| Literature DB >> 33527031 |
Hsin-I Tsai1,2, Chi-Jen Lo3, Chao-Wei Lee2,4, Jr-Rung Lin5, Wei-Chen Lee4,6, Hung-Yao Ho3,7,8, Chia-Yi Tsai1, Mei-Ling Cheng3,9,8, Huang-Ping Yu1,2.
Abstract
Early allograft dysfunction (EAD) is associated with graft failure and mortality after living donor liver transplantation (LDLT). In this study, we report biomarkers superior to other conventional clinical markers in the prediction of EAD and all-cause in-hospital mortality in LDLT patient cohort. Blood samples of living donor liver transplant recipients were collected on postoperative day 1 and analyzed by liquid chromatography coupled with mass spectrometry (LC-MS). Significant metabolites associated with the prediction of EAD were identified using orthogonal projection to latent structures-discriminant analysis (OPLS-DA). A few lipids, more specifically, lysoPC (16:0), PC (18:0/20:5), betaine and palmitic acid (C16:0) were found to effectively differentiate EAD from non-EAD on postoperative day 1. A combination of these four metabolites showed an AUC of 0.821, which was further improved to 0.846 by the addition of a clinical parameter, total bilirubin. The panel exhibits a high prognostic accuracy in prediction of all-cause in-hospital mortality and mortality within 7 postoperative days with AUCs of 0.843 and 0.954. These results show the combination of metabolomics-derived biomarkers and clinical parameters demonstrates the power of panels in diagnostic and prognostic evaluation of LDLT. AJTREntities:
Keywords: Lipidomics; betaine; early allograft dysfunction; living donor liver transplantation; lysophosphatidylcholines; phosphatidylcholines
Year: 2021 PMID: 33527031 PMCID: PMC7847515
Source DB: PubMed Journal: Am J Transl Res ISSN: 1943-8141 Impact factor: 4.060