人体系统性炎症的自主调节:一项多中心、盲法观察性队列研究。
Autonomic regulation of systemic inflammation in humans: A multi-center, blinded observational cohort study.
机构信息
William Harvey Research Institute, Queen Mary University of London, UK; Centre for Cardiovascular and Metabolic Neuroscience, Department of Neuroscience, Physiology and Pharmacology, University College London, UK.
Department of Anaesthesia, Derriford Hospital, Plymouth Hospitals NHS Trust, Peninsula Schools of Medicine and Dentistry, Plymouth University, Plymouth, UK.
出版信息
Brain Behav Immun. 2018 Jan;67:47-53. doi: 10.1016/j.bbi.2017.08.010. Epub 2017 Aug 12.
OBJECTIVE
Experimental animal models demonstrate that autonomic activity regulates systemic inflammation. By contrast, human studies are limited in number and exclusively use heart rate variability (HRV) as an index of cardiac autonomic regulation. HRV measures are primarily dependent on, and need to be corrected for, heart rate. Thus, independent autonomic measures are required to confirm HRV-based findings. Here, the authors sought to replicate the findings of preceding HRV-based studies by using HRV-independent, exercise-evoked sympathetic and parasympathetic measures of cardiac autonomic regulation to examine the relationship between autonomic function and systemic inflammation.
METHODS
Sympathetic function was assessed by measuring heart rate changes during unloaded pedaling prior to onset of exercise, divided into quartiles; an anticipatory heart rate (AHRR) rise during this period is evoked by mental stress in many individuals. Parasympathetic function was assessed by heart rate recovery (HRR) 60s after finishing cardiopulmonary exercise testing, divided into quartiles. Parasympathetic dysfunction was defined by delayed heart rate recovery (HRR) ≤12.beats.min, a threshold value associated with higher cardiovascular morbidity/mortality in the general population. Systemic inflammation was primarily assessed by neutrophil-lymphocyte ratio (NLR), where a ratio >4 is prognostic across several inflammatory diseases and correlates strongly with elevated plasma levels of pro-inflammatory cytokines. High-sensitivity C-reactive protein (hsCRP) was also measured.
RESULTS
In 1624 subjects (65±14y; 67.9% male), lower HRR (impaired vagal activity) was associated with progressively higher NLR (p=0.004 for trend across quartiles). Delayed HRR, recorded in 646/1624 (39.6%) subjects, was associated with neutrophil-lymphocyte ratio >4 (relative risk: 1.43 (95%CI: 1.18-1.74); P=0.0003). Similar results were found for hsCRP (p=0.045). By contrast, AHRR was not associated with NLR (relative risk: 1.24 (95%CI: 0.94-1.65); P=0.14).
CONCLUSIONS
Delayed HRR, a robust measure of parasympathetic dysfunction, is independently associated with leukocyte ratios indicative of systemic inflammation. These results further support a role for parasympathetic modulation of systemic inflammation in humans.
目的
实验动物模型表明自主活动可调节全身炎症。相比之下,人类研究数量有限,仅将心率变异性(HRV)用作心脏自主调节的指标。HRV 测量主要取决于心率,并且需要进行校正。因此,需要独立的自主测量来确认基于 HRV 的发现。在这里,作者试图使用独立于 HRV 的、运动诱发的交感和副交感自主调节的心脏测量来复制先前基于 HRV 的研究结果,以检查自主功能与全身炎症之间的关系。
方法
通过测量运动前无负荷踩踏期间的心率变化来评估交感神经功能,分为四分之一;在此期间,许多人会在精神压力下引起预期的心率(AHRR)升高。通过心肺运动测试结束后 60 秒的心率恢复(HRR)来评估副交感神经功能,分为四分之一。副交感神经功能障碍定义为心率恢复(HRR)延迟≥12 次/分,这是一般人群中心血管发病率/死亡率较高的一个阈值。全身炎症主要通过中性粒细胞与淋巴细胞比值(NLR)评估,其中比值>4 与几种炎症性疾病的预后相关,并与促炎细胞因子的血浆水平升高密切相关。还测量了高敏 C 反应蛋白(hsCRP)。
结果
在 1624 名受试者(65±14 岁;67.9%为男性)中,较低的 HRR(迷走神经活动受损)与 NLR 逐渐升高相关(趋势 p=0.004)。在 1624 名受试者中的 646 名(39.6%)记录到 HRR 延迟,与中性粒细胞与淋巴细胞比值>4 相关(相对风险:1.43(95%CI:1.18-1.74);P=0.0003)。hsCRP 也有类似的结果(p=0.045)。相比之下,AHRR 与 NLR 无关(相对风险:1.24(95%CI:0.94-1.65);P=0.14)。
结论
HRR 延迟是副交感神经功能障碍的可靠测量指标,与全身炎症的白细胞比值独立相关。这些结果进一步支持副交感神经调节全身炎症在人类中的作用。
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