Effect of micronization on olive pomace biotransformation in the static model of colonic fermentation
Metadatos
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Sant’Anna Monteiro, Camila; Colpo Bortolazzo, Paula; Amorim Bonini, Camila Araujo; Tamires Dluzniewski, Luana; Trivisiol da Silva, Dariane; Baranzelli, Julia; Aline Smaniotto, Aline Smaniotto; Augusto Ballus, Cristiano; Lozano Sánchez, Jesús; Somacal, Sabrina; Emanuelli, TatianaEditorial
Elsevier
Fecha
2023-03-10Referencia bibliográfica
Published version: Sant’Anna Monteiro, Camila et al. Effect of micronization on olive pomace biotransformation in the static model of colonic fermentation. Food Chemistry Volume 418, 30 August 2023, 135921. https://doi.org/10.1016/j.foodchem.2023.135921
Patrocinador
CNPq 435932/2018-7; 303654/2017-1; 422700/2021-5; CAPES Finance code 001; Estado do Rio Grande do Sul DCIT 41/2017; MCIN/AEI/10.13039/501100011033; European Union NextGenerationEU/PRTR TED2021-132489A-100Resumen
The effect of granulometric fractionation and micronization of olive pomace (OP) on the biotransformation of
phenolic compounds by intestinal microbiota was investigated in vitro. Three types of powdered OP samples were
incubated with human feces to simulate colonic fermentation, after a sequential static digestion: non-fractionated
OP (NF), granulometrically fractionated OP (GF) and granulometrically fractionated and micronized OP (GFM).
GF and GFM favored the release of hydroxytyrosol, oleuropein aglycone, apigenin and phenolic acid metabolites
in the first hours of colonic fermentation compared to NF (up to 41-fold higher). GFM caused higher release of
hydroxytyrosol than GF. GFM was the only sample to release tyrosol and sustained tyrosol levels up to 24 h of
fermentation. Micronization associated with granulometric fractionation was more efficient than granulometric
fractionation alone to increase the release of phenolic compounds from the OP matrix during simulated colonic
fermentation and can be further studied for nutraceutical purposes.