期刊文献+
任意字段
题名或关键词
题名
关键词
文摘
作者
第一作者
机构
刊名
分类号
参考文献
作者简介
基金资助
栏目信息

核受体PXR、CAR、LXR和FXR作为代谢性疾病治疗靶点的研究进展 被引量:7

Nuclear receptors PXR,CAR,LXR and FXR as therapeutic targets of metabolic diseases:research advance
原文传递
导出
摘要 PXR、CAR、LXR和FXR是核受体家族的重要成员,在体内广泛分布,经配体活化后调控众多机体代谢相关的酶、转运蛋白和信号途径,在糖异生、脂类代谢及其胆汁平衡中扮演着重要的角色。通过主要介绍核受体家族主要成员PXR、CAR、LXR和FXR在糖异生、脂类代谢以及胆汁平衡中的调控作用,从而可能为糖脂代谢和胆汁平衡紊乱相关代谢性疾病的药物治疗提供新依据。 PXR,CAR,LXR and FXR,widely distributed in the body,are important members of nuclear receptors(NRs)family.Metabolism related enzymes,transporter protein and signal pathways can be regulated by the activated NRs,which play important roles in gluconeogenesis,lipid metabolism and bile homeostasis.This review described the research progress of NR family members PXR,CAR,FXR and LXR,and regulating effects of gluconeogenesis,lipid metabolism and bile homeostasis,which might provide a new reference for clinical medication of metabolic diseases.
作者 马彦荣 张国强 武新安
机构地区 兰州大学第一医院药剂科 兰州大学药学院
出处 《中国医院药学杂志》 CAS CSCD 北大核心 2015年第7期659-663,共5页 Chinese Journal of Hospital Pharmacy
关键词 核受体 代谢性疾病 靶点 糖异生 脂类代谢 胆汁平衡 nuclear receptor metabolic diseases targets gluconeogenesis lipid metabolism bile homeostasis
分类号 R969 [医药卫生—药理学]
  • 相关文献

参考文献42

  • 1Nakae J, Kitamura T, Silver DL, etal. The forkhead tran- scription factor Foxol (Fkhr) confers insulin sensitivity onto glueose-6-phosphatase expression[J]. J Clin Invest, 2001, 108(9) : 1359-1367. 被引量:1
  • 2Seo HY, Kim MK, Min AK, et al. Endoplasmic retieulum stress induced activation of activating transcription factor 6 de- creases cAMP-stimulated hepatie glueoneogenesis via inhibi- tion of CREB[J]. Endocrinology, 2010, 151(2): 561-568. 被引量:1
  • 3Park JM, Kim TH, Bae JS, et al. Role of resveratrol in FOXOl-mediated gluconeogenic gene expression in the liver [J]. Biochem Biophys Res Commun, 2010, 403(3-4): 329- 334. 被引量:1
  • 4Kodama S, Moore R, Yamamoto Y, et al. Human nuclear pregnane X receptor cross-talk with CREB to repress cAMP activation of the glucose-6 phosphatase gene[J].Biochem J, 2007, 407(3): 373-381. 被引量:1
  • 5Bhalla S, Ozalp C, Fang S, etal. Ligand-activated pregnane X receptor interferes with HNF-4 signaling by targeting a com- mon coactivator PGC-1alpha. Functional implications in hepat- ic cholesterol and glucose metabolism[J]. J Biol Chem, 2004, 279(43) : 45139-45147. 被引量:1
  • 6Miao J, Fang S, Bae Y, et al. Functional inhibitory cross-talk between constitutive androstane receptor and hepatic nuclear factor-4 in hepatic lipid/glucose metabolism is mediated by competition for binding to the DR1 motif and to the common coactivators, GRIP-1 and PGC-lalpha[J]. J Biol Chem, 2006, 281 (21) : 14537-14546. 被引量:1
  • 7Nakamura K, Moore R, Negishi M, et al. Nuclear pregnane X receptor cross-talk with FoxA2 to mediate drug-induced reg- ulation of lipid metabolism in fasting mouse liver[J]. J Biol Chem, 2007, 282(13).. 9768-9776. 被引量:1
  • 8Zhou J, Fehbraio M, Wada T, et al. Hepatic fatty acid trans- porter Cd36 is a common target of LXR, PXR, and PPAR- gamma in promoting steatosis[J]. Gastroenterology, 2008, 134(2) : 556-567. 被引量:1
  • 9Zhai Y, Pal HV, Zhou J, et al. Activation of pregnane X re- ceptor disrupts glueocortieoid and mineralocorticoid homeosta- sis[J]. Mol Endoerinol, 2007, 21(1): 138-147. 被引量:1
  • 10Zhou J, Zhai Y, Mu Y, et al. A novel pregnane X receptor- mediated and sterol regulatory element-binding protein-inde- pendent lipogenic pathway[J]. J Biol Chem, 2006, 281 (21): 15013-15020. 被引量:1

同被引文献99

引证文献7

二级引证文献47

中国医院药学杂志
2015年 第7期

相关作者

内容加载中请稍等...

相关机构

内容加载中请稍等...

相关主题

内容加载中请稍等...

浏览历史

内容加载中请稍等...
;
使用帮助 返回顶部