4.6 Article

Profiling of Serum Metabolites of Acute Intermittent Porphyria and Asymptomatic HMBS Mutation Carriers

Journal

CELLS
Volume 10, Issue 10, Pages -

Publisher

MDPI
DOI: 10.3390/cells10102579

Keywords

porphobilinogen deaminase; metabolomic profiling; metabolic reprogramming; heme metabolism; delta-aminolevulinic acid; porphobilinogen

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Funding

  1. Health Promotion Administration, Ministry of Health and Welfare, Taiwan [KMRPB3J008]
  2. Chang Gung Memorial Hospital [CMRPG3H1761, CMRPG3J1751]

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This study aimed to present serum metabolite profiles of patients with Acute Intermittent Porphyria (AIP) and identify specific metabolites that could discriminate between AIP, asymptomatic HMBS mutation carriers, and healthy individuals. The results showed significant differences in 15 variables between AIP patients and normal controls, suggesting potential biomarkers for monitoring AIP symptoms.
This study aims to present the serum metabolite profiles of patients with acute intermittent porphyria (AIP) and identify specific metabolites that could potentially discriminate between AIP, asymptomatic HMBS mutation carriers, and healthy individuals. The study cohort included 46 female participants: 21 AIP patients, 5 asymptomatic carriers, and 20 'normal' participants (without HMBS gene mutation). Serum samples were analyzed for 157 selected metabolites or clinical variables using an assay combining liquid chromatography MS/MS and direct flow injection. AUC analysis was used to distinguish unique variables between the three groups. A total of 15 variables differed significantly between the AIP and normal control group (VIP score > 1.0 and p < 0.05 with FDR correction). In AIP patients, the levels tyrosine, valine, and eGFR were significantly lower, and the levels of sphingomyelin C16:0, C24:0, C24:1, phosphatidylcholine diacyl C32:1, C36:1, C36:3, ornithine, sarcosine, citrulline, blood urea nitrogen AST, and ALT were significantly higher. The AUC of these 15 variables in discriminating between normal and AIP patients ranged between 0.73 and 0.94 (p < 0.05). In conclusion, serum metabolic profiles differ between normal individuals and patients carrying the HMBS mutation. The unique metabolites associated with AIP identified in this study may be useful for monitoring the development of AIP symptoms.

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