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Tuesday, December 3, 2019
Neurodegenerative diseases may be caused by transportation failures inside neurons
DECEMBER 3, 2019 by Katherine Fenz, Rockefeller University
When the system that transports molecules through the long branches of neurons (pink) breaks down, chaos slowly ensues. Credit: Rockefeller University
All neurodegenerative diseases have a common thread: the appearance of protein clumps in the brain such as amyloid-beta plaques in Alzheimer's disease and alpha synuclein aggregates in Parkinson's. The root cause of this buildup has been hard to pinpoint, but Rockefeller scientists have identified a likely culprit that opens up a new avenue for developing treatments.
In a pair of studies carried out in flies and mice, the researchers discovered that the issue lies in the system that transports proteasomes, the molecular machinery that breaks down proteins, to specific locations within a cell.
"This is the first study to find a mechanism by which the proteasomes are moved to nerve endings to do their job," says Hermann Steller, the Strang Professor at Rockefeller. "When this mechanism gets disrupted, there are severe consequences for the function and long-term survival of nerve cells."
Location, location, location
Proteasomes are made in the cell body of a neuron and need to be transported over long distances to reach the nerve endings where the neuron connects with other cells—a journey of more than one meter in some cases. When proteasomes fail to reach these critical communication hubs, the cell descends into turmoil.
"Instead of being degraded, damaged proteins in these sites hang around long enough to interact with other binding partners, form aggregates, and disrupt cell function," Steller says. Over time, this causes degeneration of nerve fibers and ultimately cell death.
When Steller and his team began investigating the proteasome transportation system in fruit flies, they identified a protein called PI31, which plays a crucial role in loading the proteasomes onto the cellular components that ferry them around. In research published in Developmental Cell, they show that PI31 enhances binding and promotes movement of proteasomes with cellular motors. Without it, transport is halted. This is the case in both fly and mouse neurons, suggesting that the transport mechanism is common between many species.
Digging deeper into what happens when PI31 is defective, the scientists worked with Mary Beth Hatten's lab to generate mice whose PI31 gene was switched off in two groups of brain cells with particularly long extensions. In research published in the Proceedings of the National Academy of Sciences, they found that without PI31, proteasomes cannot travel, resulting in abnormal proteins levels at the tips of neuronal branches. The PI31-lacking neurons also looked peculiar, both with respect to their branches and to their synapses, the structures where branches from two neurons connect.
"Notably, these structural changes became progressively more severe with age," says Steller. "Inactivation of PI31 in these neurons was reminiscent of the severe behavioral and anatomical defects we see in some human neurogenerative disease."
Opportunities for therapy
There are other reasons to suspect that the lab's findings could inform the treatment of neurodegenerative diseases. For example, mutations in a human gene called PARK15, which is critical for PI31 activity, have been identified in a severe form of early-onset Parkinson's disease; and mutations in the PI31 gene itself have been linked to Alzheimer's disease.
Steller and his team are now working to determine if PI31, or molecules that affect its activity, are viable drug targets. The fact that PI31 appears to be involved in the early stages of nerve cell degeneration is especially compelling, as it could mean that drugs blocking this protein might have the potential to halt brain damage early on in the process.
As for what actually causes brains to degenerate, Steller believes the formation of aggregates is likely not the direct disease mechanism, but rather a symptom of bigger problems. "Our work suggests that it really starts with a local defect in proteasomes, resulting in the failure to degrade proteins that are critical for nerve function" he says. "These undigested proteins subsequently form aggregates and activate additional damage control pathways. But eventually, these clearance systems are overwhelmed, which causes a slow but steady progression to a detectable disease."
Steller and his colleagues are now investigating ways to stimulate the transportation pathway to get proteasomes out to the distal branches—work they believe could have a broad impact on the treatment of neurodegenerative diseases.
More information:Adi Minis et al, The proteasome regulator PI31 is required for protein homeostasis, synapse maintenance, and neuronal survival in mice,Proceedings of the National Academy of Sciences(2019).DOI: 10.1073/pnas.1911921116
Kai Liu et al. PI31 Is an Adaptor Protein for Proteasome Transport in Axons and Required for Synaptic Development, Developmental Cell (2019). DOI: 10.1016/j.devcel.2019.06.009
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i was diagnosed of parkinson disease 5 years ago,i started azilect,then mirapex as the disease progressed in february last year,and i started on parkinson disease Herbal medicine from ultimate herbal home,few months into the treatment i made a significant recovery,almost all my symptoms are gone,great improvement with my movement and balance,it been a year and life has been so good for me,contact them at ultimatehealthhome@gmail.com
My dad was diagnosed with Alzheimer's diseases this neuron disease started 25 years before being revealed it was triggered the moment we started eating sugars including any and almost all carbs that break down to glycerol,and he was placed on the best medical treatment approved by united states,(FDA) he has been taking Cholinesterase,Memantine to treat his memory loss,confusion and the problems with his thinking and reasoning.just to help slow the progression and manage the symptoms,as no cure exists I read through with interest. I once believed Alzheimer disease has no cure. Well it is true with English medicine, but not with herbal medicine. My Dad's experience opened my eyes to the reality of a cure through herbs. My Father was a vibrant man before his encounter with Alzheimer. He was a scientist, hence his mental capability was never in doubt. In 2013, he was diagnosed with Alzheimer. The symptoms manifested through repeating conversation and gradually forgetting things. It became progressive from finding the right words during conversation, to significant confusion and forgetting details about himself. It was not a good experience, seeing your father whose brilliance had no match, totally became a shadow of himself. His doctors said the disease has no cure, just medications for treatment which had a lot of side effects were administered to him. Early 2016, while on the internet, I bumped into a story of Alzheimer, and I read about a cure through herbs with interest. I researched more to be sure it was not a hoax. In my quest, Doctor James herbal mix medicine was mentioned in the testimony. I contacted him on his email that was provided (drjamesherbalmix@gmail.com) and I got his herbal mix medicine for my father.He told me that his herbal mix medicine will help my Dad to reduce the abnormal protein fold inside his neurons,and regulate the nutrients and molecules in his body system,and as well stop the progressive disorder that build up in damaging his brain cells,and help his weak cells that causes brain shrinking to function well,it's a good herbal drinks for cell repairing.This doctor James is super great man and his herbal mix medicine is wonderful and works effectively as he said,with no side effects. It's been 4 years and my Dad is perfectly okay and back to his laboratory work even at old age. For your loved ones with Alzheimer or Dementia, take them off English medicine and use Dr. James herbal mix medicine for treatment. if you have any kinds of health challenges or diseases such as..Parkinson's disease,Schizophrenia,Lung Cancer,Breast Cancer,Colo-Rectal Cancer,Blood Cancer,Prostate Cancer ,Epilepsy Dupuytren's disease ,Coeliac disease,Creutzfeldt–Jakob disease,Cerebral Amyloid Angiopathy, Ataxia,Arthritis,Amyotrophic Lateral Sclerosis,Fibromyalgia,Fluoroquinolone Toxicity
ReplyDeleteSyndrome Fibrodysplasia Ossificans ProgresS sclerosis,Seizures,Alzheimer's disease,Adrenocortical carcinoma.Asthma,Allergic diseases ,Copd,Glaucoma., Cataracts,Macular degeneration,Cardiovascular disease,Lung disease.Enlarged prostate,Osteoporosis,Lupus,Cushing’s disease,Heart failure,Multiple Sclerosis,Hypertension,Lyme Disease,Blood Cancer,Brain Cancer,Breast Cancer,Lung Cancer,Kidney Cancer, HIV/AIDS, Herpes Virus,Hepatitis B, Liver Inflammatory,Diabetes,Fibroid. just reach him on his Email [drjamesherbalmix@gmail.com]. and get your permanent cure.he's a good man and he will help you.
i was diagnosed of parkinson disease 5 years ago,i started azilect,then mirapex as the disease progressed in february last year,and i started on parkinson disease Herbal medicine from ultimate herbal home,few months into the treatment i made a significant recovery,almost all my symptoms are gone,great improvement with my movement and balance,it been a year and life has been so good for me,contact them at ultimatehealthhome@gmail.com
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