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Twin Study Identifies Early Immunological and Metabolic Dysregulation of CD8 + T Cells in Multiple Sclerosis

Vladyslav Kavaka, Luisa Mutschler, Clara de la Rosa Del Val, Klara Eglseer, Ana M Gómez Martínez,Andrea Flierl-Hecht, Birgit Ertl-Wagner,Daniel Keeser, Martin Mortazavi,Klaus Seelos, Hanna Zimmermann,Jürgen Haas,Brigitte Wildemann, Tania Kümpfel,Klaus Dornmair,Thomas Korn,Reinhard Hohlfeld,Martin Kerschensteiner, Lisa Ann Gerdes,Eduardo Beltrán

Science immunology(2024)

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摘要
Multiple sclerosis (MS) is an inflammatory neurological disease of the central nervous system with a subclinical phase preceding frank neuroinflammation. CD8 + T cells are abundant within MS lesions, but their potential role in disease pathology remains unclear. Using high-throughput single-cell RNA sequencing and single-cell T cell receptor analysis, we compared CD8 + T cell clones from the blood and cerebrospinal fluid (CSF) of monozygotic twin pairs in which the cotwin had either no or subclinical neuroinflammation (SCNI). We identified peripheral MS-associated immunological and metabolic alterations indicative of an enhanced migratory, proinflammatory, and activated CD8 + T cell phenotype, which was also evident in cotwins with SCNI and in an independent validation cohort of people with MS. Together, our in-depth single-cell analysis indicates a disease-driving proinflammatory role of infiltrating CD8 + T cells and identifies potential immunological and metabolic therapeutic targets in both prodromal and definitive stages of the disease.
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