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A drug that extends life span prevents Alzheimer's deficits (rapamycin)
University of Texas Health Science Center at San Antonio ^ | Apr 1, 2010 | Unknown

Posted on 04/01/2010 2:31:26 PM PDT by decimon

Rapamycin proves mettle in second model of memory-robbing disease

SAN ANTONIO (April 1, 2010) — If research results continue to be repeated and are turned into clinical trials, a drug already approved for some uses could be marshaled — sooner than we expect — to prevent Alzheimer's disease in humans and improve health to the end of life.

A few weeks after a report that rapamycin, a drug that extends lifespan in mice and that is currently used in transplant patients, curbed the effects of Alzheimer's disease in mice, a second group is announcing similar results in an entirely different mouse model of early Alzheimer's.

Both reports are from The University of Texas Health Science Center at San Antonio, where the rapamycin studies are conducted in the Sam and Ann Barshop Institute for Longevity and Aging Studies and in basic science departments.

The second report, to be published later this afternoon (April 1) by the Public Library of Science, showed that administration of rapamycin improved learning and memory in a strain of mice engineered to develop Alzheimer's. The improvements in learning and memory were detected in a water maze activity test that is designed to measure learning and spatial memory. The improvements in learning and memory correlated with lower damage in brain tissue.

Less sticky

"Rapamycin treatment lowered levels of amyloid-beta-42, a major toxic species of molecules in Alzheimer's disease," said Veronica Galvan, Ph.D., assistant professor from the Barshop Institute and the Department of Physiology. "These molecules, which stick to each other, are suspected to play a key role in the early memory failure of Alzheimer's."

This strain of mice has been engineered to have defects in the genes that make amyloid precursor protein, ultimately resulting in the abnormal accumulation of amyloid-beta-42 that dampens synaptic connections. Synapses are junctions where neurons communicate with each other, providing the essential "wiring" for normal function of the brain. Without this communication, neurons die, leading to the memory losses seen in Alzheimer's.

Longer life for mice

In July 2009, Barshop Institute researchers and colleagues at two other institutions reported that microencapsulated rapamycin extended the life span of mice, possibly by delaying aging. A bacterial product first isolated from soil of Easter Island, rapamycin is approved by the U.S. Food & Drug Administration to prevent organ rejection in transplant patients. Rapamycin is the first pharmacologic intervention shown to extend life in an animal model of aging.

If rapamycin treatment indeed delays aging in mice, are age-associated diseases, such as Alzheimer's, delayed or blocked? The new study, authored by Spilman et al, sought to answer this question. In the study, the same rapamycin-supplemented diet as in the life span study was fed to groups of the Alzheimer's-susceptible mice and their normal littermates. A non-rapamycin diet was fed to control groups. Rapamycin feeding began at 4 months of age, when the susceptible mice show high amyloid-beta-42 levels and synaptic dysfunction, but do not yet have amyloid beta plaques or spatial memory impairments.

Get out of the water

After 13 weeks of treatment, all groups were trained in the water maze exercise to see how quickly they could learn to exit the water via a hidden platform. Doing so requires the use of spatial cues, such as patterned posters or photos, positioned all around the water tank. The Alzheimer's model mice that were fed the control diet predictably showed significant losses in learning and memory and reduced performance.

"Strikingly, the Alzheimer's mice treated with rapamycin displayed improved performance on the maze, even reaching levels that were indistinguishable from their normal littermates," Dr. Galvan said. "Levels of amyloid-beta-42 were also reduced in these mice after treatment, and we are seeing preserved numbers of synaptic elements in the brain areas of Alzheimer's disease mice that are ravaged by the disease process."

Intriguingly, differences in resistance to swimming in the middle of the pool (a measure of anxiety) and in floating (a measure of hopelessness) were not observed among groups. "This suggests that improved performance in rapamycin-treated, Alzheimer's-susceptible mice is a result of effects on purely cognitive processes but is not due to effects related to non-cognitive components of behavior, such as helplessness and anxiety," Dr. Galvan said.

Changing a toxic process

"The fact that we are seeing identical results in two vastly different mouse models of Alzheimer's disease," Dr. Galvan added, in reference to the recent study by Caccamo et al, "provides robust evidence that rapamycin treatment is effective and is acting by changing a basic pathogenic process of Alzheimer's that is common to both mouse models. This suggests that it may be an effective treatment for Alzheimer's in humans, who also have very diverse genetic makeup and life histories."

###

Grants from the Alzheimer's Association and the National Institute on Aging supported the study. Co-authors are Drs. Patricia Spilman, Natalia Podlutskaya, Matthew J. Hart, Jayanta Debnath, Olivia Gorostiza, Dale Bredesen, Arlan G. Richardson, Randy Strong and Veronica Galvan. Collaborating institutions are the UT Health Science Center San Antonio (Barshop Institute, departments of Physiology, Pharmacology, Cellular and Structural Biology, and Molecular Medicine); the South Texas Veterans Health Care System (Geriatric Research, Education and Clinical Center and Research Service); the University of California, San Francisco (Department of Pathology); and the Buck Institute for Age Research, Novato, Calif.

About the UT Health Science Center San Antonio

The University of Texas Health Science Center at San Antonio, one of the country's leading health sciences universities, ranks in the top 2 percent of all U.S. institutions receiving federal funding. Research and other sponsored program activity totaled a record $259 million in fiscal year 2009. The university's schools of medicine, nursing, dentistry, health professions and graduate biomedical sciences have produced 27,000 graduates. The $753 million operating budget supports six campuses in San Antonio, Laredo, Harlingen and Edinburg. For more information on the many ways "We make lives better®," visit www.uthscsa.edu.


TOPICS: Health/Medicine; Science
KEYWORDS: alzheimers; medicine; rapamycin; science

1 posted on 04/01/2010 2:31:26 PM PDT by decimon
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To: neverdem; DvdMom; grey_whiskers

Ping.


2 posted on 04/01/2010 2:32:21 PM PDT by decimon
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To: decimon

You’ll need a ‘cadillac plan’.


3 posted on 04/01/2010 2:32:54 PM PDT by Spirochete (Texas is an anagram for Taxes)
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To: decimon

bump


4 posted on 04/01/2010 2:45:50 PM PDT by dangerdoc
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To: Spirochete

If people live longer, they will cost the system more money. Dr. Emanuel said as much. This must not be an Obamao-care funded research effort and I’m sure it’s funds will soon be drastically cut.

Unimpaired older folks will take better care of themselves and maybe even exercise to enhance their longevity. This is a crisis in the making. What are these scientists thinking? Don’t they know the Hippocratic Oath has been rescinded?

Call the CBO, call the FDA, call Dr Kervorkian, call Pelosi. This will totally skew the numbers and make 0 look bad.


5 posted on 04/01/2010 2:46:47 PM PDT by downtownconservative
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To: Spirochete
You’ll need a ‘cadillac plan’.

Depends on how much you need. And, perhaps, if you can get fresh or, perhaps, freshly frozen grapefruit juice.

The story is here: Grapefruit juice shows promise in some cancer treatments

6 posted on 04/01/2010 2:57:22 PM PDT by decimon
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To: downtownconservative
Maybe they will outlaw all taxes on cigarettes, and also give a huge rebate on the annual tax return to those who smoke the most cigarettes.

LOL

7 posted on 04/01/2010 3:05:58 PM PDT by hennie pennie
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To: decimon

Is this one that John McCain is trying to control, too?


8 posted on 04/01/2010 3:20:02 PM PDT by unspun (PRAY & WORK FOR FREEDOM - investigatingobama.blogspot.com)
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To: decimon
For fans of The 4400: Rapamycin also inhibits the special ability of breaking out in hip-hop lyrics, when under stress.
9 posted on 04/01/2010 3:26:08 PM PDT by unspun (PRAY & WORK FOR FREEDOM - investigatingobama.blogspot.com)
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To: Spirochete

This from Wikipedia: “The U.S. patent for sirolimus (5,665,7220, 1993) has expired, so it is available in generic formulations. Rapamune costs about $37 a day for a 4 mg dose. Generic sirolimus is available from Canadian pharmacies, manufactured in India, for $20 a day. For patients who have difficulty paying that, the dose can be adjusted by combining it with grapefruit juice.[22]”


10 posted on 04/01/2010 3:47:29 PM PDT by decimon
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To: unspun
Is this one that John McCain is trying to control, too?

No, it's already controlled.

11 posted on 04/01/2010 3:48:34 PM PDT by decimon
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To: decimon

Also used as an immunosuppressant in organ transplants.


12 posted on 04/01/2010 5:36:34 PM PDT by Born Conservative ("I'm a fan of disruptors" - Nancy Pelosi)
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To: decimon
Inhibition of mTOR by Rapamycin Abolishes Cognitive Deficits and Reduces Amyloid-β Levels in a Mouse Model of Alzheimer's Disease
13 posted on 04/04/2010 11:12:06 PM PDT by neverdem (Xin loi minh oi)
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