Amna Al-Nesf scite author profile

Amna Al-Nesf

2Publications

5Citation Statements Received

50Citation Statements Given

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Untargeted Metabolomics Identifies a Novel Panel of Markers for Autologous Blood Transfusion

et al. 2022

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Untargeted metabolomics was used to analyze serum and urine samples for biomarkers of autologous blood transfusion (ABT). Red blood cell concentrates from donated blood were stored for 35–36 days prior to reinfusion into the donors. Participants were sampled at different time points post-donation and up to 7 days post-transfusion. Metabolomic profiling was performed using ACQUITY ultra performance liquid chromatography (UPLC), Q-Exactive high resolution/accurate mass spectrometer interfaced with a heated electrospray ionization (HESI-II) source and Orbitrap mass analyzer operated at 35,000 mass resolution. The markers of ABT were determined by principal component analysis and metabolites that had p < 0.05 and met ≥ 2-fold change from baseline were selected. A total of 11 serum and eight urinary metabolites, including two urinary plasticizer metabolites, were altered during the study. By the seventh day post-transfusion, the plasticizers had returned to baseline, while changes in nine other metabolites (seven serum and two urinary) remained. Five of these metabolites (serum inosine, guanosine and sphinganine and urinary isocitrate and erythronate) were upregulated, while serum glycourdeoxycholate, S-allylcysteine, 17-alphahydroxypregnenalone 3 and Glutamine conjugate of C6H10O2 (2)* were downregulated. This is the first study to identify a panel of metabolites, from serum and urine, as markers of ABT. Once independently validated, it could be universally adopted to detect ABT.

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Reproductibility of a Metabolite Risk Score to Predict Coronary Heart Disease in a Middle Eastern Population

El‐Menyar¹,

Ullah²,

Kunji³

et al. 2021

Journal of the American College of Cardiology

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Amna Al-Nesf

Untargeted Metabolomics Identifies a Novel Panel of Markers for Autologous Blood Transfusion

Reproductibility of a Metabolite Risk Score to Predict Coronary Heart Disease in a Middle Eastern Population

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