Department of Biological Chemistry, Weizmann Institute of Science, Rehovot 76100, Israel.
FEBS Lett. 2013 Apr 17;587(8):1046-52. doi: 10.1016/j.febslet.2013.01.007. Epub 2013 Jan 18.
Traditionally, biochemical studies are performed in dilute homogenous solutions, which are very different from the dense mixture of molecules found in cells. Thus, the physiological relevance of these studies is in question. This recognition motivated scientists to formulate the effect of crowded solutions in general, and excluded volume in particular, on biochemical processes. Using polymers or proteins as crowders, it was shown that while crowding tends to significantly enhance the formation of complexes containing many subunits, dimerizations are only mildly affected. Computer simulations, together with experimental evidence, indicate soft interactions and diffusion as critical factors that operate in a concerted manner with excluded volume to modulate protein binding. Yet, these approaches do not truly mimic the cellular environment. In vivo studies may overcome this shortfall. The few studies conducted thus far suggest that in cells, binding and folding occur at rates close to those determined in dilute solutions. Obtaining quantitative biochemical information on reactions inside living cells is currently a main challenge of the field, as the complexity of the intracellular milieu was what motivated crowding research to begin with.
传统上,生物化学研究是在稀单相溶液中进行的,这与细胞中存在的密集分子混合物有很大的不同。因此,这些研究的生理相关性存在疑问。这种认识促使科学家们提出了一般拥挤溶液的影响,特别是排除体积对生化过程的影响。使用聚合物或蛋白质作为拥挤剂,结果表明,虽然拥挤往往会显著增强含有许多亚基的复合物的形成,但二聚化的影响则较为温和。计算机模拟和实验证据表明,软相互作用和扩散是协同作用的关键因素,与排除体积一起调节蛋白质结合。然而,这些方法并不能真正模拟细胞环境。体内研究可能会克服这一不足。迄今为止进行的少数研究表明,在细胞中,结合和折叠的速率接近在稀溶液中确定的速率。在活细胞内获取关于反应的定量生化信息目前是该领域的主要挑战,因为细胞内环境的复杂性正是促使拥挤研究开始的原因。
