Progressive Increase of Inflammatory Biomarkers in Chronic Kidney Disease and End-Stage Renal Disease

Sharain, Korosh; Hoppensteadt, Debra; Bansal, Vinod; Singh, Ajay K.; Fareed, Jawed

doi:10.1177/1076029612454935

Cited by 28 publications

(26 citation statements)

References 28 publications

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“…Additional risks have been attributed to the presence of nontraditional risk factors, such as inflammation, which have been shown to promote proliferation and infiltration of inflammatory cells into the tunica intima of small arteries, leading to the development of atherosclerosis and stenosis [10]. An association between a decline in RRF in patients with CKD and progressively increased level of systemic inflammatory burden which is most marked in those receiving renal replacement therapy, such as haemodialysis, has been well established [11, 12]. At present, there is no clear evidence to suggest any significant difference in the systemic inflammatory burden based on the type of dialysis modality received (i.e., haemodialysis versus peritoneal dialysis) [13].…”

Section: Introductionmentioning

confidence: 99%

Clinical Causes of Inflammation in Peritoneal Dialysis Patients

Cho

Hawley

Johnson

2014

International Journal of Nephrology

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Inflammation at both systemic and local intraperitoneal levels commonly affects peritoneal dialysis (PD) patients. Interest in inflammatory markers as targets of therapeutic intervention has been considerable as they are recognised as predictors of poor clinical outcomes. However, prior to embarking on strategies to reduce inflammatory burden, it is of paramount importance to define the underlying processes that drive the chronic active inflammatory status. The present review aims to comprehensively describe clinical causes of inflammation in PD patients to which potential future strategies may be targeted.

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Section: Introductionmentioning

confidence: 99%

Clinical Causes of Inflammation in Peritoneal Dialysis Patients

Cho

Hawley

Johnson

2014

International Journal of Nephrology

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“…The main finding of our study, conducted in a large, hospital‐based dialysis center, is that the prevalence of positive D‐dimer values is high not only in the general hemodialysis population (75% of positive values), but also in patients without additional acute or chronic predisposing disease (52% of positive values), which limits its usefulness for exclusion of VTE in everyday clinical practice. Several previous studies have shown that patients with chronic kidney disease not on dialysis have higher D‐dimer values than healthy population, but still within normal range, and that D‐dimer levels correlate with the level of renal function . In dialysis patients, a high prevalence of positive values was reported in patients without symptoms of VTE .…”

Section: Discussionmentioning

confidence: 97%

“…Several previous studies have shown that patients with chronic kidney disease not on dialysis have higher D-dimer values than healthy population, but still within normal range, and that D-dimer levels correlate with the level of renal function. 10,11 In dialysis patients, a high prevalence of positive values was reported in patients without symptoms of VTE. 12 Furthermore, in a study of patients referred to computed tomography angiography to rule out pulmonary embolism, none of the 29 patients with eGFR <30 mL/min had a negative D-dimer, although in only 17% of them pulmonary embolism was confirmed.…”

Section: Discussionmentioning

confidence: 99%

D‐dimer levels in maintenance hemodialysis patients: High prevalence of positive values also in the group without predisposing diseases

Gubenšek

Lolic

Ponikvar

et al. 2015

Hemodialysis International

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We aimed to estimate the prevalence of elevated D-dimer levels in all chronic hemodialysis patients and those without additional disease, and to identify factors associated with increased D-dimer. In 167 chronic hemodialysis patients from our center, D-dimer was measured before dialysis. The effects of age, C-reactive protein (CRP), recent acute illness, vascular access, anticoagulation type, dialysis vintage, and chronic diseases, considered to predispose for increased D-dimer levels, were analyzed. The median D-dimer in the whole group was 966 (inter-quartile range [IQR] 524-1947) μg/L and was positive (>500 μg/L) in 75% of cases. D-dimer was positive in 91% of patients with acute illness, 76% of those with predisposing chronic diseases, but was still positive in 52% of patients without additional disease (i.e., acute illness or predisposing chronic diseases) - median D-dimer was 538.5 (IQR 359-966) μg/L. D-dimer was correlated to patients' age, but not dialysis vintage. In univariate analysis, the D-dimer levels were significantly higher in patients with atrial fibrillation, ischemic heart disease, recent acute illness, increased CRP, dialyzed over a catheter, and on citrate anticoagulation. Multivariate logistic regression showed that only age >65 years (odds ratio [OR] 2.93), catheter (OR 4.86), and positive CRP (OR 4.07) were independently associated with positive D-dimer at 500 μg/L cut-off, while the significance of age disappeared at 2000 μg/L cut-off. To conclude, the high prevalence of positive D-dimer values even in hemodialysis patients without additional disease limits the use of D-dimer for exclusion of thromboembolic diseases in hemodialysis patients.

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“…Thus, soluble TM (sTM) identifiable in plasma not only reflects endothelial injury, but also inflammation [30]. Nevertheless, the clinical predictive value of sTM has been reported in sepsis [31], metabolic syndrome [32] and chronic kidney disease [33].…”

Section: Biomarkers Of the Endothelial Dysfunctionmentioning

confidence: 99%

Towards a comprehensive endothelial biomarkers profiling and endothelium-guided pharmacotherapy

Walczak

Suraj

Kuś

et al. 2015

Pharmacological Reports

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Endothelial dysfunction has prognostic, diagnostic and therapeutic significance in cardiovascular disease, but the endothelial phenotype is still not measured routinely to stratify the cardiovascular risk and tailor therapy. Flow-mediated dilation (FMD), the gold-standard technique for the functional assessment of endothelial function that is increasingly used in clinical settings measures the nitric oxide (NO)-dependent function only. However, the endothelial dysfunction involves a plethora of pathophysiologically important biochemical changes beyond alterations in the NO bioavailability. Still, in many diseases, some plasma protein biomarkers reflecting the pro-thrombotic and the pro-inflammatory endothelial phenotypes have poor selectivity, specificity, and a weak predictive value if they are used alone. Therefore, a multi biomarker strategy seems to be a reasonable and promising alternative. Here, we propose a multi-biomarker strategy to diagnose the endothelial dysfunction and to monitor the efficacy of an endothelium-targeted therapy. This strategy is based on the panel of endothelial biomarkers, reflecting various aspects and mechanisms of dysfunctional endothelium. The potential of an advanced analytical platform like the ultra-high performance liquid chromatography (UHPLC) coupled to mass spectrometry-based multiple reaction monitoring for simultaneous quantification of multiple endothelial biomakers is also discussed.

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Progressive Increase of Inflammatory Biomarkers in Chronic Kidney Disease and End-Stage Renal Disease

Cited by 28 publications

References 28 publications

Clinical Causes of Inflammation in Peritoneal Dialysis Patients

Clinical Causes of Inflammation in Peritoneal Dialysis Patients

D‐dimer levels in maintenance hemodialysis patients: High prevalence of positive values also in the group without predisposing diseases

Towards a comprehensive endothelial biomarkers profiling and endothelium-guided pharmacotherapy

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