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Predicting dyslipidemia after liver transplantation: A significant role of recipient metabolic inflammation profile

机译:肝移植后预测血脂血症:受体代谢炎症谱的重要作用

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BACKGROUND Post-transplant dyslipidemia (PTDL) is a common complication in liver recipients and can cause morbidity and threaten graft function. The crosstalk between metabolic inflammation and dyslipidemia has been recently revealed. However, the role of grafts’ and recipients’ metabolic status in the development of PTDL has not been evaluated. AIM To investigate the association of recipients’ metabolic inflammation status with PTDL and construct a predictive model. METHODS A total of 396 adult patients who received primary liver transplantation between 2015 and 2017 were enrolled. Metabolomics and cytokines were analyzed using recipients’ pre-transplant peripheral blood in a training set ( n = 72). An integrated prediction model was established according to the clinical risk factors and metabolic inflammation compounds and further verified in a validation set ( n = 144). RESULTS The serum lipid profile took 3 mo to reach homeostasis after liver transplantation. A total of 278 (70.2%) liver recipients developed PTDL during a follow-up period of 1.78 (1.00, 2.97) years. The PTDL group showed a significantly lower tumor-free survival and overall survival than the non-PTDL group in patients with hepatocellular carcinoma ( n = 169). The metabolomic analysis showed that metabolic features discriminating between the PTDL and non-PTDL groups were associated with lipid and glucose metabolism-associated pathways. Among metabolites and cytokines differentially expressed between the two groups, interleukin-12 (p70) showed the best diagnostic accuracy and significantly increased the predictive value when it was incorporated into the clinical model in both training and validation sets. CONCLUSION Recipients’ pre-transplant serum interleukin-12 (p70) level is associated with the risk of PTDL and has potential clinical value for predicting PTDL.
机译:背景技术移植后血脂血症(PTDL)是肝脏受体中的常见并发症,可以引起发病率和威胁的移植功能。最近已经揭示了代谢炎症和血脂血症之间的串扰。然而,尚未评估移植物的代谢状态在PTDL发展中的作用。目的探讨接受者的代谢炎症状态与PTDL的关联,构建预测模型。方法共有2015年至2017年间接受初级肝移植的396名成年患者。在训练组中使用受者的预移植前外周血(n = 72)分析代谢组科和细胞因子。根据临床风险因素和代谢炎症化合物建立了一体化预测模型,并在验证组中进一步验证(n = 144)。结果血清脂质型材服用3mo肝移植后达到稳态。共有278名(70.2%)肝脏受援人员在1.78(1.00,2.97)年后续期间开发了PTDL。 PTDL组在肝细胞癌(n = 169)中显示出比非PTDL组显着降低肿瘤生存和总存活。代谢组分析表明,PTDL和非PTDL基团之间区分的代谢特征与脂质和葡萄糖代谢相关途径有关。在两组之间差异表达的代谢物和细胞因子中,白细胞介素-12(P70)显示了最佳的诊断准确性,并且当在训练和验证集中纳入临床模型时显着提高了预测值。结论接受者的移植前血清白细胞介素-12(P70)水平与PTD1的风险有关,并且具有预测PTD1的潜在临床价值。

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