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Publication : Cellular architecture of evolving neuroinflammatory lesions and multiple sclerosis pathology.

First Author  Kukanja P Year  2024
Journal  Cell Volume  187
Issue  8 Pages  1990-2009.e19
PubMed ID  38513664 Mgi Jnum  J:347632
Mgi Id  MGI:7621043 Doi  10.1016/j.cell.2024.02.030
Citation  Kukanja P, et al. (2024) Cellular architecture of evolving neuroinflammatory lesions and multiple sclerosis pathology. Cell 187(8):1990-2009.e19
abstractText  Multiple sclerosis (MS) is a neurological disease characterized by multifocal lesions and smoldering pathology. Although single-cell analyses provided insights into cytopathology, evolving cellular processes underlying MS remain poorly understood. We investigated the cellular dynamics of MS by modeling temporal and regional rates of disease progression in mouse experimental autoimmune encephalomyelitis (EAE). By performing single-cell spatial expression profiling using in situ sequencing (ISS), we annotated disease neighborhoods and found centrifugal evolution of active lesions. We demonstrated that disease-associated (DA)-glia arise independently of lesions and are dynamically induced and resolved over the disease course. Single-cell spatial mapping of human archival MS spinal cords confirmed the differential distribution of homeostatic and DA-glia, enabled deconvolution of active and inactive lesions into sub-compartments, and identified new lesion areas. By establishing a spatial resource of mouse and human MS neuropathology at a single-cell resolution, our study unveils the intricate cellular dynamics underlying MS.
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