health (10)

The 5G that everyone fears is in the high, millimeter Wave (mmWave) band (above 20 GHz) and it is beam-formed. That type of 5G is only being deployed on certain streets in downtowns and surrounding residential neighborhoods in select cities. It is also being deployed in sports stadiums, arenas, airports, college campuses, metro stops and other places where large numbers of people congregate.

That mmWave 5G signal is on-demand, meaning it is only transmitted when a smart phone enabled with 5G for mmWave service asks for a connection. The mmWave 5G cell signal sent out by that antenna is only 10 degrees or so wide. If you live next door to a house where that 5G-enabled phone is calling for service and you don't have one of those 5G-enabled phones yourself, that signal to your neighbor's 5G-enabled phone will not come into your house.

It is important to realize that mmWave 5G service is only expected to be successful as primarily an outdoor service in select areas within urban areas. It is not considered by industry to be a "coverage spectrum", as is the case with 4G and 5G service in the low and mid bands (see below). 5G service in the mmWave band is more limited and does not work well indoors. Customers of mmWave service, particularly with Verizon, will have their data service seamlessly switched back and forth between 5G and 4G, because mmWave 5G service is still quite spotty...all four cell carriers (Verizon, T-Mobile, AT7T, Spring) with 5G service in the mmWave band are planning to expand their 5G service in each city that they currently serve and to add new cities.

You lose the mmWave 5G connection on a 5G-enabled phone when you move the phone around. When you move the phone, it connects back to 4G LTE service. 5G is primarily for downloading data, not voice service.

The bulk of 5G service in the US, on the other hand, is being broadcast in the low and mid bands (600 MHz to 6 GHz) from 5G small cell radios and antennas. These are being placed at existing 4G LTE macro cell sites, which are located roughly 1-1.5 miles apart, and in residential neighborhoods as stand alone small cell antennas across the country. T-Mobile and AT&T have 5G holdings in the low band and are in the process of installing low band 5G radios and transmitters, which do not send out beam-formed signals (but are highly modulated—see below) over large areas. T-Mobile plans to cover up to two-thirds of the U.S. population with their low band 5G service, and AT&T wants to provide low band 5G service, called "5G Evolution" or "5Ge" to all their customers nationwide by mid-2020.

Sprint's 5G holdings are exclusively in the mid band, at 2.5 GHz. They can use beam-formed signals, which, again, are only on-demand and narrow.

Existing 3G and 4G macro cell antennas transmit cell signals at up to 1,000 Watts. These macro cell antennas spray always-on RF signals out into a neighborhood in a cone that is roughly 120 degrees wide and high, stretching for miles. This is what we have had for a couple of decades. This 4G network is the foundation of 5G and will remain in place. New 4G macro antennas are being installed, and 5G antennas are being placed on existing 4G cell tower arrays. Existing 4G equipment at macro cell sites is also being upgraded.

Many more new small cell antennas are also being installed between macro cell sites on residential streets. These new 4G LTE-Advanced and 5G small cell radios and antennas broadcasting in the low and mid bands likewise send out RF signals that are always-on with a 120 degree-wide signal that passes deep into nearby houses and apartments.

These 4G and low and mid band 5G radios and antennas transmit signals that are lower power than macro cell sites, at 10 to 100+ Watts, but they are much closer to people's homes. As a result, we are now measuring higher RF levels in client's homes, especially in second story bedrooms, up to tens to hundreds of thousands of microWatts/meter squared (uW/m2) from these new antennas. The building biology profession and EMF experts around the world say 10 microWatts per meter squared or less is safe for sleeping areas (actually, 0.1 uW/m2 is our “No Anomaly” level for sleeping areas).

The real danger is that these 4G LTE-Advanced and low and mid band 5G cell signals are far more modulated than 3G and 4G signals were in the past. That means, more data is being sent into the same airspace at the same power density and frequency but at faster download speeds. 5G signals in the mmWave are also highly modulated. 

This modulation of 4G LTE-Advanced and 5G cell signals at all frequencies makes them more biologically active and potentially harmful for all biological life, including humans.

In addition to all that, your cell phone and the myriad wireless devices in your home and personal space emit RF signals close to you and your family that are also highly modulated. These devices include all the things people like to use these days, such as cell phones, tablets, WiFi-enabled routers, TV streaming devices, computers, printers, baby monitors, thermostats and many others. What people don't understand is that these signals are just as harmful to us as 4G and 5G cell signals coming in from outside, particularly because they are also now more modulated than in the past. WiFi is a heavily modulated signal, and therefore particularly harmful on a cellular level.

All RF signals are invisible, silent and odorless. You don't know they are there until you purchase an RF meter and measure them for yourself or hire an EMF professional to evaluate your home for EMFs. For most people, that is the only way they realize RF signals exist at high levels in their living and work space, and at schools.

We say, pay attention to wireless devices in your homes, offices and schools at the same time as you organize to oppose small cell antennas in your neighborhood.

Remember three strategies regarding the use of wireless devices: reduce use, increase distance, and favor hardwired connections whenever and wherever possible, such as when you are home.

Source: Create Healthy Homes

Additional Sources:
Former Cell Phone Company Boss Blows Whistle on 5G Coronavirus | BitChute: https://libertyinternational.wordpress.com/2021/04/23/former-cell-phone-company-boss-blows-whistle-on-5g-coronavirus-bitchute/ 

Electromagnetic Radiation Due to Cellular, Wi-Fi and Bluetooth Technologies: How Safe Are We? | Children’s Health Defense:  https://libertyinternational.wordpress.com/2020/04/07/electromagnetic-radiation-due-to-cellular-wi-fi-and-bluetooth-technologies-how-safe-are-we-childrens-health-defense/

Most countries already have limited access to 5G networks | Lifewire: https://libertyinternational.wordpress.com/2020/04/13/most-countries-already-have-limited-access-to-5g-networks-lifewire/

OOKLA 5G Map: https://libertyinternational.wordpress.com/2020/04/22/ookla-5g-map/

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By Thomas E. Levy, MD, JD

Canceling the Spike Protein: Striking Visual Evidence

Reprinted with permission: see archives and subscribe to the Orthomelcular.org newsletter

OMNS (Oct. 18, 2021) No issue in the history of medicine has been as strident and polarized as that of the risk/benefit profiles of the various COVID vaccines being administered around the world. This article does not seek to clarify this issue to the satisfaction of either the pro-vaccine or the anti-vaccine advocates. However, all parties should realize that some toxicity does result in some vaccinated individuals some of the time, and that such toxicity can sometimes be unequivocally attributed to the preceding administration of the vaccine. Whether this toxicity occurs often enough and with great enough severity in vaccinated persons to be of greater concern than dealing with the contraction and evolution of COVID infections remains the question for many people.

Practically speaking, it does not matter whether an adverse event that occurs after a vaccination gets “blamed” on the vaccination. Such a matter may never get resolved. The issue of greatest concern is whether that adverse event can be clinically resolved if not effectively prevented, and whether any long-term damage to the body can be prevented once an adverse event is recognized. The remainder of this article will address the etiologies of such damage along with measures that can mitigate or even resolve such damage.

Toxins and Oxidative Stress

All toxins ultimately inflict their damage by directly oxidizing biomolecules, or by indirectly resulting in the oxidation of those biomolecules (proteins, sugars, fats, enzymes, etc.). When biomolecules becomes oxidized (lose electrons) they can no longer perform their normal chemical or metabolic functions. No toxin can cause any clinical toxicity unless biomolecules end up becoming oxidized. The unique array of biomolecules that become oxidized determines the nature of the clinical condition resulting from a given toxin exposure. There is no “disease” present in a cell involved in a given medical condition beyond the distribution and degree of biomolecules that are oxidized. Rather than “causing” disease, the state of oxidation in a grouping of biomolecules IS the disease.

When antioxidants can donate electrons back to oxidized biomolecules (reduction), the normal function of these biomolecules is restored (Levy, 2019). This is the reason why sufficient antioxidant therapy, such as can be achieved by highly-dosed intravenous vitamin C, has proven to be so profoundly effective in blocking and even reversing the negative clinical impact of any toxin or poison. There exists no toxin against which vitamin C has been tested that has not been effectively neutralized (Levy, 2002). There is no better way to save a patient clinically poisoned by any agent than by immediately administering a sizeable intravenous infusion of sodium ascorbate. The addition of magnesium chloride to the infusion is also important to protect against sudden life-threatening arrhythmias that can occur before a sufficient number of the newly-oxidized biomolecules can be reduced and any remaining toxin is neutralized and excreted.

Abnormal Blood Clotting

Both the COVID vaccine and the COVID infection have been documented to provoke increased blood clotting [thrombosis] (Biswas et al., 2021; Lundstrom et al., 2021). Viral infections in general have been found to cause coagulopathies resulting in abnormal blood clotting (Subramaniam and Scharrer, 2018). Critically ill COVID ICU patients demonstrated elevated D-dimer levels roughly 60% of the time (Iba et al., 2020). An elevated D-dimer test result is almost an absolute confirmation of abnormal blood clotting taking place somewhere in the body. Such clots can be microscopic, at the capillary level, or much larger, even involving the thrombosis of large blood vessels. Higher D-dimer levels that persist in COVID patients appear to directly correlate with significantly increased morbidity and mortality (Naymagon et al., 2020; Paliogiannis et al., 2020; Rostami and Mansouritorghabeh, 2020).

Platelets, the elements of the blood that can get sticky and both initiate and help grow the size of blood clots, will generally demonstrate declining levels in the blood at the same time D-dimer levels are increasing, since their stores are being actively depleted. A post-vaccination syndrome known as vaccine-induced prothrombotic immune thrombocytopenia (VIPIT) with these very findings has been described (Favaloro, 2021; Iba et al., 2021; Scully et al., 2021; Thaler et al., 2021). Vaccinations have also been documented to cause bleeding syndromes due to autoimmune reactions resulting in low platelet levels (Perricone et al., 2014).

This can create some confusion clinically, as chronically low platelet levels by themselves can promote clinical syndromes of increased bleeding rather than increased blood clotting. As such, some primary low platelet disorders require pro-coagulation measures to stop bleeding, while other conditions featuring primary increased thrombosis with the secondary rapid consumption of platelet stores end up needing anticoagulation measures to stop that continued consumption of platelets (Perry et al., 2021). Significant thrombosis post-vaccination in the absence of an elevated D-dimer level or low platelet count has also been described (Carli et al., 2021). In platelets taken from COVID patients, platelet stickiness predisposing to thrombosis has been shown to result from spike protein binding to ACE2 receptors on the platelets (Zhang et al., 2021).

Of note, a D-dimer test that is elevated due to increased blood clotting will usually only stay elevated for a few days after the underlying pathology provoking the blood clotting has been resolved. Chronic, or “long-haul” COVID infections, often demonstrate persistent evidence of blood clotting pathology. In one study, 25% of convalescent COVID patients who were four months past their acute COVID infections demonstrated increased D-dimer levels. Interestingly, these D-dimer elevations were often present when the other common laboratory parameters of abnormal blood clotting had returned to normal. These other tests included prothrombin time, partial thromboplastin time, fibrinogen level, and platelet count. Inflammation parameters, including C-reactive protein and interleukin-6, typically also had returned to normal (Townsend et al., 2021).

Persistent evidence of blood clotting (increased D-dimer levels) in chronic COVID patients might be a reliable way to determine the persistent presence/production of the COVID spike protein. Another way, discussed below, might be dark field microscopy to look for rouleaux formation of the red blood cells (RBCs). At the time of the writing of this article, the correlation between an increased D-dimer level and rouleaux formation of the RBCs remains to be determined. Certainly, the presence of both should trigger the greatest of concern for the development of significant chronic COVID and post-COVID vaccination complications.

Is Persistent Spike Protein the Culprit?

Spike proteins are the spear-like appendages attached to and completely surrounding the central core of the COVID virus, giving the virion somewhat of a porcupine-like appearance. Upon binding to the angiotensin converting enzyme 2 (ACE2) receptors on the cell membranes of the target cells, dissolving enzymes are released that then permit entry of the complete COVID virus into the cytoplasm, where replication of the virus can ensue (Belouzard et al., 2012; Shang et al., 2020).

Concern has been raised regarding the dissemination of the spike protein throughout the body after vaccination. Rather than staying localized at the injection site in order to provoke the immune response and nothing more, spike protein presence has been detected throughout the body of some vaccinated individuals. Furthermore, it appears that some of the circulating spike proteins simply bind the ACE2 receptors without entering the cell, inducing an autoimmune response to the entire cell-spike protein entity. Depending on the cell type that binds the spike protein, any of a number of autoimmune medical conditions can result.

While the underlying pathology remains to be completely defined, one explanation for the problems with thrombotic tendencies and other symptomatology seen with chronic COVID and post-vaccination patients relates directly to the persistent presence of the spike protein part of the coronavirus. Some reports assert that the spike protein can continue to be produced after the initial binding to the ACE2 receptors and entry into some of the cells that it initially targets. The clinical pictures of chronic COVID and post-vaccine toxicity appear very similar, and both are likely due to this continued presence, and body-wide dissemination, of the spike protein (Mendelson et al., 2020; Aucott and Rebman, 2021; Levy, 2021; Raveendran, 2021).

Although they are found on many different types of cells throughout the body, the ACE2 receptors on the epithelial cells lining the airways are the first targets of the COVID virus upon initial encounter when inhaled (Hoffman et al., 2020). Furthermore, the concentration of these receptors is especially high on lung alveolar epithelial cells, further causing the lung tissue to be disproportionately targeted by the virus (Alifano et al., 2020). Unchecked, this avid receptor binding and subsequent viral replication inside the lung cells leads directly to low blood oxygen levels and the adult respiratory distress syndrome [ARDS] (Batah and Fabro, 2021). Eventually there is a surge of intracellular oxidation known as the cytokine storm, and death from respiratory failure results (Perrotta et al., 2020; Saponaro et al., 2020; Hu et al., 2021).

COVID, Vaccination, and Oxidative Stress

Although some people have prompt and clear-cut negative side effects after COVID vaccination, many appear to do well and feel completely fine after their vaccinations. Is this an assurance that no harm was done, or will be done, by the vaccine in such individuals? Some striking anecdotal evidence suggests otherwise, while also indicating that there exist good options for optimal protection against side effects in both the short- and long-term.

Under conditions of inflammation and systemically increased oxidative stress, RBCs can aggregate to varying degrees, sometimes sticking together like stacks of coins with branching of the stacks seen when the stickiness is maximal. This is known as rouleaux formation of the RBCs (Samsel and Perelson, 1984). When this rouleaux formation is pronounced, increased blood viscosity (thickness) is seen, and there is increased resistance to the normal, unimpeded flow of blood, especially in the microcirculation (Sevick and Jain, 1989; Kesmarky et al., 2008; Barshtein et al., 2020; Sloop et al., 2020).

With regard to the smallest capillaries through which the blood must pass, it needs to be noted that individual RBCs literally need to fold slightly to pass from the arterial to the venous side, as the capillary diameter at its narrowest point is actually less than the diameter of a normal RBC, or erythrocyte. It is clear that any aggregation of the RBCs, as is seen with rouleaux formation, will increase resistance to normal blood flow, and it will be more pronounced as the caliber of the blood vessel decreases. Not surprisingly, rouleaux formation of the RBCs is also associated with an impaired ability of the blood to optimally transport oxygen, which notably is another feature of COVID spike protein impact (Cicco and Pirrelli, 1999). Increased RBC aggregation has been observed in a number of different microcirculatory disorders, and it appears to be linked to the pathophysiology in these disorders.

Rouleaux formation is easily visualized directly with dark field microscopy. When available, feedback is immediate, and there is no need to wait for a laboratory to process a test specimen. It is a reliable indicator of abnormal RBC stickiness and increased blood viscosity, typically elevating the erythrocyte sedimentation test (ESR), an acute phase reactant test that consistently elevates along with C-reactive protein in a setting of generalized increased oxidative stress throughout the body (Lewi and Clarke, 1954; Ramsay and Lerman, 2015). As such, it can never be dismissed as an incidental and insignificant finding, especially in the setting of a symptom-free individual post-vaccination appearing to be normal and presumably free of body-wide increased inflammation and oxidative stress. States of advanced degrees of increased systemic oxidative stress, as is often seen in cancer patients, can also display rouleaux formation among circulating neoplastic cells and not just the RBCs (Cho, 2011).

Rouleaux Formation Post-COVID Vaccination

The dark field blood examinations seen below come from a 62-year-old female who had received the COVID vaccination roughly 60 days earlier. The first picture reveals mild rouleaux formation of the blood. After a sequence of six autohemotherapy ozone passes, the second picture shows a completely normal appearance of the RBCs.

v17n24-pic1a-300x244 Reversing mRNA Damage: Canceling the Spike Protein, Blood Clotting with Ozone Therapyv17n24-pic1b-300x234 Reversing mRNA Damage: Canceling the Spike Protein, Blood Clotting with Ozone Therapy

A second patient, a young adult male who received his vaccination 15 days earlier without any side effects noted and feeling completely well at the time, had the dark field examination of his blood performed. This first examination seen below revealed severe rouleaux formations of the RBCs with extensive branching, appearing to literally involve all of the RBCs visualized in an extensive review of multiple different microscopic fields. He then received one 400 ml ozonated saline infusion followed by a 15,000 mg infusion of vitamin C. The second picture reveals a complete and immediate resolution of the rouleaux formation seen on the first examination. Furthermore, the normal appearance of the RBCs was still seen 15 days later, giving some reassurance that the therapeutic infusions had some durability, and possibly permanency, in their positive impact.

v17n24-pic2a-300x232 Reversing mRNA Damage: Canceling the Spike Protein, Blood Clotting with Ozone Therapyv17n24-pic2b-300x265 Reversing mRNA Damage: Canceling the Spike Protein, Blood Clotting with Ozone Therapy

A third adult who received the vaccination 30 days earlier also had severe rouleaux formation on her dark field examination, and this was also completely resolved after the ozonated saline infusion followed by the vitamin C infusion. Of note, similar abnormal dark field microscopy findings were found in other individuals following Pfizer, Moderna, or Johnson & Johnson COVID vaccinations.

Preventing and Treating Chronic COVID and COVID Vaccine Complications

In addition to the mechanisms already discussed by which the spike protein can inflict damage, it appears the spike protein itself is significantly toxic. Such intrinsic toxicity (ability to cause the oxidation of biomolecules) combined with the apparent ability of the spike protein to replicate itself like a complete virus greatly increases the amount of toxic damage that can potentially be inflicted. A potent toxin is bad enough, but one that can replicate and increase its quantity inside the body after the initial encounter represents a unique challenge among toxins. And if the mechanism of replication can be sustained indefinitely, the long-term challenge to staying healthy can eventually become insurmountable. Nevertheless, this toxicity also allows it to be effectively targeted by high enough doses of the ultimate antitoxin, vitamin C, as discussed above. And even the continued production of spike protein can be neutralized by a daily multi-gram dosing of vitamin C, which is an excellent way to support optimal long-term health, anyway.

As was noted in an earlier article (Levy, 2021), there appear to be multiple ways to deal with spike protein effectively. The approaches to preventing and treating chronic COVID and COVID vaccine complications are similar, except that it would appear that a completely normal D-dimer blood test combined with a completely normal dark field examination of the blood could give the reassurance that the therapeutic goal has been achieved.

Until more data is accumulated on these approaches, it is probably advisable, if possible, to periodically reconfirm the normalcy of both the D-dimer blood test and the dark field blood examination to help assure that no new spike protein synthesis has resumed. This is particularly important since some patients who are clinically normal and symptom-free following COVID infection have been found to have the COVID virus persist in the fecal matter for an extended period of time (Chen et al., 2020; Patel et al., 2020; Zuo et al., 2020). Any significant immune challenge or new pathogen exposure facilitating a renewed surge of COVID virus replication could result in a return of COVID symptoms in such persons if the virus cannot be completely eliminated from the body.

Suggested Protocol (to be coordinated with the guidance of your chosen health care provider):

  1. For individuals who are post-vaccination or symptomatic with chronic COVID, vitamin C should be optimally dosed, and it should be kept at a high but lesser dose daily indefinitely.
    • Ideally, an initial intravenous administration of 25 to 75 grams of vitamin C should be given depending on body size. Although one infusion would likely resolve the symptoms and abnormal blood examination, several more infusions can be given if feasible over the next few days.
    • An option that would likely prove to be sufficient and would be much more readily available to larger numbers of patients would be one or more rounds of vitamin C given as a 7.5 gram IV push over roughly 10 minutes, avoiding the need for a complete intravenous infusion setup, a prolonged time in a clinic, and substantially greater expense (Riordan-Clinic-IVC-Push-Protocol, 10.16.14.pdf).
    • Additionally, or alternatively if IV is not available, 5 grams of liposome-encapsulated vitamin C (LivOn Labs) can be given daily for at least a week.
    • When none of the above three options are readily available, a comparable positive clinical impact will be seen with the proper supplementation of regular forms of oral vitamin C as sodium ascorbate or ascorbic acid. Either of these can be taken daily in three divided doses approaching bowel tolerance after the individual determines their own unique needs (additional information, see Levy, vitamin C Guide in References; Cathcart, 1981).
    • An excellent way to support any or all of the above measures for improving vitamin C levels in the body is now available and very beneficial clinically. A supplemental polyphenol that appears to help many to overcome the epigenetic defect preventing the internal synthesis of vitamin C in the liver can be taken once daily. This supplement also appears to provide the individual with the ability to produce and release even greater amounts of vitamin C directly into the blood in the face of infection and other sources of oxidative stress (www.formula216.com).
  2. Hydrogen peroxide (HP) nebulization (Levy, 2021, free eBook) is an antiviral and synergistic partner with vitamin C, and it is especially important in dealing with acute or chronic COVID, or with post-COVID vaccination issues. As noted above, the COVID virus can persist in the stool. In such cases, a chronic pathogen colonization (CPC) of COVID in the throat continually supplying virus that is swallowed into the gut is likely present as well, even when the patient seems to be clinically normal. This will commonly be the case when specific viral eradication measures were not taken during the clinical course of the COVID infection. HP nebulization will clear out this CPC, which will stop the continued seeding of the COVID virus in the gut and stool as well. Different nebulization approaches are discussed in the eBook.
  3. When available, ozonated saline and/or ozone autohemotherapy infusions are excellent. Conceivably, this approach alone might suffice to knock out the spike protein presence, but the vitamin C and HP nebulization approaches will also improve and maintain health in general. Ultraviolet blood irradiation and hyperbaric oxygen therapy will likely achieve the same therapeutic effect if available.
  4. Ivermectin, hydroxychloroquine, and chloroquine are especially important in preventing new binding of the spike protein to the ACE2 receptors that need to be bound in order for either the spike protein alone or for the entire virus to gain entry into the target cells (Lehrer and Rheinstein, 2020; Wang et al., 2020; Eweas et al., 2021). These agents also appear to have the ability to directly bind up any circulating spike protein before it binds any ACE2 receptors (Fantini et al., 2020; Sehailia and Chemat, 2020; Saha and Raihan, 2021). When the ACE2 receptors are already bound, the COVID virus cannot enter the cell (Pillay, 2020). These three agents also serve as ionophores that promote intracellular accumulation of zinc that is needed to kill/inactivate any intact virus particles that might still be present.
  5. Many other positive nutrients, vitamins, and minerals are supportive of defeating the spike protein, but they should not be used to the exclusion of the above, especially the combination of highly-dosed vitamin C and HP nebulization.

Summary

As the pandemic continues, there is an increasing number of chronic COVID patients and patients post-COVID vaccination with a number of different symptoms. Furthermore, there is increasing number of vaccinated individuals who still end up contracting a COVID infection. This is resulting in a substantial amount of morbidity and mortality around the world. The presence and persistence of the COVID spike protein, along with the chronic colonization of the COVID virus itself in the aerodigestive tract as well as in the lower gut, appear to be major reasons for illness in this group of patients.

Persistent elevation of D-dimer protein in the blood and the presence of rouleaux formation of the RBCs, especially when advanced in degree, appear to be reliable markers of persistent spike protein-related illness. The measures noted above, particular the vitamin C and HP nebulization, should result in the disappearance of the D-dimer in the blood while normalizing the appearance of the RBCs examined with dark field microscopy. Even though new research is taking place daily that may modify therapeutic recommendations, it appears that taking the measures to eliminate D-dimer from the blood and to maintain a consistently normal morphological appearance of the blood is a very practical and efficient way to curtail the ongoing morbidity and mortality secondary to the persistent spike protein presence seen in chronic COVID and in post-COVID vaccination patients.

There are many vaccinated individuals who feel well yet remain cautious about potential future side effects, and who really have no easy access to D-dimer testing or dark field examination of their blood. Such persons can follow a broad-spectrum supplementation regimen featuring vitamin C, magnesium chloride, vitamin D, zinc, and a good multivitamin/multimineral supplement free of iron, copper, and calcium. Periodic but regular HP nebulization should be included as well. This regimen will offer good spike protein protection while optimizing long-term health. Furthermore, such a long-term supplementation regimen is advisable regardless of how much of the protocol discussed above is followed.

(OMNS Contributing Editor Dr. Thomas E. Levy is board certified in internal medicine and cardiology. He is also an attorney, admitted to the bar in Colorado and in the District of Columbia. The views presented in this article are the author’s and not necessarily those of all members of the Orthomolecular Medicine News Service Editorial Review Board.)

Ozone treatment is also supported by other research groups and papers:

The paper titled, “Rationale for ozone-therapy as an adjuvant therapy in COVID-19: a narrative review” by Giovanni Tommaso Ranaldi , Emanuele Rocco Villani, * , Laura Franza.  (https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8086623/pdf/MGR-10-134.pdf).

The paper titled, “Potential Role of Oxygen–Ozone Therapy in Treatment of COVID-19 Pneumonia” by AE 1 Alberto Hernández F 2 Montserrat Viñals F 3 Tomas Isidoro E 3 Francisco Vilás.  (https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7476746/pdf/amjcaserep-21-e925849.pdf)

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Lehrer S, Rheinstein P (2020) Ivermectin docks to the SARS-CoV-2 spike receptor-binding domain attached to ACE 2. In Vivo 34:3023-3026. PMID: 32871846

Levy T Guide-to-Optimal-Admin-of-IVC-10-18-2021.pdf

Levy T (2002) Curing the Incurable. Vitamin C, Infectious Diseases, and Toxins Henderson, NV: MedFox Publishing

Levy T (2019) Magnesium, Reversing Disease Chapter 12, Henderson, NV: MedFox Publishing

Levy T (2021) Resolving “Long-Haul COVID” and vaccine toxicity: neutralizing the spike protein. Orthomolecular Medicine News Service, June 21, 2021. http://orthomolecular.org/resources/omns/v17n15.shtml

Levy T (2021) Rapid Virus Recovery: No need to live in fear! Henderson, NV: MedFox Publishing. Free eBook download (English or Spanish) available at https://rvr.medfoxpub.com/

Lewi S, Clarke K (1954) Rouleaux formation intensity and E.S.R. British Medical Journal 2:336-338. PMID: 13182211

Lundstrom K, Barh D, Uhal B et al. (2021) COVID-19 vaccines and thrombosis-roadblock or dead-end street? Biomolecules 11:1020. PMID: 34356644

Mendelson M, Nel J, Blumberg L et al. (2020) Long-COVID: an evolving problem with an extensive impact. South African Medical Journal 111:10-12. PMID: 33403997

Naymagon L, Zubizarreta N, Feld J et al. (2020) Admission D-dimer levels, D-dimer trends, and outcomes in COVID-19. Thrombosis Research 196:99-105. PMID: 32853982

Paliogiannis P, Mangoni A, Dettori P et al. (2020) D-dimer concentrations and COVID-19 severity: a systematic review and meta-analysis. Frontiers in Public Health 8:432. PMID: 32903841

Patel K, Patel P, Vunnam R et al. (2020) Gastrointestinal, hepatobiliary, and pancreatic manifestations of COVID-19. Journal of Clinical Virology 128:104386. PMID: 32388469

Perricone C, Ceccarelli F, Nesher G et al. (2014) Immune thrombocytopenic purpura (ITP) associated with vaccinations: a review of reported cases. Immunologic Research 60:226-235. PMID: 25427992

Perrotta F, Matera M, Cazzola M, Bianco A (2020) Severe respiratory SARS-CoV2 infection: does ACE2 receptor matter? Respiratory Medicine 168:105996. PMID: 32364961

Perry R, Tamborska A, Singh B et al. (2021) Cerebral venous thrombosis after vaccination against COVID-19 in the UK: a multicentre cohort study. Lancet Aug 6. Online ahead of print. PMID: 34370972

Pillay T (2020) Gene of the month: the 2019-nCoV/SARS-CoV-2 novel coronavirus spike protein. Journal of Clinical Pathology 73:366-369. PMID: 32376714

Ramsay E, Lerman M (2015) How to use the erythrocyte sedimentation rate in paediatrics. Archives of Disease in Childhood. Education and Practice Edition 100:30-36. PMID: 25205237

Raveendran A (2021) Long COVID-19: Challenges in the diagnosis and proposed diagnostic criteria. Diabetes & Metabolic Syndrome: Clinical Research & Reviews 15:145-146. PMID: 33341598

Rostami M, Mansouritorghabeh H (2020) D-dimer level in COVID-19 infection: a systematic review. Expert Review of Hematology 13:1265-1275. PMID: 32997543

Saha J, Raihan M (2021) The binding mechanism of ivermectin and levosalbutamol with spike protein of SARS-CoV-2. Structural Chemistry Apr 12. Online ahead of print. PMID: 33867777

Samsel R, Perelson A (1984) Kinetics of rouleau formation. II. Reversible reactions. Biophysical Journal 45:805-824. PMID: 6426540

Saponaro F, Rutigliano G, Sestito S et al. (2020) ACE 2 in the era of SARS-CoV-2: controversies and novel perspectives. Frontiers in Molecular Biosciences 7:588618. PMID: 33195436

Scully M, Singh D, Lown R et al. (2021) Pathologic antibodies to platelet factor 4 after ChAdOx1 nCoV-19 vaccination. The New England Journal of Medicine 384:2202-2211. PMID: 33861525

Sehailia M, Chemat S (2021) Antimalarial-agent artemisinin and derivatives portray more potent binding of Lys353 and Lys31-binding hotspots of SARS-CoV-2 spike protein than hydroxychloroquine: potential repurposing of artenimol for COVID-19. Journal of Biomolecular Structure & Dynamics 39:6184-6194. PMID: 32696720

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Shang J, Wan Y, Luo C et al. (2020) Cell entry mechanisms of SARS-CoV-2. Proceedings of the National Academy of Sciences of the United States of America 117:11727-11734. PMID: 32376634

Sloop G, De Mast Q, Pop G et al. (2020) The role of blood viscosity in infectious diseases. Cureus 12:e7090. PMID: 32226691

Subramaniam S, Scharrer I (2018) Procoagulant activity during viral infections. Frontiers in Bioscience 23:1060-1081. PMID: 28930589

Thaler J, Ay C, Gleixner K et al. (2021) Successful treatment of vaccine-induced prothrombotic immune thrombocytopenia (VIPIT). Journal of Thrombosis and Haemostasis 19:1819-1822. PMID: 33877735

Townsend L, Fogarty H, Dyer A et al. (2021) Prolonged elevation of D-dimer levels in convalescent COVID-19 patients is independent of the acute phase response. Journal of Thrombosis and Haemostasis 19:1064-1070. PMID: 33587810

Wang N, Han S, Liu R et al. (2020) Chloroquine and hydroxychloroquine as ACE2 blockers to inhibit viropexis of 2019-nCoV spike pseudotyped virus. Phytomedicine: International Journal of Phytotherapy and Phytopharmacology 79:153333. PMID: 32920291

Zhang S, Liu Y, Want X et al. (2021) SARS-Cov-2 binds platelet ACE2 to enhance thrombosis in COVID-19. Journal of Hematology & Oncology 13:120. PMID: 32887634

Zuo T, Zhang F, Lui G et al. (2020) Alterations in gut microbiota of patients with COVID-19 during time of hospitalization. Gastroenterology 159:944-955. PMID: 32442562

Source: Business Game Changers

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By Rick Cantrell, PhD, MD, PsyD

The below is absolutely 100% true and as a doctor I have been telling people this for 15 years now. No one wants to listen. Folks need to wake up. Cancer treatment is about making money. It is a 120 billion dollar a year industry in the United States alone and estimated to be a 600 billion dollar a year industry worldwide.

A successful cancer case according to the American Cancer Society and the American College of Oncology and Hematology means that the person survives for 5 years. Both the American Cancer Society and the American College of Oncology and Hematology admit that a person is likely to survive cancer for 7 to 10 years even if they do absolutely NOTHING. Of course, only the doctors get those magazines - not you, the cancer patient.

Alternative medicine's track record of curing cancer is 10 times higher than that of conventional medicine. Note that I say CURE.

Remember another thing. A TUMOR is just a symptom. It is not the cause of cancer.

Science is cause and effect. Remove the cause and the effect disappears.

I am in my third battle with cancer right now. I have not done any chemotherapy or radiation or surgery for any of my bouts with cancer. I survived leukemia, I survived Non Hodgkins Lymphoma and now I have Glioblastoma which is supposedly an incurable form of brain cancer. I was given two months to live 5 months ago.

I have been using Chinese herbs, high doses of vitamin C, acupuncture, chiropractic, homeopathy and nutritional changes. Yes, at first it got worse. It had metastasized to my lymph nodes, my lungs and my bones. As of this week, I am happy to say that there is no evidence now of any cancer in my lymph system or my bones. I had 6 tumors in my lungs, now there are only two. The tumors in my brain have shrunken tremendously. I never did any of their chemo, radiation or surgery.

Here is a very interesting statistic that you can only have access to by being a doctor. Every year more than 1,000 doctors oncologists (cancer doctors) are diagnosed with cancer. Less than 10% of them choose to do the treatment that they have been giving to their patients. Sort of like the fact that less than 25% of all pediatricians vaccinate their own children because of the fact that the risk of sudden death or serious side effects from the vaccination is higher than the risk of catching the disease one is being vaccinated for. This is not bullshit people - it is truth.

Medicine is about money, not about your health and the system traps people, especially the elderly, disabled and poor into a deadly treatment regime that puts them in an early grave. Meanwhile, all the jet set billionaires are flying off to Europe and paying big bucks for alternative treatments and getting cured.

Does alternative medicine work all the time? No. Of course not. Nothing works all the time. But there is a reason for that. You don't die until it's your time to die. Nothing can make you live longer than that time.

However quality of life comes into play. Those cancer patients who use alternative therapies for their cancer, yet still die from the illness, suffer a much higher quality of life. They die able to spend time with their families and even recognize their family members. They don't become emaciated like those who do chemotherapy or radiation do and rarely is a person who goes under the treatment of chemotherapy able to recognize anyone for the last few days of their lives. Their bodies become ravaged to the point that you can't even recognize them either. They suffer at a much much higher rate and they have one let down after another as doctors tell them, ahhh - it's looking good, only to tell them on the next visit it's looking worse, you need more chemo and radiation.

What is criminal about this is that YOUR DOCTORS KNOW THIS SHIT.

I took an oath as a physician. I have always followed it. That has certainly not made me successful financially as a doctor because I have consistently refused to go along with conventional medicine's bullshit.

- Rick Cantrell, PhD, MD, PsyD

Cancer Update from Rick Cantrell:

  1. \Every person has cancer cells in the body. These cancer cells do not show up in the standard tests until they have multiplied to a few billion. When doctors tell cancer patients that there are no more cancer cells in their bodies after treatment, it just means the tests are unable to detect the cancer cells because they have not reached the detectable size.
  2. Cancer cells occur between 6 to more than 10 times in a person's lifetime.
  3. When the person's immune system is strong the cancer cells will be destroyed and prevented from multiplying and forming tumors.
  4. When a person has cancer it indicates the person has nutritional deficiencies. These could be due to genetic, but also to environmental, food and lifestyle factors.
  5. To overcome the multiple nutritional deficiencies, changing diet to eat more adequately and healthy, 4-5 times/day and by including supplements will strengthen the immune system.
  6. Chemotherapy involves poisoning the rapidly-growing cancer cells and also destroys rapidly-growing healthy cells in the bone marrow, gastrointestinal tract etc, and can cause organ damage, like liver, kidneys, heart, lungs etc.
  7. Radiation while destroying cancer cells also burns, scars and damages healthy cells, tissues and organs.
  8. Initial treatment with chemotherapy and radiation will often reduce tumor size. However prolonged use of chemotherapy and radiation do not result in more tumor destruction.
  9. When the body has too much toxic burden from chemotherapy and radiation the immune system is either compromised or destroyed, hence the person can succumb to various kinds of infections and complications.
  10. Chemotherapy and radiation can cause cancer cells to mutate and become resistant and difficult to destroy. Surgery can also cause cancer cells to spread to other sites.
  11. An effective way to battle cancer is to starve the cancer cells by not feeding it with the foods it needs to multiply. CANCER CELLS FEED ON:
    > Sugar substitutes like NutraSweet, Equal, Spoonful, etc are made with Aspartame and it is harmful. A better natural substitute would be Manuka honey or molasses , but only in very small amounts. Table salt has a chemical added to make it white in color Better alternative is Bragg's aminos or sea salt.
    > Milk causes the body to produce mucus, especially in the gastro-intestinal tract. Cancer feeds on mucus. By cutting off milk and substituting with unsweetened soy milk cancer cells are being starved.
    > Cancer cells thrive in an acid environment. A meat-based diet is acidic and it is best to eat fish, and a little other meat, like chicken. Meat also contains livestock antibiotics, growth hormones and parasites, which are all harmful, especially to people with cancer.
    > A diet made of 80% fresh vegetables and juice, whole grains, seeds, nuts and a little fruits help put the body into an alkaline environment. About 20% can be from cooked food including beans. Fresh vegetable juices provide live enzymes that are easily absorbed and reach down to cellular levels within 15 minutes to nourish and enhance growth of healthy cells. To obtain live enzymes for building healthy cells try and drink fresh vegetable juice (most vegetables including bean sprouts) and eat some raw vegetables 2 or 3 times a day. Enzymes are destroyed at temperatures of 104 degrees F (40 degrees C)..
    > Avoid coffee, tea, and chocolate, which have high caffeine Green tea is a better alternative and has cancer fighting properties. Water-best to drink purified water, or filtered, to avoid known toxins and heavy metals in tap water. Distilled water is acidic, avoid it.
  12. Meat protein is difficult to digest and requires a lot of digestive enzymes. Undigested meat remaining in the intestines becomes putrefied and leads to more toxic buildup.
  13. Cancer cell walls have a tough protein covering. By refraining from or eating less meat it frees more enzymes to attack the protein walls of cancer cells and allows the body's killer cells to destroy the cancer cells.
  14. Some supplements build up the immune system (IP6, Flor-ssence, Essiac, anti-oxidants, vitamins, minerals, EFAs etc.) to enable the bodies own killer cells to destroy cancer cells.. Other supplements like vitamin E are known to cause apoptosis, or programmed cell death, the body's normal method of disposing of damaged, unwanted, or unneeded cells.
  15. Cancer is a disease of the mind, body, and spirit. A proactive and positive spirit will help the cancer warrior be a survivor. Anger, un-forgiveness and bitterness put the body into a stressful and acidic environment. Learn to have a loving and forgiving spirit. Learn to relax and enjoy life.
  16. Cancer cells cannot thrive in an oxygenated environment. Exercising daily, and deep breathing help  to get more oxygen down to the cellular level. Oxygen therapy is another means employed to destroy cancer cells.
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The-Boutenkos-288.jpg?width=288By Happy Oasis, Raw Spirit Community News

We were honored to enjoy an afternoon with Victoria Boutenko in Ashland's lovely Lithia Park this week. Victoria's authentic presence gladdens my heart, the way she looks into the soul of a person, fully listens and really sees. Victoria shared sumptuous cups of her papaya nettles smoothie. Just two ingredients, yet powerpacked with flavor and nutrition! We brought fresh-picked blackberries. Just one ingredient! :) Victoria also gifted us her four newest children's books, among her latest creations.

Victoria Boutenko's books for kids are precious, refreshing ways to joyfully introduce our little whippersnappers to the natural fun of enjoying raw greens and smoothies via playful paintings of hip animals eating greens. If you dare read them, be prepared to grin and giggle and to start your blender! Why believe me when you can have a look for yourself and purchase these essential, uplifting-while-edutaining reads at www.RawFamily.com?

The perennial researcher, Victoria, also relayed to us her current focus of enthusiasm: encouraging us Americans to read more of the classics. In contrast to best-sellers which may be more often about marketing hype than an author's genius, Victoria reminded me that reading classical literature with a deep mind, can ignite spiritual insights and more profound understandings. Yes, please.

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EarthImage.png?width=288By Happy Oasis, Raw Spirit Community News

Happy: What an unusual name, Hasher pronounced (Ah-sure) Eyanu?
Ashay :
My name is rooted in a Hebrew prayer of giving thanks when one comes upon an unexpected special blessing.
Happy:
Beautiful. What inspired you to create your first New Earth Festival coming up Sept 14 - 16th?
Ashay:
The intention is to plant a seed in the fabric of reality.
Happy:
Which seed?
Ashay:
The seed of consciously-cooperative culture. Many of us live a compulsively competitive lifestyle, engrained to compete and be highly individualistic. The New Earth Festival is an example of how we can live every day consciously cooperating and collaborating.
Happy:
So refreshing. This reminds me of the inspiration behind the Raw Spirit Festival as it leapt into being. Ashay, you are a promising (young) man of many talents - a raw chocolatier, a gardener of this juicy organic watermelon that I'm about to enjoy with friends among other fruits and organic vegetable people grown on your one-acre farm. I see that you also make reputedly wicked home brews, mostly herbs with minimal hops or alcohol, among many other creative offerings.
Ashay:
I am also a cranial sacral practitioner practicing in a private membership health group that inspired me to make the festival owned by private community members. Another project I recently created is this weekly CommunityShare market, where everyone who participates pays $1 to become a member every Saturday from 10 am to 2 pm here at the Stone House, in Nevada City, CA. In these days of ever greater restrictions, this kind of organization allows us more regulatory freedom with buying and selling produce, other goods and services. Happy, I'm looking forward to your "PlayShop For Blissologists" at The New Earth Fest!
www.NewEarthFest.info

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DrElizabethLambaer.png?width=288By Happy Oasis, Raw Spirit Community News

Happy:
Dr. Elizabeth, What's the bliss?
Dr. Elizabeth:
I'm completing my first book, Skinnydipping In The Fountain of Youth: Seven Keys to Eternal Radiance.
H:
What a fantastic title. I'm inspired to read it already. When will it be finished?
Dr. E:
It will be finished, as you love to say, in "PDT", Perfect Divine Timing.
H:
Dr. Elizabeth, you live up to your exuberant book title. I'm wondering why you are so dang energized and so incredibly beautiful? Have you ever fasted?
Dr. E:
Yes, after doing the first juice fast, it was as if I had plugged myself into a light socket. My cells get so excited to receive such food in this way.
H:
Which foods are you referring to that give you the greatest strength?
Dr. E: I've been on 100% living foods for years. Fruits and vegetables.
H:
Besides strength, joy, health and beauty, what else does dining on fruits and vegetables do for you?
Dr. E:
Living foods burst my pineal gland wide open. It helped me to remember my inherent intuition. I'm a second generation medical intuitive. I can now help guide people. My father is very third dimensional, rooted in religion, and a phenomenal diagnostic physician. Due to his keen perceptions, I asked him not so long ago if he uses a power greater than himself. "Do you use your intuition?", I asked. He answered, "I always get  a hunch."
H:
What else have you learned from your father?
Dr. E:
That if challenges arise with family members, we can remember to ask, "What is the gift in this relationship?"
H:
What are your healthiest habits?
Dr. E:
Being willing to be open to the possibility of saying "Yes" when I've previously been saying "No"; living from the heart, and dancing. I started dancing at age 40. I started interviewing people who have done extraordinary things. When I turned 50, I was told I would be a circuit speaker within 6 months. And I was! Part of my mission is to demonstrate that a woman can be more beautiful in her 50s than she ever has been in her life. There are a zillion expressions of beauty. The question is, is she in her joy? Any woman who is in her joy is absolutely radiant and also absolutely undeniable. I love boogie boarding and swimming in the ocean.  I love to see how much stronger I can be today than yesterday. I am going to dance rehearsal tonight with women who are half of my age. I love being on stage because I know that the Universe expresses its love and joy through me. It is about shifting our choices from fear to love. I rely on joy and also on service. If i can inspire and remind people to do whatever they love, that is delicious to me. We can all ask, "How much younger, stronger, kinder, deeper, more loving, more radiant, more beautiful can I express today?"
H:
Wow. Inspiring.
Dr. E:
It's so much fun realizing that we have the capacity to get better every day.
H:
What is your observation of what is happening in America these days and do you have any suggestions?
Dr. E: I am going to the place that is health and wellness. I am observing people committing to jobs they don't' love, and lives they don't love by watching tv, eating dead (cooked) foods, and consuming pharmaceuticals. I would love to see everyone opening up to what gift that each would love to give to the world. I suggest that each of us move forward with our heart, just doing what we love. If everyone chooses to live and lead with lovingkindness, compassion and joy, together we can create heaven on Earth.
HO:
I can hear the angels applauding.
Dr. E:
I was so inspired being part of the Wise Wild Women's Panel at Raw Spirit Fest this last New Year's in Phoenix, Arizona. Happy, let's have a Wise Wild Women's Panel soon on the Dr. Elizabeth show!
Contact: Speaker@DrElizabeth.com • Call: 310.383.8764 • Website: www.DrElizabeth.com

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10895903890?profile=originalEditor's Note: Given the rampant fear since the nuclear incident in Japan we though it important to provide access to a source of detoxified iodine for thyroid health and to alleviate any fear of radiation entering the body.

 

PRODUCT: Detoxified Iodine

 

IodineSource.com is your source for detoxified iodine. Our iodine is reduced to a 1% concentration in 100% ethyl alcohol and electro-magnetically transmuted (while being suspended in a wet bath containing a mild acid solution) into the Atomic state. From there it is bottled in 1/2 oz. (amber) dropper bottles and unless otherwise indicated, labeled and sealed with a full bottle heat shrink.

 

USAGE/DIRECTIONS:


Detoxified Iodine 1/2 oz: 4-6 week supply
Take 1 drop in 3 to 6 oz water or topically for the first day, increasing 1 drop each day for 5 days. Give yourself 2 days off and then repeat for five days. Follow this routine for three weeks. Then you can take 5 drops daily and work your way up slowly as long as there is no discomfort. Most people stabilize at 8 to 10 drops daily; some may need up to 12 to 15 drops. Once you have raised your levels, it may be okay to cut back a bit and it's okay to skip a day once in a while.

 

RECOMMENDED:


8 am to 12 noon on an empty stomach 30 minutes before or 1 hour after meals, medications and/or supplements. Taking it after 4 PM could raise your energy levels and leave you not being able to sleep at night.

 

INGREDIENTS:


1% Iodine Crystals in Ethyl Alcohol
(200 micrograms iodine per drop)

 

ORDER:


You can order a 1/2 oz bottle today for $25 (postpaid) at: www.iodinesource.com/Products.php

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10895904457?profile=originalHoping to sidestep these unpleasant effects, many people turn to natural remedies. Here are seven that may be effective for you. Read more...

  • Tai chi. The movements in Tai chi are slow and gentle, which makes the exercise perfect for arthritis patients. Early studies have found that Tai chi helped RA patients improve muscle function and stiffness, as well as reduce pain and stress levels. Numerous studies have agreed that exercise always helps, but Tai chi combines movement with focus, helping to not only improve joint function, but relax the body as a whole, which helps reduce pain.
  • Acupuncture. Several studies indicate that acupuncture is a good option for those with arthritis. One from China found that both traditional and electrical acupuncture reduced tenderness in patients with RA, and another from Germany found that acupuncture helped patients with OA to feel less pain and stiffness, and to enjoy improved joint function.
  • Magnets. A Harvard University study found that people with knee OA who wore a sleeve containing a high-powered magnet over the affected knee reported greater pain relief after four hours than those wearing a placebo knee sleeve. Other studies have been inconclusive. Magnets are said to work by stimulating the release of the body’s natural painkillers and increasing blood flow to the tissue. Many arthritis sufferers report that magnetic therapy is helpful. You can read more about it in the research reports of William Philpott, M.D., called “Magic of Magnetic Healing—The Real Magic Bullet.”
  • Ginger. Some studies have found evidence that ginger helps relieve arthritis pain. Japanese researchers note that red ginger (Zingiber officinale var. Rubra) is regularly used in Indonesian traditional medicine as a painkiller for arthritis. Other studies have found ginger to be comparable to non-steroidal anti-inflammatory drugs, as it also inhibits Cox 1 and Cox 2 enzymes related to pain. Ginger extract also helps inhibit inflammation, and has been found in studies to relieve muscle pain. Try fresh ginger on foods, ginger tea, and ginger supplements of 30-500 mg daily.
  • Sam-e. A naturally occurring chemical in the body, Sam-e has been found in many studies to treat pain, stiffness, and joint swelling, while improving mobility and rebuilding cartilage. Clinical studies have found the supplement to work as well as non-steroidal anti-inflammatory drugs (NSAIDs). A U.S. study found that it took longer to take effect, but when it did, it was as effective as Celebrex in reducing pain and improving joint function. Recommended doses are 400–1,200 mg per day—check with your doctor to avoid potentially dangerous interactions with other medications.
  • Omega-3 fatty acids. The Mayo Clinic states that foods rich in omega-3 fatty acids can help reduce RA pain and stiffness. A 2011 study found that omega-3 in fish oil could substantially and significantly reduce the signs and symptoms of OA, as well as slow the progression of the disease. An earlier study also indicated that omega-3s can improve symptoms of RA, helping patients to rely less on NSAID pain relievers. Recommended dose is about 2,000 mg of omega-3 supplement 3 times a day, or one tablespoon of flaxseed oil a day.
  • Capsaicin cream. Capsaicin is an active compound in hot peppers, and when applied topically, has shown to help relieve the pain of arthritis. A 1991 study found that capsaicin cream was a safe and effective treatment for arthritis, reducing pain for most participants. A more recent study found that applying 0.0125% concentration capsaicin-containing gel over the knee three times a day for four weeks gives more pain relief compared to a placebo. Those with sensitive skin, however, should try just a small amount first, as some patients reported burning and stinging at the application site.

Source: Renegade Health

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The Miracle of Ozone | Health Reporting

By Linda Cotrufello

THE OZONE STEAM SAUNA

Ozone, from the Greek, is a form of oxygen so important that the translation means, "The Breath of God." Medical grade ozone has many uses that are widely published on the internet. It has been used for over 50 years successfully in Germany for a variety of diseases, including Aids, cancer, hepatitis, genital herpes, chronic fatigue syndrome...the list goes on and on. A dear friend of mine has been fighting breast cancer for 7 months and was never told about ozone therapy due to suppression by our government. She is now heading for surgery, frustrated by diet and holistic methods. Wouldn't it be wonderful if people in need could access this incredible option? There are no practitioners that I am aware of in Ashland who administer ozone to the public.

With this sorry fact in mind, I have taken it upon myself to purchase a very powerful home unit in hopes of selling them and empowering others to use this modality. It emits 3500mg per hour of pure cold plasma ozone in conjunction with steam. The body is immersed in a sauna to the neck and ozone fed into the unit. I also recommend detox foot spa treatments to enhance the electrical signature of the body. These two powerful units are available from me at www.healthytransformation.com
Keep in mind I am not able to make medical claims but am giving information commonly available on the internet.

For more info please call me at 541-324-7971 or "google" medical grade ozone therapy.

WHAT DOES OZONE DO?
  • Inactivates viruses; oxidizes bacteria, yeast, fungi, parasites, protozoa, cancer cells
  • Stimulates the immune system, speeds healing
  • Cleans arteries and veins, improving circulation
  • Purifies the blood and the lymph
  • Oxidizes toxins, facilitating their excretion
  • Normalizes hormone and enzyme production
  • Reduces inflammation
  • Reduces pain, calms nerves
  • Prevents shock
  • Prevents stroke damage
  • Reduces cardiac arrhythmia
  • Improves brain function and memory
  • Scavenges free radicals
  • Chelates heavy metals, working well in conjunction with EDTA
  • Stimulates production of protective cell enzymes
HOW DOES OZONE WORK BIOCHEMICALLY?
  1. Inactivation of bacteria, viruses, fungi, yeast and protozoa: Ozone disrupts the integrity of the bacterial cell envelope through oxidation of the phospholipids and lipoproteins. In fungi, ozone inhibits cell growth at certain stages. With viruses, the ozone damages the viral capsid and upsets the reproductive cycle by disrupting the virus-to-cell contact with peroxidation. The weak enzyme coatings on cells which make them vulnerable to invasion by viruses make them susceptible to oxidation and elimination from the body, which then replaces them with healthy cells.
  2. Enhancement of circulation: In circulatory disease, a clumping of red blood cells hinders blood flow through the small capillaries and decreases oxygen absorption due to reduced surface area. Ozone reduces or eliminates clumping and red cell flexibility is restored, along with oxygen carrying ability. Oxygenation of the tissues increases as the arterial partial pressure increases and viscosity decreases. Ozone also oxidizes the plaque in arteries, allowing the removal of the breakdown products, unclogging the blood vessels.
  3. Stimulation of oxygen metabolism: Ozone causes an increase in the red blood cell glycolysis rate. This leads to the stimulation of 2,3-diphosphoglycerate (2,3-DPG) which leads to an increase in the amount of oxygen released to the tissues. Ozone activates the Krebs cycle by enhancing oxidative carboxylation of pyruvate, stimulating production of ATP. Ozone also causes an increase in the NADH reducing process and helps to oxidize cytochrome C. There is a stimulation of the production of the enzymes which act as free radical scavengers and cell wall protectors: glutathione peroxidase, glutathione reductase, catalase, and superoxide dismutase. Production of prostacyclin, a platelet aggregation inhibitor, and a vasodilator, is also induced by ozone.
  4. Formation of peroxides: Ozone reacts with the unsaturated fatty acids of the lipid layer in cellular membranes, forming hydro peroxides. There is a synergistic effect with cellular-formed H2O2. Lipid peroxidation products include alkoxyl and peroxyl radicals, singlet oxygen, ozonides, carbonides, carbonyls, alkanes and alkenes.
  5. Dissolution of malignant tumors: Ozone inhibits tumor metabolism. In addition, ozone oxidizes the outer lipid layer of malignant cells and destroys them through cell lysis (break-down). Phagocytes produce H2O2 and hydroxyl and ozone to kill bacteria and viruses. The generation of hydroxyl by killer cells is critical to their cytotoxic capability. Ozone stimulates conversion of arginine to citrulline, nitrite and nitrate by phagocytes, promoting their action on tumors. 6. Activation of the immune system: Ozone administered at a concentration of between 30 and 55 ug/cc causes the greatest increase in the production of interferon and the greatest output of tumor necrosis factor (TNF) and interleukin 2. The production of interleukin 2 launches an entire cascade of subsequent immunological reaction.
Here's another tidbit from the same site:

In 1933, the American Medical Association, headed up by Morris Fishbein, set out to eliminate all medical treatments that were competitive to drug therapy. The suppression of ozone therapy in the US began then, and continues to this day, except in ten US states, where doctors are protected by state laws. At the behest of the AMA, the FDA began seizing generators in the 1940s.

Source: Healthy Transformation
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Five months of intensive research, collating 670 research and news sources, are compacted in this succinct, readable and entertaining 167-page compendium about the “pandemic”. It provides a comprehensive overview for those with an open mind, still willing to learn, to expand perspectives far beyond media tidbits. This is the Dawning of the Corona Age. 

May we remove our masks - and blindfolds - to take notice of what is actually rapidly happening around us to navigate how we can still “live free in an unfree world”.

This newly released book is dedicated to you. Thank you for educating yourself, “thinking twice before you think”, calmly sharing your insights, acting wisely and thereby reclaiming authority over your life!

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