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  • Madrigal-Ruiz, P. M.Universidad de Guadalajara, Guadalajara, Mexico (author)

The unbalance of adiponectin oligomers, RvE1 and chemerin levels are associate with increase of adiposopathy status and insulin resistance in obesity

  • Article/chapterEnglish2019

Publisher, publication year, extent ...

  • 2020
  • Open Access Text,2019
  • printrdacarrier

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  • LIBRIS-ID:oai:DiVA.org:oru-109534
  • https://urn.kb.se/resolve?urn=urn:nbn:se:oru:diva-109534URI
  • https://doi.org/10.15761/jts.1000323DOI

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  • Language:English
  • Summary in:English

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  • Subject category:vet swepub-contenttype
  • Subject category:art swepub-publicationtype

Notes

  • Funding Agencies:CONACyT FOINS No. 2250-6 "Investigación en Fronteras de la Ciencia 2015-2" 4/XIV-E/2015 FON.INST./276/2016 to MVM/RENH. PNPC-CONACyT UdG Doctoral Training in Biomedical Sciences to FICM 2014-2017 Scholarship No. 305864. Grant No. 237662, UDG-Programa de Fortalecimiento de la Investigación y el Posgrado 2016 to MVM/RENH. Grant PRODEP No. 245256 to PMMR.
  • Objective: The aim was to establish if the balance adiponectin-oligomers, resolvin-E1 and chemerin levels could contribute to the insulin resistance (IR) setting of subjects with obesity, based on their serum levels and its relationship with inflammatory markers, metabolic profile and adiposopathy status.Methods: This study included 230 individuals, classified according to World Health Organization criteria by body mass index (BMI) kg/m2 in two groups: without-obesity (from 18.5 to 29.9) and with-obesity (from 30.0 to 39.9). Body fat mass distribution, metabolic and inflammatory markers were measured by anthropometric, enzymatic and immuno-turbidimetry methods, respectively. Serum insulin, resolvin-E1, chemerin, and adiponectin-oligomers were evaluating by ELISA method. Analysis performed were correlations IR-indexes with adiposity, receiver operating characteristic (ROC) curves and the adiponectin-oligomers, resolvin-E1 and chemerin tertiles.Results: Subjects’ with-obesity showed adiposopathy status, characterized by metabolic dysregulation and a subclinical inflammatory profile. They presented higher levels (`x ±SD, ng/mL) of resolvin-E1 (1227 ±668 versus 909 ±769, P= 0.017), chemerin (91 ±31 versus 79 ±23, P= 0.013) and LMW-Adiponectin (2257 ±797 versus 1030 ±1055, P= 0.011), whereas HMW-Adiponectin was lower (2470 ±1095 versus 3236 ±1848, P= 0.010), compared to the without-obesity individuals. Individuals’ with-obesity also displayed positive correlation of IR markers (rho from 0.163 to 0.479) along body fat measurements, metabolic and inflammation profiles. Moreover, a negative correlation of HMW-Adiponectin (rho from –0.564 to –0.214) with body fat measurements, metabolic and inflammation profiles. IR-indexes, LMW-Adiponectin and resolvin-E1/chemerin relationship showed differences between groups’ with-obesity and without-obesity, but not with gender. ROC curves shown potential ability of the LMW-Adiponectin levels to differentiate IR from non-IR individuals, with AUC of 0.815, P<0.0001 (95%, CI: 0.726-0.903).Conclusion: The present study shown that LMW-Adiponectin-resolvinE1-chemerin serum unbalance establishes a specific relationship with adiposopathy in individuals with obesity, which could be a way to identify risk factors in early stages of IR.

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  • Corona-Meraz, F. I.Universidad de Guadalajara, Guadalajara, Mexico; Centro Universitario de Tonalá, Tonalá Jalisco, Mexico (author)
  • Petri, Marcelo H.,1979-Vascular center, Skane University Hospital, Malmö, Sweden(Swepub:oru)pims (author)
  • Vazquez-Del, Mercado M.Universidad de Guadalajara, Guadalajara, Mexico; Hospital Civil Dr. Juan I, Menchaca, Guadalajara, Jalisco, Mexico (author)
  • Guzman-Ornelas, Guzman-OrneM. O.lasCentro Universitario de Tonalá, Tonalá Jalisco, Mexico (author)
  • Macias-Lopez, G. G.Universidad de Guadalajara, Guadalajara, Mexico (author)
  • Diaz-Rubio, G. I.Universidad de Guadalajara, Guadalajara, Mexico (author)
  • Navarro-Hernandez, R. E.Universidad de Guadalajara, Guadalajara, Mexico (author)
  • Universidad de Guadalajara, Guadalajara, MexicoUniversidad de Guadalajara, Guadalajara, Mexico; Centro Universitario de Tonalá, Tonalá Jalisco, Mexico (creator_code:org_t)

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  • In:Journal of Translational Science: Open Access Text52059-268X

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