Effect of fermented red ginseng on gut microbiota dysbiosis- or immobilization stress-induced anxiety, depression, and colitis in mice

Yoon-Jung Shin; Dong-Yun Lee; Joo Yun Kim; Keon Heo; Jae-Jung Shim; Jung-Lyoul Lee; Dong-Hyun Kim

Journal of Ginseng Research (Mar 2023)

Effect of fermented red ginseng on gut microbiota dysbiosis- or immobilization stress-induced anxiety, depression, and colitis in mice

Yoon-Jung Shin,
Dong-Yun Lee,
Joo Yun Kim,
Keon Heo,
Jae-Jung Shim,
Jung-Lyoul Lee,
Dong-Hyun Kim

Affiliations

Yoon-Jung Shin: Neurobiota Research Center, College of Pharmacy, Kyung Hee University, Seoul, Republic of Korea
Dong-Yun Lee: Neurobiota Research Center, College of Pharmacy, Kyung Hee University, Seoul, Republic of Korea
Joo Yun Kim: R&BD Center, hy Co.Ltd., Yongin, Republic of Korea
Keon Heo: R&BD Center, hy Co.Ltd., Yongin, Republic of Korea
Jae-Jung Shim: R&BD Center, hy Co.Ltd., Yongin, Republic of Korea
Jung-Lyoul Lee: R&BD Center, hy Co.Ltd., Yongin, Republic of Korea
Dong-Hyun Kim: Neurobiota Research Center, College of Pharmacy, Kyung Hee University, Seoul, Republic of Korea; Corresponding author. Department of Pharmacy, Kyung-Hee University, Seoul, 02447, Republic of Korea.

Journal volume & issue: Vol. 47, no. 2
pp. 255 – 264

Abstract

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Background: Red ginseng (RG) alleviates psychiatric disorders. Fermented red ginseng (fRG) alleviates stress-induced gut inflammation. Gut dysbiosis causes psychiatric disorders with gut inflammation. To understand the gut microbiota-mediated action mechanism of RG and fRG against anxiety/depression (AD), we investigated the effects of RG, fRG, ginsenoside Rd, and 20(S)-β-D-glucopyranosyl protopanaxadiol (CK) on gut microbiota dysbiosis-induced AD and colitis in mice. Methods: Mice with AD and colitis were prepared by exposing to immobilization stress (IS) or transplanting the feces of patients with ulcerative colitis and depression (UCDF). AD-like behaviors were measured in the elevated plus maze, light/dark transition, forced swimming, and tail suspension tests. Results: Oral gavage of UCDF increased AD-like behaviors and induced neuroinflammation, gastrointestinal inflammation, and gut microbiota fluctuation in mice. Oral administration of fRG or RG treatment reduced UCDF-induced AD-like behaviors, hippocampal and hypothalamic IL-6 expression, and blood corticosterone level, whereas UCDF-suppressed hippocampal BDNF+NeuN+ cell population and dopamine and hypothalamic serotonin levels increased. Furthermore, their treatments suppressed UCDF-induced colonic inflammation and partially restored UCDF-induced gut microbiota fluctuation. Oral administration of fRG, RG, Rd, or CK also decreased IS-induced AD-like behaviors, blood IL-6 and corticosterone and colonic IL-6 and TNF-α levels, and gut dysbiosis, while IS-suppressed hypothalamic dopamine and serotonin levels increased. Conclusion: Oral gavage of UCDF caused AD, neuroinflammation, and gastrointestinal inflammation in mice. fRG mitigated AD and colitis in UCDF-exposed mice by the regulation of the microbiota-gut-brain axis and IS-exposed mice by the regulation of the hypothalamic-pituitary-adrenal axis.

Published in Journal of Ginseng Research

ISSN: 1226-8453 (Print)
Publisher: Elsevier
Country of publisher: Korea, Republic of
LCC subjects: Science: Botany
Website: http://www.journals.elsevier.com/journal-of-ginseng-research/

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