Preventing cell loss. Top: Dopamine cells (green) in the substantia nigra of healthy mice. Middle: Dopamine cells degenerate in mice exposed to misfolded Ī±-synuclein. Bottom: In mice lacking mGluR4 and NPDC1, dopamine cells are preserved after exposure to misfolded Ī±-synuclein. Credit: Yale School of Medicine
Two proteins found ā¦
Preventing cell loss. Top: Dopamine cells (green) in the substantia nigra of healthy mice. Middle: Dopamine cells degenerate in mice exposed to misfolded Ī±-synuclein. Bottom: In mice lacking mGluR4 and NPDC1, dopamine cells are preserved after exposure to misfolded Ī±-synuclein. Credit: Yale School of Medicine
Two proteins found on the surface of motor neurons in the brain may be essential in the progression of Parkinsonās disease, according to new Yale School of Medicine (YSM) research.
Parkinsonās disease is a neurodegenerative condition where neurons in the brain slowly break down and die. Cell death is caused by the accumulation of a misfolded protein called Ī±-synuclein, which spreads from neuron to neuron.
The mechanism by which Ī±-synuclein spreads among cells, however, remains unknown. Now, a new study published in Nature Communications suggests that two membrane proteinsāmGluR4 and NPDC1āare major players in transporting misfolded Ī±-synuclein into healthy neurons after it escapes from dying neurons.
The finding could help develop more effective treatments for Parkinsonās disease, says senior author Stephen Strittmatter, MD, Ph.D., Vincent Coates Professor of Neurology and chair of the Department of Neuroscience at YSM.
Misfolded Ī±-synuclein is "the pathologic hallmark of Parkinsonās disease," he says. "If we understood how it gets into neurons, we could perhaps block or slow down the progression of the disease," he adds. But to do that, "we need to understand the molecular mechanism of how it spreads."
Transporting Ī±-synuclein
Neurodegenerative diseases like Alzheimerās and Parkinsonās are a growing health concern in the United States. The Parkinsonās Foundation currently estimates that around 1.1 million Americans are diagnosed with Parkinsonās disease, and nearly 90,000 more people join their ranks every year.
People with Parkinsonās disease often experience motor issues, such as tremors, trouble with balance, and slowed movement. These symptoms are caused by the accumulation of misfolded Ī±-synuclein in motor cells in the brain. As Ī±-synuclein spreads between neurons, symptoms worsen.
One way Ī±-synuclein could enter new cells is by binding to surface proteins. To determine whether this was the case, Strittmatter and his colleagues created 4,400 batches of cells, each expressing different cell surface proteins, and observed whether they bound to misfolded Ī±-synuclein.
Most cell surface proteins did not. But 16 did, including two found in the human dopamine neurons of the substantia nigra, a region of the brain that degenerates in Parkinsonās disease. The researchers found that these two, called mGluR4 and NPDC1, transported misfolded Ī±-synuclein into the cell.
Preventing the spread of Parkinsonās pathology
These results suggested to Strittmatter and his colleagues that the two cell surface proteins could be involved in moving Ī±-synuclein from neuron to neuron. To test this, the researchers genetically modified mice to have nonfunctional copies of either mGluR4 or NPDC1 and then introduced misfolded Ī±-synuclein.
In regular mice, misfolded Ī±-synuclein accumulated in their brains once introduced, and the mice developed Parkinsonās-like symptoms. But mice without working mGluR4 or NPDC1 didnāt. The researchers also found that knocking out the genes for these two cell surface proteins in a mouse model of Parkinsonās disease helped reduce the risk of death and progression of symptoms.
Altogether, the researchersā experiments suggest that mGluR4 and NPDC1 work together to move misfolded Ī±-synuclein into neurons in mice.
The findings offer a potential avenue for treating Parkinsonās disease, Strittmatter says. Current Parkinsonās disease interventions focus on reducing symptoms but do not effectively prevent progression of the disease. Going directly after the spread of Ī±-synuclein could provide treatments to slow or halt the course of Parkinsonās disease, he says.
New, effective treatments will be especially important in the coming decades. Parkinsonās and other neurodegenerative diseases largely impact older people. The number of Americans over the age of 65 is expected to increase over the next few decadesāmeaning that more people will be at risk of developing Parkinsonās disease.
"We have an aging population. How we can stop or slow neurons from dying is an enormous problem," says Strittmatter. "This is really the time to make some inroads into figuring out how to slow it down."
More information
Azucena Perez-Canamas et al, mGluR4āNPDC1 complex mediates Ī±-synuclein fibril-induced neurodegeneration, Nature Communications (2025). DOI: 10.1038/s41467-025-67731-3
Journal information: Nature Communications
Citation: Proteins that spread Parkinsonās pathology in the brain identified (2026, January 6) retrieved 6 January 2026 from https://medicalxpress.com/news/2026-01-proteins-parkinson-pathology-brain.html
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