PEOPLE WITH PARKINSON'S DISEASE, PAIN IS A MAJOR COMPLAINT

Pain is the most common reason people in the United States visit their doctors each year. Although
pain is highly subjective and difficult to describe, a working definition is “an unpleasant sensory and emotional
experience associated with actual or potential physical damage.” Its components are physical, cognitive,
behavioral, emotional and perceptual. Among people who have Parkinson’s disease (PD), pain is a
major complaint. In fact, up to 85 percent of people with Parkinson’s report pain as a troubling symptom.
Some of these people experience pain as an early symptom of Parkinson’s, before their disease has even
been diagnosed. Yet, pain in Parkinson’s disease often remains undiagnosed and untreated. Thus, it is important
to understand that pain can be part of the Parkinson’s experience and to learn ways to manage it.

STRAIGHTENING THE MIS-FOLDED PROTEINS OF ALPHA-SYNUCLEIN

 

 

 

Straightening the Mis-Folded Proteins of Alpha-Synuclein

Alpha-synuclein if the protein molecule that is found in Lewy bodies and is one culprit that is thought to be responsible for the symptoms of PARKINSON’S DISEASE.  Scientists have been working hard to understand how alpha-synuclein infiltrates the cells and neurons and exactly what its role is in human biology.  It is known that alpha synuclein is at the root of many of the problems of neurodegenerative diseases, but how to remove or suppress this protein has proven extremely elusive and resistant to the best of scientific techniques.

Dr. James Shorter, an associate professor of Biochemistry and Biophysics from the Perelman School of Medicine at the University of Pennsylvania may have discovered a unique and interesting approach that could help solve the alpha synuclein dilemma.  His research looked at yeast proteins, and he discovered a specific yeast protein Hsp104 that is able to dissolve mis-folded proteins of alpha-synuclein in the plasma of cells.

Unfortunately, it is not so simple and straightforward.  Hsp104 is one of the better known proteins on our planet; however, it does not exist in humans or animals.  Dr. Shorter says “We don’t understand why animals have lost the gene for Hsp104, but at the same time, we’ve been wondering:  ‘Is there a therapeutic opportunity in this?’”  His research has shown that although Hsp104 is effective, it is not perfectly effective and increasing the effectiveness of this protein is the new direction in his research.

His lab has been re-engineering variants of Hsp104.  Finding the right variant that can suppress the mis-folded alpha synuclein while also improving the function of the cell is the challenge.  While any number of variants might to the job, they might also do more than prevent the clumping of alpha-synuclein and therein would lie some serious problems.  So it is no easy task to engineer this particular protein to become an accurate therapeutic product with a focused target.  It is also a protein that is foreign to animal and humans, so side effects or toxicity are also important considerations.

His research up until now has been with yeast models, and has been successful.  The next step was to test it in a more sophisticated, multi-cellular model, for which a primitive worm model was chosen.  This work was a collaboration with Dr. Guy Caldwell from the University of Alabama.  And it was successful.  The next challenge is to move to even more complex animal models, such as mice.

Although this research is still in some very early stages, it is exciting that a foreign molecule can be engineered to obtain therapeutic benefit and holds the promise that perhaps eventually it will become an important agent for ameliorating the symptoms or possibly eliminating the cause of those symptoms in PARKINSON’S DISEASE and other neurodegenerative diseases.

Jackrel, M.E., M.E. DeSantis, B.A. Martinez, L.M. Castellano, R.M. Stewart, K.A. Caldwell, G.A. Caldwell, and J. Shorter^. (2014). Potentiated Hsp104 variants antagonize diverse proteotoxic misfolding events. Cell. 156:170–182

PD affects everyone differently

Parkinson's More Than Motion PD affects everyone differently, so sometimes it can be difficult to describe your specific PD symptoms. This is where the Parkinson’s Well-Being Map™ comes in by helping you document motor and non-motor symptoms in detail. Your doctor can use this information to assess your symptoms and consider your individual needs. Clink on the link below to begin filling out your own map! https://www.parkinsons-voices.eu/wbm/index_us.html

More Alpha-Synuclein in Spinal Fluid Linked to Faster Cognitive Decline

FoxFeed Blog

Posted by  Maggie McGuire, March 17, 2014

Alpha-synuclein — the protein that clumps in the cells of Parkinson’s patients — is currently the major focus of Parkinson’s biomarker studies. Researchers are analyzing biosamples (spinal fluid, blood, tissue) to make a connection between alpha-synucleinand risk, onset or progression of Parkinson’s disease (PD). The latest findings, published in The American Journal of Pathology, report that patients with higher levels in spinal fluid experienced faster cognitive decline.

In a project funded by The Michael J. Fox Foundation (MJFF), Jing Zhang, MD, PhD, and his team at the University of Washington in Seattle examined samples and data from PD patients obtained in the DATATOP study. Led by the Parkinson’s Study Group in the late 1980s, the deprenyl and tocopherol antioxidative therapy of parkinsonism (DATATOP) study collected samples and clinical data from PD subjects for up to eight years.

In this latest analysis, researchers compared alpha-synuclein levels to scores from tests of cognition, such as verbal learning and memory, visuospatial memory and processing speed, among 304 PD patients. They found that patients with higher levels of alpha-synuclein in spinal fluid had faster cognitive decline.

“This is a surprising conclusion,” says Mark Frasier, PhD, MJFF vice president of research programs. “One would think that people with more cognitive problems would have less alpha-synuclein in spinal fluid because more would be caught up in the brain causing those problems.”

Zhang’s group also reported that while alpha-synuclein levels decreased significantly over two years, that decline could not predict motor symptoms. These findings join a list of observations about how alpha-synuclein in spinal fluid relates to PD. Initial analysis from the MJFF-sponsored Parkinson’s Progression Markers Initiative (PPMI) reported last year that PD patients had lower alpha-synuclein levels in spinal fluid compared to controls. They also found that patients with posture/gait disturbance averaged lower alpha-synuclein than patients with tremor-dominant PD.

Further investigation into alpha-synuclein continues in PPMI and other studies. Zhang and his coauthors cited PPMI as a potential source for validation of their cognition findings. Since PPMI includes healthy controls, researchers could test whether those results are PD-specific or seen in healthy aging adults with cognitive decline, too.

To accelerate research around PD biomarkers, MJFF spearheaded an effort to make data and samples from varied Parkinson’s studies available to investigators. The Foundation also offers funding to use the data and samples, such as to Zhang for the DATATOP analysis.

Register now for our May 15 Webinar titled “Taking Inventory of Parkinson’s and Alzheimer’s Disease,” where experts will discuss cognitive decline.

TAGS: Cognitive Changes, Dementia, Alpha-Synuclein, UPDRS, Biomarkers, Research News,Washington, Research Grants, Parkinson's Progression Markers Initiative

PARKINSON'S DISEASE INCREASES THE RISK OF INJURIES

23rd March 2014 - New research

European Journal of Neurology [2014] Mar 17 [Epub ahead of print] (H.C.Wang, C.C.Lin, C.I.Lau, A.Chang, F.C.Sung, C.H.Kao)

People with Parkinson's Disease have been found to increase their likelihood of most accidental injuries, especially head injuries. The risk of injury increases with age.

People with Parkinson's Disease were found to have the following increased likelhood of injuries times what is normal : head injury 1.9, bone fracture and dislocation 1.4, all injuries 1.3, injury to spinal cord, plexus and nerves 1.25, superficial injuries and contusions 1.20, burns 1.0. The injury risk for those people with Parkinson's Disease who were 69-79 years old was significantly higher than those who were 50-69 years old.

So people with Parkinson's Disease demonstrate a significantly elevated risk of developing all accidental injury types except injuries caused by burns. The risk of injury increases as age increases.

http://www.viartis.net/parkinsons.disease/news/140323.pdf mail@viartis.net
©2014 Viartis 

THE EFFECT OF AGE OF ONSET ON PARKINSON'S DISEASE

22nd March 2014 - New research

Parkinsonism Related Disorders [2014] Feb 22 [Epub ahead of print] (R.Mehanna, S.Moore, J.G.Hou, A.I.Sarwar, E.C.Lai)

The clinical features and development of Parkinson's Disease has been found to differ in many respects according to the age of onset of Parkinson's Disease. The age of onset can be roughly divided in to young onset (49 years old or younger), middle onset (50 to 69 years old), and late onset (70 years old or later).

Data collected included age at symptom onset, year of onset, family history of Parkinson's disease in first and second degree relatives, predominant first symptom, first anti parkinsonian medication prescribed, frequency of L-dopa-induced dyskinesia, therapy related dystonia, therapy related gastrointestinal side effects, hallucinations, dementia, depression and apathy. In numbers, the middle onset was the largest group (51%), followed by those with late onset (39%) and then those with young onset (10%).

Those with young onset were found to have a more frequent family history of Parkinson's disease and longer survival. Symptoms other than tremor were more frequent as the initial symptom of the young onset group. Depression was more frequent in the young onset group than middle onset or old onset. The frequency of tremor as the first symptom increased with advancing age at onset. The frequency of treatment related dyskinesia or dystonia decreased with advancing age at onset.
http://www.viartis.net/parkinsons.disease/news/140322.pdf mail@viartis.net
©2014 Viartis