Joyce Kaitlyn M, Wong Carmen P, Scriven Ian A, Olson Dawn A, Doerge Daniel R, Branscum Adam J, Sattgast Lara H, Helferich William G, Turner Russell T, Iwaniec Urszula T
Botanical Research Center, Department of Food Science and, Human Nutrition, University of Illinois at Urbana-Champaign, Urbana, IL, 61801, USA.
Skeletal Biology Laboratory, School of Biological and Population Health Sciences, Oregon State University, Corvallis, OR, 97331, USA.
Mol Nutr Food Res. 2022 Jun;66(11):e2100974. doi: 10.1002/mnfr.202100974. Epub 2022 Apr 5.
A dose-ranging study is performed using young estrogen-depleted rats to determine whether dietary isoliquiritigenin (ILQ) alters bone metabolism and if the effects are associated with estrogen receptor signaling.
Six-week-old rats (ovariectomized at 4 weeks of age) are fed diets containing 0, 100, 250, or 750 ppm ILQ (n = 5/treatment) for 7 days. Gene expression in femur and uterus, blood markers of bone turnover, body composition, and uterine weight and epithelial cell height are determined. Because ILQ lowers bone resorption, the effect of ILQ on in vitro differentiation of osteoclasts from bone marrow of mice is assessed. Treatment resulted in a dose-dependent increases in serum ILQ but no changes in serum osteocalcin, a marker of global bone formation. Contrastingly, ILQ administration results in reduced serum CTX-1, a marker of global bone resorption, and reduces tartrate resistant acid phosphatase expression in osteoclast culture. ILQ treatment and endogenous estrogen production had limited overlap on gene expression in femur and uterus. However, uterine epithelial cell hyperplasia is observed in two of five animals treated with 750 ppm.
In conclusion, dietary ILQ reduces bone resorption in vivo and osteoclast differentiation in vitro, by mechanisms likely differing from actions of ovarian hormones.
利用年轻的雌激素缺乏大鼠进行剂量范围研究,以确定膳食异甘草素(ILQ)是否会改变骨代谢,以及这些影响是否与雌激素受体信号传导相关。
六周龄大鼠(4周龄时进行卵巢切除)分别喂食含0、100、250或750 ppm ILQ的饲料(每组n = 5只),持续7天。测定股骨和子宫中的基因表达、骨转换的血液标志物、身体组成、子宫重量和上皮细胞高度。由于ILQ降低了骨吸收,因此评估了ILQ对小鼠骨髓破骨细胞体外分化的影响。治疗导致血清ILQ呈剂量依赖性增加,但血清骨钙素(一种整体骨形成的标志物)没有变化。相反,给予ILQ会导致血清CTX-1(一种整体骨吸收的标志物)降低,并降低破骨细胞培养物中抗酒石酸酸性磷酸酶的表达。ILQ治疗和内源性雌激素产生在股骨和子宫的基因表达上有有限的重叠。然而,在接受750 ppm治疗的五只动物中有两只观察到子宫上皮细胞增生。
总之,膳食ILQ通过可能与卵巢激素作用不同的机制,在体内降低骨吸收,在体外降低破骨细胞分化。