Session: 898 APS Respiratory Dysfunction in Neurological Disease and Injury: Mechanisms and Potential Therapeutics Poster Session
(898.6) Single Nuclear RNA Sequencing Reveals Activation of Neuroinflammation Within the Pre-Bötzinger Complex Following Repeated Seizures
Tuesday, April 5, 2022
10:15 AM – 12:15 PM
Location: Exhibit/Poster Hall A-B - Pennsylvania Convention Center
Poster Board Number: E409
Wasif Osmani (Medical College of Wisconsin), Erin Duffy (Medical College of Wisconsin), Anna Manis (Medical College of Wisconsin), Neil Rohde (Medical College of Wisconsin), Gary Mouradian (Medical College of Wisconsin), Hubert Forster (Medical College of Wisconsin), Alexander Staruschenko (Medical College of Wisconsin), Matthew Hodges (Medical College of Wisconsin)
Epilepsy is one of the most common neurological diseases in the world. Treatment with anti-epileptic drugs (AEDs) prevents recurrent seizures in ~70% of patients with epilepsy, but the remaining 30% of patients with refractory epilepsies continue to experience seizures. The consequences of repeated seizures include, but are not limited to, a high risk of post-ictal cardiorespiratory failure and Sudden Unexpected Death in Epilepsy (SUDEP). Fundamental gaps exist in understanding how repeated seizures disrupt the vital cardiorespiratory control system in refractory epilepsy. A factor commonly identified in many neurological conditions is neuroinflammation, which may support beneficial health functions but is dysregulated in neurological disease. Key cells within the CNS that mediate beneficial and/or pathological neuroinflammation are resident microglia and astrocytes, which have been shown to be dysfunctional in human epilepsy and alter neuronal function. However, it is not known what mechanistic role they play in contributing to epilepsy-related impairment in cardiorespiratory control or increased SUDEP risk. Here, we tested the hypothesis that repeated seizures lead to activation of neuroinflammation mediated by microglia and astrocytes in CNS regions of cardiorespiratory control, leading to a progressive decline in neurologic function. Preliminary data in our novel rat model with genetic mutations in Kcnj16, a gene encoding an inwardly-rectifying potassium channel Kir5.1 in Dahl salt-sensitive rat (SSkcnj16-/-) show that repeated sound-induced seizures lead to a progressively more severe post-ictal suppression of breathing frequency and heart rate. Single nuclear RNA sequencing of pre-Bötzinger Complex/Nucleus Ambiguous cells (roughly 80,000) was performed from rats exposed to 0, 3, 7, or 10 seizures to measure cell type-specific gene expression changes induced by seizures. Bioinformatic analyses of transcriptomic changes in microglia, neuronal, and glial cells within these regions point to activation of specific inflammatory pathways following repeated seizures such as IL-1 signaling and Toll-like Receptor signaling. Afterwards, cytokine-chemokine array was performed in brain regions regulating cardiorespiratory control after rats were exposed to 0, 3, 7, or 10 seizures and confirmed the presence of neuroinflammation after seizure induction. Identifying neuroinflammatory signals/pathways induced by repeated seizures within distinct neural circuits will enhance understanding of pathophysiological consequences of uncontrolled seizures in patients with refractory epilepsy and hold the potential for identifying new therapeutic targets aimed at improving cardiorespiratory function to reduce the risk of SUDEP.
