Perhaps I should clarify the situation. Kati is basically right. I will try to sort out some of the further confusions. For anyone who is not aware I will just remind people that the autoimmune dose for rituximab was devised by me for very specific reasons to do with mechanisms of autoimmunity.
Firstly, there is no significant difference between standard oncological dose and autoimmune dose. The exact dosages may be calculated differently and the total amount may be divided into four rather than two infusions, but there is no material difference.
Secondly, there is no justification for using a low dose on the basis of 'prudence'. As has been pointed out I have previously noted that the standard dose may be more than a lot of people need to get full depletion for three months. However, to be of much use one needs to deplete for six months and both in routine RA care and in the Haukeland studies doctors have moved towards maintaining B cell depletion for much longer periods, which on balance makes sense, even if there are issues that need keeping an eye on. We also have some quite good evidence for even the standard dose not being as potent as we would really like and not giving full depletion for a small proportion of patients. So justification for reducing the dose would need to be based on a formal dose comparison study.
We have already heard Dr Beiger and Dr Mikovits talking about low doses of rituximab in a way that indicated clearly that neither of them knew what they were talking about. I strongly suspect that Dr De Meirleir has picked up on this. Giving small doses of rituximab is not 'prudent'. In order to break a cycle of autoantibody production even for a period of months you need complete depletion - both on theoretical grounds and based on experience in particular in lupus. Anything less than about 90% depletion tends to have no clinical benefit at all, as one would theoretically expect. The reasons are to do with complicated immunology. However, it is not too difficult to follow. If a self-controlling system has got into a vicious cycle then gentle actions are more likely to interfere with the remaining good functions of the system than hit the vicious cycle. If you blow gently at a snowball rolling down a hill you do not stop the snowball getting bigger, you just blow away the snow around it.
Moreover, the real dangers with rituximab are of post-infusion allergic reactions and pneumonitis and as far as we know these are UNRELATED to dose - they occur after the first infusion, even if small.
So giving small doses for 'prudence' is in my view stupid meddling. I also have reason to be angry about this.When I developed B cell depletion therapy for RA I thought it might do a lot of good but I realised that in the hands of stupid and irresponsible physicians it might do a lot of harm. We went through that with physicians in France and probably Belgium giving rituximab without monitoring adequately. The lesson was learnt but not without harm being done. I consider myself responsible at least in part for harm done by usage of the drug. As a result I am only too happy to act as an expert witness for the plaintiff in cases of negligence in relation to inappropriate use. The very last thing I, and also Oystein Fluge and Olav Meall, want to see in ME/CFS is usage by phsyciains who do not understand what they are doing. I sincerely hope that Dr De Meirleir is not playing around with it.
