Hypothalamic POMC deficiency leads to obesity and metabolic deficiencies， largely due to the loss of melanocortin peptides. However， POMC neurons in the arcuate nucleus (ARC) are comprised of glutamatergic and GABAergic subpopulations. The developmental program， relative proportion and function of these two subpopulations are unresolved. To test whether glutamatergic POMC neurons serve a distinct role in maintaining energy homeostasis， we activated expression Cre- dependently in -expressing neurons of mice with conditionally silenced alleles. The - restored mice had normal ARC mRNA levels， POMC immunoreactivity， as well as body weight and body composition at age 12 weeks. Unexpectedly， the cumulative total of glutamatergic- and - neurons detected by hybridization (ISH) exceeded 100% in both - restored and control mice， indicating that a subpopulation of neurons must express both neuronal markers. Consistent with this hypothesis， triple ISH of C57BL/6J hypothalami revealed that 35% of ARC neurons were selectively ， 21% were selectively ， and 38% expressed both and . The single and neurons were most prevalent in the rostral ARC， while the dual-phenotype cells predominated in the caudal ARC. A lineage trace using Ai9-tdTomato reporter mice to label fluorescently all -expressing neurons showed equal numbers of tdTomato and tdTomato POMC immunoreactive neurons. Together， these data suggest that POMC neurons exhibit developmental plasticity in their expression of glutamatergic and GABAergic markers， enabling re-establishment of normal energy homeostasis in the - restored mice.