There is currently, yet another post, about being newly diagnosed and wanting to be med free (a much abused term - many of the "Med Free's" get their levadopa from macuna instead of a pharmacy. That's like buying paracetemol from Tesco instead of a doctors prescription, and saying "I don't use pharmaceuticals")

Now - I joined this forum because I wanted to be Med Free - and feared conventional medications carried a cost of accelerated disease decline. The short version, is I still use some "off-neurologist" stuff (Vit B & D supplements, Curcumin, Doxazosin, red light hat, and others on and off) but my conclusion is that the balance of probability is that the "scare story" drug problems are the progression of a disease (syndrome) which manifests dramatically differently in different individuals. It's a snowflake disease - no 2 versions are the same. I don't count exercise as "off-neurologist" - all 3 of the neuros I have seen have emphasised its importance

I had participated in a Cure Parkinsons Trust (CPT) webinar about Exanatide, and subsequent email correspondence with the team, and been asked to look in on this forum. I saw my neurologist, told him I wanted to avoid conventional symptomatic meds, and find disease modifying remedies and was offered Rasagiline, which might maybe be neuroprotective a bit. I wanted off-label exanatide. I ended up with a referral to Christine Brefel at Toulouse, strong endorsement from CPT - and ended up on Biogens BIIB054 trial at Toulouse.

And for the first 30 months post diagnosis was not on conventional meds, and doing OK. There are more than a few of us in this club. I could almost certainly manage without medication now. Manage, but live a much diminished life.

So, coming to the points,

1) many of us can manage without meds in the early stages, but this is a progressive disease, and most of us grow out of this.

2) There can be enormous quality of life benefits to getting good symptomatic medication for a fair lump of the earlier part of the disease (which is going to progress anyway). In my case, I am 61. Maybe I can use conventional meds to improve my quality of life until I'm 70. I won't get to live those 9 years twice

3) So if I machismo choose not to use medication until I'm 70 - I would be choosing my handicap and my reduced quality of life. Why? Because, in the absence of any very good evidence, I have bought the story - that declines in later PD, and reduced efficacy of the drug, are due to the drug poisoning me - instead of the natural progression of the disease. That's almost certainly wrong

I am inspired to write this, because of a few months of drug experimentation, and what I think I've learned from it in terms of degrees of "cured". I started on 1mg Pramipexole ER once a day whilst seeing Dr Brefel at Toulouse. I didn't get the big nasties (hallucinations, compulsive behaviours etc) but , maybe it made me cough, made me tired at midday, made my chest tight (it didn't actually cause me breathing difficulties, I just felt odd), and maybe I got light headed bending down, and maybe that was orthostatic hypotension. I wanted to try regular Sinemet as a contrast, and having ended the Toulouse trial, and switched back to my neurologist in Carcassonne, he agreed to help me experiment . I had started adding 2xmacuna 60mg ldopa TDS.

Trying to keep it short, I switched first to .5mg Pramipexole twice a day, and Sinemet 10/100 tds (Having just checked my neurologists report, in French, I see now he intended that to be 2 sinemet tablets TDS. Oops. No wonder I have a stock of them! Then, I faded out the Pramipexole, reducing by 0.26mg every 10 days until down to NIL and added Sinemet ER 25/100 once a day and Sinemet 25/250 tds.

I was due a neuro appointment this week, but he has vanished until November. So I saw my GP, explained the problem, and that I was undermedicated, and had increased the Sinemet ER 25/100 from once a day to TDS. He gave me a 6 month prescription for this latest mix, and commented it was a lot of medication. Which it was, relative to what I had intended.

Part of the problem, is C/L in Europe is no longer available in 25/100 immediate release - which is what I had planned to take. It's either 10/100, 25/250 or 25/100ER.

So, I have cut back to 25/100 ER TDS only. Then, after a week added 1 macuna 60mg TDS. And this week switched the 1 macuna for half a 25/250 sinemet TDS

And I have once again achieved a sweet spot. Although, maybe not sweet enough for my wife (she would like me to try mixing in some Pramipexole again - and if I can get a neuro onside, I might)

What defines the sweet spot for me? I can touch type absolutely as fast as I ever could previously. And I can play guitar. This has turned out to be a really precise measurement tool. And really emphasises the point about missing out on life by avoiding or delaying medication. The guitar thing is quite bizarre - I can not only make chord changes which I was unable to do quickly enough - I can form some chords which I couldn't before. My fingers grow!

The point being - living for today - with the help of medication - effectively I don't have Parkinsons. Or more precisely - I do not suffer the handicap which Parkinsons would otherwise be inflicting on me

You only get one life . I don't want to waste mine being handicapped in the belief, contrary to most of the science, that I am making things worse in the future

Added to that - there is a ton of good stuff happening in Parkinsons research. By the time I'm 70, who knows what will be available?

Carpe Diem