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#1 | |||
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Elder
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according to the NY Times.
http://www.nytimes.com/2012/07/18/he...fVCA1E7drZJjNQ The most widely prescribed drug for treating multiple sclerosis has little or no effect on a patient’s progression to disability, a new study has found. The medicine, interferon beta, does help reduce the development of brain lesions and limit the frequency of relapses, but until now there have been few well-controlled long-term studies demonstrating its effectiveness at preventing the onset of irreversible disability. Researchers at the University of British Columbia prospectively collected data on 868 M.S. patients treated with interferon beta, comparing them with 1,788 patients who never took the drug. Using a well-validated scale, they found that those who took interferon beta were no less likely to suffer long-term disability than those who took none. Interferon beta drugs are commonly used to treat relapsing-remitting M.S., the most common form of the disease. M.S. is an autoimmune disease that damages the myelin sheath surrounding the nerve cells. Its course varies widely, but it is usually a relapsing illness that produces a variety of symptoms, including muscle spasms and difficulty walking, bladder and bowel problems, vision and hearing disturbances, speech problems, difficulties with reasoning and attention span and more. The disorder is chronic and incurable, and its outcome is variable and hard to predict. But life expectancy can be normal, and many people live with the disease for decades, still able to walk and work with minimal disability. The senior author, Helen Tremlett, an associate professor of neurology at the University of British Columbia, cautioned that the study, published online on Tuesday in the Journal of the American Medical Association, does not show that interferon beta is useless. “These drugs were licensed because they reduce relapse and have a better outcome with lesions,” she said. “That has not changed.” Other experts found the study discouraging. “It’s an interesting paper and an important paper,” said Dr. David A. Hafler, chairman of the neurology department at Yale. “If interferon does have an effect on disability, then it’s a relatively small effect.” Dr. Claire Riley, director of the Multiple Sclerosis Clinical Care & Research Center at Columbia University, was equally impressed with the work and somewhat troubled by its results. “It’s a little dispiriting to see this well-designed, well-conducted assessment showing no association between reduction of disability progression and interferon use,” she said. “But the key is that all M.S. is not created equal, and we now have eight approved drugs in four different classes that allow us to better react to patients who are not having a response to therapy.” Previous studies have found that interferon beta does prevent disability, but the authors point out that many of them were marred by methodological problems — the use of control groups too ill to start medication, for example — that this study avoided. At the same time, they acknowledge certain weaknesses of their own study, in particular the problem that people who take no medicine are also likely to be among those who are the least ill and therefore least likely to become disabled in any case. But after controlling for sex, age at onset, disease duration, relapse rate and other factors, they could find no association between taking interferon beta and any reduction in progression to disability. Relapses and brain lesions do not, apparently, drive disability, Dr. Tremlett said. “There may be other processes at work,” she added. “In an ideal world, we want drugs that target whatever is driving long-term disability. We need other drugs aiming at other targets in the brain.” A version of this article appeared in print on July 18, 2012, on page A14 of the New York edition with the headline: Multiple Sclerosis Drug Doesn’t Prevent Onset of Disability, Study Finds.
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RRMS 3/26/07 . Betaseron 5/18/07 . Elevated LFTs Beta DC 7/07 Copaxone 8/7/07 . . |
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#2 | ||
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Junior Member
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I'm curious how much it impacts the time to onset of disability. That seems to be an important question too.
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"Thanks for this!" says: | Mariel (07-25-2012) |
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#3 | ||
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Junior Member
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Reading a little more about this study, I came across this:
Quote:
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#4 | |||
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In Remembrance
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Thanks Dej...and MissJ also posted this to the "To drug or not drug" thread.
It's exactly as I expected, except, that Beta still does help a select few. We need to pinpoint these drugs more, as to the exact type of MS they help!!!! Too much money is being spent on drugs that are not meeting our specific disease needs. ![]() ![]()
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~Love, Sally . "The best way out is always through". Robert Frost ~If The World Didn't Suck, We Would All Fall Off~ |
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#5 | |||
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Elder
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Maybe this also suggests that the medical community isn't on the right track as to what really causes MS and it's (more than likely) outcome of disability...
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Instant Karma's gonna get you-gonna knock you right in the head...John Lennon |
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#6 | |||
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Wisest Elder Ever
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It didn't work for me. Made me sicker than I was without it. And cost a fortune. What's wrong with this picture?
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These forums are for mutual support and information sharing only. The forums are not a substitute for medical advice, diagnosis or treatment provided by a qualified health care provider. Always consult your doctor before trying anything you read here. |
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#7 | ||
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n/a
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from delawareonline I found this
The data’s implications may be limited because the study was designed to show a 40 percent risk reduction with interferon treatment, more than the 30 percent shown in trials of the interferon beta therapies or Copaxone, Kappos and Tobias Derfuss, also of University Hospital in Basel, wrote in their editorial. hmmmm |
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#8 | |||
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Member
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Well....
That's eight years of my life (on Beta) that I will never get back. The side effects were awful - but I do have to say it stopped the aggressive MRI activity in its tracks......but maybe it would have stopped anyway. That is what I hate - you can't gauge what nobody will ever know, and that is the same with all of these drugs - A B C R and T. Lyn
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Lyn . Multiple Sclerosis Dx 2001 Craniotomy to clip brain aneurysm 2004. ITP 1993. |
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#9 | ||
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Member
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Quote:
But if you read the literature of the companies who produce this drug, you would get a totally different outlook. Ah the importance of marketing and how it can influence people to use something even though it may not give you what was inferred. The CRAB drug producers have been doing this for years and making a ton of money along the way. Too bad most MS patients haven't benefited much if at all. |
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#10 | |||
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Member
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Gotta remember - making money is what they are all about. Sucks for us, but that is capitalism in a nutshell.
Lyn
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Lyn . Multiple Sclerosis Dx 2001 Craniotomy to clip brain aneurysm 2004. ITP 1993. |
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