Multiple Sclerosis and helminthic therapy

Every one of our Relapsing Remitting Multiple Sclerosis clients who has maintained a therapeutic population of hookworm has reported achieving near or complete remission within twenty-four months, most show an improvement within six to nine months.

Every. Single. One.

I recently spoke with the gentleman who sent me the email quoted below, and he has agreed to write up an account of his experiences with helminthic therapy. I will post that here as soon as I get it.

Nor are our results always entirely subjective, although this one is typical of the emails I get from our MS clients, in this case their response is documented by their neurologist using pre- and post-helminthic therapy MRIs.

Start of email:

Hi Jasper, I just recently had a brain MRI and I wanted to share the great results with you. This is the letter from my neurologist:

“Just a short note to let you know about the results of your recent MRI of the brain done 5/30/10. We were finally able to get it compared to your previous MRI done 6/22/07 done at Kaiser Woodland Hills. Here’s a copy of the report: “Comparison exam dated 6/22/07 from outside institution is now available for review. Compared to this study, a lesion in the lateral aspect of the right thalamus has significantly decreased in size. A previous lesion in the right brachium pontis is not seen. Other white matter lesions are without significant change. Hyperintensity in the left optic nerve was not definitely seen on the prior but this area was not seen clearly given technique. No new lesion has developed.”

So things are actually improved and no new lesions are seen! This is great news! I think we can safely reduce your Copaxone to every other day provided you have an annual MRI. What are your thoughts?”

This is better news than I could have hoped for. It looks like the mild symptoms I was having were not an actual relapse. Some people get these flare ups when they get too hot, but I think that I may get them when I don’t get enough sleep. From what I understand, it is not actually disease activity, but more like a “short circuit” caused by existing scar tissue in the brain when it is exposed to certain stresses. I definitely think that the hookworms are a big part of the reason that I am doing so well. So thank you again for all the sacrifices that you’ve made to make this treatment available.

End of email.

You can read another quite incredible account on our page devoted to Multiple Sclerosis and Helminthic Therapy. The one you want is by “Ric”. He was in the very first cohort of clients, on September 25, 2007. Reading his account just now I realised I need to get him to update it, and have emailed him so we can bring it up-to-date.

If you want more than anecdote there is plenty of research, in particular that of Correale and Farez over the last decade, theirs is some of the best research into helminth’s impact on any disease there is, even now. If what is available here is not sufficient a search of PubMed, the online medical research database maintained by the National Institutes for Health is a great resource.

Correale and Farez’s work is superb(1,2,3), as you can see for yourself below, the full text of one of the papers below is available for free. See link below also.

What their work shows is that just about any infection with a helminth will slow or stop the progress of Relapsing Remitting Multiple Sclerosis.

Furthermore, their work examines some of the mechanisms explaining the impact of helminth infection on the immune systems of those with Relapsing Remitting Multiple Sclerosis. Explaining how the improvement of symptoms of those with Relapsing Remitting Multiple Sclerosis who are infected with helminths is caused by the helminths.

Taken together this has enormous potential to treat, or to eliminate, Multiple Sclerosis.

Relapsing Remitting Multiple Sclerosis is about 85% of all cases of Multiple Sclerosis.

Secondary Progressive Multiple Sclerosis is what Relapsing Remitting Multiple Sclerosis turns into after a few years or decades. Secondary Progressive Multiple Sclerosis forms about 10% of all cases of Multiple Sclerosis.

So, Relapsing Remitting Multiple Sclerosis is responsible for about 95% of all cases of Multiple Sclerosis.

Summarising, based on our 100% response rate treating Relapsing Remitting Multiple Sclerosis using hookworm alone, supported by powerful results from a series of well-designed and executed studies showing similar results for a variety of helminths, that provide at least part of the reason for the beneficial effects of helminth infection on the course of Relapsing Remitting Multiple Sclerosis, it appears reasonable to believe that it is possible, using tools and techniques we have right now, to prevent or to “cure” approximately 95% of all cases of Multiple Sclerosis.

But is it safe?

One branch of the United States Federal Government says so. The Centers for Disease Control.

The Centers for Disease Control, a department of the National Institutes for Health in the United States, recommends US doctors not treat light infections of hookworm (see diagnosis and treatment algorithm published by the CDC/NIH here).

Light infections being all that is required to treat Multiple Sclerosis, it is hard to understand why there is so little excitement about all this.

Source: Public Health Image Library, ID#:52454

Unfortunately the CDC is not the portion of the US Government that is concerned with regulating, and deciding what are, drugs. Sadly, for us, that portion of the Federal Government, the FDA, has decided that helminths are a drug.

According to various estimates that can be found on the web, a disease not worth treating according to the CDC is in fact a potentially dangerous drug requiring years, decades, of research likely to cost approximately $800,000,000.00, this according to sources quoted on Wikipedia. It is hard to imagine a drug company undertaking such a task to gain approval for the therapy that it could not patent, and that would supplant some of the most expensive drugs on the market today.

Take Tysabri as an example, a drug used in the USA to treat Relapsing Remitting Multiple Sclerosis. One estimate I have read on the internet states that the cost of five years treatment with Tysabri costs $140,00.00, that is the drug alone. It does not include the blood tests and doctor’s visits required by use of the drug. The cost of hookworm currently for five years benefit? $3,050.00.

Put another way, treatment with hookworm for Relapsing Remitting Multiple Sclerosis is 2.1% of the cost of Tysabri over a five year period.

While I understand why no drug companies are championing this approach for treating Multiple Sclerosis, given that doing so would amount to financial suicide, what i don’t understand is why Multiple Sclerosis sufferers, and the Charities that represent them, are not.

I don’t understand why everyone with Relapsing Remitting Multiple Sclerosis is not aware of the potential of helminthic therapy to treat Multiple Sclerosis. Why aren’t the charities championing research or promoting the use of this therapy right now?

It’s safe, remember?

Because of the universal response among our Multiple Sclerosis clients, and the excellent science available courtesy of Correale and Farez, we have decided that Multiple Sclerosis is the route to gaining wider acceptance of helminthic therapy. To persuading the medical and scientific establishment to treat the subject with the seriousness and resources it deserves.

If anyone with experience writing grant proposals, for research in particular. Or with experience working with charities wants to help, or to advise us in these efforts, please contact me by leaving a message in the comments section here, or by visiting http://autoimmunetherapies.com/contact.html.

This is absolutely the most important thing we have attempted since starting to sell helminthic therapy in September, 2007.

Success with a study will help us towards our ultimate goal, the transformation of the practice of medicine o include the use of benign infectious organisms to prevent and to treat disease. We might even help accelerate the eradication of Multiple Sclerosis, too.

Jasper Lawrence

References:

(1) The impact of parasite infections on the course of multiple sclerosis.

Correale J, Farez MF.

Abstract: Previously, we demonstrated that helminth-infected MS patients showed significantly lower number of relapses, reduced disability scores, and lower MRI activity compared to uninfected MS subjects. In the current study, 12 patients with diagnosis of relapsing remitting MS presenting parasite infections were prospectively followed during 90months; due to exacerbation of helminth-infection symptoms after 63months of follow-up, 4 patients received anti-parasite treatment. Helminth-infection control was associated with significant increase in clinical and radiological MS activities. Moreover, these patients showed significant increase in the number of IFN-γ and IL-12 producing cells, and a fall in the number of TGF-β and IL-10 secreting cells, as well as CD4+CD25+FoxP3+ Treg cells evident 3months after anti-helminth treatment began. These new observations on parasite infections associated to MS indicate that parasite regulation of host immunity can alter the course of MS.

Copyright © 2011 Elsevier B.V. All rights reserved.

PMID: 21277637 Link to PubMed Entry

(2) Helminth antigens modulate immune responses in cells from multiple sclerosis patients through TLR2-dependent mechanisms.

Correale J, Farez MF.

Abstract: To better understand the link between parasite infections and the course of multiple sclerosis (MS), we studied the role of TLRs in helminth product recognition by dendritic cells (DCs) and B cells. Baseline expression of TLR2 was significantly higher in infected-MS patients compared with uninfected MS subjects or healthy controls. Moreover, cells exposed to TLR2 agonists or to soluble egg Ag (SEA) from Schistosoma mansoni resulted in significant TLR2 up-regulation. SEA suppressed the LPS-induced DCs production of IL-1beta, IL-6, IL-12, and TNF-alpha and enhanced TGF-beta as well as IL-10 production. Similarly, after exposure to SEA, anti-CD40-activated B cells increased IL-10 production. Both processes were MyD88 dependent. In addition, SEA down-regulated the expression of LPS-induced costimulatory molecules on DCs in a MyD88-independent manner. DCs stimulation by SEA and TLR2 agonists induced increasing phosphorylation of the MAPK ERK1/2. Neither stimulus showed an effect on p38 and JNK1/2 phosphorylation, however. Addition of the ERK1/2 inhibitor U0126 was associated with dose-dependent inhibition of IL-10 and reciprocal enhancement of IL-12. Finally, cytokine effects and changes observed in DCs costimulatory molecule expression after SEA exposure were lost when TLR2 expression was silenced. Overall, these findings indicate that helminth molecules exert potent regulatory effects on both DCs and B cells through TLR2 regulation conducted via different signaling pathways. This knowledge could prove critical in developing novel therapeutic approaches for the treatment of autoimmune diseases such as MS.

PMID: 19812189 Link to free copy of complete paper.

(3) Helminth infections associated with multiple sclerosis induce regulatory B cells.

Correale J, Farez M, Razzitte G.

Abstract

OBJECTIVE: To assess the importance of B-cell control during parasite infections in multiple sclerosis (MS) patients.

METHODS:

Peripheral blood CD19+ B cells from 12 helminth-infected MS patients, 12 MS patients without infection, 10 patients infected with Trypanosoma cruzi, 8 subjects infected with Paracoccidioides brasiliensis, and 12 healthy control subjects were purified using magnetic cell sorting. Interleukin (IL)-4, IL-6, IL-10, tumor necrosis factor-alpha, lymphotoxin, transforming growth factor-beta, brain-derived neurotrophic factor, and nerve growth factor secretion were evaluated after stimulation with CDw32 L cells and CD40 antibody using enzyme-linked immunosorbent assays. The production of anti-myelin oligodendrocyte glycoprotein IgG and IgM antibodies was evaluated by enzyme-linked immunosorbent spot assays. Cell phenotype was assessed by flow cytometry.

RESULTS:

Helminth infections in MS patients created a B-cell population producing high levels of IL-10, dampening harmful immune responses through a mechanism mediated, at least in part, by the ICOS-B7RP-1 pathway. The IL-10-producing B-cell phenotype detected expressed high levels of CD1d and was similar to the one observed in mature naive B2 cells (namely, CD11b(-), CD5(-), CD27(-), and IgD+). Moreover, B cells isolated from helminth-infected MS patients also produced greater amounts of brain-derived neurotrophic factor and nerve growth factor compared with those of normal subjects, T. cruzi-infected subjects, P. brasiliensis-infected subjects, or uninfected MS patients, raising the possibility that these cells may exert a neuroprotective effect on the central nervous system.

INTERPRETATION:

Increased production of B-cell-derived IL-10 and of neurotrophic factors are part of the parasite’s regulation of host immunity and can alter the course of MS, potentially explaining environmental-related MS suppression observed in areas with low disease prevalence.

PMID: 18655096 Link to PubMed Entry

(4) For those wanting to find the hookworm diagnosis and treatment algorithm image for themselves it is impossible to bookmark, I expect the CDC does not want their servers being used by sites like this one to host their images and to provide their bandwidth. But you can find it at http://phil.cdc.gov/phil/home.asp, use the search field to search on “hookworm” and the image is about halfway down on the right.

2 thoughts on “Multiple Sclerosis and helminthic therapy

  1. I have had MS since I was a teenager but not diagnosed til I was 39, I am 62 now and walk with a cane my body won’ t allow me to take standard treatments at this time I think your treatment does the same to the genes in the cells as the gene therapy the Bristol University has discover I think you should compare notes, in the meantime how do I access your therapy
    Thomas Forsmark

    1. Hi Thomas, I am sure we could talk for hours, I am not a fan of unnecessary therapies or invasive ones, like gene therapy. But that is for another time and place. You can learn more by sending a completed questionnaire you can download and submit from http://autoimmunetherapies.com/contact.html, but I have to warn you even if we succeed in arresting or slowing significantly the course of your MS that you will not regain any function lost to nerve damage. I believe you likely know this already, but it has to be said.

      You can also request one, and they will send you some documentation to speed things along as well as the questionnaire, by emailing enquiries@auto….pies.com, be sure to put Regarding Helminthic Therapy as your subject so it gets past our spam filters.

      Thanks for the comment,

      jasper

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