The ability to decide adaptively between immediate vs. delayed gratification (intertemporal choice) is critical for well-being and is associated with a range of factors that influence quality of life. In contrast to young adults, many older adults show enhanced preference for delayed gratification; however, the neural mechanisms underlying this age difference in intertemporal choice are largely un-studied. Changes in signaling through GABA receptors (GABARs) mediate several age-associated differences in cognitive processes linked to intertemporal choice. The current study used a rat model to determine how GABARs in two brain regions known to regulate intertemporal choice (prelimbic cortex; PrL and basolateral amygdala; BLA) contribute to age differences in this form of decision making in male rats. As in humans, aged rats showed enhanced preference for large, delayed over small, immediate rewards during performance in an intertemporal choice task in operant test chambers. Activation of PrL GABARs via microinfusion of the agonist baclofen increased choice of large, delayed rewards in young adult rats but did not influence choice in aged rats. Conversely, infusion of baclofen into the BLA strongly reduced choice of large, delayed rewards in both young adult and aged rats. Aged rats further showed a significant reduction in expression of GABAR1 subunit isoforms in the prefrontal cortex, a discovery that is consonant with the null effect of intra-PrL baclofen on intertemporal choice in aged rats. In contrast, expression of GABAR subunits was generally conserved with age in the BLA. Jointly, these findings elucidate a role for GABARs in intertemporal choice and identify fundamental features of brain maturation and aging that mediate an improved ability to delay gratification.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9297337PMC
http://dx.doi.org/10.1016/j.neuropharm.2022.109001DOI Listing

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