State Key Laboratory of Natural and Biomimetic Drugs; Department of Chemical Biology, Peking University School of Pharmaceutical Sciences, 38 Xueyuan Road, Haidian District, Beijing, 100191, People's Republic of China.
Department of Pharmaceutics, Ernest Mario School of Pharmacy, Rutgers, The State University of New Jersey, Room 228 160 Frelinghuysen Road, Piscataway, NJ, 08854, USA.
AAPS J. 2017 Nov;19(6):1703-1714. doi: 10.1208/s12248-017-0133-1. Epub 2017 Aug 21.
Oxidative stress is an important pathogenic factor in various hepatic diseases. Nuclear factor-erythroid 2-related factor-2 (Nrf2), which coordinates the expression of an array of antioxidant and detoxifying genes, has been proposed as a potential target for prevention and treatment of liver disease. Dibenzoylmethane (DBM) is a minor ingredient in licorice that activates Nrf2 and prevents various cancers and oxidative damage. In the present study, the mechanisms by which DBM activates Nrf2 signaling were delineated, and its protective effect against carbon tetrachloride (CCl)-induced liver injury was examined. DBM potently induced the expression of HO-1 in cells and in the livers of mice, but this induction was diminished in Nrf2-deficient mice and cells. Overexpression of Nrf2 enhanced DBM-induced HO-1 expression, while overexpression of a dominant-negative fragment of Nrf2 inhibited this induction. DBM treatment resulted in dissociation from Keap1 and nuclear translocation of Nrf2. Moreover, DBM activated Akt/protein kinase B, mitogen-activated protein kinases, and AMP-activated protein kinase and increased intracellular calcium levels. Inhibition of JNK, AMPK, or intracellular calcium signaling significantly suppressed the induction of HO-1 expression by DBM. Finally, DBM treatment significantly inhibited CCl-induced acute liver injury in wild-type but not in Nrf2-deficient mice. Taken together, our results revealed the mechanisms by which DBM activates Nrf2 and induces HO-1 expression, and provide molecular basis for the design and development of DBM and its derivatives for prevention or treatment of liver diseases by targeting Nrf2.
氧化应激是各种肝脏疾病的重要致病因素。核因子-红细胞 2 相关因子 2(Nrf2)协调抗氧化和解毒基因的表达,被认为是预防和治疗肝脏疾病的潜在靶点。二苯甲酰甲烷(DBM)是甘草中的一种次要成分,可激活 Nrf2 并预防各种癌症和氧化损伤。在本研究中,阐明了 DBM 激活 Nrf2 信号通路的机制,并研究了其对四氯化碳(CCl)诱导的肝损伤的保护作用。DBM 可强力诱导细胞和小鼠肝脏中 HO-1 的表达,但在 Nrf2 缺陷型小鼠和细胞中,这种诱导作用减弱。Nrf2 的过表达增强了 DBM 诱导的 HO-1 表达,而 Nrf2 的显性负片段的过表达抑制了这种诱导。DBM 处理导致 Nrf2 与 Keap1 解离并向核内转位。此外,DBM 激活 Akt/蛋白激酶 B、丝裂原活化蛋白激酶和 AMP 激活的蛋白激酶,并增加细胞内钙水平。JNK、AMPK 或细胞内钙信号的抑制显著抑制了 DBM 诱导的 HO-1 表达。最后,DBM 处理可显著抑制野生型小鼠而非 Nrf2 缺陷型小鼠中 CCl 诱导的急性肝损伤。综上所述,我们的研究结果揭示了 DBM 激活 Nrf2 并诱导 HO-1 表达的机制,并为设计和开发 DBM 及其衍生物提供了分子基础,可通过靶向 Nrf2 预防或治疗肝脏疾病。
