Switching gene expression “on” and “off” is of utmost importance when studying gene function in the adult nervous system. In the early 1990s, scientists described a tetracycline-controlled gene expression systems (Tet systems), which allow the regulation of gene expression by externally applied substances. The Tet-regulated gene expression can be used to analyze involvement of genes for example in cognition in the mouse, as was shown in key studies from 1996. But in spite of the published success, others scientists report some difficulties: in some experiments the full reactivation of Tet-regulated genes failed. Mazahir T. Hasan and colleagues at the Max Planck Institute for Medical Research in Heidelberg have therefore systematically examined individual components of the Tet systems and delineated the necessary conditions for reversible control of gene expression in neurons.
In the June 20th issue of the online, open-access journal PLoS ONE, they report that genes which had been inactive in neurons during early mouse development become functionally silenced in the adult brain. Intriguingly, Hasan and colleagues found that gene silencing in the adult brain can be avoided by making neurons produce high levels of gene-specific activators which facilitate “un-silencing” of previously silenced genes. These findings have important implications in experimental research that makes use of reversible gene expression tools to switch genes on and off. Neuroscientists need such gene switches to investigate the cause-and-effect relationship between gene activity, neuronal physiology, and animal behavior. Hence, this new research is an important step in both the development of highly reliable gene-switches for experimental neuroscience and in our understanding of mechanisms governing gene regulation in the brain. Indeed, the epigenetic mechanisms in charge of switching genes “on” or “off” play an essential role when our brain learns and stores information, and when our brain reacts to injury and disease.







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