PROJECT SUMMARY In the United States, one in three women of reproductive age is obese. In epidemiologic studies, maternal obesity is associated with neurodevelopmental morbidity in children, including cognitive deficits, autism spectrum disorder, anxiety and depression, disordered eating, and attention deficit hyperactivity disorder. Many of these disorders have a sex bias, and aberrant brain immune activation (microglial priming, or “trained immunity”), has been implicated in their pathogenesis. While direct evaluation of microglial function in a living human fetus or neonate is impossible, resident placental macrophages (Hofbauer cells) and microglia have a common origin in the fetal yolk sac. “Fetal Brain-Placental Immune Activation in Maternal Obesity” is a pre-clinical R01 that tests the hypothesis that maternal obesity-associated inflammatory priming of fetal brain microglia and placental Hofbauer cells is a targetable mechanism underlying offspring cognitive deficits. A key translational aspect of the funded project is the use of single-cell RNA sequencing (scRNA-Seq) to determine whether Hofbauer cells represent a novel biologic surrogate for microglial immunoreactivity in the setting of maternal obesity. In 2019, we were funded to complete the following specific aims: Aim 1a: Determine whether maternal obesity primes fetal brain and placental resident macrophages to overrespond to an immune challenge. Aim 1b: Evaluate whether Hofbauer cells can serve as a biologic surrogate for brain microglial priming, using scRNA-Seq and flow cytometry. Aim 2: Determine if targeted ablation of pro-inflammatory signaling in fetal resident tissue macrophages (including microglia and placental Hofbauer cells) rescues hippocampal learning deficits in offspring, using a novel Cx3cr1-CreBT:MyD88f/f transgenic mouse. Both sexes are evaluated in all experiments, except the scRNA-Seq in Aim 1b. We have completed initial sequencing for 16 male brain and placental macrophage samples from obese and lean dams. We have demonstrated novel gene programs and cell states that define male microglia and Hofbauer cells in the context of maternal obesity. This administrative supplement proposal aims to expand the scRNA-Seq experiments in Aim 1b of the parent grant to include female fetal microglia and placental macrophages. This will allow us to test whether maternal obesity induces sex-specific alterations in fetal microglial and Hofbauer cell programs, and whether Hofbauer cell subsets can serve as a biologic surrogate for fetal brain microglial priming in the setting of maternal obesity. Determination of how fetal sex impacts microglial and placental macrophage gene programs and cell states will generate key insights into how obesity-associated brain and placental immune activation influences sex-specific neurodevelopmental outcomes. If Hofbauer cells can serve as a more accessible cell type that provides information about brain microglial function in maternal obesity, t...