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Bile acids, farnesoid X receptor, atherosclerosis and metabolic control.

机译:胆汁酸,法尼醇X受体,动脉粥样硬化和代谢控制。

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PURPOSE OF REVIEW: Bile acids are amphiphilic molecules synthesized from cholesterol exclusively in the liver that are essential for effective absorption of dietary fat. In addition to this 'classical role', bile acids act as signalling molecules that control their own metabolism by activating the nuclear receptor, farnesoid X receptor. RECENT FINDINGS: Recent work demonstrates that farnesoid X receptor exerts metabolic control beyond bile acid homeostasis, notably effects on HDL, triglyceride and glucose metabolism. Farnesoid X receptor influences insulin sensitivity of tissues that are not part of the enterohepatic circulation, for example, adipose tissue. Certain metabolic effects in the liver appear to be mediated via farnesoid X receptor-stimulated release of an intestinal growth factor. In addition, novel signalling pathways independent of farnesoid X receptor have been identified that may contribute to bile acid-mediated metabolic regulation. SUMMARY: Farnesoid X receptor represents a potentially attractive target for treatment of various aspects of the metabolic syndrome and for prevention of atherosclerosis. Yet, in view of its pleiotropic effects and apparent species-specificity, it is evident that successful interference of the farnesoid X receptor signalling system will require the development of gene-specific and/or organ-specific farnesoid X receptor modulators and extensive testing in human models of disease.
机译:审查的目的:胆汁酸是仅在肝脏中由胆固醇合成的两亲性分子,对有效吸收膳食脂肪至关重要。除了这种“经典作用”外,胆汁酸还可以作为信号分子,通过激活核受体(法呢素X受体)来控制自身的代谢。最近的发现:最近的研究表明,法尼醇X受体发挥了胆汁酸稳态之外的代谢控制作用,特别是对HDL,甘油三酸酯和葡萄糖代谢的影响。 Farnesoid X受体影响不属于肝肠循环的组织(例如脂肪组织)的胰岛素敏感性。肝脏中的某些代谢作用似乎是由法呢素X受体刺激的肠生长因子释放介导的。另外,已经确定了独立于法呢素X受体的新型信号传导途径,其可能有助于胆汁酸介导的代谢调节。概述:法尼醇X受体代表了潜在的有吸引力的靶标,用于治疗代谢综合征的各个方面以及预防动脉粥样硬化。然而,鉴于其多效性作用和明显的物种特异性,显然,成功干扰法呢素X受体信号传导系统将需要开发基因特异性和/或器官特异性法呢素X受体调节剂,并在人体中进行广泛的测试。疾病模型。

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