Pre-transplant Biomarkers of Immune Dysfunction Improve Risk Assessment of Post-transplant Mortality Compared With Conventional Clinical Risk Scores.
J Esli Medina-MoralesGuergana G PanayotovaDuc T NguyenEdward A GravissGagan S PrakashJeffery A MarshSopio SimonishviliYash ShahTumininu AyorindeYong QinLianhua JinTheofano ZoumpouLaurie J MinzeFlavio PaternoArpit AminGrace Lee RiddleR Mark GhobrialJames V GuarreraKeri E LunsfordPublished in: Research square (2023)
Introduction: There is a critical need to accurately stratify liver transplant (LT) candidates' risk of post-LT mortality prior to LT to optimize patient selection and avoid futility. Here, we compare current pre -LT clinical risk scores with the recently developed Liver Immune Frailty Index (LIFI) for prediction of post -LT mortality. LIFI measures immune dysregulation based on pre-LT plasma HCV IgG, MMP3 and Fractalkine. LIFI accurately predicts post-LT mortality, with LIFI-low corresponding to 1.4% 1-year post-LT mortality compared with 58.3% for LIFI-high (C-statistic=0.85). Methods : LIFI was compared to MELD, MELD-Na, MELD 3.0, D-MELD, MELD-GRAIL, MELD-GRAIL-Na, UCLA-FRS, BAR, SOFT, P-SOFT, and LDRI scores on 289 listed patients (T 0 ). Survival, hazard of early post-LT death, and discrimination power (C-statistic) were assessed (Stata v17). Results : LIFI showed superior discrimination (highest C-statistic) of post-LT mortality when compared to all other risk scores, irrespective of biologic MELD. On univariate analysis, the LIFI showed a significant correlation with mortality at 3- and 6-months, as well as 1-, 3-, and 5-years. No other pre-LT scoring system significantly correlated with post-LT mortality . On bivariate adjusted analysis, African American race and pre-LT cardiovascular disease were significantly associated with early- and long-term post-LT mortality (p<0.05). Patients who died within 1-yr following LT had a significantly higher incidence of infections, including 30-day and 90-day incidence of any infection, pneumonia, abdominal infections, and UTI (p<0.05). Conclusions : LIFI, which measures pre-LT biomarkers of immune dysfunction, more accurately predicts risk of post-LT futility compared with current clinical predictive models. Pre-LT assessment of immune dysregulation may be critical in predicting mortality after LT and may optimize selection of candidates with lowest risk of futile outcomes.
Keyphrases
- cardiovascular events
- risk factors
- cardiovascular disease
- risk assessment
- african american
- rheumatoid arthritis
- oxidative stress
- intensive care unit
- end stage renal disease
- chronic kidney disease
- case report
- adipose tissue
- human immunodeficiency virus
- newly diagnosed
- skeletal muscle
- free survival
- heavy metals
- data analysis
- acute respiratory distress syndrome
- cell migration