Neuron-binding antibody responses are associated with Black ethnicity in multiple sclerosis during natalizumab treatment

Author:

Telesford Kiel M1ORCID,Smith Chad2,Mettlen Marcel3,Davis Melissa B4,Cowell Lindsay5,Kittles Rick6,Vartanian Timothy1,Monson Nancy2

Affiliation:

1. Weill Cornell Medicine, Brain and Mind Research Institute , New York, NY 10065 , USA

2. University of Texas Southwestern Medical Center, O’Donnell Brain Institute , Dallas, TX 75390 , USA

3. University of Texas Southwestern Medical Center, Department of Cell Biology , Dallas, TX 75390 , USA

4. Morehouse School of Medicine, Department of Community Health and Preventative Medicine , Atlanta, GA 30310 , USA

5. University of Texas Southwestern Medical Center, Peter O-Donnell Jr. School of Public Health , Dallas, TX 75390 , USA

6. Morehouse School of Medicine, Institute of Genomic Medicine , Atlanta, GA 30310 , USA

Abstract

Abstract Multiple sclerosis is an inflammatory degenerative condition of the central nervous system that may result in debilitating disability. Several studies over the past twenty years suggest that multiple sclerosis manifests with a rapid, more disabling disease course among individuals identifying with Black or Latin American ethnicity relative to those of White ethnicity. However, very little is known about immunologic underpinnings that may contribute to this ethnicity-associated discordant clinical severity. Given the importance of B cells to multiple sclerosis pathophysiology, and prior work showing increased antibody levels in the cerebrospinal fluid of Black-identifying, compared to White-identifying multiple sclerosis patients, we conducted a cohort study to determine B cell subset dynamics according to both self-reported ethnicity and genetic ancestry over time. Further, we determined relationships between ethnicity, ancestry, and neuron-binding IgG levels. We found significant associations between Black ethnicity and elevated frequencies of class-switched B cell subsets, including memory B cells; double negative two B cells; and antibody-secreting cells. The frequencies of these subsets positively correlated with West African genetic ancestry. We also observed significant associations between Black ethnicity and increased IgG binding to neurons. Our data suggests significantly heightened T cell-dependent B cell responses exhibiting increased titres of neuron-binding antibodies among individuals with multiple sclerosis identifying with the Black African diaspora. Factors driving this immunobiology may promote the greater demyelination, central nervous system atrophy and disability more often experienced by Black-, and Latin American-identifying individuals with multiple sclerosis.

Funder

National Center for Advancing Translational Sciences Weill Cornell Medicine Fellowship

National Institute of Allergy and Infectious Diseases

National Institute of Neurological Disorders and Stroke

Publisher

Oxford University Press (OUP)

Subject

Neurology,Cellular and Molecular Neuroscience,Biological Psychiatry,Psychiatry and Mental health

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