阻塞性睡眠呼吸暂停患者血液中未发现氧化剂生成增加的证据。
No evidence of enhanced oxidant production in blood obtained from patients with obstructive sleep apnea.
作者信息
Grabska-Kobylecka Izabela, Kobylecki Andrzej, Bialasiewicz Piotr, Krol Maciej, Ehteshamirad Golsa, Kasielski Marek, Nowak Dariusz
机构信息
Sleep and Respiratory Disorders Center of Chair of Experimental and Clinical Physiology, Medical University of Lodz, 92-215 Lodz, Mazowiecka St. 6/8, Poland.
出版信息
J Negat Results Biomed. 2008 Nov 25;7:10. doi: 10.1186/1477-5751-7-10.
BACKGROUND
Obstructive sleep apnea syndrome (OSAS) is a recognized risk factor for cardiovascular morbidity and mortality, perhaps due to causative exacerbations of systemic oxidative stress. Putative oxidative stress related to numerous episodes of intermittent hypoxia, may be an oxidants chief driving force in OSAS patients.
METHODS
We assessed the resting and n-formyl-methionyl-leucyl-phenylalanine (fMLP)- induced whole blood chemiluminescence (as a measure of oxidant production by polymorphonuclear leukocytes and monocytes), ferric reducing ability of plasma (FRAP) and H2O2 generation in the whole blood of 27 untreated OSAS patients, 22 subjects after a night of CPAP therapy and 11 controls without OSAS. All of them were matched to age, BMI (body mass index) and smoking habits. All parameters were measured before and after polysomnography-controlled sleep, individual results were obtained as a mean from duplicated experiments.
RESULTS
No significant differences were distinguished between evening and morning blood chemiluminescence, H2O2 activity and FRAP within and between all three study groups.For instance patients with untreated OSAS had similar morning and evening resting whole blood chemiluminescence (2.3 +/- 2.2 vs. 2.4 +/- 2.2 [aU.10-4 phagocytes]), total light emission after stimulation with fMLP (1790 +/- 1371 vs. 1939 +/- 1532 [aU.s.10-4 phagocytes]), as well as FRAP after 3 min. plasma incubation (602 +/- 202 vs. 671 +/- 221 [uM]). Although, in the subgroup of 11 patients with severe OSAS (apnea/hypopnea index 58 +/- 18/h and oxygen desaturation index 55 +/- 19/h), the morning vs. evening resting chemiluminescence and total light emission after stimulation with fMLP observed a propensity to elevate 2.5 +/- 2.7 vs. 1.9 +/- 1.8 [aU.10-4 phagocytes] and 1778 +/- 1442 vs. 1503 +/- 1391 [aU.s.10-4 phagocytes], respectively, these did not attain statistical significance (p > 0.05).
CONCLUSION
Our investigation exposed no evidence in the overproduction of oxidants via circulating phagocytes, once considered a culprit in the oxidative stress of OSAS patients.
背景
阻塞性睡眠呼吸暂停综合征(OSAS)是心血管疾病发病和死亡的公认危险因素,可能是由于全身氧化应激的致病性加重。与多次间歇性缺氧相关的假定氧化应激可能是OSAS患者氧化剂的主要驱动力。
方法
我们评估了27例未经治疗的OSAS患者、22例接受一晚持续气道正压通气(CPAP)治疗的受试者和11例无OSAS的对照者静息和N-甲酰甲硫氨酰-亮氨酰-苯丙氨酸(fMLP)诱导的全血化学发光(作为多形核白细胞和单核细胞产生氧化剂的指标)、血浆铁还原能力(FRAP)和全血中过氧化氢的生成情况。所有受试者在年龄、体重指数(BMI)和吸烟习惯方面相匹配。所有参数在多导睡眠图监测的睡眠前后进行测量,个体结果取重复实验的平均值。
结果
在所有三个研究组内和组间,傍晚和早晨的血液化学发光、过氧化氢活性和FRAP均无显著差异。例如,未经治疗的OSAS患者早晨和傍晚的静息全血化学发光相似(2.3±2.2对2.4±2.2 [aU·10⁻⁴吞噬细胞]),fMLP刺激后的总发光量(1790±1371对1939±1532 [aU·s·10⁻⁴吞噬细胞]),以及血浆孵育3分钟后的FRAP(602±202对671±221 [μM])。尽管在11例重度OSAS患者亚组(呼吸暂停/低通气指数58±18/小时和氧饱和度下降指数55±19/小时)中,早晨与傍晚的静息化学发光和fMLP刺激后的总发光量有升高趋势,分别为2.5±2.7对1.9±1.8 [aU·10⁻⁴吞噬细胞]和1778±1442对1503±1391 [aU·s·10⁻⁴吞噬细胞]),但这些差异未达到统计学意义(p>0.05)。
结论
我们的研究没有发现通过循环吞噬细胞过度产生氧化剂的证据,而循环吞噬细胞曾被认为是OSAS患者氧化应激的罪魁祸首。
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