LAQV, REQUIMTE, Laboratório de Química Aplicada, Departamento de Ciências Químicas, Faculdade de Farmácia, Universidade do Porto, Porto, Portugal.
UCIBIO, REQUIMTE, Laboratório de Bioquímica, Departamento de Ciências Biológicas, Faculdade de Farmácia, Universidade do Porto, Porto, Portugal.
Sci Rep. 2021 Jul 20;11(1):14768. doi: 10.1038/s41598-021-94075-x.
Chronic inflammation plays an important role in the progression and outcome of chronic kidney disease (CKD). The circulating levels of the inflammatory biomarkers interleukin 6 (IL6) and pentraxin 3 (PTX3) are enhanced in CKD patients, and are associated with the progression of the disease and with higher risk for cardiovascular events, the major cause of death in CKD patients. Our aim was to study how specific polymorphisms of IL6 and PTX3 encoding genes affect the inflammatory response and outcome of end-stage renal disease (ESRD) patients on dialysis. Methodology included the analysis of two single nucleotide polymorphisms (SNP), namely the IL6 (rs1800795) polymorphism in the promoter region (-174G > C), and the PTX3 (rs2305619) polymorphism in the intron 1 (+ 281A > G), which were analyzed in ESRD patients on dialysis and in a group of heathy individuals. The allelic frequencies, genotype distribution and their association with circulating levels of the inflammatory markers C-reactive protein (CRP), IL6, growth differentiation factor 15 (GDF15) and PTX3, were determined in ESRD patients. Events of death were recorded along one year, to assess the association of the studied SNPs with all-cause mortality and the inflammatory biomarkers, in ESRD patients. Results showed that the allelic frequencies and genotype distribution for IL6 and PTX3 SNPs in the control group and ESRD patients were similar and in agreement with other European reports. For the IL6 polymorphism, we found a trend towards higher levels of high-sensitivity (hs) CRP, IL6 and PTX3 in the homozygous genotypes; the CC genotype also showed the highest levels of GDF15. The mortality rate after the 1-year follow-up was 10.4%. The CC genotype (IL6 SNP) was associated to a higher risk of mortality and deceased patients carrying this genotype also showed the highest levels of hsCRP. Regarding the studied PTX3 SNP, the AA genotype was linked to an enhanced inflammatory response, showing the highest values of hsCRP and IL6. Nevertheless, this genotype had no significant impact on the mortality rate. In conclusion, both studied SNPs seem to modulate the inflammatory response in ESRD and may, therefore, be determinant on disease progression and patients' outcome. Our data also highlights the importance of research on genetic variants that, although less frequent, may have significant biological value.
慢性炎症在慢性肾脏病 (CKD) 的进展和结局中起着重要作用。循环中白细胞介素 6 (IL6) 和五聚素 3 (PTX3) 等炎症生物标志物的水平在 CKD 患者中升高,与疾病的进展以及心血管事件风险增加相关,心血管事件是 CKD 患者的主要死亡原因。我们的目的是研究 IL6 和 PTX3 编码基因的特定多态性如何影响透析终末期肾病 (ESRD) 患者的炎症反应和结局。方法包括分析两个单核苷酸多态性 (SNP),即启动子区域 (-174G > C) 的 IL6 (rs1800795) 多态性和内含子 1 中的 PTX3 (rs2305619) 多态性 (+ 281A > G),这些 SNP 分别在透析 ESRD 患者和一组健康个体中进行分析。确定 ESRD 患者的等位基因频率、基因型分布及其与循环中炎症标志物 C 反应蛋白 (CRP)、IL6、生长分化因子 15 (GDF15) 和 PTX3 的关系。记录一年中所有的死亡事件,以评估研究 SNP 与 ESRD 患者全因死亡率和炎症标志物的关系。结果表明,对照组和 ESRD 患者的 IL6 和 PTX3 SNP 的等位基因频率和基因型分布相似,与其他欧洲报告一致。对于 IL6 多态性,我们发现同型基因型中 hs-CRP、IL6 和 PTX3 的水平较高呈趋势;CC 基因型也显示出 GDF15 的最高水平。随访 1 年后的死亡率为 10.4%。CC 基因型 (IL6 SNP) 与更高的死亡率风险相关,携带该基因型的死亡患者也显示出 hs-CRP 水平最高。关于研究的 PTX3 SNP,AA 基因型与增强的炎症反应相关,hs-CRP 和 IL6 的值最高。然而,该基因型对死亡率没有显著影响。总之,这两个研究 SNP 似乎调节 ESRD 中的炎症反应,因此可能是疾病进展和患者预后的决定因素。我们的数据还强调了研究遗传变异的重要性,尽管这些遗传变异不太常见,但它们可能具有重要的生物学价值。
