Martín-Vírgala Julia, Miranda-Prieto Daniel, Fernández-Villabrille Sara, Martín-Carro Beatriz, González-García Nerea, Bande-Fernández Joaquín, Díaz-Corte Carmen, Fernández-Martín José Luis, Alonso-Montes Cristina, Suárez Ana, Panizo Sara, Naves-Díaz Manuel, Rodríguez-Carrio Javier, Carrillo-López Natalia
Metabolismo Óseo, Vascular y Enfermedades Inflamatorias Crónicas, Instituto de Investigación Sanitaria del Principado de Asturias (ISPA), Oviedo, Spain.
Bone and Mineral Research Unit, Hospital Universitario Central de Asturias, Oviedo, Spain.
Front Med (Lausanne). 2024 Dec 9;11:1460021. doi: 10.3389/fmed.2024.1460021. eCollection 2024.
Cardiovascular disease is the major cause of premature death in chronic kidney disease (CKD) and vascular damage is often detected belatedly, usually evaluated by expensive and invasive techniques. CKD involves specific risk factors that lead to vascular calcification and atherosclerosis, where inflammation plays a critical role. However, there are few inflammation-related markers to predict vascular damage in CKD. This study aimed to investigate immune populations in pre-dialysis patients to (i) identify subset alterations, (ii) assess longitudinal changes, and (iii) evaluate their applicability as biomarkers of subclinical vascular indices.
43 pre-dialysis CKD patients in stages CKD-2 to CKD-5 and 38 controls were recruited at baseline and after 18-month follow-up. Aortic stiffness was determined by carotid-femoral pulse wave velocity (PWV) and abdominal aortic calcification was quantified by the Kauppila index on X-rays. Carotid intima-media thickness, the number of carotid plaques and adventitial neovascularization were evaluated by Superb Microvascular Imaging. Peripheral blood mononuclear cells were isolated and immune cell populations were assessed by flow cytometry: senescent T cells (CD4CD28), Tang (CD3CD31CD184) and derived subsets, and monocyte subsets (classical, intermediate and non-classical; and ACE expression).
Senescent T cells were increased in CKD. Despite Tang levels were unchanged compared to controls, this subset exhibited enhanced immunosenescence traits (CD28 and inverted CD4CD8 ratio) in CKD. Furthermore, Tang were negatively correlated with CKD progression. Slight alterations within monocyte subsets were observed. These findings were validated at the 18-month follow-up. Tang were correlated with several subclinical indices, and further analyses revealed an independent effect on PWV and their potential value as biomarkers. Intermediate monocytes were positively correlated with PWV.
Pre-dialysis CKD stages are hallmarked by alterations in immune cell populations related to vascular homeostasis, including early T-cell immunosenescence traits and a stage-dependent Tang depletion, which was independently related to vascular stiffness. All these features were replicated upon follow-up, thus providing validation toward our results. Our findings pave the ground for future studies addressing the functional contribution of these cellular mediators at the local level, assessing their potential predictive value in the long-term and implementing preventive strategies in the clinical setting.
心血管疾病是慢性肾脏病(CKD)过早死亡的主要原因,血管损伤往往发现较晚,通常通过昂贵且有创的技术进行评估。CKD涉及导致血管钙化和动脉粥样硬化的特定危险因素,炎症在其中起关键作用。然而,用于预测CKD血管损伤的炎症相关标志物很少。本研究旨在调查透析前患者的免疫细胞群体,以(i)识别亚群改变,(ii)评估纵向变化,以及(iii)评估它们作为亚临床血管指标生物标志物的适用性。
招募了43例CKD-2至CKD-5期的透析前CKD患者和38例对照,在基线和18个月随访后进行研究。通过颈股脉搏波速度(PWV)测定主动脉僵硬度,通过X线片上的考皮拉指数对腹主动脉钙化进行量化。通过超微血管成像评估颈动脉内膜中层厚度、颈动脉斑块数量和外膜新生血管形成。分离外周血单个核细胞,通过流式细胞术评估免疫细胞群体:衰老T细胞(CD4CD28)、Tang细胞(CD3CD31CD184)及其衍生亚群,以及单核细胞亚群(经典型、中间型和非经典型;以及ACE表达)。
CKD患者中衰老T细胞增加。尽管与对照组相比Tang细胞水平未改变,但该亚群在CKD中表现出增强的免疫衰老特征(CD28和倒置的CD4CD8比值)。此外,Tang细胞与CKD进展呈负相关。观察到单核细胞亚群有轻微改变。这些发现在18个月随访时得到验证。Tang细胞与几个亚临床指标相关,进一步分析揭示了其对PWV的独立影响及其作为生物标志物的潜在价值。中间型单核细胞与PWV呈正相关。
透析前CKD阶段的特征是与血管稳态相关的免疫细胞群体改变,包括早期T细胞免疫衰老特征和与血管僵硬度独立相关的阶段依赖性Tang细胞耗竭。所有这些特征在随访中都得到了重复,从而验证了我们的结果。我们的发现为未来研究奠定了基础,这些研究将探讨这些细胞介质在局部水平的功能作用,评估它们在长期的潜在预测价值,并在临床环境中实施预防策略。
