Anecdote, if dr Wheldon or guys at Vanderbilt says so, that is a proof. I do not think that with such a serious illness like PPMS or SPMS we should wait years to state something based on clinical trials. E.g. everyone knows how progressive patients control groups performed in other clinical trials ( close to zero). So 75% is much better. If he has any experience with PPMS patients I would be grateful for that. How did they do? I am 35 and have PPMS.I could say that out of the more than a hundred people that my husband has treated who have SPMS, three quarters have stopped progression ad many of these have improved, but not being part of a trial, there is no proof.
Did your husband or at Vanderbilt where they have neurologist on board have any opinion on connection with PPMS? As far as I see the pathogenesis of PPMS is totally different from the other types. Any experience on what symptoms or signs might suggest that someone's MS might be caused by CPN or other infection? As you know PPMS patients have no inflammation, no flair-upsAnecdote wrote:Gogo, I imagine you are ill and frightened because you feel you are getting worse.I was that way when I started treatment. Now, since the nineteen sixties, MS has become known as an auto-immune disease whereas before neurologists were willing to believe that it was maybe caused by an infection. It's one thing believing that but totally something else to know what the infection is.
In the nineteen sixties, Chlamydia pneumoniae was known about but was not known to cause anything more than a walking pneumonia.
If you read page one of David's MS site you will see that he talks about the historical Vanderbilt trial and how people responded. The second one had to be stopped because too many people dropped out, being charmed away by the newest of auto-immune drugs. Neither of them included metronidazole, though: suppliers of money for trials want quick results and you don't get that with this treatment.
I could say that out of the more than a hundred people that my husband has treated who have SPMS, three quarters have stopped progression ad many of these have improved, but not being part of a trial, there is no proof.
Maybe one day he and Stratton will write this all up as a case note study, but maybe for the moment there are more important things to do.
Now, you say that taking drugs for years should not be solely the choice of the patient, but I disagree: nobody can be forced to take anything and it is a great pity that so many people drop out of taking long-term treatment for tuberculosis, but they can't be forced to take the stuff, more is the pity, so TB remains as a constant threat to any people.
Sarah
I am asking all these questions as I think only dr Wheldon and the Vanderbilt team have knowledge and experience in this subject. I think even without clinical trials we can conclude things. In medical history things were based on experience and not clinical trials. Imagine Hippocrates and others doing clinical trials!
They still did much more for their patients than neuros today. So, I greatly value the experince of Dr Wheldon and others and I would be happy getting any info from themHere's an article on it:
http://espace.library.uq.edu.au/eserv.p ... 1_7_04.pdf
