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快速上升至高原后高原综合征的分析及与急性高原病相关的潜在基因多态性。

Analysis of High-altitude Syndrome and the Underlying Gene Polymorphisms Associated with Acute Mountain Sickness after a Rapid Ascent to High-altitude.

机构信息

Institute of Cardiovascular Diseases of PLA, Xinqiao Hospital, Third Military Medical University, Chongqing, China.

出版信息

Sci Rep. 2016 Dec 16;6:38323. doi: 10.1038/srep38323.

Abstract

To investigated the objective indicators and potential genotypes for acute mountain sickness (AMS). 176 male subjects were evaluated for symptoms scores and physiological parameters at 3700 m. EPAS1 gene polymorphisms were explored and verified effects of potential genotypes on pulmonary function by inhaled budesonide. The incidence of AMS was 53.98% (95/176). The individuals who suffered from headache with anxiety and greater changes in heart rate (HR), the forced vital capacity (FVC), and mean flow velocity of basilar artery (Vm-BA), all of which were likely to develop AMS. The rs4953348 polymorphism of EPAS1 gene had a significant correlation with the SaO2 level and AMS, and a significant difference in the AG and GG genotype distribution between the AMS and non-AMS groups. The spirometric parameters were significantly lower, but HR (P = 0.036) and Vm-BA (P = 0.042) significantly higher in the AMS subjects with the G allele than those with the A allele. In summary, changes in HR (≥82 beats/min), FVC (≤4.2 Lt) and Vm-BA (≥43 cm/s) levels may serve as predictors for diagnosing AMS accompanied by high-altitude syndrome. The A allele of rs4953348 is a protective factor for AMS through HR and Vm-BA compensation, while the G allele may contribute to hypoxic pulmonary hypertension in AMS.

摘要

为了研究急性高原病(AMS)的客观指标和潜在基因型。在 3700 米处评估了 176 名男性受试者的症状评分和生理参数。探讨了 EPAS1 基因多态性,并通过吸入布地奈德验证了潜在基因型对肺功能的影响。AMS 的发病率为 53.98%(95/176)。头痛伴焦虑、心率(HR)、用力肺活量(FVC)和基底动脉平均流速(Vm-BA)变化较大的个体,均可能发生 AMS。EPAS1 基因 rs4953348 多态性与 SaO2 水平和 AMS 显著相关,且 AMS 组和非 AMS 组之间的 AG 和 GG 基因型分布存在显著差异。AMS 组的肺功能参数明显降低,但 HR(P=0.036)和 Vm-BA(P=0.042)均高于 A 等位基因。总之,HR(≥82 次/分钟)、FVC(≤4.2Lt)和 Vm-BA(≥43cm/s)水平的变化可能是诊断伴有高原综合征的 AMS 的预测指标。rs4953348 的 A 等位基因通过 HR 和 Vm-BA 补偿,是 AMS 的保护因素,而 G 等位基因可能导致 AMS 低氧性肺动脉高压。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0794/5159877/e21f872ae008/srep38323-f1.jpg

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