Department of Biochemistry, School of Medicine, Gachon University, Incheon 21999, Republic of Korea.
Department of Biochemistry, College of Medicine, Ewha Womans University, Seoul 07985, Republic of Korea.
Int J Mol Med. 2018 Mar;41(3):1715-1723. doi: 10.3892/ijmm.2017.3326. Epub 2017 Dec 15.
Gallstone disease is one of the most prevalent and costly gastrointestinal disorders worldwide. Gallstones are formed in the biliary system by cholesterol secretions in bile, which result from excess cholesterol, a deficiency in bile salts or a combination of the two. The present study examined the effects of proteasome inhibition on gallstone formation using the proteasome inhibitors bortezomib (BT) and carfilzomib (CF). C57BL/6J mice were fed a lithogenic diet to generate gallstones and injected with BT or CF for 12 weeks. After 12 weeks of the lithogenic diet, 8 out of the 10 mice in the control group had developed gallstones, whereas none of the mice who received proteasome inhibitors had developed gallstones. Notably, the expression of genes associated with cholesterol synthesis (sterol regulatory element‑binding protein‑2 and 3‑hydroxy‑3‑methylglutaryl‑CoA reductase), cholesterol secretion [ATP‑binding cassette subfamily G member 5 (ABCG5) and ABCG8] and bile acid synthesis [cytochrome P450 family 7 subfamily A member 1 (Cyp7a1), Cyp7b1, Cyp27a1 and Cyp8b1] was reduced in the livers of mice injected with BT or CF. Cyp7a1 encodes cholesterol 7α‑hydroxylase, the rate‑limiting enzyme in the synthesis of bile acid from cholesterol. The present study therefore measured the expression levels of transcription factors that are known to inhibit Cyp7a1 expression, namely farnesoid X receptor (FXR), pregnane X receptor (PXR) and small heterodimer partner (SHP). Although FXR, PXR and SHP expression was predicted to increase in the presence of proteasome inhibitors, the expression levels were actually reduced; thus, it was concluded that they were not involved in the proteasome inhibition‑induced regulation of Cyp7a1. Further investigation of the mitogen‑activated protein kinase and protein kinase A (PKA) signaling pathways in human hepatoma cells revealed that proteasome inhibition‑induced c‑Jun N‑terminal kinase (JNK) phosphorylation reduced CYP7A1 and CYP27A1 expression. In addition, reduced PKA phosphorylation as a result of proteasome inhibition regulated ABCG5 and ABCG8 expression. In conclusion, these findings suggest that proteasome inhibition regulates cholesterol and biliary metabolism via the JNK and PKA pathways, and is a promising therapeutic strategy to prevent gallstone disease.
胆石病是全球最普遍和代价最高的胃肠道疾病之一。胆石在胆汁中的胆固醇分泌作用下在胆道系统中形成,这是由于胆固醇过多、胆汁盐缺乏或两者的结合所致。本研究使用蛋白酶体抑制剂硼替佐米(BT)和卡非佐米(CF)研究了蛋白酶体抑制对胆石形成的影响。C57BL/6J 小鼠喂食致石饮食以产生胆石,并注射 BT 或 CF 12 周。在致石饮食 12 周后,对照组的 10 只小鼠中有 8 只发展为胆石,而接受蛋白酶体抑制剂治疗的小鼠均未发展为胆石。值得注意的是,与胆固醇合成(固醇调节元件结合蛋白-2 和 3-羟-3-甲基戊二酰基辅酶 A 还原酶)、胆固醇分泌[三磷酸腺苷结合盒亚家族 G 成员 5(ABCG5)和 ABCG8]和胆汁酸合成[细胞色素 P450 家族 7 亚家族 A 成员 1(Cyp7a1)、Cyp7b1、Cyp27a1 和 Cyp8b1]相关的基因在注射 BT 或 CF 的小鼠肝脏中表达减少。Cyp7a1 编码胆固醇 7α-羟化酶,是胆固醇合成胆汁酸的限速酶。因此,本研究测量了已知抑制 Cyp7a1 表达的转录因子的表达水平,即法尼醇 X 受体(FXR)、孕烷 X 受体(PXR)和小异二聚体伴侣(SHP)。尽管预计在存在蛋白酶体抑制剂时 FXR、PXR 和 SHP 表达会增加,但实际上表达水平降低;因此,结论是它们不参与蛋白酶体抑制诱导的 Cyp7a1 调节。进一步研究人肝癌细胞中的丝裂原活化蛋白激酶和蛋白激酶 A(PKA)信号通路表明,蛋白酶体抑制诱导的 c-Jun N-末端激酶(JNK)磷酸化降低了 CYP7A1 和 CYP27A1 的表达。此外,蛋白酶体抑制导致的 PKA 磷酸化减少调节 ABCG5 和 ABCG8 的表达。总之,这些发现表明蛋白酶体抑制通过 JNK 和 PKA 途径调节胆固醇和胆汁代谢,是预防胆石病的一种有前途的治疗策略。
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