Relationships of oxidative stress and systemic inflammation markers depending on the degree and duration of hypertension

T. Ashcheulova, N. Gerasimchuk
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引用次数: 1

Abstract

Arterial hypertension (AH) is a heterogenic and multisystem disease. It has been suggested that oxidative stress (OS) and systemic non-specific inflammation may be involved in pathogenesis of cardiovascular pathology including AH. The aim of our study was to characterize the plasma C-reactive protein (CRP) level as a marker of systemic inflammation in relation to OS development (on the base of 8-isoprostane level assessment), depending on duration and degree of AH. We examined 117 persons, of which 102 patients from 30 to 65 years old (average age – 54.7 years) who had previously not been receiving regular antihypertensive therapy had I–III degrees of essential hypertension and 15 healthy persons (average age – 48.7 years). In 34 patients from this group the degree of OS activity was determined by 8-isoprostane level as the main marker of OS. The control group consisted of 10 healthy persons, by age and gender comparable with the study group. Determination of plasmatic CRP levels and the level of 8-isoprostane in the serum was performed by ELISA. The study established an increase of the plasmatic CRP levels in patients with hypertension, and a statistically significant increase of serum 8-isoprostane content in hypertensive patients compared to the control group. When assessing the relationship of 8-isoprostane and CRP content in patients with different degrees of hypertension we found that the strongest positive relationship between their levels was observed in the case of I degree hypertension. This may indicate the role of oxidative stress in the pathogenesis of hypertension as a damaging mechanism which contributes to the activation of immune mechanisms and further progression of the disease. Increased CRP and 8-isoprostane levels confirm the involvement of autoimmune mechanisms and oxidative stress in the pathogenesis of hypertension. The level of C-reactive protein is dependent on the duration of hypertension, while the 8-isoprostane levels – only on degree of hypertension. A raised level of C-reactive protein can be used as an independent marker of systemic inflammation in patients with arterial hypertension.
氧化应激和全身炎症标志物与高血压程度和持续时间的关系
动脉高血压(AH)是一种异质多系统疾病。氧化应激(OS)和全身性非特异性炎症可能参与包括AH在内的心血管病理的发病机制。我们研究的目的是根据AH的持续时间和程度,将血浆c反应蛋白(CRP)水平作为与OS发展相关的全身炎症的标志物(基于8-异前列腺素水平评估)。我们检查了117人,其中102例患者年龄在30 - 65岁(平均年龄54.7岁),以前没有接受常规降压治疗,有I-III级原发性高血压,15例健康人(平均年龄48.7岁)。本组34例患者以8-异前列腺素水平作为OS的主要标志物,测定OS活性程度。对照组由10名健康的人组成,按年龄和性别与研究组相当。ELISA法测定血浆CRP水平和血清8-异前列腺素水平。研究证实高血压患者血浆CRP水平升高,与对照组相比,高血压患者血清8-异前列腺素含量升高具有统计学意义。在评估不同程度高血压患者8-异前列腺素与CRP含量的关系时,我们发现,在1度高血压患者中,它们之间的正相关关系最强。这可能表明氧化应激在高血压发病机制中的作用,作为一种损伤机制,有助于激活免疫机制和疾病的进一步进展。升高的CRP和8-异前列腺素水平证实了自身免疫机制和氧化应激参与高血压的发病机制。c反应蛋白水平与高血压持续时间有关,而8-异前列腺素水平仅与高血压程度有关。c反应蛋白水平升高可作为动脉性高血压患者全身性炎症的独立标志物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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