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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.
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Saturday, November 23, 2019
Understanding the Relationship as Sanctuary
Glassy Carbon Electrodes Safer Than Metal in MRIs, Study Suggests
Dystonia Researchers Awarded Bachmann-Strauss Prize for Excellence
Friday, November 22, 2019
Mount Sinai researchers uncover new genetic drivers of Parkinson's disease
Defects in the STMN2 gene cause nine other genes related to Parkinson's disease to become overly active, a new study reports. (CC0 Creative Commons)
Only about 20% of Parkinson’s diagnoses can be tied to genetic mutations, making the disease difficult to address with targeted therapies. Researchers at the Mount Sinai Icahn School of Medicine hope to change that by using brain samples from Parkinson’s patients to identify gene networks that drive the disease.
A new study out of Mount Sinai takes that effort one step further.
The Mount Sinai scientists examined postmortem analyses from 83 patients in eight studies and identified the gene STMN2 as a key regulator of Parkinson’s disease. They went on to show that when the gene is knocked down in the brains of mice, nine other genes that had been previously tied to Parkinson’s became overly active. They published the finding in the journal Nature Communications.
"The new genes we identified suggest that new pathways should be considered as potential targets for drug development,” particularly for Parkinson's cases that have no known cause, said Zhenyu Yue, Ph.D., Professor of Neurology and Neuroscience at the Icahn School, in a statement.
The team focused in on the substantia nigra, the region of the brain that’s most negatively affected by Parkinson’s. They compared brain tissue from the 83 patients to tissue taken from 70 people who had been healthy. They then applied a statistical method called multiscale gene network analysis (MGNA) to both sample sets, which allowed them to identify gene networks associated with Parkinson’s.
n healthy people, the STMN2 gene is expressed in neurons that produce dopamine, the critical neurotransmitter that’s lacking in the brains of people with Parkinson’s. When they knocked down STMN2 in the substantia nigra of mice, the animals struggled to complete motor tasks, such as balancing on a rod. Their dopamine-producing neurons started to break down, and there was an increase in a toxic protein called alpha-synuclein in their brains, the Mount Sinai team reported.
The STMN2 gene is of great interest to researchers studying neurodegenerative diseases. Earlier this year, a Harvard team reported a newly discovered connection between STMN2 and TDP-43, a gene that’s mutated in some cases of amyotrophic lateral sclerosis (ALS). They’re now examining whether repairing the STMN2 gene can slow or stop the progression of ALS.
The next step for the Mount Sinai researchers is to validate their observations related to STMN2 and Parkinson’s disease in larger studies. “Our approach is expected to be improved with comprehensive longitudinal studies, increased sample size, and better diagnosis” of Parkinson’s, they wrote in the study.
https://www.fiercebiotech.com/research/mount-sinai-researchers-uncover-new-genetic-drivers-parkinson-s-disease
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Accelerating Medicines Partnership launches data knowledge portal for Parkinson’s disease
Increased use of antibiotics may predispose to Parkinson's disease
Thursday, November 21, 2019
Royal recognition for neuroscience research at the University of Sheffield
- The University of Sheffield has been awarded the Queen's Anniversary Prize for innovation in neuroscience
- The prize is the highest national honour that recognises outstanding work by UK universities and colleges that demonstrate quality and innovation in their research
- Sheffield has been recognised for improving patient outcomes for people living with neurodegenerative diseases such as Parkinson's Disease and Motor Neurone Disease
- a new orthotic device, 'HeadUp', for patients living with MND who suffer from muscle weakness in their neck
- ground-breaking clinical stem cell clinical trials for MS patients
- research which has improved the life-expectancy and quality of life for those living with MND
- the discovery of a biomarker linked to the development of Alzheimer's Disease for the first time, which has the potential for earlier diagnosis and has sparked the development of new therapies
- drug discovery programmes to develop new treatments for Parkinson's Disease
- new gene therapy experimental medicine studies for MND which are showing promising early results.
- Find more information about the Royal Anniversary Prizes here: https:/
/ www. queensanniversaryprizes. org. uk/ - The awards were announced at a ceremony at St. James's Palace in the City of Westminster on Thursday 21 November 2019.
Tiny Crystals May Help Scientists Trace Causes of Brain Inflammation in Parkinson’s, Study Reports
Human Participants In Experimentation On The Brain? They Better Be Treated Well.
The MRI of a patient suffering from Dystonia, who received implants within the brain. UNIVERSAL IMAGES GROUP VIA GETTY IMAGES
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A patient undergoes surgery to implant an electrode in the brain as a treatment for Parkinson's ... [+]UNIVERSAL IMAGES GROUP VIA GETTY IMAGES
The final ethical point, and one that has not been investigated in depth before, is what happens after the trial is over? Participants often think that the cost of their care after the trial is over will be covered, but this is not always the case. Imagine if the battery of the implant needs to be replaced after the trial. Who pays? What if the patient is benefiting from the implant? Who covers the cost of treatment after the trial ends? Health insurance many times will not cover expenses like this, so the authors encourage researchers to plan for care of the participants even after the trial is completed.
“Such studies are only possible because research participants generously contribute,” says Ramos and co-authors. Their interests should be guarded, both during and after the trial.
https://www.forbes.com/sites/fernandezelizabeth/2019/11/21/human-participants-in-experimentation-on-the-brain-they-better-be-treated-well/#61302c2d2d55
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