Obesity hypoventilation syndrome (OHS) is a severe form of sleep disordered breathing (SDB) characterized by daytime hypercapnia and hypoventilation during sleep. OHS is driven by chronically decreased CO2 sensitivity and depressed ventilatory responses to CO2 (hypercapnic ventilatory response, HCVR). Non-invasive ventilation restores CO2 sensitivity and treats OHS. However, adherence to this treatment is poor. There is no effective pharmacotherapy for OHS. Leptin increases HCVR and treats hypoventilation in leptin deficient ob/ob mice. Diet-induced obese (DIO) mice emulate all features of human OHS, including awake hypercapnia, upper airway obstruction during sleep and sleep hypoventilation. However human and mouse DIO become resistant to leptin limiting leptin as a pharmacotherapy. This proposal is focused on identifying pharmacological targets downstream of the leptin network to treat OHS. Leptin upregulates pro-opiomelanocortin, which is a pre- hormone post-transcriptionally processed into several peptides, including α melanocyte stimulating hormone, a ligand for the melanocortin 4 receptor (MC4R) promoting energy expenditure. The MC4R agonist setmelanotide has been approved for treatment of genetic forms of obesity linked to mutations in the POMC/MC4R/leptin pathways. The role of MC4R in control of breathing remains unknown. Our exciting preliminary data shows that setmelanotide augments the HCVR and treats SDB in DIO mice, that chemogenetic activation of MC4R (+) neurons in the parafacial region containing the chemosensitive retrotrapezoid nucleus (RTN) increases baseline ventilation and HCVR without any effect on metabolism; and that MC4R (+) parafacial neurons project to brainstem respiratory premotor neurons, that, in turn, project to the phrenic motor nucleus. Our overarching hypothesis is that MC4R agonists treat OHS by augmenting hypercapnic sensitivity in MC4R+ neurons in the parafacial region, which is a major center of CO2 sensitivity. In Specific Aim 1, we will determine the therapeutic benefits of the MC4R agonist setmelanotide in OHS in DIO mice. We hypothesize that (A) a single dose will acutely; and (B) a three-month course of setmelanotide will chronically augment HCVR and abolish SDB in randomized placebo-controlled trials; and that (C) the effect of setmelanotide on ventilation will be prevented by the MC4R blocker SHU9119. In Specific Aim 2, we will use DIO Mc4r-Cre mice to examine if the respiratory effects of MC4R activation by setmelanotide can be mimicked by chemogenetic activation and attenuated by chemogenetic inhibition of MC4R+ parafacial neurons. In in vitro Specific Aim 3, we will examine the synaptic neurotransmission from MC4R (+) neurons in the parafacial region to the rostral ventral respiratory group (rVRG) neurons that project to the phrenic motor nucleus using selective expression of ChR2 in Mc4r-Cre parafacial neurons, retrograde identification of spinally projecting rVRG neurons and patch clamp electroph...