Novel 3D human cell-based model uncovers immune cell involvement in Alzheimer's disease progression, offering insights for accelerated treatment testing.
By studying immune cell behavior, a fresh 3D human cell-based model of Alzheimer's disease sheds light on progression, potentially hastening the development of effective treatments (1✔ ✔Trusted Source
Infiltrating CD8+ T cells exacerbate Alzheimer's disease pathology in a 3D human neuroimmune axis model
Go to source). Also, immune cells outside of the brain, //particularly T cells, can enter the brain and worsen AD pathology, but studying this process has been difficult.
‘Revealing how immune cells impact Alzheimer's disease, a newly developed 3D human cell-based model aids in understanding progression and expediting treatment trials.
#alzheimersdisease, #immunecells
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Now, a team led by researchers at Massachusetts General Hospital (MGH) has engineered a novel 3D human cellular model that mimics the intricate interactions between brain cells and these immune invaders. The work, which builds on previous 3D models of AD developed by the team, is described in Nature Neuroscience.
In the new study, the team used the model to demonstrate that as Alzheimer’s pathology accumulates in the brain, specific types of immune cells called CT8+ T Cells surge into the brain and amplify the destruction caused by neuroinflammation.
The team also identified the molecular mechanisms that drive the infiltration of T cells to the brain and showed that blocking these mechanisms reduced the destructive effects of T cell infiltration.
The findings could lead to new therapies for Alzheimer’s patients that target immune cell infiltration in the brain.
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“We hope our work contributes to developing a more physiologically relevant human Alzheimer’s disease model in a dish,” adds co–senior author Doo Yeon Kim, Ph.D., associate professor of Neurology at MGH.
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The model is an extension of previous work done by the research team to create and validate 3D lab models of AD that better replicate the hallmark plaques and tangles of the disease in a three-dimensional environment—much, in the same way, the disease develops in the brain.
Revolutionizing Alzheimer's Treatment Testing
In addition to observing higher levels of T cells in AD brain models, the team identified a pathway between a chemokine (CXCL10) and a chemokine receptor (CXCR3) that plays a key role in regulating T cell infiltration.Blocking this pathway largely prevented T-cell infiltration and neurodegeneration in AD cultures.
The findings could help in identifying new therapeutic targets that slow or halt the infiltration of T cells into the brains of Alzheimer’s patients, and potentially reduce the devastating cognitive impacts of the disease.
"his multidisciplinary research approach identified the different behaviors of distinct cell types in this disease context, and we aim to shed light on the underlying mechanisms to identify strategies for intervention that could lead to more effective treatments," said co–lead author Joseph Park, Ph.D., instructor in Neurology at MGH.
Additional targets may be identified with continued experiments with this model.
“Perhaps, what is most exciting about this study is that we have identified a new drug target on T cells, outside of the brain, which would be more accessible to novel treatments, especially since it has been traditionally difficult to get drugs into the brain,” says senior author Rudolph Tanzi, PhD, director of the Genetics and Aging Research Unit at MGH.
Reference:
- Infiltrating CD8+ T cells exacerbate Alzheimer’s disease pathology in a 3D human neuroimmune axis model - (https://www.nature.com/articles/s41593-023-01415-3)
Source-Eurekalert