Antioxidants (Mar 2024)

Fucoidan Supplementation Improves Antioxidant Capacity via Regulating the <i>Keap1/Nrf2</i> Signaling Pathway and Mitochondrial Function in Low-Weaning Weight Piglets

  • Chenggang Yin,
  • Qingyue Bi,
  • Wenning Chen,
  • Chengwei Wang,
  • Bianca Castiglioni,
  • Yanpin Li,
  • Wenjuan Sun,
  • Yu Pi,
  • Valentino Bontempo,
  • Xilong Li,
  • Xianren Jiang

DOI
https://doi.org/10.3390/antiox13040407
Journal volume & issue
Vol. 13, no. 4
p. 407

Abstract

Read online

Fucoidan (FC) is known for its antioxidant properties, but it has unclear effects and mechanisms on weaned piglets. Two experiments were conducted to determine the optimal FC dosage in piglet diets and its protective effect against lipopolysaccharide (LPS)-induced oxidative stress. In experiment one, 24 low weight weaned piglets were randomly assigned to four dietary treatments: a basal diet (FC 0), or a diet supplemented with 150 (FC 150), 300 (FC 300), or 600 mg/kg FC (FC 600). In experiment two, 72 low-weaning weight piglets were randomly allocated into four treatments: a basal diet (CON), or 300 mg/kg of fucoidan added to a basal diet challenged with LPS (100 µg LPS/kg body weight) or not. The results showed that FC treatments increased the G:F ratio, and dietary FC 300 reduced the diarrhea incidence and increased the plasma IGF-1 concentrations. In addition, FC 300 and FC 600 supplementation increased the plasma SOD activity and reduced the plasma MDA concentration. LPS challenge triggered a strong systemic redox imbalance and mitochondrial dysfunction. However, dietary FC (300 mg/kg) supplementation increased the activity of antioxidant enzymes, including SOD, decreased the MDA concentration in the plasma and liver, down-regulated Keap1 gene expression, and up-regulated Nrf2, CAT, MFN2, SDHA, and UQCRB gene expression in the liver. These results indicated that dietary fucoidan (300 mg/kg) supplementation improved the growth performance and antioxidant capacity of low-weaning weight piglets, which might be attributed to the modulation of the Keap1/Nrf2 signaling pathway and the mitochondrial function in the liver.

Keywords