸与穿孔阳性CD3 +γδ-T细胞的减少有关。虽然在没有间歇性缺氧的瘦患者中检测到这种发现,但减少在肥胖患者严重OSA患者中只有统计学意义。因为CD3 +γδ-T细胞在肿瘤细胞的控制中发挥着重要作用,因此我们的研究结果与OSA和癌症协会的研究直接相关。

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