Previous reports have shown that running wheel activity or voluntary exercise prevents
hyperphagia and
obesity in various animal models of
obesity, but such effects seem only minimal in obese animals lacking
leptin or
leptin receptors. The mechanisms underlying this ineffectiveness remain unclear. Here, we identified the action of neuronal activation in the dorsomedial hypothalamus (
DMH) in modulating physical activity, food intake and
body weight using
leptin receptor mutant obese Zucker (Lepr(fa), ZF) and Koletsky (Lepr(fak), SHROB) rats. Ad lib-fed SHROB rats with locked running wheels became hyperphagic and gained
body weight rapidly. These alterations were not ameliorated in ad lib-fed SHROB rats with voluntary access to running wheels, but the
body weight of SHROB rats with running wheel access was significantly decreased when they were pair-fed to the amounts consumed by lean controls. Determinations of hypothalamic gene expression revealed that sedentary ad lib-fed SHROB rats had increased expression of
neuropeptide Y (Npy) and decreased expression of
pro-opiomelanocortin (
Pomc) in the arcuate nucleus (
ARC). Both
ARC Npy and
Pomc expression were further altered under running and pair-fed conditions, indicating that both genes are appropriately regulated in response to increased energy demands or alterations caused by running activity and food restriction. Strikingly, c-Fos immunohistochemistry revealed that while voluntary running activity elevated the number of c-Fos positive cells in the
DMH (particularly in the ventral and caudal subregions) of intact rats, such activation was not observed in ZF rats. Using adeno-associated virus (AAV)-mediated expression of the designer receptors hM3D(Gq) in the ventral and caudal
DMH of ZF rats, we found that chemogenetic stimulation of neurons in these
DMH subregions via injection of the
designer drug clozapine N-oxide (CNO) significantly increased their running activity and reduced their food intake and
body weight. Together, these results demonstrate that activation of ventral and caudal
DMH neurons promotes physical activity and decreases food intake and
body weight and suggest that intact
DMH neural signaling is likely crucial for exercise-induced reductions of food intake and
body weight in obese rats lacking
leptin receptors.