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Comparative effects of dietary stigmasterol and oxidised stigmasterol on cholesterol absorption and metabolism in mice

Published online by Cambridge University Press:  16 October 2025

Yui Ohara*
Affiliation:
Department of Agricultural Chemistry, School of Agriculture, Meiji University Graduate School, 1-1-1 Higashimita, Tama-ku, Kawasaki, Kanagawa 214-8571, Japan
Kyoichi Osada
Affiliation:
Department of Agricultural Chemistry, School of Agriculture, Meiji University Graduate School, 1-1-1 Higashimita, Tama-ku, Kawasaki, Kanagawa 214-8571, Japan
*
Corresponding author: Yui Ohara; Email: cf240114@meiji.ac.jp
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Abstract

Dietary phytosterols exert hypocholesterolemic effects by inhibiting cholesterol absorption in the small intestine. However, oxidised phytosterols exert harmful effects. In this study, we compared the effects of dietary stigmasterol or oxidised stigmasterol (OS) on cholesterol absorption and metabolism in mice. Institute of Cancer Research (ICR) male mice were fed one of the following diets: a standard American Institute of Nutrition (AIN) diet; the standard diet plus 0·25 % cholesterol; the standard diet plus 0·25 % cholesterol and 0·25 % stigmasterol or the standard diet plus 0·25 % cholesterol and 0·25 % OS. Stigmasterol, but not OS, decreased plasma total cholesterol levels. Unlike stigmasterol, dietary OS increased the cholesterol levels in micellar solutions. Thus, OS could not exert hypocholesterolemic effects as it could not displace cholesterol in micellar solutions. In contrast, dietary OS downregulates the mRNA expression of genes involved in cholesterol synthesis and upregulates the mRNA expression of genes involved in cholesterol catabolism in mice fed cholesterol. In addition, dietary stigmasterol and OS increased the levels of faecal-neutral steroids by downregulating the mRNA expression of Niemann-Pick C1-like 1 protein (NPC1L1) in the small intestine. Dietary stigmasterol may directly regulate the mRNA expression of NPC1L1, whereas dietary OS may reduce the mRNA expression of sterol regulatory element-binding protein 2 and act as a Liver X receptor α agonist, reducing the mRNA expression of NPC1L1. Therefore, OS may affect cholesterol absorption and metabolism through a mechanism different from that of stigmasterol.

Information

Type
Research Article
Creative Commons
Creative Common License - CCCreative Common License - BY
This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (https://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution and reproduction, provided the original article is properly cited.
Copyright
© The Author(s), 2025. Published by Cambridge University Press on behalf of The Nutrition Society
Figure 0

Table 1. Diet composition

Figure 1

Table 2. Effect of dietary stigmasterol or oxidised stigmasterol on growth parameters

Figure 2

Figure 1. Effects of dietary stigmasterol or oxidised stigmasterol on plasma and hepatic cholesterol levels. Data are presented as the mean and sem of 5–6 mice in each group. Significant differences between values of the St and C groups at P < 0·01**. abValues without a common superscript letter are significantly different among values of the C, S and OS groups at P < 0·05. Other abbreviations are the same as shown in Table 1. Plasma cholesterol level was the level per dl of plasma, and hepatic cholesterol level was the level per gram of tissue.

Figure 3

Table 3. Effects of dietary stigmasterol or oxidised stigmasterol on faecal neutral steroid levels

Figure 4

Table 4. Effects of dietary stigmasterol or oxidised stigmasterol on faecal acidic steroid levels

Figure 5

Figure 2. Effects of dietary stigmasterol or oxidised stigmasterol on the mRNA expression of enzymes and nuclear receptors involved in cholesterol synthesis and catabolism in the liver. Data are presented as the mean and sem of 5–6 mice in each group. Significant differences between values of the St and C groups at P < 0·01**. abValues without a common superscript letter are significantly different among values of the C, S and OS groups at P < 0·05. Other abbreviations are the same as shown in Table 1. Each relative expression level was calculated by comparing the expression level of the target gene to that of the reference β-actin, with the C group set to 1.

Figure 6

Figure 3. Effects of dietary stigmasterol or oxidised stigmasterol on the mRNA expression of transporters involved in sterol absorption in the mucosa of the small intestines. Data are presented as the mean and sem of 5–6 mice in each group. Significant differences between values of the St and C groups at P < 0·01**. abValues without a common superscript letter are significantly different among values of the C, S and OS groups at P < 0·05. Other abbreviations are the same as shown in Table 1. Each relative expression level was presented using the same calculation method as described in the footnote of Figure 2.

Figure 7

Figure 4. Effect of stigmasterol or oxidised stigmasterol on the incorporation of cholesterol into micellar solutions. Data are presented as the mean and sem of 4 samples in each group. abValues without a common superscript letter are significantly different among values of the C, S and OS groups at P < 0·05. Other abbreviations are the same as shown in Table 1.