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Therapeutic B-cell depletion reverses progression of Alzheimer’s disease

Medicine and Health

Therapeutic B-cell depletion reverses progression of Alzheimer’s disease

K. Kim, X. Wang, et al.

This groundbreaking research explores the crucial role of B cells in Alzheimer's disease (AD), revealing their accumulation and infiltration in the brain, and suggesting that targeting these cells may provide a promising therapeutic strategy for AD patients. Conducted by leading experts including Ki Kim, Xin Wang, and others from the National Institute on Aging, this study highlights the potential for B cell depletion to reshape the future of AD treatment.

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Abstract
The function of B cells in Alzheimer’s disease (AD) is not fully understood. While immunoglobulins that target amyloid beta (Aβ) may interfere with plaque formation and hence progression of the disease, B cells may contribute beyond merely producing immunoglobulins. Here we show that AD is associated with accumulation of activated B cells in circulation, and with infiltration of B cells into the brain parenchyma, resulting in immunoglobulin deposits around Aβ plaques. Using three different murine transgenic models, we provide counterintuitive evidence that the AD progression requires B cells. Despite expression of the AD-fostering transgenes, the loss of B cells alone is sufficient to reduce Aβ plaque burden and disease-associated microglia. It reverses behavioral and memory deficits and restores TGFβ⁺ microglia, respectively. Moreover, therapeutic depletion of B cells at the onset of the disease retards AD progression in mice, suggesting that targeting B cells may also benefit AD patients.
Publisher
Nature Communications
Published On
Apr 12, 2021
Authors
Ki Kim, Xin Wang, Emeline Ragonnaud, Monica Bodogai, Tomer Illouz, Marisa DeLuca, Ross A. McDevitt, Fedor Gusev, Eitan Okun, Evgeny Rogaev, Arya Biragyn
Tags
Alzheimer's disease
B cells
immunoglobulin
amyloid-beta
therapeutic strategy
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