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AuthorElashi, Asma A.
AuthorRazzaq, Aleem
AuthorAnwardeen, Najeha
AuthorNaja, Khaled
AuthorAlshafai, Mashael
AuthorDiboun, Ilhame
AuthorAlbagha, Omar
AuthorElrayess, Mohamed A.
Available date2025-12-20T16:52:02Z
Publication Date2025-09-28
Publication NameHuman Molecular Genetics
Identifierhttp://dx.doi.org/10.1093/hmg/ddaf152
CitationElashi, A. A., Razzaq, A., Anwardeen, N., Naja, K., Alshafai, M., Diboun, I., ... & Elrayess, M. A. (2025). N-Lactoyl amino acids: insights from metabolite genome-wide association studies and phenome-wide association analysis. Human Molecular Genetics, 34(22), 1865-1873.
ISSN0964-6906
URIhttps://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=105020801948&origin=inward
URIhttp://hdl.handle.net/10576/69208
AbstractN-lactoyl-amino acids (Lac-AA) are emerging as important metabolites with diverse physiological roles. This study integrates metabolomics and genomics to investigate the genetic determinants and clinical relevance of three Lac-AA: N-Lactoyl phenylalanine (Lac-Phe), N-Lactoyl tyrosine (Lac-Tyr), and N-Lactoyl valine (Lac-Tyr). We conducted a metabolome-wide association study (mGWAS) on 2811 participants followed by a phenome-wide association study (PheWAS) and pathway enrichment analysis. Our mGWAS revealed modest genetic contributions to Lac-AA levels, with genome-wide significant loci identified for Lac-Tyr and Lac-Val, but not for Lac-Phe. PheWAS analysis linked these genetic variants to key clinical traits, including white blood cell count, platelet count, and glucose levels. Pathway enrichment highlighted the involvement of Lac-AA in immune-metabolic crosstalk, particularly in inflammation and energy metabolism. These findings suggest that Lac-AA levels are primarily influenced by dynamic metabolic or inflammatory states rather than fixed genetic factors. Our results underscore the potential of Lac-AA as metabolic sensors and biomarkers at the intersection of cellular energy states and systemic inflammation, opening new avenues for research in metabolic and inflammatory disorders.
SponsorThis research was funded by Qatar Research, Development and Innovation (QRDI) Council, grant number PPM-06-0516-230030. Open Access funding provided by the Qatar National Library
Languageen
PublisherOxford University Press
SubjectMetabolomics
mGWAS
N-Lactoyl amino acids
PheWAS
TitleN-Lactoyl amino acids: insights from metabolite genome-wide association studies and phenome-wide association analysis
TypeArticle
Pagination1865-1873
Issue Number22
Volume Number34
ESSN1460-2083
dc.accessType Open Access


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