Serum miR-92a is Elevated in Children and Adults with Obstructive Sleep Apnea.

Journal of molecular biomarkers & diagnosis Pub Date : 2020-01-01 Epub Date: 2020-07-27

Brendan Gongol, Fenqing Shang, Ming He, Yingshuai Zhao, Weili Shi, Manli Cheng, John Yj Shyy, Liuyi Wang, Atul Malhotra, Rakesh Bhattacharjee

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Abstract

Background: Obstructive Sleep Apnea (OSA) is a highly prevalent condition that is associated with several comorbidities including cardiovascular disease (CVD). Recent studies have revealed mixed results as to whether standard OSA therapy reverses CVD in adult patients. Thus, many advocate for earlier recognition of OSA induced CVD, as early as childhood, to prompt treatment antecedent to the onset of irreversible CVD. Here we investigated if the serum level of miR-92a, a known biomarker for CVD, can be used to identify patients with OSA in both children and adults.

Methods: Consecutive snoring patients undergoing polysomnography were recruited for determination of circulating miR-92a, in addition to inflammatory and metabolic profiles. We assessed whether circulating miR-92a was associated with OSA severity.

Results: Using two separate cohorts of adults (n=57) and children (n=13), we report a significant increase in the serum level of miR-92a in patients with severe OSA (p=0.021) and further demonstrate a significant correlation (Spearman rank correlation 0.308, p=0.010) with serum miR-92a levels and the apnea hypopnea index (AHI), a primary measure of OSA severity. Stepwise regression analysis revealed that serum miR-92a levels were independently associated with AHI (ß=0.332, p=0.003), age (ß=0.394, p=0.002) and LDL cholesterol levels (ß=0.368, p=0.004).

Conclusion: Our study is the first to establish that miR-92a is a useful biomarker for OSA severity in both children and adults. Given the canonical role of miR-92a on endothelial dysfunction, miR-92a may be useful to identify early onset CVD in OSA patients or stratify patient CVD risk to identify those that may benefit from earlier OSA treatment.

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儿童和成人阻塞性睡眠呼吸暂停患者血清miR-92a升高

背景:阻塞性睡眠呼吸暂停(OSA)是一种非常普遍的疾病，与包括心血管疾病(CVD)在内的几种合并症有关。最近的研究显示，标准的OSA治疗是否能逆转成人患者的CVD，结果好坏参半。因此，许多人主张尽早识别OSA诱发的CVD，早在儿童时期，以便在不可逆CVD发生之前及时治疗。在这里，我们研究了miR-92a(一种已知的CVD生物标志物)的血清水平是否可以用于识别儿童和成人OSA患者。方法:招募接受多导睡眠描记术的连续打鼾患者，以测定循环miR-92a，以及炎症和代谢谱。我们评估了循环miR-92a是否与OSA严重程度相关。结果:通过对成人(n=57)和儿童(n=13)两组独立队列的研究，我们发现严重OSA患者血清miR-92a水平显著升高(p=0.021)，并进一步证实血清miR-92a水平和呼吸暂停低通气指数(AHI)(衡量OSA严重程度的主要指标)之间存在显著相关性(Spearman秩相关0.308,p=0.010)。逐步回归分析显示，血清miR-92a水平与AHI (ß=0.332, p=0.003)、年龄(ß=0.394, p=0.002)和LDL胆固醇水平(ß=0.368, p=0.004)独立相关。结论:我们的研究首次证实miR-92a是儿童和成人OSA严重程度的有用生物标志物。鉴于miR-92a在内皮功能障碍中的典型作用，miR-92a可能有助于识别OSA患者的早发性CVD或分层患者CVD风险，以识别那些可能从早期OSA治疗中获益的患者。

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Journal of molecular biomarkers & diagnosis

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