Guerrero Fátima, Carmona Andrés, Jiménez Maria Jose, Ariza Francisco, Obrero Teresa, Berdud Isabel, Carrillo-Carrión Carolina, Rodríguez Mariano, Soriano Sagrario, Muñoz-Castañeda Juan R, Martín-Malo Alejandro
Maimonides Biomedical Research Institute of Cordoba (IMIBIC), University of Córdoba, Reina Sofía University Hospital, Córdoba, Spain.
Dialysis Satellite Unit, Fresenius Medical Care Services Andalucía, Córdoba, Spain.
Clin Kidney J. 2025 Jul 10;18(8):sfaf223. doi: 10.1093/ckj/sfaf223. eCollection 2025 Aug.
The first year of haemodialysis (HD) carries the highest risk of mortality, which to a large extent is attributed to the aggravation of inflammation. However, traditional markers such as C-reactive protein and interleukin-6 show only minor changes during the first year, suggesting that there are other factors involved. The present study evaluates the effect of HD on microinflammation and oxidative stress of uremic patients.
We conducted a prospective observational longitudinal study including 30 incident HD patients. Blood samples were collected at baseline and 6 and 12 months. Pro-inflammatory monocytes were quantified using flow cytometry. Proteomic analysis (Olink) was performed on serum. Concentrations of indoxyl sulphate (IS), growth differentiation factor 15 (GDF-15), oxidative status and circulating microRNA (miRNA) expression were also determined.
A new population of activated monocytes was identified that progressively increased at 1 year of HD. In addition, an increase in the serum concentration of up to 29 inflammation-related proteins was detected, including interleukins, chemokines, tumour necrosis factor family molecules, cell activation molecules and apoptosis-related proteins. Conversely, leukaemia inhibitory factor receptor was downregulated. The concentration of IS was positively correlated with GDF-15 levels. Furthermore, patients exhibited decreased expression of miRNA-126-3p, -130a-3p, -146a-5p, 223-3p, -let7a-5p and -let7b-5p.
This study highlights the impact of HD on inflammation and oxidative stress, manifested by an increase in activated monocytes and inflammatory markers. The observed subclinical inflammation associated to HD treatment may help in understanding the mechanisms of cardiovascular damage in patients on HD.
血液透析(HD)的第一年死亡率最高,这在很大程度上归因于炎症的加重。然而,传统标志物如C反应蛋白和白细胞介素-6在第一年仅显示微小变化,这表明还有其他因素参与其中。本研究评估了HD对尿毒症患者微炎症和氧化应激的影响。
我们进行了一项前瞻性观察性纵向研究,纳入30例新接受HD治疗的患者。在基线、6个月和12个月时采集血样。使用流式细胞术对促炎单核细胞进行定量。对血清进行蛋白质组分析(Olink)。还测定了硫酸吲哚酚(IS)、生长分化因子15(GDF-15)的浓度、氧化状态和循环微小RNA(miRNA)表达。
鉴定出一群新的活化单核细胞,其在HD治疗1年后逐渐增加。此外,检测到血清中多达29种炎症相关蛋白的浓度升高,包括白细胞介素、趋化因子、肿瘤坏死因子家族分子、细胞活化分子和凋亡相关蛋白。相反,白血病抑制因子受体下调。IS的浓度与GDF-15水平呈正相关。此外,患者表现出miRNA-126-3p、-130a-3p、-146a-5p、223-3p、-let7a-5p和-let7b-5p表达降低。
本研究强调了HD对炎症和氧化应激的影响,表现为活化单核细胞和炎症标志物增加。观察到的与HD治疗相关的亚临床炎症可能有助于理解HD患者心血管损伤的机制。
