Cross-Sensitization between Binge Eating and Binge Drinking in a Novel C57BL/6NJ Murine Model of Disease Comorbidity Requires PDE4B Activation.

在新型 C57BL/6NJ 小鼠疾病共病模型中,暴食和暴饮之间的交叉致敏作用需要 PDE4B 激活

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作者:Madory Lauren E, Kazerani Ida, Lee Edward C, Denning Christopher J E, Mosqueda De Rosas Estevan, Nguyen Dylan T, Feng Elwin, Kotlyar Daniel, Kharwa Aadithya, Munn-Chernoff Melissa A, Bryant Camron D, Szumlinski Karen K
There is a high rate of comorbidity between binge eating (BE) and binge drinking (BD) behaviors, suggesting a common neuropathology. Recently, phosphodiesterase 4B (PDE4B) was identified as a pleiotropic gene associated with comorbid alcohol use disorder (AUD) and anorexia nervosa with BE in a genome-wide association study, implicating PDE4B as a potential contributor to shared genetic risk between these disorders. Here, we developed a novel mouse model of comorbid BE and BD in C57BL/6NJ mice in which mice underwent 10†d of BE, followed by 10†d of BD. Females exhibited cross-sensitization from BE to BD, which was apparent on the first day of ethanol access, whereas cross-sensitization emerged in males over multiple trials of BD. Accordingly immunoblotting of the nucleus accumbens tissue indicated a female-selective increase in PDE4B protein expression that was apparent on both the first and last day of BD in mice with a prior BE history. Acute pretreatment with the selective PDE4B inhibitor A33 (1.0†mg/kg) reduced the expression of cross-sensitization to BD in females on Day 1, and this effect was maintained during a 5†d A33 treatment regimen. The 5†d A33 treatment regimen also reduced expression of cross-sensitization to BD that had emerged in males over repeated sessions. These results provide preclinical, functional validation of PDE4B as a driver of food-ethanol cross-sensitization in a novel model for BE and BD comorbidity and support PDE4B in the shared genetic risk for these behavioral pathologies and as a target for pharmacotherapeutic intervention in comorbid AUD and BE behaviors.

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