Clinical and pathogenetic features of the development of endothelial dysfunction in patients with chronic kidney disease and its contribution to the development of cognitive impairments

M. G. Panchenko, M. Gasanov, M. M. Batyushin, A. A. Kazanskaya, G. I. Appakov
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Abstract

THE AIM: to study the clinical and pathogenetic features of the development of endothelial dysfunction (ED) in patients with chronic kidney disease stages 3A-5D and its contribution to the development of cognitive impairment.PATIENTS AND METHODS: The study included 80 patients with CKD stages 3A-5D aged from 26 to 79 years (average age 58.9 ± 1.4 years): 43 women (average age 60.1 ± 1.9 years) and 37 men (average age 57.4±2.3 years). The patients were divided into 2 groups: group 1 included 40 patients with CKD 3A-5 (average age 59.9 ± 2.1 years), group 2 included 40 patients with CKD 5D (average age 58.1 ± 2 years). All patients underwent common and biochemical blood tests, the levels of endothelial nitric oxide synthase 3 (eNOS-3) and endothelin-1 (END-1) were determined, an endothelium-dependent vasodilation test (EDVD) was performed, testing for the presence and severity of cognitive disorders using the Montreal Cognitive Assessment Scale (MoCA) and the Mini Mental State Examination (MMSE).RESULTS: The prevalence of ED in the overall cohort of patients based on the results of a positive test with EDVD was 55 % of cases. ED was statistically significantly more often detected in the group of patients receiving hemodialysis treatment compared to patients in group 1: 70  % versus 40 %, respectively (p=0.007). The level of eNOS-3 in group 1 was higher compared to group 2 and amounted to 1.01±0.5 ng/ml versus 0.76±0.3 ng/ml (p=0.008). While the level of END-1 was statistically significantly lower in patients of group 1 compared to group 2 and amounted to 45.4±9.1 pg/ml versus 54.9±4.7 pg/ml (p<0.001). Cognitive impairments were identified in the general cohort: according to MMSE – in 67.5 % of cases, according to MoCA – in 71.3 %, and were more common in group 2. There were no statistically significant relationships between the results of the EDVD test and testing on the MoCA and MMSE scales. The level of eNOS-3 was lower in the subgroup of patients with cognitive impairment according to MoCA compared to the subgroup without it: 0.73±0.1 ng/ ml versus 0.94±0.2 ng/ml (p=0.127). The content of END-1 was statistically significantly higher in the subgroup of patients with cognitive impairment according to MoCA – 52.98±1.2 pg/ml compared to the subgroup without it – 47.67±1.5 pg/ml (p=0.043). When assessing the relationship between the levels of eNOS-3 and END-1 and the results of the EDVD test, it was found that in patients with a positive test in group 1, the level of eNOS-3 was statistically significantly higher compared to group 2 (p=0.01). An inverse relationship was observed for END-1; its level was lower in patients of group 1 compared to group 2 (p<0.01).CONCLUSION. Thus, the study revealed a high prevalence of endothelial dysfunction in patients with CKD stages 3A-5D. Progressive loss of renal function leads to dysregulation of the molecular mechanisms controlling vascular tone and the development of ED. eNOS-3 and END-1 have demonstrated high sensitivity for ED verification, and their detection improves the quality of the EDVD test. The development and progression of ED in patients with CKD is a multifactorial process that leads to hemodynamic disturbances in various organs and tissues, their damage and has a negative impact on the patient’s quality of life, his cognitive status and life expectancy.
慢性肾病患者发生内皮功能障碍的临床和病理特征及其对认知障碍发展的贡献
目的:研究慢性肾脏病 3A-5D 期患者发生内皮功能障碍 (ED) 的临床和病理特征及其对认知障碍发展的贡献:其中女性 43 人(平均年龄为 60.1±1.9 岁),男性 37 人(平均年龄为 57.4±2.3 岁)。患者分为两组:第一组包括 40 名 CKD 3A-5 患者(平均年龄(59.9±2.1)岁),第二组包括 40 名 CKD 5D 患者(平均年龄(58.1±2)岁)。所有患者都接受了普通和生化血液检测,测定了内皮一氧化氮合酶 3(eNOS-3)和内皮素-1(END-1)的水平,进行了内皮依赖性血管舒张试验(EDVD),并使用蒙特利尔认知评估量表(MoCA)和迷你精神状态检查(MMSE)检测了认知障碍的存在和严重程度。结果:根据 EDVD 阳性测试结果,ED 在所有患者中的发病率为 55%。与第一组患者相比,接受血液透析治疗的患者中发现 ED 的比例明显更高:分别为 70% 对 40% (P=0.007)。第 1 组患者的 eNOS-3 水平高于第 2 组,分别为 1.01±0.5 纳克/毫升和 0.76±0.3 纳克/毫升(P=0.008)。与第二组相比,第一组患者的END-1水平明显降低,为45.4±9.1 pg/ml对54.9±4.7 pg/ml(P<0.001)。在总体队列中发现了认知障碍:根据 MMSE,67.5% 的病例存在认知障碍,根据 MoCA,71.3% 的病例存在认知障碍,并且在第 2 组中更为常见。 EDVD 测试结果与 MoCA 和 MMSE 量表测试结果之间没有显著的统计学关系。与无认知障碍的亚组相比,有认知障碍(MoCA)的亚组患者的 eNOS-3 水平较低:0.73±0.1纳克/毫升对0.94±0.2纳克/毫升(P=0.127)。从统计学角度看,MoCA 结果显示有认知障碍的亚组患者的END-1含量为(52.98±1.2)pg/ml,而无认知障碍的亚组患者的END-1含量为(47.67±1.5)pg/ml(p=0.043)。在评估 eNOS-3 和 END-1 的水平与 EDVD 测试结果之间的关系时发现,在测试结果呈阳性的第 1 组患者中,eNOS-3 的水平在统计学上明显高于第 2 组(p=0.01)。END-1呈反向关系;与第2组相比,第1组患者的END-1水平较低(P<0.01)。因此,该研究显示,在 CKD 3A-5D 期患者中,内皮功能障碍的发病率很高。肾功能的逐渐丧失导致控制血管张力的分子机制失调,并导致 ED 的发生。eNOS-3 和 END-1 对 ED 的验证具有较高的灵敏度,它们的检测提高了 EDVD 检测的质量。慢性肾功能衰竭患者 ED 的发生和发展是一个多因素过程,会导致各种器官和组织的血流动力学紊乱及其损伤,并对患者的生活质量、认知状态和预期寿命产生负面影响。
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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