Urinary pro-thrombotic, anti-thrombotic, and fibrinolytic molecules as biomarkers of lupus nephritis

Abstract Objective This study evaluates the utility of urinary pro-thrombotic molecules such as tissue factor (TF), anti-thrombotic molecules such as tissue factor pathway inhibitor (TFPI), and fibrinolytic molecules such as plasmin and d-dimer as biomarkers of lupus nephritis (LN). Methods Urine sa...

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Main Authors: Ling Qin, Samantha Stanley, Huihua Ding, Ting Zhang, Van Thi Thanh Truong, Teja Celhar, Anna-Marie Fairhurst, Claudia Pedroza, Michelle Petri, Ramesh Saxena, Chandra Mohan
Format: Article
Language:English
Published: BMC 2019-07-01
Series:Arthritis Research & Therapy
Subjects:
Online Access:http://link.springer.com/article/10.1186/s13075-019-1959-y
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spelling doaj-044571c0897943c58b272ca0ea9499562020-11-25T03:11:58ZengBMCArthritis Research & Therapy1478-63622019-07-0121111010.1186/s13075-019-1959-yUrinary pro-thrombotic, anti-thrombotic, and fibrinolytic molecules as biomarkers of lupus nephritisLing Qin0Samantha Stanley1Huihua Ding2Ting Zhang3Van Thi Thanh Truong4Teja Celhar5Anna-Marie Fairhurst6Claudia Pedroza7Michelle Petri8Ramesh Saxena9Chandra Mohan10Department of Nephrology & Rheumatology, Shanghai Tenth People’s Hospital, Tongji University School of MedicineDepartment of Biomedical Engineering, University of HoustonDepartment of Biomedical Engineering, University of HoustonDepartment of Biomedical Engineering, University of HoustonDepartment of Pediatrics, UT HoustonSingapore Immunology Network, Agency for Science, Technology, and ResearchSingapore Immunology Network, Agency for Science, Technology, and ResearchDepartment of Pediatrics, UT HoustonDepartment of Rheumatology, John Hopkins Medical UniversityDepartment of Nephrology, UT Southwestern Medical CenterDepartment of Biomedical Engineering, University of HoustonAbstract Objective This study evaluates the utility of urinary pro-thrombotic molecules such as tissue factor (TF), anti-thrombotic molecules such as tissue factor pathway inhibitor (TFPI), and fibrinolytic molecules such as plasmin and d-dimer as biomarkers of lupus nephritis (LN). Methods Urine samples from 113 biopsy-proven LN patients (89 active LN and 24 inactive LN), 45 chronic kidney disease patients, and 41 healthy controls were examined for d-dimer, plasmin, TF, and TFPI levels by ELISA. The area under the receiver operating characteristic curve (AUC) analysis, multivariate regression analysis, and Bayesian network analysis were performed to assess the diagnostic value of the assayed molecules in LN. Results Although urinary d-dimer, plasmin, TF, and TFPI were all elevated in active LN compared to all control groups, and correlated with rSLEDAI and SLICC RAS disease activity indices, urine plasmin emerged as the strongest independent predictor of eGFR and renal disease status, by multivariate regression analysis and Bayesian network analysis. Whereas urine plasmin discriminated active LN from inactive disease with an AUC of 0.84, the combination of urine plasmin and TFPI discriminated ALN from ILN with an AUC of 0.86, with both surpassing the specificity and positive predictive value of traditional markers such as anti-dsDNA and complement C3. Conclusion Both thrombogenic and thrombolytic cascades appear to be upregulated in lupus nephritis, with proteins from both cascades appearing in the urine. Of the coagulation cascade proteins surveyed, urine plasmin emerges as the strongest predictor of eGFR and clinical renal disease in patients with LN.http://link.springer.com/article/10.1186/s13075-019-1959-yLupus nephritisBiomarkersPlasminTissue factorTissue factor pathway inhibitorD-dimer
collection DOAJ
language English
format Article
sources DOAJ
author Ling Qin
Samantha Stanley
Huihua Ding
Ting Zhang
Van Thi Thanh Truong
Teja Celhar
Anna-Marie Fairhurst
Claudia Pedroza
Michelle Petri
Ramesh Saxena
Chandra Mohan
spellingShingle Ling Qin
Samantha Stanley
Huihua Ding
Ting Zhang
Van Thi Thanh Truong
Teja Celhar
Anna-Marie Fairhurst
Claudia Pedroza
Michelle Petri
Ramesh Saxena
Chandra Mohan
Urinary pro-thrombotic, anti-thrombotic, and fibrinolytic molecules as biomarkers of lupus nephritis
Arthritis Research & Therapy
Lupus nephritis
Biomarkers
Plasmin
Tissue factor
Tissue factor pathway inhibitor
D-dimer
author_facet Ling Qin
Samantha Stanley
Huihua Ding
Ting Zhang
Van Thi Thanh Truong
Teja Celhar
Anna-Marie Fairhurst
Claudia Pedroza
Michelle Petri
Ramesh Saxena
Chandra Mohan
author_sort Ling Qin
title Urinary pro-thrombotic, anti-thrombotic, and fibrinolytic molecules as biomarkers of lupus nephritis
title_short Urinary pro-thrombotic, anti-thrombotic, and fibrinolytic molecules as biomarkers of lupus nephritis
title_full Urinary pro-thrombotic, anti-thrombotic, and fibrinolytic molecules as biomarkers of lupus nephritis
title_fullStr Urinary pro-thrombotic, anti-thrombotic, and fibrinolytic molecules as biomarkers of lupus nephritis
title_full_unstemmed Urinary pro-thrombotic, anti-thrombotic, and fibrinolytic molecules as biomarkers of lupus nephritis
title_sort urinary pro-thrombotic, anti-thrombotic, and fibrinolytic molecules as biomarkers of lupus nephritis
publisher BMC
series Arthritis Research & Therapy
issn 1478-6362
publishDate 2019-07-01
description Abstract Objective This study evaluates the utility of urinary pro-thrombotic molecules such as tissue factor (TF), anti-thrombotic molecules such as tissue factor pathway inhibitor (TFPI), and fibrinolytic molecules such as plasmin and d-dimer as biomarkers of lupus nephritis (LN). Methods Urine samples from 113 biopsy-proven LN patients (89 active LN and 24 inactive LN), 45 chronic kidney disease patients, and 41 healthy controls were examined for d-dimer, plasmin, TF, and TFPI levels by ELISA. The area under the receiver operating characteristic curve (AUC) analysis, multivariate regression analysis, and Bayesian network analysis were performed to assess the diagnostic value of the assayed molecules in LN. Results Although urinary d-dimer, plasmin, TF, and TFPI were all elevated in active LN compared to all control groups, and correlated with rSLEDAI and SLICC RAS disease activity indices, urine plasmin emerged as the strongest independent predictor of eGFR and renal disease status, by multivariate regression analysis and Bayesian network analysis. Whereas urine plasmin discriminated active LN from inactive disease with an AUC of 0.84, the combination of urine plasmin and TFPI discriminated ALN from ILN with an AUC of 0.86, with both surpassing the specificity and positive predictive value of traditional markers such as anti-dsDNA and complement C3. Conclusion Both thrombogenic and thrombolytic cascades appear to be upregulated in lupus nephritis, with proteins from both cascades appearing in the urine. Of the coagulation cascade proteins surveyed, urine plasmin emerges as the strongest predictor of eGFR and clinical renal disease in patients with LN.
topic Lupus nephritis
Biomarkers
Plasmin
Tissue factor
Tissue factor pathway inhibitor
D-dimer
url http://link.springer.com/article/10.1186/s13075-019-1959-y
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