Microglia Exacerbate Damage in APOE4 Model of Alzheimer’s
New research shows that microglia, which usually clear debris, cause inflammation in the presence of APOE4 protein.
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In healthy brains, immune cells called microglia patrol for damage, clearing away debris and harmful proteins. But in the presence of the APOE4 protein—the most important genetic risk factor for Alzheimer’s disease—the same cells cause harmful inflammation and clumps of misfolded proteins, according to a new study by scientists at Gladstone Institutes.
The team created a new research model for studying Alzheimer’s that involved transplanting human neurons producing the APOE4 protein into the brains of mice.
When they removed microglia from the brains, they discovered that the APOE4 protein no longer triggered as many deposits of amyloid or tau—two types of misfolded proteins that are hallmarks of Alzheimer’s disease.
“The study underscores the importance of microglia, in concert with APOE4 produced by human neurons, in Alzheimer’s,” says Gladstone Senior Investigator Yadong Huang, MD, PhD, who supervised the new study published in Cell Stem Cell. “Our findings suggest that drugs reducing microglia may eventually be useful in treating the disease.”
A Human-Like Model
There are three major forms of APOE protein in humans. Compared with the most common version of the protein—APOE3—the APOE4 protein increases risk and APOE2 decreases risk for Alzheimer’s disease.
About one in four Americans has at least one copy of the APOE4 gene, and roughly 3 percent have two copies, making those individuals especially susceptible to the disease.
“People with two copies of the APOE4 gene have a 12-fold greater risk of developing Alzheimer’s disease than those with APOE3,” says Huang, who is also director of the Center for Translational Advancement at Gladstone and a professor in the Departments of Neurology and Pathology at UC San Francisco.
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Subscribe for FREEIn the new study, Huang’s team developed a “chimeric” mouse model that not only carries human APOE genes, but also contains human neurons that are transplanted into the brain. Importantly, the neurons are transplanted after the brain matures, allowing the researchers to mimic late-onset Alzheimer’s disease.
Previous attempts to establish a mouse model that expresses the characteristics of late-onset Alzheimer’s have been unsuccessful when they used only the APOE4 protein, without transplanted human neurons.
“Creating this mouse model gave us a much more realistic way to study how human neurons carrying the APOE4 gene contribute to Alzheimer’s disease in the living brains of older adults,” says Antara Rao, a graduate student in Huang’s lab who led the experiments for the new study.
Huang and his colleagues already knew that APOE4 leads to higher-than-usual levels of amyloid plaques and tau tangles in human brains. In the new chimeric mouse model, the researchers confirmed that the presence of human APOE4 neurons leads to high levels of both amyloid and tau deposits as the mice aged.
They also showed that human APOE3 neurons lead to moderate levels of the aggregates, and human neurons lacking the APOE gene altogether resulted in fewer tau aggregates and scattered amyloid deposits rather than dense, harmful aggregates.
“It turns out that more accurately modeling late-onset Alzheimer’s disease requires human neurons, rather than mouse neurons, producing APOE4 in mouse brains,” says Huang.
Protective Effect of Reducing Microglia
Huang’s group previously found that mouse neurons producing human APOE4 release molecular signals that activate microglia. This time, they used the new mouse model to probe in more detail the connection between microglia and human neurons producing APOE4.
The researchers used a drug to selectively remove microglia from the brains of the chimeric mice. In mice with human APOE4 neurons, they found that levels of the amyloid and tau aggregates were significantly reduced, indicating that APOE4 and microglia work together to drive key attributes of Alzheimer’s disease.
The team then turned to single-cell RNA sequencing—a powerful technique to study gene activity in individual cells—to determine what genes were activated in the microglia of each mouse model.
They found that in the presence of human neurons containing APOE4 and APOE3, levels of inflammatory molecules in microglia increased. Microglia with the most inflammatory molecular signatures made up 30 percent of all microglia in mice with human APOE4 neurons, 20 percent of all microglia in mice with human APOE3 neurons, and only 8 percent of all microglia in mice that had human neurons lacking the APOE gene.
“Together, these results suggest that microglia are being activated by human neuron–produced APOE4 and, in turn, are potentially helping form the misfolded protein aggregates we see in Alzheimer’s,” says Rao.
A Path Toward New Treatments
The findings give researchers new inroads to understand how microglia go awry in Alzheimer’s, flipping from its normally protective state to a harmful state in the presence of APOE4 produced by human neurons.
The study also suggests that drugs that can reduce levels of APOE4 in neurons or target microglia—either by reducing the number of microglia or their level of inflammatory activity—could be a promising strategy for slowing or preventing Alzheimer’s disease progression in people with the APOE4 gene.
Still, more work is needed to show whether these potential strategies would be effective in humans, what the side effects of targeting neuronal APOE4 or microglia would be, and how the timing of such treatment would work.
The researchers also hope to use their new chimeric mouse to study the roles of other cell types in Alzheimer’s disease.
“Our new mouse model, along with these initial results, offers a path forward to better understanding Alzheimer’s disease, especially in the context of APOE4, and developing new drugs that could treat it,” says Huang.
Reference: Rao A, Chen N, Kim MJ, et al. Microglia depletion reduces human neuronal APOE4-related pathologies in a chimeric Alzheimer’s disease model. Cell Stem Cell. 2024. doi: 10.1016/j.stem.2024.10.005
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