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Título
Multiomic‐based immune response profiling in migraine, vestibular migraine and Meniere's disease
Autor(es)
Palabras clave
Meniere disease
Autoinflammation
Cytokines
Migraine
Monocytes
Clasificación UNESCO
2412 Inmunología
Fecha de publicación
2024-12-01
Editor
wiley
Citación
Cruz‐Granados, P., Frejo, L., Perez‐Carpena, P., Amor‐Dorado, J. C., Dominguez‐Duran, E., Fernandez‐Nava, M. J., ... & Lopez‐Escamez, J. A. (2024). Multiomic‐based immune response profiling in migraine, vestibular migraine and Meniere's disease. Immunology, 173(4), 768-779.
Resumen
[EN]Migraine (MI) is the most common neurological disease, affecting with 20% of the world population. A subset of 25% of MI patients showcase concurrent vestibular symptoms, which may classify as vestibular migraine (VM). Meniere's disease (MD) is a complex inner ear disorder defined by episodes of vertigo associated with tinnitus and sensorineural hearing loss with a significant autoimmune/autoinflammatory contribution, which symptoms overlap with VM. Blood samples from 18 patients with MI (5), VM (5) and MD (8) and 6 controls were collected and compared in a case–control study. Droplet-isolated nuclei from mononuclear cells used to generate scRNAseq and scATACseq data sets from MI, VM and MD. MI and VM have no differences in their immune transcriptome; therefore, they were considered as a single cluster for further analyses. Natural Killer (NK) cells transcriptomic data support a polarisation triggered by Type 1 innate immune cells via the release of interleukin (IL)-12, IL-15 and IL-18. According to the monocyte scRNAseq data, there were two MD clusters, one inactive and one driven by monocytes. The unique pathways of the MI + VM cluster were cellular responses to metal ions, whereas MD monocyte-driven cluster pathways showed responses to biotic stimuli. MI and MD have different immune responses. These findings support that MI and VM have a Type 1 immune lymphoid cell response, and that there are two clusters of MD patients, one inactive and one Monocyte-driven.
URI
ISSN
0019-2805
DOI
10.1111/imm.13863
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