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Lapp Reports XMRV is Found in CFS Using Genome Detection Technology/Ampligen News

Messages
13,774
They're mentioned here:

http://www.genomeweb.com/sequencing...s-chronix-biomedical-caris-life-sciences-babr

"Chronix Biomedical said that it has launched a new disease detection and monitoring service for cancer researchers using its Apoptotic DNA Blood Test, which analyzes apoptotic DNA from dead and dying cells to identify and track ongoing changes associated with specific cancers and other chronic diseases. "

Not really able to see much about them though.

edit: Bad googling. Actually, there are a few things about that make them look credible. I was worried they were just a lab out to scam people, but it doesn't look like that's the case.

Stuff like this looks promising:

Study validates Chronix Biomedical’s serum DNA blood tests for early, accurate detection of breast cancer

http://www.news-medical.net/news/20...arly-accurate-detection-of-breast-cancer.aspx
 

lansbergen

Senior Member
Messages
2,512
richvank;166713 It's a fact that apoptosis is increased in ME/CFS.[/QUOTE said:
If it is apoptosis something is wrong with it.

I wonder whether it is not apoptosis but lysis.
 

xchocoholic

Senior Member
Messages
2,947
Location
Florida
Hi, all.

It's a fact that apoptosis is increased in ME/CFS. There are published papers on this. It's also a fact that the level of cell-free DNA is higher in PWMEs/PWCs than in normal, healthy people, but not as high as in cancer patients. Dr. John McLaren Howard of Acumen Lab in the UK offers a test for cell-free DNA. He has noted that when apoptosis occurs normally, it is a programmed cell death, and the components of the cell are disassembled in an orderly way, so that the amount of cell-free DNA that arises is small. This is not the case in ME/CFS, and especially not in cancer.

I think it's very plausible that retroviruses could be reponsible for early cell death in ME/CFS, and if so, I think it's very plausible that their complementary DNA would show up in DNA fragments in the blood. I think this is very interesting work.

Best regards,

Rich

I'm way over my head here but are these related ? Don't all of us have insane allergic reactions to foods, chemicals, etc ... x

http://ec2-174-129-232-51.compute-1...-contribute-autism-theoharis-theoharides-md-p

Mast cells disrupt the gut-blood-brain barriers and contribute to autism by Theoharis Theoharides, MD, PhD

Many autism spectrum disorder (ASD) patients have a history of "allergic" symptoms and food intolerance, suggesting activation of mast cells, now recognized as master regulators of the immune system.

Activation of intestinal and brain mast cells by immune, infectious, stress or toxic triggers could lead to gut-blood-brain-barrier disruption, permitting brain inflammation and autism. This is more likely to occur in children up to 3 years old, who are more susceptible to infections, and when their gut-blood-brain barriers are still developing.

Moreover, perinatal stress has been associated with ASD development, and we have shown that corticotropin-releasing hormone (CRH) secreted under stress and during premature labor can induce mast cells to release vascular endothelial growth factor (VEGF), which increases blood-brain-barrier permeability.

We have also shown that mercury causes release of VEGF from human mast cells. Mast cells are critical in the disease mastocytosis, characterized by an increased number of hypersensitive mast cells in many tissues. Children with mastocytosis also present with skin allergies, diarrhea, learning disabilities, hyperactivity and difficulty focusing, reminiscent of ASD.


A survey of the Mastocytosis Society's members (www.tsmforacure.org) indicated that the rate of autism in children with mastocytosis is at least 10-fold higher than that reported for the general population.

Mastocytosis patients also have high blood levels of interleukin-6 (IL-6), which has recently been implicated in an "animal model" of autism, and which we have shown derives entirely from mast cells. We have also shown that the naturally occurring flavonoids luteolin and quercetin can inhibit human mast cell release of IL-6 and other inflammatory molecules.



Theoharis Theoharides, MD, PhD is a professor of pharmacology, Internal Medicine and Biochemistry, and the director of the Laboratory of Molecular Immunopharmacology and Drug Discovery; Department of Pharmacology and Experimental Therapeutics, Tufts University School of Medicine. He trained in allergy and clinical immunology at Yale and internal medicine at New England Medical Center.

Dr. Theoharides was director of medical pharmacology at Tufts (1986-1993), and became full professor in 1995. He has 300 publications and 3 books, including a Textbook of Pharmacology. Dr. Theoharides was the first to show mast cells and acute stress promote inflammation in autism, cancer, interstitial cystitis, migraines and multiple sclerosis.



Mast cells ...

http://www.ncbi.nlm.nih.gov/pubmed/9354811

Mast cells are found resident in tissues throughout the body, particularly in association with structures such as blood vessels and nerves, and in proximity to surfaces that interface the external environment.

Mast cells are bone marrow-derived and particularly depend upon stem cell factor for their survival. Mast cells express a variety of phenotypic features within tissues as determined by the local environment.

Withdrawal of required growth factors results in mast cell apoptosis. Mast cells appear to be highly engineered cells with multiple critical biological functions. They may be activated by a number of stimuli that are both Fc epsilon RI dependent and Fc epsilon RI independent.

Activation through various receptors leads to distinct signaling pathways. After activation, mast cells may immediately extrude granule-associated mediators and generate lipid-derived substances that induce immediate allergic inflammation.

Mast cell activation may also be followed by the synthesis of chemokines and cytokines. Cytokine and chemokine secretion, which occurs hours later, may contribute to chronic inflammation.

Biological functions of mast cells appear to include a role in innate immunity, involvement in host defense mechanisms against parasitic infestations, immunomodulation of the immune system, and tissue repair and angiogenesis.
 

SOC

Senior Member
Messages
7,849
Hi Rich,
Now, since I became ill I noticed that my nails changed, more particularly my lunulas(the half moon on your fingernails). The appeared and disappeared continuously and I always atrributed that to cell apoptosis, but since a month now, they don't disappear anymore. I guess, Gc-Maf is doing it's work and cell apoptosis is not happening anymore to full scale. Of course, that's just an assumption...

Whadda ya know... my lunulas have disappeared too. How strange. I never noticed that before. So is this another oddity of ME/CFS?
 

justy

Donate Advocate Demonstrate
Messages
5,524
Location
U.K
Hi, all.

It's a fact that apoptosis is increased in ME/CFS. There are published papers on this. It's also a fact that the level of cell-free DNA is higher in PWMEs/PWCs than in normal, healthy people, but not as high as in cancer patients. Dr. John McLaren Howard of Acumen Lab in the UK offers a test for cell-free DNA. He has noted that when apoptosis occurs normally, it is a programmed cell death, and the components of the cell are disassembled in an orderly way, so that the amount of cell-free DNA that arises is small. This is not the case in ME/CFS, and especially not in cancer.

I think it's very plausible that retroviruses could be reponsible for early cell death in ME/CFS, and if so, I think it's very plausible that their complementary DNA would show up in DNA fragments in the blood. I think this is very interesting work.

Best regards,

Rich

Thanks for bringing this up Rich, i was wondering about the link too. I had the testing with the Acumen lab also and like Garcia i had a pretty high cell free DNA. Its a useful test in that it mirrors somewhat how you are feeling, so the test validates your illness, but i couldnt find out much more info about what its really telling you than that.
My reading of the in the near future means that the very quick testing for $100 is not yet available or may not be for some time, i think its normal to say something will be developed without being 100% sure how or when.
I am so excited by the news, just when i was beginning to think it was all a dead end.
 

WillowJ

คภภเє ɠรค๓թєl
Messages
4,940
Location
WA, USA
Ok, that bit about testing blood for dead cells and the pathogens in them is really cool. Cellular disease is really developing as a field. I wished I could be well and be a part of that revolution, but I certainly don't want it to wait for me. There are a lot of cellular diseases in addition to ours, that can really benefit from this sort of technology. Wow. Imaginary happy dance here!

I had seen the Lapp newsletter and I'm pleased that Ampligen is deemed approvable. :) I also wish they'd hurry up about it. Both HEB and FDA.
 

WillowJ

คภภเє ɠรค๓թєl
Messages
4,940
Location
WA, USA
Hi, all.

It's a fact that apoptosis is increased in ME/CFS. There are published papers on this. It's also a fact that the level of cell-free DNA is higher in PWMEs/PWCs than in normal, healthy people, but not as high as in cancer patients. Dr. John McLaren Howard of Acumen Lab in the UK offers a test for cell-free DNA. He has noted that when apoptosis occurs normally, it is a programmed cell death, and the components of the cell are disassembled in an orderly way, so that the amount of cell-free DNA that arises is small. This is not the case in ME/CFS, and especially not in cancer.

I think it's very plausible that retroviruses could be reponsible for early cell death in ME/CFS, and if so, I think it's very plausible that their complementary DNA would show up in DNA fragments in the blood. I think this is very interesting work.

Best regards,

Rich

very interesting (as your posts always are), thanks much
 

Bob

Senior Member
Messages
16,455
Location
England (south coast)
Maybe i'm missing something here, but i can't quite understand what there is to get excited about here... Is there something I'm missing?

As I understand it, Ampligen has a long history of not getting FDA approval, and this CFS study is one among many trials that they've carried out, and all the others have not met FDA approval. The FDA approval scheme is so complex and expensive, that I'm not sure this is something that is ever going to happen.
The side effect that they mention worries me... "Flu-like" symptoms... Well, that's something I'm trying to get rid of, so I'm not very encouraged by that, especially because I tend to get a strong reaction to drugs.
The other thing is that only a third of patients are responding 'very significantly', which means that two thirds might not be seeing any significant effects. Even the term 'very significant' doesn't mean much unless they clarify exactly what they mean. 'Very significant' might just mean that patients see a very small improvement. A 'very significant improvement' does not necessarily equate to a 'very effective' treatment. It might just mean a slightly effective treatment, or a minimally effective treatment. (I learnt all this about the use of wording in medical trials, from the PACE Trial, which talked about 'moderately effective treatments', which when analysed, actually meant 'very minimally effective.')

And then there's the blood tests that they are talking about... It's all so vague, that i'm not sure exactly what they are offering us... And are they offering it to us now, or some vague time in the future? Are they going to publish their results? Unfortunately a patent request does not mean that they are going to have any actual results for us in the near future... It might be a speculative patent request.

If they really have found an XMRV-Human DNA 'chimera', then that is obviously really big news, but it does seem to be somewhat speculative, with no hard evidence at this stage.

If anyone can give any clarity to any of this, then I'd be grateful.
 

WillowJ

คภภเє ɠรค๓թєl
Messages
4,940
Location
WA, USA
Ampligen is not going to help everyone, but there is a potential to significantly (by any fair definition of the word, no studyspeak) help some patients. Some patients get a portion of their life back, get out of wheelchairs, etc. Not everyone is helped. Some people do worse, actually. It is still not a magic bullet.

The blood tests are cool because generally you have to have identifiable organ damage, demyelination, or something like that in order for a doctor to notice you are sick. But some disease happen inside the cells. I refer to this as cellular disease.

Doctors know about a few of these cellular diseases, such as some channelopathies like Myasthenia Gravis. However, they generally only test you for this if you have a visible sign like droopy eyelid (even though it is a known fact that you can have MG without that). They are supposed to also test you if you go into respiratory distress, but if they arbitrarily decide that the respiratory distress is some kind of anxiety or panic attack (perhaps due to a handy psychosomatic label like CFS), they might not even note this in your chart, much less test you for serious disease like MG.

With a blood test for dysfunctional dead cells like this, they can potentially identify cellular disease--like ours: long on cellular dysfunctions like channelopathy, inappropriate apoptosis, cellular transport issues, probably cell communication issues, and the like, but short on what doctors easily identify as disease like shriveled organs, tar in the lungs, scar tissue building up, and other macro issues.

Sounds to me like one could immediately prove inappropriate cell death was ocurring, and labs would perhaps have a novel tool for identifying specific disease processes or at least genetic differences (point mutations, foreign material such as viruses, bacteria, fungus) in the dead cells.
 

Dan_USAAZ

Senior Member
Messages
174
Location
Phoenix, AZ
Maybe i'm missing something here, but i can't quite understand what there is to get excited about here... Is there something I'm missing?

As I understand it, Ampligen has a long history of not getting FDA approval, and this CFS study is one among many trials that they've carried out, and all the others have not met FDA approval. The FDA approval scheme is so complex and expensive, that I'm not sure this is something that is ever going to happen.

Bob,
While I hope Ampligen works out for some, I think I am less excited about the Ampligen announcement and more excited about their claim that they can detect XMRX chimeras that are spilled into the blood as a result of cell apoptosis. If I am interpreting this correctly, it suggests that they can show XMRV integrated into human DNA and answers the question as to whether XMRV truly exists in the human population or if it was just a lab contaminant.

If they can prove the XMRV DNA integration within chimeras and others can replicate the findings, I would assume that the science would be able to move forward and start looking at whether XMRV is a pathogen that causes disease. I know many researchers have already moved ahead, but I am referring to the holdouts who still claim that XMRX is a lab contaminant.

I assumed most of the excitement in this thread was related more to the chimeras and less about Ampligen, but maybe not, I would like to hear from others on this. Also, if I am misinterpreting the implications of XMRV integrated into chimeras, please let me know that as well.

Thanks,
Dan
 

Guido den Broeder

Senior Member
Messages
278
Location
Rotterdam, The Netherlands
What Ampligen does is point the immune system in the right direction. This may not be enough; some patients may need strong antivirals of the kind that Lerner prescribes (valacyclovir, valgancyclovir). It is also entirely possible that not all the patients in the Ampligen trials really had/have ME. Remember that CFS is nothing more that a way to select patients for trials, it is not the disease itself.

Apoptosis in ME has been known for decades, and is believed to be the result of defects in the immune system. Normally, a sick cell will first try and repair itself and will only end its life cycle when that fails. There are reports of finding lots of dead cell material in tissue samples of ME patients.
 

anne_likes_red

Senior Member
Messages
1,103
Mine are gone too, except for both thumbs, there they are normal. I never thought much about it, even though i've realized i don't have them anymore. Interesting...

Mine went years ago....just a hint of them left on my thumbs too. I wonder why the thumbs are special? :)
 

SOC

Senior Member
Messages
7,849
Mine are gone too, except for both thumbs, there they are normal. I never thought much about it, even though i've realized i don't have them anymore. Interesting...

Same here, gone except for on thumbs. What on earth can this have to do with cell apoptosis or anything else related to ME/CFS?

So many oddities with this illness.
 

kday

Senior Member
Messages
369
Whadda ya know... my lunulas have disappeared too. How strange. I never noticed that before. So is this another oddity of ME/CFS?

I noticed this before any treatment. Mine were completely gone on every nail. Mentioned this many times.

Methylation treatment makes them grow much larger on the thumbs, and in my case, if I get my methylation cycle to go continuously, they appear on my index and middle fingers as well.

I notice as they grow, it usually correlates with improvements in the nervous system. Shrinkage doesn't ever seem to be a good sign.
 

SpecialK82

Ohio, USA
Messages
993
Location
Ohio, USA
Yep, no lunulas here either except for the thumbs.

Another sign of cell apoptosis is a disappereance of fingerprints. Dr. Lapp has noted that many of his patients no longer have their fingerprints. If you look at your fingertips, they are either pruned up (like when you just get out of water) or they are shiny looking and smooth. My fingers vary between the two. I've also noticed the soles of my feet are doing the same thing - smoothing out, they are more slippery when walking in bare feet.
 
Messages
49
I just checked my fingernails and I'm missing lunulas too - I only have them on my thumbs and one finger on my right hand. This is very interesting! My fingerprints had mostly disappeared by 1989, especially on the smaller fingers, and they've been like that ever since.


I hope Chronix isn't being overly optimistic about their test becoming available "soon". Hemispherx does have a problem with overstating things. But if Dr. Lapp is excited, that's a good sign - it's like when Dr. Bell's socks "start rolling up and down".
 

insearchof

Senior Member
Messages
598
Hi Bob

Agree with your concerns and the article detailing the history of the drug someone posted earlier was very interesting.

I think though, Willow also makes valid points with respect to this treatment. Like most of what is being mooted and or offered, the long term efficacy of these treatments remains unknown. What you raise is important, and necessary to know and understand in order to do a risk/benefits analysis and go with what we feel most comfortable with (which is never easy when you're as chronically and sometimes critically ill and are concerned that something might lead to a further deterioration in your health). It is, a burdensome undertaking for many of us, severely ill, and already shouldering far too much of this burden alone.

What saddens me, is that patients and researchers remain at this juncture 25 yrs (CFS) or 50 yr ( ME) on. If these illnesses had not been manipulated, reclassified or reassigned to areas of medicine where they were left to languish, we might not have to seek out cutting edge treatments, and struggle to weigh up the unpalatable acceptance of unnecessary risk, in the mere hope of some improvement in health and quality of life.:(

On a more positive note I would like to learn more about this:

If they really have found an XMRV-Human DNA 'chimera', then that is obviously really big news, but it does seem to be somewhat speculative, with no hard evidence at this stage.
.