|
VA Watchdog Stuff
cups, hats, shirts
click here to
support the site
Be sure to get all five
VA Watchdog dot Org
RSS feeds --
Daily VA
News Flashes
House CVA
Veterans' News
Senate CVA
Veterans' News
VA Press
Releases
VSO Press
Releases
Download
your
free copy of the
2007 VA benefits
handbook here...
|
Printer-Friendly Version
VA RESEARCH: MODIFIED PROTEIN MAY LEAD TO CURE
FOR CIRRHOSIS OF THE LIVER -- Researchers have
proven in animal studies that fibrosis in the
liver
can be not only stopped, but reversed.
For more about VA research, use the VA Watchdog
search engine...click here...
http://www.yourvabenefits.org/sessearch.php?q=va+research&op=ph
Story here...
http://www.sciencedai
ly.com/releases/2007/12/071226225538.htm
Story below:
-------------------------
Modified Protein May Lead To First Cure For
Cirrhosis Of The Liver
ScienceDaily — University of California, San Diego researchers have proven
in animal studies that fibrosis in the liver can be not only stopped, but
reversed. Their discovery, to be published in PLoS Online on December 26,
opens the door to treating and curing conditions that lead to excessive
tissue scarring such as viral hepatitis, fatty liver disease, cirrhosis,
pulmonary fibrosis, scleroderma and burns.
Six years ago, the UC San Diego School of Medicine research team
discovered the cause of the excess fibrous tissue growth that leads to
liver fibrosis and cirrhosis, and developed a way to block excess scar
tissue in mice. At that time, the best hope seemed to be future
development of a therapy that would prevent or stop damage in patients
suffering from the excessive scarring related to liver or lung disease or
severe burns.
Article continues below:
"ASK
THE BUILDER" VIDEOS -- HOME IMPROVEMENT TIPS
(use left/right arrows in screen to view more videos)
|
In their current study, Martina Buck, Ph.D.,
assistant professor of medicine at UCSD and the Veterans Affairs San Diego
Healthcare System, and Mario Chojkier, M.D., UCSD professor of medicine
and liver specialist at the VA, show that by blocking a protein linked to
overproduction of scar tissue, they can not only stop the progression of
fibrosis in mice, but reverse some of the cell damage that already
occurred.
In response to liver injury -- for example, cirrhosis caused by alcohol --
hepatic stellate cell (HSC) activated by oxidative stress results in large
amounts of collagen. Collagen is necessary to heal wounds, but excessive
collagen causes scars in tissues. In this paper, the researchers showed
that activation of a protein called RSK results in HSC activation and is
critical for the progression of liver fibrosis. They theorized that the
RSK pathway would be a potential therapeutic target, and developed an RSK
inhibitory peptide to block activation of RSK.
The scientists used mice with severe liver fibrosis -- similar to the
condition in humans with cirrhosis of the liver -- that was induced by
chronic treatment with a liver toxin known to cause liver damage. The
animals, which continued on the liver toxin, were given the RSK-inhibitory
peptide. The peptide inhibited RSK activation, which stopped the HSC from
proliferating. The peptide also directly activated the caspase or
"executioner" protein, which killed the cells producing liver cirrhosis
but not the normal cells.
"All control mice had severe liver fibrosis, while all mice that received
the RSK-inhibitory peptide had minimal or no liver fibrosis," said Buck.
Buck explained that the excessive collagen response is blocked by the RSK-inhibitory
peptide, but isn't harmful to the liver. "The cells continue to do their
normal, healing work but their excess proliferation is controlled," Buck
said. "Remarkably, the death of HSC may also allow recovery from liver
injury and reversal of liver fibrosis."
The researchers found a similar activation of RSK in activated HSC in
humans with severe liver fibrosis but not in control livers, suggesting
that this pathway is also relevant in human liver fibrosis. Liver biopsies
from patients with liver fibrosis also showed activated RSK.
The study expands on work reported in 2001 in the journal Molecular Cell
announcing that a team led by Buck had found that a small piece of an
important regulatory protein called C/EBP beta was responsible for fibrous
tissue growth, or excessive scar tissue following injury or illness. When
normal scarring goes awry, excessive build-up of fibrous tissue can
produce disfiguring scars or clog vital internal organs and lead to
serious complications. Buck and colleagues developed a mutated protein
that stopped this excessive fibrous tissue growth.
"Six years ago, we showed a way to prevent or stop the excessive scarring
in animal models," said Buck. "Our latest finding proves that we can
actually reverse the damage."
Worldwide, almost 800,000 people die from liver cirrhosis each year, and
there is currently no treatment for it. Excessive tissue repair in chronic
liver disease induced by viral, toxic, immunologic and metabolic disorders
all result in excessive scar tissue, and could benefit from therapy
developed from the UCSD researchers' findings.
The research was supported by grants from the National Institutes of
Health, the Department of Veterans Affairs and UCSD's Medical Research
Foundation. Buck is the recipient of a Howard Temin Award from the
National Cancer Institute.
Adapted from materials provided by University of California - San Diego.
-------------------------
Larry Scott --
Don't forget to read all of today's VA
News Flashes (click here)
Click here to make VA Watchdog dot Org your homepage
email Larry
(go
back to VA Watchdog dot Org Home Page) |
VA Watchdog Stuff
cups, hats, shirts
click here to
support the site
|
