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Risk Management and Healthcare Policy Volume 13, 2020 - Issue
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Original Research

Presepsin Level Correlates with the Development of Moderate Coronary Artery Calcifications in Hemodialysis Patients: A Preliminary Cross-Section Design Study

Ahmed F ElhabashiBahrain Defense Force Hospital, Royal Medical Services, Riffa, Kingdom of BahrainCorrespondence[email protected]
,
Leena SulaibeekhBahrain Defense Force Hospital, Royal Medical Services, Riffa, Kingdom of BahrainORCID Iconhttps://orcid.org/0000-0002-3536-5486
ORCID Icon,
Nahed SeddiqBahrain Defense Force Hospital, Royal Medical Services, Riffa, Kingdom of Bahrain
,
Salman AlaliBahrain Defense Force Hospital, Royal Medical Services, Riffa, Kingdom of Bahrain
,
Amjad K AbdulmajeedBahrain Defense Force Hospital, Royal Medical Services, Riffa, Kingdom of Bahrain
&
Nuria S PerezBahrain Defense Force Hospital, Royal Medical Services, Riffa, Kingdom of Bahrain
Pages 999-1006 | Published online: 03 Aug 2020
 
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Abstract

Purpose

End-stage renal disease patients have a high mortality rate linked to cardiovascular complications, and one of these complications is vascular calcification. This study was performed to test if presepsin, an inflammatory marker, is a predictor of coronary artery calcification (CAC) in hemodialysis (HD) patients.

Patients and Methods

This study was a cross-sectional design involving 48 HD patients and 13 control subjects. Coronary artery calcification score (CACs) was evaluated by a high resolution, ECG synchronized computed tomography of the heart using a CT calcium scoring. Presepsin and other laboratory analyses were performed on blood samples drawn before HD.

Results

Presepsin levels in HD patients were 14 times higher than healthy controls (P<0.01). Also, all laboratory tests except for vitamin D were significantly different than controls. Presepsin, phosphorus levels, and calcium-phosphate product were positively correlated with increasing CACs within groups of zero to moderate calcifications (p<0.05, R=0.459 and <0.01, R=0.591, respectively). These correlations were not seen with eGFR, PTH, calcium, vitamin D, CRP, or ESR levels. Furthermore, the log-transformed data of presepsin correlated with 1–15 months of HD vintage (p<0.05, R=0.482), whereas CACs data correlated with 1–20 months of HD vintage (p<0.05, R=0.425).

Conclusion

Although this study is preliminary and has a limited number of patients, it shows that presepsin, as an inflammatory marker, correlates with the development of moderate CAC in HD patients and may predict CAC development. Therefore, measuring presepsin and managing inflammation before and during the early phases of HD may lower coronary calcification development. However, more clinical studies in this direction are essential.

Disclosure

The authors report no conflicts of interest for this work.

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