4.2 Article

An assessment of executive function in two different rat models of attention-deficit hyperactivity disorder: Spontaneously hypertensive versus Lphn3 knockout rats

期刊

GENES BRAIN AND BEHAVIOR
卷 20, 期 8, 页码 -

出版社

WILEY
DOI: 10.1111/gbb.12767

关键词

Adgrl3; ADHD; CRISPR; Cas9; delayed spatial alternation; differential reinforcement of low rates; externalizing behavior; inhibitory control; Latrophilin-3; Lphn3; working memory

资金

  1. National Institute of Environmental Health Sciences [R01ES032270]
  2. University of Cincinnati Graduate School Dean's Disseration Completion Award
  3. University of Memphis

向作者/读者索取更多资源

The study explored the impact of Lphn3 deletion on behavioral control associated with ADHD and externalizing behaviors in rats. Results showed deficits in impulsive action and working memory in Lphn3(-/-) rats compared to control rats, suggesting a role for Lphn3 in modulating inhibitory control and working memory. Further research on the role of Lphn3 in externalizing disorders is warranted.
Attention-deficit/hyperactivity disorder (ADHD) a common neurodevelopmental disorder of childhood and often comorbid with other externalizing disorders (EDs). There is evidence that externalizing behaviors share a common genetic etiology. Recently, a genome-wide, multigenerational sample linked variants in the Lphn3 gene to ADHD and other externalizing behaviors. Likewise, limited research in animal models has provided converging evidence that Lphn3 plays a role in EDs. This study examined the impact of Lphn3 deletion (i.e., Lphn3(-/-)) in rats on measures of behavioral control associated with externalizing behavior. Impulsivity was assessed for 30 days via a differential reinforcement of low rates (DRL) task and working memory evaluated for 25 days using a delayed spatial alternation (DSA) task. Data from both tasks were averaged into 5-day testing blocks. We analyzed overall performance, as well as response patterns in just the first and last blocks to assess acquisition and steady-state performance, respectively. Positive control measures on the same tasks were measured in an accepted animal model of ADHD-the spontaneously hypertensive rat (SHR). Compared with wildtype controls, Lphn3(-/-) rats exhibited deficits on both the DRL and DSA tasks, indicative of deficits in impulsive action and working memory, respectively. These deficits were less severe than those in the SHRs, who were profoundly impaired on both tasks compared with their control strain, Wistar-Kyoto rats. The results provide evidence supporting a role for Lphn3 in modulating inhibitory control and working memory, and suggest additional research evaluating the role of Lphn3 in the manifestation of EDs more broadly is warranted.

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