Proteomic Identification of Biomarkers Associated with Eating Control and Bariatric Surgery Outcomes in Patients with Morbid Obesity
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2018-11-13
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Springer
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Background The current therapeutics of morbid obesity could be significantly improved after the identification of
novel biomarkers associated with the food addiction endophenotype of obesity and with bariatric surgery outcomes.
Methods We applied differential expression proteomics and enzyme-linked immunosorbent confirmatory assays to
identify (a) proteins that varied according to loss of control over eating in morbidly obese patients and (b) proteins
that varied between normoweight controls and patients before and 1 year after bariatric surgery.
Results Clusterin was the only protein that consistently varied according to eating control in patients. Patients showed
increased levels of serum amyloid P protein, apolipoprotein A4, serotransferrin, complement factors B and C3 and
haptoglobin with respect to controls; the levels of all these proteins tended to return to control values 1 year after
surgery. In contrast, apolipoprotein A1 and transthyretin were initially downregulated in patients and were scarcely
changed by surgery. Leucine-rich alpha-2-glycoprotein was markedly increased in patients only after surgery.
Conclusions Clusterin could be of interest as a putative biomarker for food addiction diagnosis in people with
morbid obesity. In addition, postsurgical normalization of the proteins initially dysregulated in obese subjects might
help monitor clinical improvements after surgery, while lasting or newly detected alterations (i.e., those affecting
transthyretin and leucine-rich alpha-2-glycoprotein) could reflect partial refractoriness and/or contribute to the early
prediction of clinical problems.
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Rodríguez-Rivera, C., Pérez-García, C., Muñoz-Rodríguez, J.R. et al. Proteomic Identification of Biomarkers Associated with Eating Control and Bariatric Surgery Outcomes in Patients with Morbid Obesity. World J Surg 43, 744–750 (2019). https://doi.org/10.1007/s00268-018-4851-z