Jutley Gurpreet Singh, Sahota Kalvin, Sahbudin Ilfita, Filer Andrew, Arayssi Thurayya, Young Stephen P, Raza Karim
NIHR Birmingham Biomedical Research Centre, University Hospitals Birmingham NHS Foundation Trust and Institute for Inflammation and Ageing, University of Birmingham, Birmingham, United Kingdom.
Research Into Inflammatory Arthritis Centre, Versus Arthritis, University of Birmingham, Birmingham, United Kingdom.
Front Immunol. 2021 Sep 28;12:676105. doi: 10.3389/fimmu.2021.676105. eCollection 2021.
Systemic inflammation in rheumatoid arthritis (RA) is associated with metabolic changes. We used nuclear magnetic resonance (NMR) spectroscopy-based metabolomics to assess the relationship between an objective measure of systemic inflammation [C-reactive protein (CRP)] and both the serum and urinary metabolome in patients with newly presenting RA.
Serum (n=126) and urine (n=83) samples were collected at initial presentation from disease modifying anti-rheumatic drug naïve RA patients for metabolomic profile assessment using 1-dimensional H-NMR spectroscopy. Metabolomics data were analysed using partial least square regression (PLS-R) and orthogonal projections to latent structure discriminant analysis (OPLS-DA) with cross validation.
Using PLS-R analysis, a relationship between the level of inflammation, as assessed by CRP, and the serum (p=0.001) and urinary (p<0.001) metabolome was detectable. Likewise, following categorisation of CRP into tertiles, patients in the lowest CRP tertile and the highest CRP tertile were statistically discriminated using OPLS-DA analysis of both serum (p=0.033) and urinary (p<0.001) metabolome. The most highly weighted metabolites for these models included glucose, amino acids, lactate, and citrate. These findings suggest increased glycolysis, perturbation in the citrate cycle, oxidative stress, protein catabolism and increased urea cycle activity are key characteristics of newly presenting RA patients with elevated CRP.
This study consolidates our understanding of a previously identified relationship between serum metabolite profile and inflammation and provides novel evidence that there is a relationship between urinary metabolite profile and inflammation as measured by CRP. Identification of these metabolic perturbations provides insights into the pathogenesis of RA and may help in the identification of therapeutic targets.
类风湿关节炎(RA)中的全身炎症与代谢变化相关。我们使用基于核磁共振(NMR)波谱的代谢组学来评估新诊断的RA患者中全身炎症的客观指标[C反应蛋白(CRP)]与血清和尿液代谢组之间的关系。
在初次就诊时,收集了未使用改善病情抗风湿药物的RA患者的血清(n = 126)和尿液(n = 83)样本,使用一维氢核磁共振波谱进行代谢组学分析。代谢组学数据采用偏最小二乘回归(PLS-R)和具有交叉验证的正交投影到潜在结构判别分析(OPLS-DA)进行分析。
使用PLS-R分析,可检测到通过CRP评估的炎症水平与血清(p = 0.001)和尿液(p < 0.001)代谢组之间的关系。同样,将CRP分为三分位数后,使用血清(p = 0.033)和尿液(p < 0.001)代谢组的OPLS-DA分析在最低CRP三分位数和最高CRP三分位数的患者之间进行了统计学区分。这些模型中权重最高的代谢物包括葡萄糖、氨基酸、乳酸和柠檬酸盐。这些发现表明,糖酵解增加、柠檬酸循环紊乱、氧化应激、蛋白质分解代谢和尿素循环活性增加是新诊断的CRP升高的RA患者的关键特征。
本研究巩固了我们对先前确定的血清代谢物谱与炎症之间关系的理解,并提供了新的证据,即尿液代谢物谱与通过CRP测量的炎症之间存在关系。识别这些代谢紊乱有助于深入了解RA的发病机制,并可能有助于确定治疗靶点。
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