| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 5040758 | Brain, Behavior, and Immunity | 2017 | 8 Pages |
â¢Binge levels of alcohol exacerbate TBI-induced neuropathology and inflammation.â¢Binge alcohol produces mild learning impairments in injured mice.â¢Injured, alcohol-treated mice have more ectopic DCX+ neurons in the dentate gyrus.
Traumatic brain injuries (TBI) are a major public health problem with enormous costs in terms of health care dollars, lost productivity, and reduced quality of life. Alcohol is bidirectionally linked to TBI as many TBI patients are intoxicated at the time of their injury and we recently reported that, in accordance with human epidemiological data, animals injured during juvenile development self-administered significantly more alcohol as adults than did sham injured mice. There are also clinical data that drinking after TBI significantly reduces the efficacy of rehabilitation and leads to poorer long-term outcomes. In order to determine whether juvenile traumatic brain injury also increased the vulnerability of the brain to the toxic effects of high dose alcohol, mice were injured at 21Â days of age and then seven weeks later treated daily with binge-like levels of alcohol 5Â g/kg (by oral gavage) for ten days. Binge-like alcohol produced a greater degree of neuronal damage and neuroinflammation in mice that sustained a TBI. Further, mice that sustained a juvenile TBI exhibited mild learning and memory impairments in adulthood following binge alcohol and express a significant increase in hippocampal ectopic localization of newborn neurons. Taken together, these data provide strong evidence that a mild brain injury occurring early in life renders the brain highly vulnerable to the consequences of binge-like alcohol consumption.
