March 28, 2011

Gene Therapy Halts Binge Drinking in Rats

Electron micrograph of a round cell with stringy filaments on its surface A human melanoma cell grown in culture. Anne Weston, LRI, CRUK, all rights reserved by Wellcome Images.

In a series of experiments in rats, researchers gained new insights into the molecular players involved in binge drinking. The findings suggest future therapeutic strategies.

Binge drinking is typically defined as having 5 or more drinks in a row for men, and 4 or more drinks in a row for women. People of all ages can engage in binge drinking, but it鈥檚 a particular problem among college students. About 2 of 5 college students 鈥 more than 40% 鈥 have engaged in binge drinking at least once during the past 2 weeks.

Molecules in the brain called GABAA receptors are known to be involved in excessive alcohol consumption and have been recognized as potential targets for therapy. The receptor鈥檚 伪1 and 伪2 subunits both seem to play a role. A part of the brain called the ventral pallidum is rich with 伪1 GABAA receptors, whereas the central nucleus of the amygdala has mostly 伪2 subunits. Researchers still don鈥檛 have a detailed understanding of the roles of these subunits and the molecular pathways they trigger.

A research team led by Dr. Harry June and Dr. Laure Aurelian at the University of Maryland School of Medicine set out to study these GABAA receptors in an established rat model for binge drinking. They also looked at Toll-like receptor 4 (TLR4), an innate immune system molecule that鈥檚 been shown to contribute to the inflammation and brain damage brought on by excessive drinking. Their work was supported by NIH鈥檚 最新麻豆视频 Institute on Alcohol Abuse and Alcoholism (NIAAA) and 最新麻豆视频 Institute of Neurological Disorders and Stroke (NINDS). The study appeared on March 15, 2011, in the Proceedings of the 最新麻豆视频 Academy of Sciences.

The researchers used molecules called small interfering RNA (siRNA), which temporarily 鈥渟ilence鈥 targeted genes in the brain regions in which they are infused. Three to 6 days after silencing 伪2 in the central amygdala, the rats had virtually no alcohol intake. Their drinking returned to previous levels 13 days after the siRNA infusion, as 伪2 levels rose once again. Silencing 伪2 in the ventral pallidum, in contrast, had no effect on the rats鈥 drinking.

The researchers noted that 伪2 silencing in the central amygdala significantly lowered levels of TLR4. To test the role of TLR4 directly, the scientists silenced TLR4 in the central amygdala and found that the rats鈥 binge drinking fell significantly. But as with 伪2, the rats鈥 drinking remained unchanged when TLR4 was silenced in the ventral pallidum.

In contrast, silencing 伪1 in the central amygdala didn鈥檛 affect drinking. But drinking was significantly reduced when 伪1 was silenced in the ventral pallidum.

Taken together, these results suggest that the 伪2 subunit of GABAA acts through TLR4 in the central amygdala during binge drinking. The 伪1 subunit also plays a role in binge drinking, but in the ventral pallidum and independent of TLR4. More research will be needed to better understand how these and other molecules contribute to binge drinking.

Gene therapy or other strategies that target these brain receptors may one day prove effective for fighting binge drinking. 鈥淭he discovery of this involvement of TLR4 in a pathway with GABA is most remarkable,鈥 Aurelian says. 鈥淭his study provides basically a totally new understanding of what TLR4 and GABA are all about. That鈥檚 exciting, but there is a lot more to learn about this pathway and where it goes beyond this point.鈥

鈥 by Harrison Wein, Ph.D.

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