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Test Systems to Study the Structure and Function of Uncoupling Protein 1: A Critical Overview

机译:测试系统去偶联蛋白的结构和功能的测试系统1:关键概述

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摘要

The discovery of active brown adipose tissue (BAT) in healthy adult humans has renewed interest in the biology of this organ. BAT is capable of distributing nutrient energy in the form of heat allowing small mammals to efficiently defend their body temperature when acutely exposed to the cold. On the other hand BAT might be a target for the treatment of obesity and related diseases, as its pharmacological activation could allow release of excess energy stored in white adipose tissue depots. Energy dissipation in BAT depends on the activity of uncoupling protein 1 (UCP1), therefore a BAT-based obesity therapy requires a detailed understanding of structure and function of UCP1. Although UCP1 has been in the focus of research since its discovery, central questions concerning its mechanistic function and regulation are not yet resolved. They have been addressed in native mitochondria but also in several test systems, which are generally used to lower inter-experimental variability and to simplify analysis conditions. Different test systems have contributed to our current knowledge about UCP1 but of course all of them have certain limitations. We here provide an overview about research on UCP1 structure and function in test systems. So far, these have nearly exclusively been employed to study rodent and not human UCP1. Considering that the amino acid sequence of mouse and human UCP1 is only 79% identical, it will be essential to test whether the human version has a similarly high catalytic activity, allowing a relevant amount of energy dissipation in human BAT. Besides the issue of comparable mechanistic function a sufficiently high expression level of human UCP1 is a further prerequisite for anti-obesity therapeutic potential. Treatments which induce BAT hyperplasia and UCP1 expression in humans might therefore be equally important to discover as mere activators of the thermogenic process.
机译:在健康的成年人体内发现活性棕色脂肪组织(BAT)引起了人们对该器官生物学的新兴趣。英美烟草能够以热量的形式分配营养能量,从而使小型哺乳动物在暴露于寒冷中时能有效地保护自己的体温。另一方面,BAT可能是治疗肥胖症和相关疾病的靶标,因为它的药理活性可以释放储存在白色脂肪组织贮库中的多余能量。 BAT中的能量耗散取决于解偶联蛋白1(UCP1)的活性,因此基于BAT的肥胖疗法需要对UCP1的结构和功能有详细的了解。尽管自发现以来,UCP1一直是研究的重点,但有关其机械功能和调节的主要问题尚未解决。它们已在天然线粒体中得到解决,但在一些测试系统中也得到解决,这些系统通常用于降低实验间的变异性并简化分析条件。不同的测试系统为我们目前对UCP1的了解做出了贡献,但是当然它们都有一定的局限性。我们在这里提供有关在测试系统中对UCP1结构和功能的研究的概述。到目前为止,这些几乎只用于研究啮齿动物,而不是人类UCP1。考虑到小鼠和人UCP1的氨基酸序列只有79%相同,因此必须测试人版本是否具有类似的高催化活性,从而在人BAT中消耗大量的能量。除了可比较的机械功能问题之外,人UCP1的足够高的表达水平是抗肥胖症治疗潜力的另一个先决条件。因此,在人类中诱导BAT增生和UCP1表达的治疗可能与发现热原过程的激活剂一样重要。

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