WELCOME TO OUR PARKINSON'S PLACE!

I HAVE PARKINSON'S DISEASES AND THOUGHT IT WOULD BE NICE TO HAVE A PLACE WHERE THE CONTENTS OF UPDATED NEWS IS FOUND IN ONE PLACE. THAT IS WHY I BEGAN THIS BLOG.

I COPY NEWS ARTICLES PERTAINING TO RESEARCH, NEWS AND INFORMATION FOR PARKINSON'S DISEASE, DEMENTIA, THE BRAIN, DEPRESSION AND PARKINSON'S WITH DYSTONIA. I ALSO POST ABOUT FUNDRAISING FOR PARKINSON'S DISEASE AND EVENTS. I TRY TO BE UP-TO-DATE AS POSSIBLE.

I AM NOT RESPONSIBLE FOR IT'S CONTENTS. I AM JUST A COPIER OF INFORMATION SEARCHED ON THE COMPUTER. PLEASE UNDERSTAND THE COPIES ARE JUST THAT, COPIES AND AT TIMES, I AM UNABLE TO ENLARGE THE WORDING OR KEEP IT UNIFORMED AS I WISH. IT IS IMPORTANT TO UNDERSTAND I AM A PERSON WITH PARKINSON'S DISEASE. I HAVE NO MEDICAL EDUCATION,

I JUST WANT TO SHARE WITH YOU WHAT I READ ON THE INTERNET. IT IS UP TO YOU TO DECIDE WHETHER TO READ IT AND TALK IT OVER WITH YOUR DOCTOR. I AM JUST THE COPIER OF DOCUMENTS FROM THE COMPUTER. I DO NOT HAVE PROOF OF FACT OR FICTION OF THE ARTICLE. I ALSO TRY TO PLACE A LINK AT THE BOTTOM OF EACH ARTICLE TO SHOW WHERE I RECEIVED THE INFORMATION SO THAT YOU MAY WANT TO VISIT THEIR SITE.

THIS IS FOR YOU TO READ AND TO ALWAYS KEEP AN OPEN MIND.

PLEASE DISCUSS THIS WITH YOUR DOCTOR, SHOULD YOU HAVE ANY QUESTIONS, OR CONCERNS. NEVER DO ANYTHING WITHOUT TALKING TO YOUR DOCTOR FIRST..

I DO NOT MAKE ANY MONEY FROM THIS WEBSITE. I VOLUNTEER MY TIME TO HELP ALL OF US TO BE INFORMED.

I WILL NOT ACCEPT ANY ADVERTISEMENT OR HEALING POWERS, HEALING FROM HERBS AND ETC. UNLESS IT HAS GONE THROUGH TRIALS AND APPROVED BY FDA. IT WILL GO INTO SPAM.

THIS IS A FREE SITE FOR ALL WITH NO ADVERTISEMENTS

THANK YOU FOR VISITING! TOGETHER WE CAN MAKE A DIFFERENCE!

TRANSLATE

Wednesday, June 15, 2016

Metabolite in MS drug seems to slow onset of Parkinson's disease

JUNE 15, 2016

Magdalena Kegel




Dimethylfumarate (Tecfidera), a drug used to harness multiple sclerosis symptoms, generates a metabolite that could be used in Parkinson’s patients to improve defenses against oxidative damage. The drug acts on Nrf2, a molecule that has frequently been suggested as a target for neuroprotective drugs in Parkinson’s, as its activation is a part of our natural defense against oxidative stress and inflammation.
The multiple sclerosis drug was approved by the U.S. FDA in 2013, and its ability to activate Nrf2 is known by scientists. But some of its side effects, including flushing, diarrhea, nausea, vomiting, abdominal pain, and brain dysfunction has made the drug particularly unsuitable for patients with Parkinson’s disease, who often have gastrointestinal problems caused by their disease.
Such problems are linked to the death of dopamine neurons also in the gut, and as is the case with other movements, the lack of the neurotransmitter prevents gut motility, effectively causing constipation. The metabolite of dimethylfumarate, called monomethylfumarate, is also known to activate Nrf2, but is not as potent. It also turned out to be less toxic.
Researchers from the Medical College of Georgia at Augusta University decided to tease out the individual contributions of the drug and its metabolite, and discovered that both substances activated Nrf2, but in contrast to its parent drug, monomethylfumarate had a range of effects further promoting neuroprotection.
The study, Distinct Nrf2 Signaling Mechanisms of Fumaric Acid Esters and Their Role in Neuroprotection against 1-Methyl-4-Phenyl-1,2,3,6-Tetrahydropyridine-Induced Experimental Parkinson’s-Like Disease, demonstrated that while dimethylfumarate depleted the anti-oxidant glutathione, decreased cell survival, and blocked the capacity of mitochondria to use oxygen and glucose to make energy, initially exposing cells to a more stressed state, its metabolite triggered the opposite changes, reversing the harmful situation the parent compound induced.
These changes were observed in cultured cells, so to study the impact of the two compounds on a living organism, the research team treated mice with a toxin called MPTP, capturing the progression of Parkinson’s disease on a short time scale. Mice exposed to the toxin lose dopamine neurons and develop symptoms within days.
The report, published in The Journal of Neuroscience, showed that mice that received either dimethylfumarate or its metabolite before they were given the toxin were largely protected against the neurodegenerative effects, also showing fewer signs of inflammation and oxidative stress. If, however, the same procedure was applied in mice lacking the Nrf2 gene, the toxin wiped out the dopamine neurons, showing that activation of Nrf2 is a key part of this neuroprotection.
While dimethylfumarate is a more potent drug, the team showed that its metabolite is good enough in protecting from neurodegeneration in Parkinson’s, activating Nrf2 in a more direct manner.
The research team now wants to bring these findings to the clinic, awaiting the formulation of monomethylfumarate and other substances mimicking its structure, for humans.
“If we can catch them early enough, maybe we can slow the disease,” co-author Dr. John Morgan, a neurologist and Parkinson’s disease specialist, said in a news release. “If it can help give five to eight more years of improved quality of life, that would be great for our patients.”
http://parkinsonsnewstoday.com/2016/06/15/parkinsons-neurodegeneration-stopped-by-multiple-sclerosis-drug-metabolite/

No comments:

Post a Comment