4.5 Article

Metabolomic profiling of early inactive hepatic alveolar and cystic echinococcosis

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ACTA TROPICA
卷 242, 期 -, 页码 -

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ELSEVIER
DOI: 10.1016/j.actatropica.2023.106875

关键词

Hepatic; Alveolar; Cysts; Echinococcosis; Metabolomic profiling; Biomarkers

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This study investigated the metabolic variations in patients with active and inactive hepatic alveolar echinococcosis (AE) and cystic echinococcosis (CE), and identified serum biomarkers that can differentiate between the two diseases. Active AE lesions strongly alter amino acid metabolism in the host, while CE lesions have an altered metabolism of oxidative stress response. These changes in metabolic pathways can serve as biomarkers for early diagnosis of AE and CE.
Hepatic alveolar echinococcosis (AE) and cystic echinococcosis (CE) are severe helminthic zoonoses and leading causes of parasitic liver damage. They pose a high mortality risk due to invisible clinical signs, especially at the early inactive stage. However, the specific metabolic profiles induced by inactive AE and CE lesions remain largely unclear. Therefore, we used gas chromatography-mass spectrometry-based metabolomic profiling to identify the global metabolic variations in AE and CE patient sera to differentiate between the two diseases and reveal the mechanisms underlying their pathogenesis. In addition, specific serum biomarkers of inactive hepatic AE and CE were screened using receiver operating curves, which can contribute to the clinical diagnosis of both diseases, especially in the earlier phase. These differential metabolites are involved in glycine, serine, tyrosine, and phenylalanine metabolism. Further analysis of key metabolic pathways showed that inactive AE lesions strongly alter amino acid metabolism in the host. CE lesions have an altered metabolism of oxidative stress response. These changes suggest these metabolite-associated pathways can serve as biomarkers to distinguish individuals with inactive AE and CE from healthy populations. This study also investigated the differences in serum metabolic profiles in patients with CE and AE. The biomarkers identified belonged to different metabolic pathways, including lipid, carnitine, androgen, and bile acid metabolism. Taken together, by investigating the different phenotypes of CE and AE with metabolomic profiling, serum biomarkers facilitating early diagnosis were identified.

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