Kalinovich Anastasia V, de Jong Jasper M A, Cannon Barbara, Nedergaard Jan
Department of Molecular Biosciences, The Wenner-Gren Institute, Stockholm University, Stockholm, Sweden.
Department of Molecular Biosciences, The Wenner-Gren Institute, Stockholm University, Stockholm, Sweden.
Biochimie. 2017 Mar;134:127-137. doi: 10.1016/j.biochi.2017.01.007. Epub 2017 Jan 18.
The possibility that brown adipose tissue thermogenesis can be recruited in order to combat the development of obesity has led to a high interest in the identification of "browning agents", i.e. agents that increase the amount and activity of UCP1 in brown and brite/beige adipose tissues. However, functional analysis of the browning process yields confusingly different results when the analysis is performed in one of two alternative steps. Thus, in one of the steps, using cold acclimation as a potent model browning agent, we find that if the browning process is followed in mice initially housed at 21 °C (the most common procedure), there is only weak molecular evidence for increases in UCP1 gene expression or UCP1 protein abundance in classical brown adipose tissue; however, in brite/beige adipose depots, there are large increases, apparently associating functional browning with events only in the brite/beige tissues. Contrastingly, in another step, if the process is followed starting with mice initially housed at 30 °C (thermoneutrality for mice, thus similar to normal human conditions), large increases in UCP1 gene expression and UCP1 protein abundance are observed in the classical brown adipose tissue depots; there is then practically no observable UCP1 gene expression in brite/beige tissues. This apparent conundrum can be resolved when it is realized that the classical brown adipose tissue at 21 °C is already essentially fully differentiated and thus expands extensively through proliferation upon further browning induction, rather than by further enhancing cellular differentiation. When the limiting factor for thermogenesis, i.e. the total amount of UCP1 protein per depot, is analyzed, classical brown adipose tissue is by far the predominant site for the browning process, irrespective of which of the two steps is analyzed. There are to date no published data demonstrating that alternative browning agents would selectively promote brite/beige tissues versus classical brown tissue to a higher degree than does cold acclimation. Thus, to restrict investigations to examine adipose tissue depots where only a limited part of the adaptation process occurs (i.e. the brite/beige tissues) and to use initial conditions different from the thermoneutrality normally experienced by adult humans may seriously hamper the identification of therapeutically valid browning agents. The data presented here have therefore important implications for the analysis of the potential of browning agents and the nature of human brown adipose tissue.
为对抗肥胖的发展而募集褐色脂肪组织产热的可能性引发了人们对识别“褐变剂”的高度兴趣,即能增加褐色和亮/米色脂肪组织中解偶联蛋白1(UCP1)数量和活性的物质。然而,当在两个替代步骤之一中进行分析时,褐变过程的功能分析得出的结果却令人困惑地不同。因此,在其中一个步骤中,使用冷适应作为一种有效的模型褐变剂,我们发现,如果在最初饲养于21°C(最常见的做法)的小鼠中追踪褐变过程,在经典褐色脂肪组织中,UCP1基因表达增加或UCP1蛋白丰度增加的分子证据很弱;然而,在亮/米色脂肪库中,有大幅增加,显然将功能性褐变仅与亮/米色组织中的事件联系起来。相反,在另一个步骤中,如果从最初饲养于30°C(小鼠的热中性温度,因此类似于正常人类状况)的小鼠开始追踪该过程,在经典褐色脂肪组织库中观察到UCP1基因表达和UCP1蛋白丰度大幅增加;然后在亮/米色组织中几乎没有可观察到的UCP1基因表达。当认识到21°C时的经典褐色脂肪组织已经基本完全分化,因此在进一步的褐变诱导下通过增殖而广泛扩张,而不是通过进一步增强细胞分化时,这个明显的难题就可以得到解决。当分析产热的限制因素,即每个脂肪库中UCP1蛋白的总量时,无论分析的是两个步骤中的哪一个,经典褐色脂肪组织都是褐变过程的主要部位。迄今为止,没有已发表的数据表明替代褐变剂会比冷适应更有选择性地促进亮/米色组织而非经典褐色组织。因此,将研究局限于仅检查适应过程仅发生有限部分的脂肪组织库(即亮/米色组织)并使用不同于成年人通常经历的热中性的初始条件,可能会严重阻碍治疗有效的褐变剂的识别。因此,这里呈现的数据对于分析褐变剂的潜力和人类褐色脂肪组织的性质具有重要意义。
