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Yale Scientists Find Telltale Alzheimer's Protein
alzheimersupport.com
02-27-2006
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BY KANYA BALAKRISHNA
Staff Reporter, Yale Daily News
As the Yale School of Medicine begins to focus greater attention on the fight against Alzheimer's and other neurological diseases, Medical School researchers working with proteins have given the investigation a shot in the arm.
Neurology professor Stephen Strittmatter published a paper in the February issue of the Journal of Neuroscience that identifies the protein NogoReceptor as a key factor in combating Alzheimer's disease. Strittmatter and his team observed that an increase in this protein has been shown to reduce the amount of disease-causing plaque in the brains of transgenic mice, animals that have been genetically altered to develop the neurodegenerative disorder.
Strittmatter, whose research primarily focused on nerve-spinal growth and axons -- the ends of neurons that conduct nerve impulses -- said he was originally attempting to determine how to stimulate nerve fibers to regrow after spinal cord injury.
But what he found, along with his colleagues, was that there were two key proteins at work in this mechanism.
"Nogo and NogoReceptor are proteins that stop axons from growing," he said. "There are ways to pharmacologically disrupt the interaction between [the two], and when this happens, the animals recover and the axons grow back."
This new knowledge, coupled with existing knowledge that nerve fibers and axons are important to Alzheimer's, led Stittmatter's team to question whether the NogoReceptor protein has anything to do with the protein buildup that is believed to be the culprit in provoking the onset of Alzheimer's disease.
"The first question we asked was whether the amyloid-beta peptide, [the protein] commonly thought to be the cause of Alzheimer's disease, interacts with NogoReceptor in a molecular sense," he said, "The answer to that was yes. Then we asked if animals without NogoReceptor would be more or less likely to experience Alzheimer's."
Strittmatter's team found that transgenic mice, pre-designated to develop the disease, were likely to do so at an increased rate in the absence of NogoReceptor. The researchers found that the reverse was true as well: Pumping extra protein into the brain would in turn slow down the progression of Alzheimer's disease in the mice.
Psychiatry professor Christopher Van Dyck, who also serves as director of the Alzheimer's Disease Research Unit at Yale, said Strittmatter's research marks a great stride for the field.
Van Dyck said all research into treatment and prevention for Alzheimer's is hugely important worldwide because as the global population ages, the disease will become more widespread. By the year 2030, he said, the population of Alzheimer's patients is likely to double, and by 2050, it could triple.
"Alzheizmer's is a massive public health problem," Van Dyck said. "Unless we want a society with a huge number of people that need to be cared for in nursing homes, we need to better preventative treatment."
Van Dyck, who performs clinical research, said a lot of work will have to go into applying Strittmatter's results to therapy for humans because treatments that work in mice often do not function the same way in people. Though it may seem like the obvious conclusion, Van Dyck said, effective treatment for Alzheimer's in humans may not mean pumping excess NogoReceptor into the brain.
Strittmatter said that while clinical testing is the long-term goal, there are currently no treatments that target the NogoReceptor in human beings, so all drug development will be from the ground up. He said issues of toxicity, possible side effects and drug delivery mechanisms still need to be addressed and that the protein used for the research was made from the genes of rats and must be customized for humans.
James Park MED '08 GRD '08, who, along with David Gimbel MED '08, worked on Strittmatter's team, said that though there is still a great deal of work to be done, the research they just published is extremely significant.
"We are implicating the molecule in Alzheimer's disease as another player in the disease's pathology," Park said. "We now have one additional target to consider."
Medical School Dean Robert Alpern said a research focus on Alzheimer's disease is necessary because of the growing number of people affected and the lack of knowledge of prevention and treatment methods.
"Fifty percent of people at 85 have Alzheimer's," Alpern said. "It's a devastating disease. There's been a lot of new research in the last 10 years, but we need more."
Alpern also said that the number of people afflicted with the disease is growing because, ironically, increased proficiency at treating other afflictions, such as cancer and heart disease, is gradually aging the population.
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DISCUSS THIS ARTICLE (1 existing comments)
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AD and Celiac disease
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Posted by: ggfarber
May 14, 2008 |
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WHY HAS THE MEDICAL COMMUNITY & ALZHEIMER'S ASSOC. IGNORED ONE DISCOVERED CAUSE & PREVENTION OF DEMENTIA?
Here are but a few of the universally obtainable websites I discovered, which indicate the possible link of celiac disease or gluten-intolerance, and dementia; some reported many years ago:
---------------------------------------------------------------------------------MAYO CLINIC DISCOVERS POTENTIAL LINK BETWEEN CELIAC DISEASE & COGNITIVE DECLINE Oct.-2006 ( http://www.mayoclinic.org/news2006-rst/3688.html-31K
Mayo Clinic neurologist Keith A. Josephs, MD says, "It is almost unheard of to see a reversal in dementia or cognitive decline." .......
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NEUROLOGICAL COMPLICATIONS OF CELIAC DISEASE:
Source: Tiege, et al, American Journal of Gastroenterology, 92:40, 1997. Lifeline, Winter 1998, Vol XVI, No 1, pp 1-2
www.csaceliacs.org/library/neurocomp.php
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CELIAC DISEASE PRESENTING WITH NEUROLOGICAL DISORDERS
National Library of Medicine www.ncbi.nlm.nih.gov/pubmed/10529537
Dept. of Neurology, Tampere Univ. Hosp., Kuopio, Finland
Eur Neurol. 1999;42(3):132-5.
It is well known that celiac disease may be associated with various neurological manifestations. We have a high index of suspicion of celiac desease during our years in our neurological clinic.
As a result 10 (7%) out of 144 of our new celiac patients were detected because of neurological symtoms. PMID: 10529537 [PubMed - indexed for MEDLINE].......
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"EMERGING EVIDENCE THAT DIETARY RESTRICTION CAN FORSTALL THE DEVELOPMENT OF AD ........PROVIDES OPTIMISM THAT THESE DEVASTATING BRAIN DISORDERS OF AGING MAY BE LARGELY PREVENTABLE." Mattson MP, Pererson WA, Duan W, Cumsee C.
Ann N Y Acad Sci. 1999;893:154-75. Review. PMID: 10672236 [PubMed - indexed for MEDLINE]
www.freeadicalscience.com/showabstract.php?pmid=10672236
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THE NEUROLOGY OF GLUTEN SENSITIVITY LLWonline 2002
Dept. of Neurology, Queen's Medical Centre, Nottingham, UK.
Wills AJ, Unsworth DJ Adrian.Wills@sdah-tr.trent.nhs.uk
Clinicolopathological features heal on a gluten-free diet and relapse when gluten is reintroduced. An immunopathology is suspected. A number of neurological syndromes may be associated with celiac disease....... This is an exciting hypothesis because it offers new therapeutic possibilities including simple exclusion diets....[PubMed- indexed for MEDLINE] www.ncbi.nih.gov/pubmed/12351994
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The shocking aspect of my genetic Celiac disease, diagnosed 6 years ago, at age 75, instigated my research of my family's medical history, resulting in unexpected discoveries that our tragic history of genetic Alzheimer's can now undoubtedly be linked to our genetic Celiac disease! ( One of many Celiac web-sites is www.celiac.com )
Alzheimer's has proven responsible for the deaths of 4 members in my maternal family, and is strongly suspected to be responsible for at least 4 fatalities of our previously-named "senile-dementia" victims. I have learned that at least 3 of these relatives also had disabling symptoms often associated with Celiac Disease. My mother was one of these victims who I have been able to definitely trace as having had at least one celiac-gene; my positive DNA test for celiac disease resulted in two identical genes, one from each parent. (my test and info from www.enterolab.com)
My sibling has also been diagnosed with Alzheimer's, and tests have indicated her possessing a Celiac-gene as well. I have been shocked that the Alzheimer Assoc. has ignored my many letters and several calls since I first contacted them about my family in '04, but I am even more baffled to learn that they have also ignored the Oct.'06 Mayo Clinic discovery- to this day.
I had been very hopeful, in Dec., '05 when I read that Dr, Richard Mayeux, at the Taub Institute for Research on Alzheimer's Disease, at Columbia Univ. was researching genetics! This lab, which employs hundreds, was described in a 10-page article, "The Gene Hunters", in The New Yorker Magazine of Dec. 12, '05. Dr. Mayeux,for nearly 20 years, "has been compiling the world's most comprehensive genetic library of families with Alzheimer's, in an effort to uncover the biological origins of a disease that effects 4.5 million Americans." ......
"There's a simple reason that no one has found a new Alzheimer's gene in more than a decade" he says,“statistics." I read that he was searching for families with genetic Alzheimer's who have additional genetic diseases which may link to AD. I wrote to Dr. Mayeux, to the New Yorker, to the Taub Institute, and to the writer of the article, Sue Halpern, in 12-'05. I received no replies.
Can it be a coinsidence that this startling info about my family statistics, which I have sent to many other AD research labs, to organizations, to the media, to legislators, & to physicians, have virtually all been simply overlooked? When my mother's autopsy finally indicated Alzheimer's Disease, in 1980, very little had been known about our family's anguish; losing her so painfully for 10 long years... And by now there have been 3 more family members in MY generation diagnosed with AD, with little more ability still, to avoid these seemingly endless tragedies. I think we have, at the very least, earned the respect of being heard.
Meanwhile, AARP notes that "The Alzheimer's Breakthrough Act of 2007"--asks congress for apprx. $1.3 BILLION in federal funds.....Apparently for more drug research, as their article ONLY defines pharmaceutical promises. (AARP thanked me for my letter, but noted that there was no room to publish it at this time.)
In the AD newsletter (Winter '07) N. Calif. Alzheimer Assoc. CEO Wm. Fisher reminds us that, "Alzheimer's costs this country $148 billion annually.....[and] threatens to bankrupt the Medicare and Medicaid systems in this country." As usual, on their full page of newsletter-research proposals- there is only mention of drug-research. (Besides our taxes & private donations, the Alzheimer Assoc. is funded by Eisai Inc. Pharmaceuticals, Pfizer Inc., and Forest Pharmaceuticals Inc.)
These warnings from the Alzheimer Assoc. came 6 months AFTER the Mayo Clinic's discovery of a Celiac-dementia link was published, and 3 years after my first letter to Mr. Fisher. I don't pretend to have proof of this family-linkage, but don't you think there is enough possibility indicated by now, so that a portion of those billions can be used for simply testing those who have been diagnosed with AD, for possible gluten-intolerance?
Gerta Farber 2951 Derby St. #113 Berkeley CA 94705 510 841-2050
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