法尼基转移酶抑制剂可降低Ras激活,并改善对乙酰氨基酚诱导的小鼠肝损伤。
Farnesyltransferase inhibitors reduce Ras activation and ameliorate acetaminophen-induced liver injury in mice.
作者信息
Saha Banishree, Nandi Dipankar
机构信息
Department of Biochemistry, Indian Institute of Science, Bangalore, India.
出版信息
Hepatology. 2009 Nov;50(5):1547-57. doi: 10.1002/hep.23180.
UNLABELLED
Hepatotoxicity due to overdose of the analgesic and antipyretic acetaminophen (APAP) is a major cause of liver failure in adults. To better understand the contributions of different signaling pathways, the expression and role of Ras activation was evaluated after oral dosing of mice with APAP (400-500 mg/kg). Ras-guanosine triphosphate (GTP) is induced early and in an oxidative stress-dependent manner. The functional role of Ras activation was studied by a single intraperitoneal injection of the neutral sphingomyelinase and farnesyltransferase inhibitor (FTI) manumycin A (1 mg/kg), which lowers induction of Ras-GTP and serum amounts of alanine aminotransferase (ALT). APAP dosing decreases hepatic glutathione amounts, which are not affected by manumycin A treatment. However, APAP-induced activation of c-Jun N-terminal kinase, which plays an important role, is reduced by manumycin A. Also, APAP-induced mitochondrial reactive oxygen species are reduced by manumycin A at a later time point during liver injury. Importantly, the induction of genes involved in the inflammatory response (including iNos, gp91phox, and Fasl) and serum amounts of proinflammatory cytokines interferon-gamma (IFNgamma) and tumor necrosis factor alpha, which increase greatly with APAP challenge, are suppressed with manumycin A. The FTI activity of manumycin A is most likely involved in reducing APAP-induced liver injury, because a specific neutral sphingomyelinase inhibitor, GW4869 (1 mg/kg), did not show any hepatoprotective effect. Notably, a structurally distinct FTI, gliotoxin (1 mg/kg), also inhibits Ras activation and reduces serum amounts of ALT and IFN-gamma after APAP dosing. Finally, histological analysis confirmed the hepatoprotective effect of manumycin A and gliotoxin during APAP-induced liver damage.
CONCLUSION
This study identifies a key role for Ras activation and demonstrates the therapeutic efficacy of FTIs during APAP-induced liver injury.
未标记
过量服用止痛和解热药物对乙酰氨基酚(APAP)导致的肝毒性是成人肝衰竭的主要原因。为了更好地理解不同信号通路的作用,在给小鼠口服APAP(400 - 500 mg/kg)后,评估了Ras激活的表达和作用。Ras - 鸟苷三磷酸(GTP)早期被诱导,且呈氧化应激依赖性。通过单次腹腔注射中性鞘磷脂酶和法尼基转移酶抑制剂(FTI)马尼霉素A(1 mg/kg)研究Ras激活的功能作用,该抑制剂可降低Ras - GTP的诱导以及血清丙氨酸转氨酶(ALT)水平。APAP给药会降低肝脏谷胱甘肽含量,而马尼霉素A治疗对此无影响。然而,马尼霉素A可降低APAP诱导的c - Jun氨基末端激酶的激活,该激酶起重要作用。此外,在肝损伤后期,马尼霉素A可降低APAP诱导的线粒体活性氧。重要的是,马尼霉素A可抑制参与炎症反应的基因(包括诱导型一氧化氮合酶、gp91phox和Fasl)的诱导以及促炎细胞因子干扰素 - γ(IFNγ)和肿瘤坏死因子α的血清水平,这些在APAP攻击后会大幅增加。马尼霉素A的FTI活性最有可能参与减轻APAP诱导的肝损伤,因为一种特异性中性鞘磷脂酶抑制剂GW4869(1 mg/kg)未显示出任何肝保护作用。值得注意的是,一种结构不同的FTI,即胶质毒素(1 mg/kg),在APAP给药后也可抑制Ras激活并降低血清ALT和IFN - γ水平。最后,组织学分析证实了马尼霉素A和胶质毒素在APAP诱导的肝损伤中的肝保护作用。
结论
本研究确定了Ras激活的关键作用,并证明了FTIs在APAP诱导的肝损伤中的治疗效果。
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