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Rituximab Phase III - Negative result

Gingergrrl

Senior Member
Messages
16,171
I think there could well be a small group of people who benefit from rituximab either because:
  • they have an as yet unidentified autoimmune disease; or
  • because rituximab is effective in another way. I am not talking about placebo. We don't understand the disease mechanism in ME/CFS; therefore, rituximab could have an indirect positive effect.
I think we should keep looking for autoimmune antibodies since the identification of antibodies would help to establish the disease mechanism and identify a (sub) group who would benefit from immune therapy.

I agree with all of this @FMMM1 but you explained it much better than I did!
 

FMMM1

Senior Member
Messages
513
I agree (but did not know enough about the statistics in phase 2 of the trial to comment). Thank you for explaining it @JES. If one third of patients went from a very low functioning score to almost 100 during the treatment (especially at the 15 week point), I cannot imagine how this is placebo if these patients were sick for 8-13 years pre- Rituximab.

To me this means that there is either a sub-group within ME/CFS that is ill because of B-cell driven autoimmunity, or there is a group that has both ME/CFS and a B-cell driven co-morbidity, or there is a completely misdiagnosed group with B-cell driven autoimmunity and no ME/CFS. Either way, identifying these people helps both the individual people and future research.

Hi [from memory] if you check out Alain Moreau's presentation at the OMF Symposium he refers to a group of people with ME/CFS who have an MiRNA which regulates the CD20 receptor which is up-regulated/down-regulated [or some such]. Rituximab targets CD20 B-cells; Alain and Fluge are going to work together on investigating whether this would identify a sub-group who are likely to respond to Rituximab. Alain's talk starts at 2:26:35 [https://livestream.com/accounts/1973198/ME-CFS-2018/videos/180981460].
 
Messages
49
Location
New Zealand
Klimas group believes there is a sub group that will respond to rituximab. I believe there is a trial with better selected patients underway, but I could be wrong...
I personally think the Norwegian researchers commit fraud. The difference between the first 2 trials and the last was so different, I suspect they fiddled the data of the first trials for extra funding for the last. This is common in scientific research. There’s a good article about how and why researchers do this. Sadly it’s very common too!

The good news is though that even if the study was fraudulent, the attention it brought to ME was huge. As the timing of new tools to measure our bodies by other unrelated researchers boomed because Rituximab was thought to prove ME was biologically. Luckily for us the unrelated researchers did indeed find massive amounts of biological differences in ME patients compared to controls. So even if the Norwegian researchers commit fraud,we still owe them gratitude for opening the floodgates into research. Timing was important too because technology finally caught up also. The evil psychiatrist Simon Weasley who suggested ME patients “didn’t want to get well” had to eat humble pie during the Rituximab trials, and then again he was shamed when other researchers showed so much unusual activity going on in the bodies of ME patients. So it’s a mixed blessing.

Disclaimer: I can’t be sure the first Rituximab trials were fraudulent I just highly suspect it.
 

FMMM1

Senior Member
Messages
513
I personally think the Norwegian researchers commit fraud. The difference between the first 2 trials and the last was so different, I suspect they fiddled the data of the first trials for extra funding for the last. This is common in scientific research. There’s a good article about how and why researchers do this. Sadly it’s very common too!

The good news is though that even if the study was fraudulent, the attention it brought to ME was huge. As the timing of new tools to measure our bodies by other unrelated researchers boomed because Rituximab was thought to prove ME was biologically. Luckily for us the unrelated researchers did indeed find massive amounts of biological differences in ME patients compared to controls. So even if the Norwegian researchers commit fraud,we still owe them gratitude for opening the floodgates into research. Timing was important too because technology finally caught up also. The evil psychiatrist Simon Weasley who suggested ME patients “didn’t want to get well” had to eat humble pie during the Rituximab trials, and then again he was shamed when other researchers showed so much unusual activity going on in the bodies of ME patients. So it’s a mixed blessing.

Disclaimer: I can’t be sure the first Rituximab trials were fraudulent I just highly suspect it.

I replied previously to you on this [https://forums.phoenixrising.me/ind...iii-negative-result.56244/page-17#post-987701].

Rituximab treatment is I assume based on the assumption that you're B-cell are producing autoantibodies i.e. which cause ME/CFS. The autoantibody test are c--p. However, one of the leading scientists (Carmen Scheibenbogen) who worked on these autoantibody tests recently published a paper showing that threes genes are upregulated in ME/CFS*. These 3 genes were able to separate a (small) group of people with ME/CFS from a (small) group of people who did not have ME/CFS i.e. healthy controls. I.e. a possible diagnostic test.
[*"The expression signature of very long non-coding RNA in myalgic encephalomyelitis/chronic fatigue syndrome" - https://translational-medicine.biomedcentral.com/articles/10.1186/s12967-018-1600-x].

That's how science works i.e. try something fail, --fail -fail-- success. Ron Davis explained this in one of his talks; I guess this is why OMF are persuing so many different approaches.

Consider lobbying for funding; there are good scientists out there (including Fluge and Mella) but they need funding.
 
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JES

Senior Member
Messages
1,320
I personally think the Norwegian researchers commit fraud. The difference between the first 2 trials and the last was so different, I suspect they fiddled the data of the first trials for extra funding for the last. This is common in scientific research. There’s a good article about how and why researchers do this. Sadly it’s very common too!

Have you actually looked at the results they reported, for example this table that provides individual level patients data highlighting the improvement of many patients? My understanding from following PACE and other messy trials is that very rarely is there actually any direct data manipulation going on. What happened in PACE was that certain thresholds and ways of calculating outcomes were adjusted to make the results seem more impressive, but actual raw data wasn't manipulated.

Regarding manipulation of individual patient data like the one in the table I provided, I don't see how it would be feasible in this day and age. First of all, any patient in such a small trial group could probably recognize himself/herself in this data, so a widely different result would most likely immediately be spotted. It just doesn't make any sense even when assuming that the researchers were corrupt, which I don't see any evidence for either.

If you want to look for a reason behind the disparity in phase 2 and 3 results, IMO a lot more likely explanation is that the patient group was much bigger in 3. If we assume that ME/CFS may be caused by several mechanisms, maybe the small group of patients in phase 2 contained a larger portion of an autoimmune subgroup that responded to rituximab.
 
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Learner1

Senior Member
Messages
6,305
Location
Pacific Northwest
Thanks! So, as @FMMM1 said, this is about a biomarker for detecting ME/CFS, I've and above the ones already found.

I'd be a lot more interested in a treatment here. If Rituximab isn't it, what is?
 

FMMM1

Senior Member
Messages
513
Thanks! So, as @FMMM1 said, this is about a biomarker for detecting ME/CFS, I've and above the ones already found.

I'd be a lot more interested in a treatment here. If Rituximab isn't it, what is?

Check out Vicky Whittemore's (NIH) presentation at the 2018 Invest in ME Conference.

From memory Vicky pointed out that in another illness she's involved with they've just found the causal gene. They can now develop drugs regarding that gene. ME/CFS isn't at that point i.e. the cause hasn't been identified with certainty.

On the flip side we may not need a drug. As Ron Davis has said the system may be intact; what we need is to find out how to re-set it.
 

Learner1

Senior Member
Messages
6,305
Location
Pacific Northwest
I am not convinced we all have the same exact problem to solve. And there seem to be multiple genes involved, so changing the expression of or editing one gene is not the answer.

It does seem to be about understanding a system of interrelated systems that have gone awry and altering the levers to cause all of the little systems to behave better together so the whole concert is more harmonious.

And figuring out one or a few biomarkers is a very long way from being able to do this. The biomarkers are more like the contrail of a jet airplane - we know the jet made it and it points backward to where the jet came from, but we still can't figure out where its going, or if it has enough fuel to get there.

From what I understand, Rituximab is helping some patients, IVIG is helping some, Valcyte is helping some, nutritional supplements are helping some, avoiding and detoxifying mold and other toxins us helping some, surgery on spinal probkems is helping some. Which biomarker is going to tell us which intervention or interventions will help which patients?

Unfortunately, we are likely many years from these answers. I don't like it, and I know scientists are working as hard as they can. But, time is ticking away for all of us, and perhaps if one is 20 now, 5 or 10 or 15 or 20 years waiting for a cure gives one hope for fulfilling life afterwards at a younger age, but for those who are 1-4 decades older, adding this wait time for a cure doesn't give us much at the end...

While I agree that research should be done properly, papers should be published, collaboration should happen, as a patient, the only thing I find relevant is any info on what tests can be done today to give clues and speculation on what theories might work to fix us, so my doctors and I can evaluate the possible risks and rewards and pick and choose those interventions that seem to provide the best chance of success. I just don't see waiting month after month, year after year for all of this research to come to fruition. So far, taking all of the clues and making educated guesses has helped a lot, hasn't cured me, but has vastly improved my quality of life and ability to function. And, my doctors have found a surprisingly long list of various problems to solve that would not likely be resolved by a magic bullet. A process maybe, as Dr. Naviaux has discussed, but no miracle cure...
 

Wishful

Senior Member
Messages
5,679
Location
Alberta
And, my doctors have found a surprisingly long list of various problems to solve that would not likely be resolved by a magic bullet. A process maybe, as Dr. Naviaux has discussed, but no miracle cure...
If you had those problems before developing ME, then curing ME probably wouldn't help. However, if the problems developed afterwards, then they might be resolved by curing or at least treating ME.
 

FMMM1

Senior Member
Messages
513
I am not convinced we all have the same exact problem to solve. And there seem to be multiple genes involved, so changing the expression of or editing one gene is not the answer.

It does seem to be about understanding a system of interrelated systems that have gone awry and altering the levers to cause all of the little systems to behave better together so the whole concert is more harmonious.

And figuring out one or a few biomarkers is a very long way from being able to do this. The biomarkers are more like the contrail of a jet airplane - we know the jet made it and it points backward to where the jet came from, but we still can't figure out where its going, or if it has enough fuel to get there.

From what I understand, Rituximab is helping some patients, IVIG is helping some, Valcyte is helping some, nutritional supplements are helping some, avoiding and detoxifying mold and other toxins us helping some, surgery on spinal probkems is helping some. Which biomarker is going to tell us which intervention or interventions will help which patients?

Unfortunately, we are likely many years from these answers. I don't like it, and I know scientists are working as hard as they can. But, time is ticking away for all of us, and perhaps if one is 20 now, 5 or 10 or 15 or 20 years waiting for a cure gives one hope for fulfilling life afterwards at a younger age, but for those who are 1-4 decades older, adding this wait time for a cure doesn't give us much at the end...

While I agree that research should be done properly, papers should be published, collaboration should happen, as a patient, the only thing I find relevant is any info on what tests can be done today to give clues and speculation on what theories might work to fix us, so my doctors and I can evaluate the possible risks and rewards and pick and choose those interventions that seem to provide the best chance of success. I just don't see waiting month after month, year after year for all of this research to come to fruition. So far, taking all of the clues and making educated guesses has helped a lot, hasn't cured me, but has vastly improved my quality of life and ability to function. And, my doctors have found a surprisingly long list of various problems to solve that would not likely be resolved by a magic bullet. A process maybe, as Dr. Naviaux has discussed, but no miracle cure...

There's a lot I agree with in your post. However, (probably repeating myself) we don't know what's causing ME/CFS. Therefore, it could require the discovery of cause and the development of new drugs. The development of a drug from scratch might take 15 years. However, as Ron Davis has pointed out, we may not need a dug i.e. since the system appears to be intact - based on the nanoneedle results which reverse when you switch from ME/CFS plasma to control plasma. As you point out, it may be a reset issue. However, you can't say, with a high degree of confidence, that it will take 20 years or 2 years i.e. for an individual who is using this forum.

Ron Davis, and Jen Brea, debated time scale recently (last 1 year?) and the argument (from memory) was pretty much the one in my previous paragraph.
 

Gingergrrl

Senior Member
Messages
16,171
Any news on this?

I was wondering this as well and am hoping someone will tag me when the Phase 3 paper comes out (in case I miss it)!

Klimas group believes there is a sub group that will respond to rituximab. I believe there is a trial with better selected patients underway, but I could be wrong...

I believe that as well and hope that there will be more research on this issue.

I personally think the Norwegian researchers commit fraud.

I disagree and why would they possibly commit fraud? Do you have any evidence to back up a statement like this? I would love to understand why the Phase 2 and Phase 3 results were so different but I do not believe that there was any sort of fraud.

Rituximab treatment is I assume based on the assumption that you're B-cell are producing autoantibodies i.e. which cause ME/CFS. The autoantibody test are c--p. However, one of the leading scientists (Carmen Scheibenbogen) who worked on these autoantibody tests recently published a paper showing that threes genes are upregulated in ME/CFS*.

I don't believe that all of the autoantibody tests are crap but I also believe that Rituximab may work in some patients in a mechanism that we just do not yet understand (in addition to B-cell depletion of autoantibodies).

maybe the small group of patients in phase 2 contained a larger portion of an autoimmune subgroup that responded to rituximab.

I agree (either a larger portion of patients in an autoimmune sub-group or some patients with a misdiagnosed autoimmune disease). Which to me means it was a more obscure autoimmune disease vs. the more common ones which would be detected by mainstream testing.

I am not convinced we all have the same exact problem to solve.

I totally agree.
 

FMMM1

Senior Member
Messages
513
Have you actually looked at the results they reported, for example this table that provides individual level patients data highlighting the improvement of many patients? My understanding from following PACE and other messy trials is that very rarely is there actually any direct data manipulation going on. What happened in PACE was that certain thresholds and ways of calculating outcomes were adjusted to make the results seem more impressive, but actual raw data wasn't manipulated.

Regarding manipulation of individual patient data like the one in the table I provided, I don't see how it would be feasible in this day and age. First of all, any patient in such a small trial group could probably recognize himself/herself in this data, so a widely different result would most likely immediately be spotted. It just doesn't make any sense even when assuming that the researchers were corrupt, which I don't see any evidence for either.

If you want to look for a reason behind the disparity in phase 2 and 3 results, IMO a lot more likely explanation is that the patient group was much bigger in 3. If we assume that ME/CFS may be caused by several mechanisms, maybe the small group of patients in phase 2 contained a larger portion of an autoimmune subgroup that responded to rituximab.

I've only skimmed through your response, but your comment that "a lot more likely explanation is that the patient group was much bigger in 3" seems sound. I'm guessing that if you looked at all phase 2, and phase 3, trials the data for this trial may well be within a few standard deviations of the mean.
 

FMMM1

Senior Member
Messages
513
I was wondering this as well and am hoping someone will tag me when the Phase 3 paper comes out (in case I miss it)!



I believe that as well and hope that there will be more research on this issue.



I disagree and why would they possibly commit fraud? Do you have any evidence to back up a statement like this? I would love to understand why the Phase 2 and Phase 3 results were so different but I do not believe that there was any sort of fraud.



I don't believe that all of the autoantibody tests are crap but I also believe that Rituximab may work in some patients in a mechanism that we just do not yet understand (in addition to B-cell depletion of autoantibodies).



I agree (either a larger portion of patients in an autoimmune sub-group or some patients with a misdiagnosed autoimmune disease). Which to me means it was a more obscure autoimmune disease vs. the more common ones which would be detected by mainstream testing.



I totally agree.

I agree that rituximab may work in some people with ME/CFS. I was being simplistic when I said that all of the antibody tests were c--p but I think that there's some evidence of false positives/negatives. I think some of these tests should be reviewed and possibly an improved immunoassay produced or an alternative test (like mass spectrometry) produced. Ron Davis has done some work on improving immunoassays [https://www.omf.ngo/2018/02/12/tweak-assay-bolster-disease-detection-stanford-medicine-news-center/].

I agree i.e.there may be a number of causes of ME/CFS; check out Ron Tompkins's presentation at the OMF (2018) OMF Community Symposium. Ron says pretty much the same thing (from memory) i.e. diseases with different causes can end up at a common end point (outcome).
 

Gingergrrl

Senior Member
Messages
16,171
I was being simplistic when I said that all of the antibody tests were c--p but I think that there's some evidence of false positives/negatives.

I understood what you meant and I agree that these tests will be improved upon in the future. It is also frustrating that the only lab that runs these tests (as far as I know?) is in Germany. I don't understand why the US is so behind and there is no lab that offers these tests here. I am very grateful to Fluge & Mella, Dr. Scheibenbogen, and Cell Trend but I wish the US was more up to speed on all of this information! I was able to seek out what I needed (regardless what country or lab) but I know that many people are too ill to do this. I wish this information was not so fragmented!
 

charityfundraiser

Senior Member
Messages
140
Location
SF Bay Area
I am wondering if the idea has been considered that Rituximab might have worked in the first patients who had both CFS and cancer because it treated the cancer, and that the cancer might have been contributing to their CFS even before they were diagnosed with cancer.

I was treated this year for a different cancer (colon) with surgery and a different chemotherapy (FOLFOX), and about 6-9 months later, my fatigue is less and there is a difference in the characteristics of the fatigue in that my PEM is mild if any now.