Cell Type-Specific Intralocus Interactions Reveal Oligodendrocyte Mechanisms in MS | Zendy

Daniel C. Factor | Zendy; Anna M. Barbeau | Zendy; Kevin Allan | Zendy; Lucille R. Hu | Zendy; Mayur Madhavan | Zendy; An T. Hoang | Zendy; Kathryn E.A. Hazel | Zendy; Parker A. Hall | Zendy; Sagar Nisraiyya | Zendy; Fadi J. Najm | Zendy; Tyler E. Miller | Zendy; Zachary S. Nevin | Zendy; Robert T. Karl | Zendy; Bruna R. Lima | Zendy; Yanwei Song | Zendy; Alexandra G. Sibert | Zendy; Gursimran Dhillon | Zendy; Christina Volsko | Zendy; Cynthia F. Bartels | Zendy; Drew Adams | Zendy; Ranjan Dutta | Zendy; Michael D. Gallagher | Zendy; William Phu | Zendy; Alexey Kozlenkov | Zendy; Stella Dracheva | Zendy; Peter C. Scacheri | Zendy; Paul J. Tesar | Zendy; Olivia Corradin | Zendy

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Cell Type-Specific Intralocus Interactions Reveal Oligodendrocyte Mechanisms in MS

Author(s) -

Daniel C. Factor,

Anna M. Barbeau,

Kevin Allan,

Lucille R. Hu,

Mayur Madhavan,

An T. Hoang,

Kathryn E.A. Hazel,

Parker A. Hall,

Sagar Nisraiyya,

Fadi J. Najm,

Tyler E. Miller,

Zachary S. Nevin,

Robert T. Karl,

Bruna R. Lima,

Yanwei Song,

Alexandra G. Sibert,

Gursimran Dhillon,

Christina Volsko,

Cynthia F. Bartels,

Drew Adams,

Ranjan Dutta,

Michael D. Gallagher,

William Phu,

Alexey Kozlenkov,

Stella Dracheva,

Peter C. Scacheri,

Paul J. Tesar,

Olivia Corradin

Publication year - 2020

Publication title -

cell

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 26.304

H-Index - 776

eISSN - 1097-4172

pISSN - 0092-8674

DOI - 10.1016/j.cell.2020.03.002

Subject(s) - biology , multiple sclerosis , oligodendrocyte , myelin , cell type , neuroscience , immune system , central nervous system , demyelinating disorder , cell , regeneration (biology) , genetics , immunology

Multiple sclerosis (MS) is an autoimmune disease characterized by attack on oligodendrocytes within the central nervous system (CNS). Despite widespread use of immunomodulatory therapies, patients may still face progressive disability because of failure of myelin regeneration and loss of neurons, suggesting additional cellular pathologies. Here, we describe a general approach for identifying specific cell types in which a disease allele exerts a pathogenic effect. Applying this approach to MS risk loci, we pinpoint likely pathogenic cell types for 70%. In addition to T cell loci, we unexpectedly identified myeloid- and CNS-specific risk loci, including two sites that dysregulate transcriptional pause release in oligodendrocytes. Functional studies demonstrated inhibition of transcriptional elongation is a dominant pathway blocking oligodendrocyte maturation. Furthermore, pause release factors are frequently dysregulated in MS brain tissue. These data implicate cell-intrinsic aberrations outside of the immune system and suggest new avenues for therapeutic development.

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