You really don’t get it ’til you get it with these denied diseases. Immune suppression diseases have been vehemently denied by the mafioso medical establishment throughout history resulting in the sacrificial genocide of innocent human victims who are caught in the cross fire of a war they did not ask to be a part of. All sufferers intuitively share the same pragmatic common ground. That common ground being more like a cliff side that we are stuck on, clinging to the jagged outcropping of rocks while our fingers bleed as we get tossed fishing line that we can’t quite grasp, instead of a rope to climb our way back to the top. We may not have asked to be in this war but one thing is for sure- we are fighters, and fight we will until every last battle has been overcome and Justice prevailed. Our own salvation is up to us as the lifelines we have been thrown act more like decoys.

This Lyme war started roughly 40 years ago when a Mom demanded someone find out why so many kids were mysteriously developing juvenile arthritis. We all know the story of how Allen Steere was the supposed puzzle-putter-togetherer and that Willy Burgdorfer was the one who saw a spirochete in the slide. What we are still contending with today is what Willy appropriately coined as the “shameful affair”. Things took a turn for the worse when greedy, truly stupid, self serving evil idiots decided it would be a good idea to make a vaccine against a relapsing fever organism. Is there a word to describe how stupid it is to think a venture such as this would ever work out, to vaccinate for an organism capable of true antigenic variation? What is equally dumbfounding is the predicament they got themselves into insisting that we need a vaccine for such a non-disease in the first place.

So we need a vaccine for a disease that doesn’t make people sick and is hard to catch and easy to treat in the first place? Lyme is just a knee but also causes victims to acquire brain degrading enzymes- so get the vaccine. Quite the quandary.

You can’t have it both ways, fellas. Nice try, though.

Another baffling aspect to this is that the good guys like ILADS and the LDA don’t mention that we are victims of such a crime. They don’t mention that OspA is Pam3Cys and that killing spirochetes won’t fix B cells. They have done a great disservice to us all. ILADS not only cannot help everyone for financial reasons, but they also have never used their platform to do the one thing that would help every single patient out there- support a criminal prosecution. They have been on national television and never mentioned it and it’s not in Horowitz’s book. The answer to “Why Can’t I Get Better?” is a simple one- because the disease isn’t about spirochetes and killing them won’t reverse the acquired immune deficiency. While they make millions and gain all of our affection there are people living outside in the cold right now because when they got too sick to work they couldn’t get disability when they were instead labeled a hypochondriac. There are children suffering greatly who are living in poverty, whose parents are constantly on the verge of getting the electricity shut off living paycheck the paycheck.

Decoys..

The kicker to this is that they know. It’s not like they just haven’t discovered it yet. They know that OspA is Pam3Cys because Kathleen told them. She wrote their original Klempner rebuttal and was a part of the organization many many years ago. As an organization they are killing us, too, by omitting the science and true mechanism of disease. What does that make them? While our doctors may have integrity and truly trying to help their patients they failed to ask a very important question. If the LYMErix vaccine caused the same disease, but had no spirochetes in it, then what is the disease really about? What is OspA?

We fight for our diagnosis and everyone turns us away and blames us. Then finally ILADS validates our suffering and offers hope that if we bust biofilm, kill the critters, detox the mold, etcetera, that we can get our lives back. Then to find out that isn’t true either, after we may have spent thousands of dollars and spent years convincing our friends and family…. Well, it’s devastating. It’s humiliating. Some people just simply won’t believe it and refuse to even look at the data and viciously attack the messenger who only wanted to show them they respect they deserved by telling them the truth. Others are relieved after being told in support groups that if they didn’t find a way to afford expensive treatments they would die. A lot of us are outraged by it all and become determined to fight this and fix it.

Tick bite victims really only need to know a few simple things. Once we all know these simple things “they” can’t *&$% with us anymore.

Dearborn was invalid

OspA is Pam3Cys, so antibiotics don’t work

This is a CRYME that needs to be prosecuted

The Cryme in one picture

If you are reading this you are likely well aware of the hell that this disease is. It is like you’re invisible in every way. You disease doesn’t show up on your test results, your family and friends don’t seem to notice the pain in your eyes, your doctors don’t believe you. It’s like being buried alive while screaming as loud as you can but everyone around you is deaf and blind, seemingly lacking even basic empathy. No one seems to hear you, or see you, or care about you. While you suffer several neurologic diseases and have an acquired immune deficiency (AIDS) the whole world turns its back on you.

We are forced to trudge through our lives like the walking dead, desperately holding on for dear life while at the same time secretly wishing we would just die already. The abandonment, the torment, days turning to weeks to months to years to decades of living in survival mode. Being misunderstood and judged becomes your normal, and you end up living defensively. By the time you figure out that you’re living with a disease that doesn’t officially exist you’re stuck in a time-loop of panic. Suicide becomes a valid treatment option.

We are completely powerless to what is happening inside of us and it spills outwardly into what happens around us. Our friends and families are quick to judge us and put plenty of energy into discrediting our misery, yet subtle are the times and ways that they actually TRY to understand what is actually wrong with the person that they are supposed to love. They can’t imagine that we could actually have a real disease after so many doctors tell us that they can’t find anything wrong. Doctors don’t even respect their own “profession” enough to use PubMed to find out what the disease is. No one wants to put their ego aside to LOOK AT THE VALID DATA, proving that these victims are the sickest people on this earth. Doing so might threaten their moral obligation to admit that they have been wrong and it’s easier to be arrogant. After all, doctors paid a lot of money to become the non-scientists that they are and God forbid they should have to understand disease mechanisms for any other reason than to throw a drug at it. Blame the patient, always, so that one never has to sacrifice the precious and easily earned jewel that is self righteous pride.

Pride hates the truth and that’s a fact.

All of the abuse, neglect, slander, oppression.. it’s all because of a scientific crime. Straight up research fraud. That is good news because it means that we can do something about it, like prosecute it. What we do have a choice in is how we react. The data that I am sharing with you in this is your rope brought to us by our favorite whistleblower, Kathleen Dickson.

Which is why I want to validate everyone here today. You’re as sick as you feel. The “experts” and the government know what these diseases are. The science says that you’re a zombie on a cellular level, 80 years old when you’re only 40. The medical term for this is Post Sepsis Syndrome (PSS) and that means that you have an acquired immune deficiency. You get bit by an infected tick and end up with spirochetes and God knows whatever else. After the initial cytokine storm your bodies way of coping is to down-regulate, or turn off. If it didn’t you would die.

Brain and nerve degrading enzymes are found in the spinal fluid of lyme victims but that didn’t make it into Klempners fraudulent re-treatment study. Lyme crook, Schoen, when pushing the LYMErix vaccine said everyone better get vaccinated because Gfap (glial fibrillary acidic protein) was an issue for tick bite victims, which is a sign of gliosis (brain destruction), but simultaneously insists that Lyme is just a bad knee. As far back as 1986 we have experts such as Paul Duray reporting findings like transformed B cells in spinal fluid that were being misinterpreted by labs as malignant lymphoma and leukemia. Allen Steere reported Lyme being like “psuedolymphoma” in the 90s but has been hell bent on saying that it’s just arthritis in a knee since Dearborn. Wormser signed off on the “Guidelines” while reporting himself that Dearborn is only only 15% accurate. They all use flagella for specificity in their patents but deny it as a biomarker for diagnosis. Also in the patents they talk about the two different outcomes but that certainly isn’t in the fraudulent guidelines.

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Let’s start with what spirochetes are, so we can know what they do. I cannot stress enough the fact that this is so much worse than persisting spiral shaped bacteria drilling through our tissues.

Spirochetes do all of the damage very early on, I’m talking’ like the first 10 days to 2 weeks. They go straight to the lymph nodes and set up shop, then straight to the brain chronically inflaming it. It has been known for the last 108 years that borrelia, which are relapsing fever organisms that undergo true antigenic variation, are permanent brain infections. Persistence is very old news. As soon as they enter the host they begin shedding, or blebbing, their outer surface proteins (Osps). The shed triacylated lipoproteins are what really mess you up being that they are fungal-like antigens, managed by TLR 2 and cause something called “immune tolerance”. This means that your body loses the ability to recognize or fight other pathogens handled by other TLRs. There is also the issue that half the cases fail even early treatment and go on to eventual disability.

OspA is Pam3Cys. Pam3cys is a molecule that when inside the body it basically STOPS the typical immunity chain reaction. This is what overwhelms, or destroys the immune system when you have Lyme disease. The effects are not undone by taking antibiotics because killing spirochetes doesn’t do anything for the immune system. “Taking the load down” doesn’t mean anything when it comes to post sepsis syndrome. Pam3Cys is an endotoxin. You can literally buy this stuff and use it for inducing experimental sepsis.

And they called it a vaccine. If something causes immune suppression that makes it the exact opposite of a vaccine. Duh.

“The magnitude of modulation was directly dependent on the quantity of OspA. OspA interferes with the response of lymphocytes to proliferative stimuli including a blocking of cell cycle phase progression.” – Gary Wormser https://www.ncbi.nlm.nih.gov/pubmed/10865170

OspA = Pam3Cys = permanent immune suppression or Post Sepsis Syndrome.

AIDS, folks.

“Tolerance means the immune system will stop responding to the antigen. Cross tolerance means spreading or expanding normal disease-combating insufficiency to other antigen types such as TLR4 agonists or TLR7/9 agonists (viruses). Exposure to shed borrelial lipoproteins causes fungal tolerance in the blood and the inability to get rid of mycoplasma/eperythrozoons (also bearers of fungal antigens like OspA) from the blood, especially from the red blood cells. It is well known that fungi infections in the blood, particularly these blood parasites, the eperythrozoa or mycoplasma, causes fatigue, because they, by attaching to the surfaces of- and within- red blood cells hijack sugar metabolism and change the osmotic potential of the red cell membrane, rendering Oxygen unable to cross the red cell membrane, starving the body cells of Oxygen.

This generalized immunosuppression as a result of exposure to borreliae and their shed varying surface antigens creates an environment where common opportunistic infections are reactivated, such as latent Epstein-Barr, and cause chronic disabling disease.” -KMD http://www.actionlyme.org/BORRELIOSIS_BASICS.htm

Here is a relatively recent report (2015) out of UCDavis from Nicole Baumgarth. This is really important because it proves that the host loses the ability to mount an immune response TOTALLY. That means that you’re not going to be making antibodies, therefore you won’t test positive for anything. Doctors only know to look for “objective signs of inflammation” to diagnose an underlying disease process. Unfortunately, this includes LLMDs.

All of this means that spirochetes cause immune suppression and the resulting collapse is life altering. We know how serious this disease is because ever since we got the “flu that changed everything” we have felt like we are dying. Now that you have an acquired immune deficiency viruses reactivate and other opportunistic infections of all kinds take advantage of the free reign. This is common knowledge, transplant victims have the same thing going on as a result of the immunosuppressive drugs they have to take like Humira and Stelara.

Carolyn Beans (NIH) on Live Science:

Surviving Sepsis: Detection and Treatment Advances

“Some people who survive sepsis can develop secondary infections days or even months later. A research team that included Richard Hotchkiss, Jonathan Green and Gregory Storch of Washington University School of Medicine in St. Louis suspected that this is because sepsis might cause lasting damage to the immune system. To test this hypothesis, the scientists compared viral activation in people with sepsis, other critically ill people and healthy individuals. The researchers looked for viruses like Epstein-Barr and herpes simplex that are often dormant in healthy people but can reactivate in those with suppressed immune systems.

[Sepsis Has Long-Term Impact for Older Adults, Study Finds]

“Of the three study groups, people with sepsis had much higher levels of these viruses, suggesting reactivation due to compromised immune responses. Immune suppression could make it difficult to defend against the reactivated viruses as well as new infections like pneumonia. The team now plans to test whether immune-boosting drugs can prevent deaths in sepsis survivors.”

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“For more than two decades, sepsis was defined as a microbial infection that produces fever (or hypothermia), tachycardia, tachypnoea and blood leukocyte changes. Sepsis is now increasingly being considered a dysregulated systemic inflammatory and immune response to microbial invasion that produces organ injury for which mortality rates are declining to 15-25%. Septic shock remains defined as sepsis with hyperlactataemia and concurrent hypotension requiring vasopressor therapy, with in-hospital mortality rates approaching 30-50%.

With earlier recognition and more compliance to best practices, sepsis has become less of an immediate life-threatening disorder and more of a long-term chronic critical illness, often associated with prolonged inflammation, immune suppression, organ injury and lean tissue wasting. Furthermore, patients who survive sepsis have continuing risk of mortality after discharge, as well as long-term cognitive and functional deficits. Earlier recognition and improved implementation of best practices have reduced in-hospital mortality, but results from the use of immunomodulatory agents to date have been disappointing. Similarly, no biomarker can definitely diagnose sepsis or predict its clinical outcome.

Because of its complexity, improvements in sepsis outcomes are likely to continue to be slow and incremental.” https://www.ncbi.nlm.nih.gov/pubmed/28117397

There are a lot of different names for this state of lymph node failure that is really an acquired immune deficiency. Mainstream it’s labeled CFS/ME, Fibromyalgia, or straight up crazy loon faker hypochondriac syndrome. The victims usually call it what they assume it had been caused by like mold/biotoxin illness, Autism/vaccine injury, Lyme, etc. The label that fits the most accurately as an umbrella term is post sepsis syndrome. PSS is all inclusive in that it describes a state of aftermath in the body from a TLR 2 agonism event leading in to immune suppression with chronic reactivation of viral syndromes and opportunistic takeover. Having wrecked germinal centers is the common ground between all of these different syndromes. It truly is a shit show.

Everything that has been done since the crime was committed was fixed around keeping up the pretense that Dearborn was valid. Lyme disease was rebranded to fit their vaccine model. They spun the disease claiming that the odd HLA-linked hypersensitivity response accounting for only 15% of total cases was the ONLY disease and cut out the majorly more common outcome that 85% of the population gets, the chronic neurologic immunosuppression disease.

Here is a list of valid biomarkers, most of which are from the real disease denialism vaccine addicted criminals themselves. <That’s a mouthful> Note that none of these were used in Klempners fraudulent re-treatment study, he used psych questionnaires instead. Studies from about the early 1990s onward are invalid because of Dearborn, so we need to pull out the time machine and travel back to a time when pathology was pathology and questionnaires were a stupid way to do science. They can’t possibly try to claim that they are so inept that ALL of their previous findings are bullshit. This is an obvious conflict against even themselves, to claim that Lyme is just a knee but a vaccine is necessary because of neurologic problems, a common mechanism in itself amongst the criminals involved.

Brain and nerve degrading enzymes-

Perides G1, Charness ME, Tanner LM, Péter O, Satz N, Steere AC, Klempner MS.

“Neurologic manifestations of Lyme disease include meningitis, encephalopathy, and cranial and peripheral neuropathy. There are no sensitive markers for neuroborreliosis, and diagnosis is often based on clinical presentation and cerebrospinal fluid (CSF) abnormalities, including intrathecal antibody production. Matrix metalloproteinase (MMP) activity in CSF was compared in patients with neuroborreliosis, patients with diverse neurologic disorders, and healthy controls. The CSF of 17 of 18 healthy subjects and 33 of 37 patients with neurologic symptoms and normal CSF and imaging studies contained only MMP2. The CSF of several patients with neurologic disorders contained MMP2, MMP9, and gelatinolytic activity at 130 and 250 kDa. The 130-kDa MMP was found without the 92- kDa MMP9 in the CSF of 11 (79%) of 14 patients with neuroborreliosis and only 7 (6%) of 118 control patients (P < .001). This pattern of CSF gelatinase activity may be a useful marker for neuroborreliosis.”

https://www.ncbi.nlm.nih.gov/pubmed/9466528 You can’t kill spirochetes- “The Lyme disease spirochete, Borrelia burgdorferi, can be recovered long after initial infection, even from antibiotic-treated patients, indicating that it resists eradication by host defense mechanisms and antibiotics.” https://www.ncbi.nlm.nih.gov/pubmed/1634816

Brain destruction- “Other peripheral neuropathies and Lyme meningitis are also seen at this stage. In late-stage disease, the central nervous system may be involved. A new diagnostic test measuring glial fibrillary acidic protein in cerebrospinal fluid may prove to be a useful tool for measuring such involvement (20).” https://www.ncbi.nlm.nih.gov/pubmed/10766685

Anti-flagellar antibodies cross reaction with myelin, very not good- “Although Borrelia burgdorferi, the causative agent of Lyme disease, is found at the site of many disease manifestations, local infection may not explain all its features. B. burgdorferi’s flagellin cross-reacts with a component of human peripheral nerve axon, previously identified as heat shock protein 60 (HSP60).” http://www.ncbi.nlm.nih.gov/pubmed/11860186

Neurophysiological abnormalities- ‘Abnormal QEEG and/or EPs were found in 75% of the active Lyme disease patients and in 54% of the post CNS Lyme disease patients. Three different types of neurophysiological abnormality were observed in these patients including QEEG slowing, possible signs of cortical hyperexcitability, and focal patterns indicating disturbed interhemispheric relationships. In patients tested before and after treatment QEEG and EP normalization was associated with clinical improvement.” https://www.ncbi.nlm.nih.gov/pubmed/7554300

Encephalopathy-

“Lyme encephalopathy (LE) presents with subtle neuropsychiatric symptoms months to years after onset of infection with Borrelia burgdorferi. Brain magnetic resonance images are usually normal.” http://www.ncbi.nlm.nih.gov/pubmed/9409364 Quinolinic Acid found in CNS, sign of infection as a byproduct of the immune system “In patients with encephalopathy, serum QUIN was elevated with corresponding increments in CSF QUIN. Lymphokine concentrations were not consistently elevated. We conclude that CSF QUIN is significantly elevated in B burgdorferi infection–dramatically in patients with CNS inflammation, less in encephalopathy. The presence of this known agonist of NMDA synaptic function–a receptor involved in learning, memory, and synaptic plasticity–may contribute to the neurologic and cognitive deficits seen in many Lyme disease patients….“

http://www.ncbi.nlm.nih.gov/pubmed/1531156

ALS and Lyme-

There appears to be a statistically significant association between ALS and immunoreactivity to B burgdorferi, at least among men living in hyperendemic areas.” https://www.ncbi.nlm.nih.gov/pubmed/2334308

Neurotoxin nitric oxide in the brain-

Borrelia burgdorferi and Escherichia coli lipopolysaccharides induce nitric oxide and interleukin-6 production in cultured rat brain cells. http://www.ncbi.nlm.nih.gov/pubmed/7513330

Anti ganglioside antibodies-

“Patients with neuroborreliosis produce antibodies, mostly of the immunoglobulin M (IgM) class, to gangliosides, particularly to those with Gal(beta 1-3)GalNac terminal sequences.” https://www.ncbi.nlm.nih.gov/pubmed/7558329

***EBV transformed cells in CSF***-

“Immature B cells can also be seen in the spinal fluid. These cells can appear quite atypical- not unlike those of transformed or neoplastic lymphocytes.” http://www.ncbi.nlm.nih.gov/pubmed/2814170

We suffer permanent brain infections and no one cares. We are ignored, our pleas for help are interpreted as an annoyance to those we confide in. One thing we do have control over are our demands, and we should all be demanding the same thing. PROSECUTION OF THE CRIMINALS THAT ARE RESPONSIBLE FOR THIS GENOCIDE. It is murder. Awareness nor antibiotics have helped us. While we lay in our beds half dead there are others out there who are bed-less. Imagine the condemnation of homelessness with this disease.. A lot of us can’t afford to pay out of pocket. We need to keep that on the top of the priority list when it comes to what we ask for.

What we ask for should be nothing short of criminal prosecution. There’s our rope, let’s put it to good use.

TruthCures.org — Read the Charge Sheets and watch the free documentary on YouTube “Lyme Cryme”. Find us on Facebook, TruthCures page.