TY - JOUR
T1 - Admission Urinary and Serum Metabolites Predict Renal Outcomes in Hospitalized Patients With Cirrhosis
AU - Bajaj, Jasmohan S.
AU - Garcia-Tsao, Guadalupe
AU - Reddy, K. Rajender
AU - O’Leary, Jacqueline G.
AU - Vargas, Hugo E.
AU - Lai, Jennifer C.
AU - Kamath, Patrick S.
AU - Tandon, Puneeta
AU - Subramanian, Ram M.
AU - Thuluvath, Paul
AU - Fagan, Andrew
AU - Sehrawat, Tejasav
AU - de la Rosa Rodriguez, Randolph
AU - Thacker, Leroy R.
AU - Wong, Florence
N1 - Funding Information:
Supported by VA Merit Review (I0CX00176) and National Center for Advancing Translational Sciences/National Institutes of Health (R21TR003095 and R21TR002024) and investigator‐initiated grants from Grifols and Mallinckrodt Pharmaceuticals.
Funding Information:
Supported by VA Merit Review (I0CX00176) and National Center for Advancing Translational Sciences/National Institutes of Health (R21TR003095 and R21TR002024) and investigator-initiated grants from Grifols and Mallinckrodt Pharmaceuticals. Potential conflict of interest: Dr. Reddy advises and received grants from Mallinckrodt. He received grants from Bristol-Myers Squibb, Gilead, Merck, Intercept, Sequana, Grifols, and Exact Sciences. Dr. O?Leary is on the speakers? bureau for Gilead and AbbVie.
Publisher Copyright:
© 2021 by the American Association for the Study of Liver Diseases.
PY - 2021/11
Y1 - 2021/11
N2 - Background and Aims: Acute kidney injury (AKI) has a poor prognosis in cirrhosis. Given the variability of creatinine, the prediction of AKI and dialysis by other markers is needed. The aim of this study is to determine the role of serum and urine metabolomics in the prediction of AKI and dialysis in an inpatient cirrhosis cohort. Approach and Results: Inpatients with cirrhosis from 11 North American Consortium of End-stage Liver Disease centers who provided admission serum/urine when they were AKI and dialysis-free were included. Analysis of covariance adjusted for demographics, infection, and cirrhosis severity was performed to identify metabolites that differed among patients (1) who developed AKI or not; (2) required dialysis or not; and/pr (3) within AKI subgroups who needed dialysis or not. We performed random forest and AUC analyses to identify specific metabolite(s) associated with outcomes. Logistic regression with clinical variables with/without metabolites was performed. A total of 602 patients gave serum (218 developed AKI, 80 needed dialysis) and 435 gave urine (164 developed AKI, 61 needed dialysis). For AKI prediction, clinical factor–adjusted AUC was 0.91 for serum and 0.88 for urine. Major metabolites such as uremic toxins (2,3-dihydroxy-5-methylthio-4-pentenoic acid [DMTPA], N2N2dimethylguanosine, uridine/pseudouridine) and tryptophan/tyrosine metabolites (kynunerate, 8-methoxykyunerate, quinolinate) were higher in patients who developed AKI. For dialysis prediction, clinical factor–adjusted AUC was 0.93 for serum and 0.91 for urine. Similar metabolites as AKI were altered here. For dialysis prediction in those with AKI, the AUC was 0.81 and 0.79 for serum/urine. Lower branched-chain amino-acid (BCAA) metabolites but higher cysteine, tryptophan, glutamate, and DMTPA were seen in patients with AKI needing dialysis. Serum/urine metabolites were additive to clinical variables for all outcomes. Conclusions: Specific admission urinary and serum metabolites were significantly additive to clinical variables to predict AKI development and dialysis initiation in inpatients with cirrhosis. These observations can potentially facilitate earlier initiation of renoprotective measures.
AB - Background and Aims: Acute kidney injury (AKI) has a poor prognosis in cirrhosis. Given the variability of creatinine, the prediction of AKI and dialysis by other markers is needed. The aim of this study is to determine the role of serum and urine metabolomics in the prediction of AKI and dialysis in an inpatient cirrhosis cohort. Approach and Results: Inpatients with cirrhosis from 11 North American Consortium of End-stage Liver Disease centers who provided admission serum/urine when they were AKI and dialysis-free were included. Analysis of covariance adjusted for demographics, infection, and cirrhosis severity was performed to identify metabolites that differed among patients (1) who developed AKI or not; (2) required dialysis or not; and/pr (3) within AKI subgroups who needed dialysis or not. We performed random forest and AUC analyses to identify specific metabolite(s) associated with outcomes. Logistic regression with clinical variables with/without metabolites was performed. A total of 602 patients gave serum (218 developed AKI, 80 needed dialysis) and 435 gave urine (164 developed AKI, 61 needed dialysis). For AKI prediction, clinical factor–adjusted AUC was 0.91 for serum and 0.88 for urine. Major metabolites such as uremic toxins (2,3-dihydroxy-5-methylthio-4-pentenoic acid [DMTPA], N2N2dimethylguanosine, uridine/pseudouridine) and tryptophan/tyrosine metabolites (kynunerate, 8-methoxykyunerate, quinolinate) were higher in patients who developed AKI. For dialysis prediction, clinical factor–adjusted AUC was 0.93 for serum and 0.91 for urine. Similar metabolites as AKI were altered here. For dialysis prediction in those with AKI, the AUC was 0.81 and 0.79 for serum/urine. Lower branched-chain amino-acid (BCAA) metabolites but higher cysteine, tryptophan, glutamate, and DMTPA were seen in patients with AKI needing dialysis. Serum/urine metabolites were additive to clinical variables for all outcomes. Conclusions: Specific admission urinary and serum metabolites were significantly additive to clinical variables to predict AKI development and dialysis initiation in inpatients with cirrhosis. These observations can potentially facilitate earlier initiation of renoprotective measures.
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U2 - 10.1002/hep.31907
DO - 10.1002/hep.31907
M3 - Article
C2 - 34002868
AN - SCOPUS:85109349586
SN - 0270-9139
VL - 74
SP - 2699
EP - 2713
JO - Hepatology
JF - Hepatology
IS - 5
ER -