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Why I Won’t Take the Johnson & Johnson Vaccine — a Scientist’s Perspective

4/12/21

Ken Biegeleisen, M.D., Ph.D., explains why he believes Johnson & Johnson cannot guarantee its COVID vaccine won’t alter your genetic code.

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EDITOR’S NOTE: As The Defender reported this morning, U.S. health officials paused vaccinations with the Johnson & Johnson vaccine following multiple reports of people who developed blood clots after receiving the vaccine. Health officials said the pause is immediate but temporary. The article below was written before J&J vaccinations were paused.

Everyone is talking about DNA/RNA vaccines. Can they alter our own genetic codes?

The vaccine lobby says “Never!” I, however — laboring beneath the weight of a Ph.D. in virology — would instead quote Gilbert and Sullivan: “Well, hardly ever.”

Most people don’t know very much about DNA or RNA, so I’ll start with a 30-second chemistry discussion. DNA and RNA are both polymers, long strings (in this case, very long strings) composed of seemingly endless repetitions of a single basic chemical building block, called a nucleotide.

The resulting structure is often likened to a string of pearls, or to the rungs of a very, very long ladder. A single human cell contains some 6 billion nucleotide building blocks in its chromosomes.

In the picture below, the DNA basic building block is on the left, and the RNA building block is on the right. Take a look and see whether or not you can discern the difference:

DNA RNA Building Blocks

Don’t see much difference? That’s because there isn’t much. The red asterisk (*) shows the primary difference. RNA has an extra “O” (the abbreviation for an Oxygen atom). That’s about it.

Viruses have no lives of their own. They can grow only in host cells, such as, for example, your cells. In order for a virus to infect you, it needs to recognize a “receptor” on your cell surfaces. If — and only if — the virus can recognize such a receptor, then it has its own clever way of attaching itself to that receptor and sneaking its DNA (or RNA — viruses can have either one) into your cells.

Once inside, the DNA (or RNA) virus chromosome proceeds to reproduce itself, giving rise to hundreds or thousands of exact copies. These are then turned into complete virus particles by being covered with a protective protein coat. Next, the cell is broken open and the new progeny viruses disperse, infecting hundreds or thousands of other cells.

It’s easy to see how a viral infection can spread like wildfire in your body.

Even though the chemical differences between DNA and RNA are relatively small, the cell is smart enough to instantly recognize those small differences and act accordingly.

DNA is replicated in our cells by means of an enzyme called “DNA polymerase.” RNA, however, will not ordinarily be replicated by our cells because that’s simply not the way things work. So how does the RNA virus reproduce?

Some RNA viruses have an enzyme called “reverse transcriptase,” which begins each new viral life cycle by converting the virus’ RNA chromosome into DNA. This DNA copy can then be replicated by the cell’s own DNA polymerase-based system.

But other RNA viruses, including the COVID-19 strain of coronavirus, bring in their own special reproductive enzyme called “RNA polymerase,” which has the ability to directly produce numerous copies of the virus’ own RNA chromosome without any help from the cell’s native DNA polymerase system.

Now let’s speak for a moment about alteration of our genetic code. The interaction between a virus and the host cell is generally classified as being one of two distinct types of interaction.

Historically, the first type of interaction (discovered in the late 19th and early 20th centuries) was what we now call, in retrospect, a “productive infection.” Here the virus reproduces and kills the cell, releasing the many progeny as described above.

It was only in the later years of the 20th century that it became clear that there is a second sort of interaction, very different in nature, known as a “transforming” interaction (also called a “latent” infection). In a transforming interaction there is no virus growth at all. Instead, the single chromosome of the virus uses its bag of genetic tricks to insert itself into one of the 46 chromosomes of the host cell. There the viral DNA remains, sometimes forever.

In some species, such as herpesviruses, the virus’ chromosome just sits there, inside the host chromosome, apparently doing nothing — unless and until some sort of stimulus causes it to “pop out” again and begin growing. This produces a “cold sore” of the lips (herpesvirus type 1) or genitalia (herpesvirus type 2).

A large number of publications have documented that many — perhaps most — human beings have, within their nervous systems, cells which quietly harbor latent herpesvirus infections, even though the majority of humans will never get a cold sore. It is a known fact that herpes type I, in the latent state, resides in the trigeminal ganglion, inside the skull near the spinal cord. It is believed to be perfectly harmless in this latent state.

Other viruses, however, are not harmless in the latent state. A good example is SV-40, a DNA virus which is known to be capable of causing cancer in many mammalian species. SV-40 infects cells, but it usually doesn’t grow. Instead, it inserts its own chromosome into one of the cell’s chromosomes (a process called “integration”), and from that new base of operations it converts the cell from a normal cell, which is subject to normal forms of growth control, to a malignant cell which respects none of the host organism’s growth controls, and thereby causes cancer. This alteration, from normal to cancerous, is referred to as a “malignant transformation.”

But the term “transformation” does not automatically connote malignancy. Although a “transformation” may be harmful in any number of ways (and not solely limited to cancer), it might in other cases be entirely inconsequential (as far as the eye can see). In special cases, it might even be beneficial.

Curiously, however, even now — 68 years after the publication of the “Watson-Crick double-helix” structure for DNA — the dream of curing disease via human genetic re-engineering, employing custom-made viruses, remains in its infancy.

On the other hand, certain questionable forms of hastily-contrived human genetic experimentation, empowered by “executive orders,” and facilitated by “fast-track” bypassing of safety protocols, have become alarmingly commonplace.

Can a DNA-based vaccine ‘transform’ a human cell into something genetically different?

With all this in mind, we can now ask the question of whether or not a DNA-based vaccine might “transform” a human cell into something genetically different.

This is no small question, because if the answer is “yes,” and if the transformation proves to be harmful, then that harm may be passed to every subsequent generation — forever.

From 1972-1978, I was an M.D. – Ph.D. student at the New York University School of Medicine. Our lab addressed a question which was current at that time: In “productive infections,” where a virus replicates in cells and ultimately destroys them, might there nevertheless be integration of viral DNA into the host cell chromosomes?

We asked that question because, at that time in virological history, it had become abundantly clear that many different types of viruses could transform many different types of cells into malignant cancer cells. Those cells, if transplanted into animal hosts, would then form cancerous growths which would quickly kill the animal.

This sort of virus-mediated malignant transformation always began with the insertion (i.e., integration) of viral DNA into the chromosomes of the host cells. (Yes, I’m talking about that which the vaccine companies “assure” us will not follow vaccination with their “fast-tracked” new products).

Once these viral genes take up residence in host cell chromosomes, they are thereby empowered to seize control of the cell’s metabolism, perverting it to their own purposes.

So the question virologists were asking in the 1970s was this: Is the insertion of viral genes into host cell chromosomes a process uniquely associated with cancerous transformations? Or might the insertion of viral genes into host cell chromosomes take place in any and every sort of viral infection, whether it was a “productive” infection leading to virus multiplication and cell death, or whether it was a “transforming” infection where there was no virus multiplication at all?

We looked into this question by studying the infection of mammalian cells by herpesviruses. In the end, we published three papers, all in leading virology journals. These papers, listed below, are very difficult reading for anyone not familiar with the peculiar jargon of the field. But for those who are interested, here are the three references:

  1. Rush MJ & Biegeleisen K.  Association of Herpes simplex virus DNA with host chromosomal DNA during productive infection. Virology, 69:246-257 (1976).  https://doi.org/10.1016/0042-6822(76)90211-7.
  2. Rush MJ, Yanagi K & Biegeleisen K.  Further studies on the association of Herpes simplex virus DNA and host DNA during productive infection.  Virology, 83:221-225 (1977).  DOI:  10.1016/0042-6822(77)90227-6.
  3. Yanagi K; Rush MG; Biegeleisen K.  Integration of herpes simplex virus type 1 DNA into the DNA of growth-arrested BHK-21 cells. Journal Of General Virology, 44(3):657-667 (1979).  DOI: 10.1099/0022-1317-44-3-657.

The first paper proved that herpesvirus genes are integrated into host cell chromosomes, but left some important questions unanswered concerning the physico-chemical nature of the linkage between viral and host DNA.

By the third paper, however, all reasonable doubt about the integration of viral DNA into host chromosomes had been laid to rest.

Another line of investigation going on at about the same time, in the laboratory of W. Munyon, led to the same conclusion. Munyon and his associates studied an enzyme called “thymidine kinase.” What that enzyme does is extraneous to this discussion. What matters is that the gene for the enzyme is normally found in human chromosomes, and also in herpesvirus chromosomes.

Munyon and his team had a mutant strain of cells that lacked the thymidine kinase gene. They infected those cells with herpesvirus that had been irradiated, and thereby rendered incapable of multiplying in and killing the cells.

But the virus did, nevertheless, carry in its own thymidine kinase gene. Upon infection, the cells were shown to suddenly have acquired that enzyme, even though they were mutants who had none of their own. Because the virus had been irradiated, it did not kill the cells, which continued growing in the laboratory.

Eight months — which is hundreds of generations — later, the progeny of those cells were still producing thymidine kinase!

So if a DNA vaccine company alleges that their vaccine will cause my cells to temporarily manufacture corona spike protein, but will not permanently “transform” my cells in any other way, what am I to think?

Or, perhaps I’m not supposed to think?

So far we’ve talked only about herpesvirus. The new Johnson & Johnson vaccine uses “reproductively incompetent” genetically engineered adenovirus as the carrier for the corona spike protein gene.

Should we worry? After all, unexpected integration of viral genes may be peculiar only to herpesvirus, and not adenovirus, right?

Unfortunately, that’s not the case. What I did not realize, at the time I was doing my own Ph.D. research on herpesvirus, was that other labs were conducting the same type of research on the adenovirus. Here’s an example of that work:

Schick J, Baczko K, Fanning E, Groneberg J, Burgert H, & Doerfler W (1975).  Intracellular forms of adenovirus DNA: Integrated form of Adenovirus DNA appears early in productive infection.  Proc Nat Acad Sci USA, 73(4):1043-1047.  DOI: 10.1073/pnas.73.4.1043.  PMID: 1063388.  PMCID: PMC430196.

Like coronavirus, there are dozens of known adenovirus types, most of which are classified as “cold viruses.” But some adenoviruses cause much more serious disease, including cancer.

In the 1970s, the adenovirus researchers were asking the same questions that the herpesvirus workers were asking. And they were coming up with the same answers: In “productive infection,” where adenovirus was supposed to only replicate and destroy the cell, there was indeed extensive integration of viral genes into the host cell chromosomes — even though there was no obvious biological reason for the virus to do that.

No guarantees, despite what vaccine makers say

It seems that in many, perhaps most viral infections, integration of viral DNA into the host cells is a very real possibility. When this occurs, there is absolutely no way to “guarantee” that the genetic code of the host cell will not be re-written.

The question then arises: If this is the case, why do vaccine manufacturers “assure” us that their marginally tested products are genetically “safe?”

I would suggest three possible explanations, all equally reprehensible:

  1. It may be that the scientists in these companies simply do not know the history of this field. What can one say? “Those that fail to learn from history are doomed to repeat it.”
  2. It may be that anything in industry which does not improve the quarterly profit report is at great risk of being ignored.
  3. It may be that calling a new vaccine “safe,” in the pharmaceutical world, means little more than that the company has the legal resources to deal with any liability claims that arise.

Which of these three possible explanations is the correct one? Or is it all three?

In any event, you now know why I shall not take the Johnson & Johnson vaccine.

What about RNA vaccines?

We’ve been discussing DNA vaccines. What about RNA vaccines, such as Pfizer and Moderna?

Although I have no personal experience working in the lab on genetic transformation of human cells by RNA viruses, it is appropriate to comment briefly on that subject before closing.

The RNA vaccines are alleged by their promoters to be genetically “safe” because RNA cannot be directly incorporated into human chromosomes.

Is that true? Yes. But does that make them “safe?” Perhaps not.

What the vaccine companies forgot to tell you is that our cells have several types of “reverse transcriptase” of their own, which can potentially convert the vaccine RNA into DNA.

In December 2020, a team of researchers from Harvard and MIT (Zhang et al) posted an article at the Cold Spring Harbor Laboratory-hosted bioRxiv preprint server showing that, in all probability, incorporation of coronavirus spike protein genes, into the chromosomes of infected cells, does indeed take place, and is mediated by the so-called “LINE-1” type of human reverse transcriptase. (For more on the Harvard-MIT study and its implications, read this article previously published by The Defender).

To be clear, this was not a vaccine study, but a study in which cells were deliberately infected with whole, non-inactivated virus, as happens in nature, and which apparently can result in genetic transformation of the cells after all.

This, suggested the authors, may account for the now-frequent observation of COVID-19 test “positivity” in people who are clearly not sick. That is, the bodies of such people are continually manufacturing corona spike protein, from the viral genes which have been permanently incorporated into their genetic codes.

It could be said, in defense of the genetics-based-vaccine lobby, that since infection with whole, functional coronavirus clearly appears capable of transforming the human genetic code, causing our cells to forever manufacture the viral spike protein, there may therefore be some justification in mimicking this natural transformation via an unnatural RNA vaccine.

In condemnation of that lobby, however, we cannot overlook the obviously unwarranted assurances of vaccine manufacturers that alteration of our genetic code “will not happen.” Such a statement casts doubt on (a) their competence in their own field, and (b) their willingness to accept the consequences of their own actions.

Moreover, reverse transcription is a known means of normal human chromosome-to-chromosome gene mobility, a fascinating process whose study goes back to the pioneering workof Barbara McClintock in the 1930s. It has thus been well-known, for the better part of a century, that the effects of moving genes around will very much depend on where they are moved, and on exactly and precisely what is moved.

In the case of the current vaccine-borne corona spike protein gene, no one has any clue as to where in our genomes it will wind up, or what it will do when it gets there.

There is a corona vaccine, Novavax, which contains no genetic material at all (i.e., no DNA or RNA), but rather consists solely of the corona spike protein. Of all the available vaccines, this is the one least likely to cause human genetic harm. But almost no one gets it, because it’s not available in most countries. Why not?

There are also at least two corona vaccines (Sinopharm, Sinovac) which are made from whole inactivated virus, analogous to the polio vaccines of the 20th century. This is a tried and tested form of technology, but very few people get those vaccines either.

Instead, we’re all being pressured into taking hastily prepared genetic vaccines, which are likely to transform our heredity, permanently. Is there any reason for this, other than countless billions of dollars in windfall profits?

It is my view that the massive and barely studied global human genetic experiment going on right now is the biological equivalent of a drunk driver, speeding down the highway with impunity at 60 mph — at night without headlights — because he says that “he knows the road.”

Most sensible people are wary about “GMO,” even in food. Now we’re going to genetically modify ourselves? Why? What madness is this?

The views and opinions expressed in this article are those of the authors and do not necessarily reflect the views of Children’s Health Defense.

Ken Biegeleisen, M.D., Ph.D.'s avatar

Ken Biegeleisen, M.D., Ph.D. 

Ken Biegeleisen, M.D., Ph.D., has studied virology and is the author of multiple studies on virology and DNA/protein structure.

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For more: https://madisonarealymesupportgroup.com/2021/04/13/warning-for-jj-and-astrazeneca-shots-variants-lethality-greatly-exaggerated-military-unveils-implantable-microchip-mask-recall/

https://madisonarealymesupportgroup.com/2020/12/21/warning-3150-injuries-in-1st-week-of-covid-vaccines-among-american-healthcare-workers-pregnant-women-included/

https://www.sciencemag.org/news/2021/02/lizards-may-be-protecting-people-lyme-disease-southeastern-united-states

Lizards may be protecting people from Lyme disease in the southeastern United States

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Lyme disease is one of the most devastating tick-borne infections in the United States, affecting more than 300,000 people each year. It’s also one of the most mysterious: The creature that spreads it—the black-legged tick—lives throughout the country. Yet the northeastern United States is home to far more cases than anywhere else. Now, researchers have identified an unexpected reason: lizards.

Black-legged ticks (Ixodes scapularis), also known as deer ticks, carry corkscrew-shaped bacteria that cause Lyme disease. The ticks pick up the pathogens—spirochetes that belong to the genus Borrelia—when they suck the blood of animals like mice, deer, and lizards. In the next stage of their life cycle, the ticks may latch onto an unlucky human. But every host transmits the microbes differently. Reptiles are worse transmitters than mammals, so ticks that have lived on reptiles are less likely to make people sick.

The north-south divide in Lyme cases is a fairly sharp line right along the border of Virginia and North Carolina. Researchers have hypothesized that disparity in cases stems from ticks feeding on different hosts in the two regions. (See link for article)

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For more:  

https://www.sciencedirect.com/science/article/pii/S0365059620303093

Prevalence of infection by Bartonella spp. in patients with psoriasis

Under a Creative Commons license
open access
Dear Editor,

Psoriasis (Ps) is a chronic multisystem inflammatory disease that, in addition to the genetic factor, has other triggers such as emotional stress, nutritional deficit, endocrine problems, and infections. The activation of immune system cells is considered an important factor in the pathogenesis of Ps, and several infectious agents have been related to this activation. To modulate the immune response in patients with Ps, the systemic treatment of the disease may be based on immunosuppressive drugs, which facilitates the spread of opportunistic infections.1

Bacteria of the genus Bartonella are fastidious Gram-negative cocobacilli distributed worldwide (Fig. 1). Currently, the genus has 45 species and subspecies, of which at least 17 are capable of infecting humans. Most of these bacteria are transmitted by hematophagous arthropods, and some of their reservoirs are domestic animals, mainly dogs and cats. Although they have been neglected, the number of studies on Bartonella spp. is increasing, as well as the recognition of their importance. These agents have been linked to a wide spectrum of clinical manifestations, ranging from asymptomatic infection to life-threatening conditions, such as endocarditis.2

Figure 1

Figure 1. Transmission electronmicroscopy photomicrograph of a colony of Bartonella henselae (ATCC 49793) after 45 days of growth on blood-enriched agar: cocoid and electrondense bacteria with a tri-laminar wall, 50,000×.

There are no diagnostic tests with sufficiently high sensitivity and specificity. In addition, bartonellosis is not included in the diagnostic hypotheses by most physicians, which contributes to the underdiagnosis of these infections.2 This study aimed to assess the prevalence of Bartonella spp. infection through molecular and microbiological tests in Ps patients and a control group of volunteers.

The project was approved by the Institutional Research Council of the Universidade Estadual de Campinas (University of Campinas), under protocol CAAE: 48057415.5.0000.5404.

Blood samples were obtained from 30 Ps patients over 18 years of age, with mild to severe manifestations in different therapeutic regimens who agreed to participate in the study, as well as 30 volunteers – Unicamp students or employees over 18 years of age who denied clinical symptoms, were not pregnant, and agreed to participate in the study.

The samples were processed as summarized in Fig. 2. Liquid enrichment cultures and solid cultures were performed as previously described.3 From whole blood and culture samples, DNA was extracted using the QIAmp DNA Mini Kit (Qiagen®).

Figure 2

Figure 2. Flowchart of the procedures performed.

From the obtained DNA, genus-specific conventional PCRs (ITS region) and Bartonella henselae-specific PCRs were performed: double amplified PCR (nested) for the ftsZ region and real-time PCR for the gltA region. The quality of the extracted DNA and the absence of amplification inhibitors were tested using conventional PCR for the GAPDH gene.

B. henselae DNA was detected in 20% (6/30) of Ps patients and in 10% (3/30) of healthy volunteers who denied symptoms at the time of blood sample collection (Table 1). Using Fisher’s exact test, no statistical difference was observed between the two groups (p = 0.23).

Ps is a multifactorial, inflammatory, and immune-mediated disease. Although there is no consensus on the exact mechanisms of action in its pathogenesis, there is strong evidence that external factors, such as super antigens, have a great capacity to stimulate the inflammatory response of the disease.1 Microorganisms have been associated with Ps (including β-hemolytic streptococci, Staphylococcus aureus, Porphyromonas gingivalis, Candida albicans, Chlamydia psittaci, human immunodeficiency virus, and hepatitis C virus), but there is limited evidence that antimicrobial therapy has any direct benefit in crisis prevention. Ps is independently associated with a higher risk of serious infections, which is increased by the use of immunomodulatory treatments.1

Infection by Bartonella spp. was documented in 3.2% of 500 blood donors using a single conventional genus-specific PCR, from samples of liquid and solid culture.4

Bartonella spp. was detected in patients with Ps and psoriatic arthritis (PsA). One patient with Ps presented with cat-scratch disease during treatment with adalimumab, and another patient with PsA presented mesenteric lymphadenopathy and splenic abscesses. Symptomatic infection by Bartonella spp. was detected in other patients who were receiving treatment with immunobiologicals.5

One in five patients with Ps and one in ten healthy volunteers presented infection by B. henselae. Despite the lack of statistical difference when compared with the control group, this information is important when considering the high prevalence of infection in patients with Ps and even in the control group. Attention is needed for any patient who requires immunobiological treatment or other immunosuppressive drugs and who presents with possible expressions of infection by Bartonella spp., such as fever of undetermined origin, cryptogenic hepatitis, lymph node enlargement, endocarditis, sepsis, and graunlomatous or angioproliferative reactions. Further studies are needed to assess whether infection by Bartonella spp. may worsen Ps expression and the risks of this infection associated with immunosuppressive treatments.

https://vitalplan.com/blog/6-subtle-signs-you-need-to-detox-how-to-get-started?

By Vital Plan Posted 04-07-2021

Reviewed by Bill Rawls, MD
Medical Director of Vital Plan

As the country slowly emerges from the pandemic and hope is in the air, our bodies may not exactly be in top shape to take on the coming spring. Over the past year, many people coped with the stress and loneliness of the pandemic by relying heavily on sugary foods, carbs, alcohol, sedentary screen time, irregular sleeping, Netflix binging, you name it. Though these types of quarantine habits may have provided some short-term stress relief, they may have put your body’s detox systems under siege. Your body’s detox system could use some relief too before it leads to other problems.

“It’s usually not just one thing that inhibits your body’s ability to get rid of toxins, but rather a combination of several,” says Dr. Bill Rawls, medical director of Vital Plan. For example, stress, being sedentary, eating excess carbs, and other lifestyle factors common during the pandemic can compromise your microbiome and lead to leaky gut syndrome. This condition allows toxins and undesirable food components to cross into your bloodstream (aka leaky gut) instead of being eliminated, which in turn can overwhelm the immune system and cause systemic inflammation.

Not eating adequate fruits and veggies, drinking enough water, or exercising regularly, or simply being sick or having a compromised immune system — any of these can also slow down or clog your lymphatic system. This network of channels running throughout your body picks up toxins and cellular debris and brings them to lymph nodes, where they’re processed and disposed of. But when lymphatic fluid isn’t flowing or the system isn’t working as it should, toxins can build up and make trouble.

Your liver, kidneys, skin (via sweat), and other organs also play a role in regularly detoxifying your system. All of them are susceptible to the same unhealthy habits mentioned above. And when they get overloaded, detoxification slows, which can compromise your immune system, trigger inflammation, slow down circulation, or cause hormonal imbalances.

And so, many people coming out of the pandemic feeling run down (or worse) and resolving to hit the refresh button may turn to extreme programs that promise to jumpstart the body’s detoxing powers. Most of these plans last only a few weeks and focus primarily on food — or, more accurately, a lack thereof. (Ahem, juice fasts.)

But regardless of their popularity, short-term, highly restrictive detox diets or cleanses aren’t going to do much for you in the long term. One review in the Journal of Human Nutrition and Dietetics reports that there’s very little evidence that commercial detox diets are effective or even necessary. Some can even do damage. For instance, extreme detoxing can lead to nutritional deficiencies that impair immune function or dangerously-low blood sugar levels in people with diabetes.

That doesn’t mean you should check “detox” off your to-do list. Life happens, and despite your best efforts, you may not be doing enough to stop the inflow of toxins and/or encourage their disposal. How to know?

“It’s tricky,” says Dr. Rawls. You could feel okay, pretty good even, while your systems are actually struggling. “Your body will always try to compensate for whatever you’re doing or what it’s experiencing — it does what it has to do to keep you going,” Dr. Rawls says. “But it will get weighed down, and sooner or later, there’s a straw that breaks the camel’s back.” It could be a virus that should manifest as simple sniffles that flattens you for days, for example, or a minor gut microbiome imbalance that throws your GI system entirely out of whack.

The key to restoring healthy detox functions before it has significant ramifications is paying close attention to the subtle signals your body sends about your health. Any of the symptoms below should be a wake-up call that it’s time to take action.

1. Lasting Fatigue

Tired multiethnic businessman sleeping in office. Middle eastern business man with eyeglasses worked late and fell asleep on the computer keyboard. Creative casual man sleeping at his working place

Being tired after a few busy days or late nights is one thing, but consistently lacking the energy and motivation to do what you want is another. Sleep is the obvious first place to look. “If you need caffeine to get going every morning, you’re probably not getting enough sleep, or the sleep you’re getting isn’t high quality, restorative rest, ” says Dr. Rawls. “Either can make it harder for your body to detoxify.”

Lingering fatigue might also be a red flag that your detox systems are already worn down from an influx of chemicals from food (i.e., pesticides or artificial additives) or environmental toxins (i.e., cleaning solutions or air pollution), and your body is burning excess energy to try to keep up. Unfortunately for a lot of people, constant fatigue is just par for the course. “It’s the number one symptom people tend to put up with or ignore,” Dr. Rawls says.

2. Brain Fog

Closeup portrait of confused mature woman squinting to see more clearly, wearing and touching glasses, trying to read book, having difficulties seeing text because of vision problems, cheking diary

Occasionally forgetting names or important to-dos is common, especially when you’re stressed and your brain is overloaded with too much information. But brain fog is different.

“It feels like everyone around you is functioning at full speed and you’re in slow motion, wading through a fog,” Dr. Rawls says. “You miss things or don’t understand them clearly. Your mental functions seem slower, and as a result, you can only focus on what’s in front of you and what’s needed to survive.”

Too much sugar and a sluggish lymphatic system can trigger cloudy or slow brain function. Brain fog is also a common symptom of a leaky gut. That’s because when toxins and food proteins you may be sensitive to or intolerant of cross the gut-blood barrier, they can travel to places in the body they don’t belong — including the brain. “Accumulation of toxins slows neurological functions and allows microbes present in the brain to flourish,” Dr. Rawls says.

3. Digestive Problems

Senior woman having a huge stomach pain in bedroom at home

Your GI system plays a crucial role in disposing of toxins, so if it’s dealing with more than usual or isn’t able to get rid of them fast enough, its functions will be sluggish and irregular, Dr. Rawls says. Likewise, if unhealthy habits and toxins have messed with the balance of good bacteria in your gut, you’ll also experience digestive issues.

Watch for bloating, gas, or discomfort in your abdomen, as well as constipation, diarrhea, or both. Anything other than formed, regular stools and a calm tummy can mean your microbiome is struggling to maintain balance and that your system may not be effectively managing toxins or properly regulating your immune system, Dr. Rawls says.

4. Sugar Cravings

Guy eating sugar with spoon, surrounded by candy

Consuming too much sugar or simple carbohydrates (processed cereal, muffins, white bread) sends insulin and blood glucose on a roller coaster that, over time, can supercharge your sweet tooth so you crave more and more. Likewise, a sugar-heavy diet can actually change how your brain registers the sweet stuff, dulling its response and triggering cravings.

The problem, of course, is that all that excess sugar sets off a domino effect that leads to inflammation and disease, plus sugar feeds pathogenic bacteria in your gut and makes your liver work overtime to deal with the excess. Bottom line: If you’re craving sweets, things have already gotten to a critical point — time to detox.

5. Achy or Stiff Joints and Muscles

Unrecognizable senior man massaging his knee suffering from arthritis pain sitting on sofa indoor. Cropped, selective focus

Joint discomfort in your knees, hips, or elsewhere can be a sign of uncontrolled inflammation in the body. Swollen and stiff joints may also signal a sluggish lymphatic system.

Your body’s lymphatic fluid helps collect pathogens, toxins, and cellular waste from around your body and carries them to your lymph nodes, which break down and dispose of the “trash.” When it’s not working properly, lymphatic fluid doesn’t flow as easily and can build up, causing stiffness.

6. Any Other Unusual Symptoms

Portrait of sad mature woman sitting on couch at home and looking down and rubbing temples trying to calm herself, copy space

Pay attention to congestion, colds, or flu-like symptoms that persist beyond the normal time frame, frequent and unexplained headaches, skin problems such as breakouts, rashes, or puffiness, and anything else that seems odd about how you feel or how your body functions. Often, just feeling “off” is a sign that your systems may be overtaxed with toxins.

Get Started with These 5 Natural Ways to Detox

If you’ve decided you need to step up your detox game, remember to steer clear of extreme plans that promise fast and amazing results. If it sounds too good to be true, odds are it is.

Instead, try these simple tips to jumpstart healthy and detoxifying daily habits. They might seem small or insignificant, but if you make them a part of your everyday life, they’ll help support your body’s natural detoxification powers long-term and steal the appeal of over-the-top cleanses.

Try Detoxifying Herbs and Natural Remedies

Wooden bowl and spoon with chlorella pills on white textured background

Chlorella is at the top of the list, Dr. Rawls says. This freshwater green algae is rich in chlorophyll, a pigment with antioxidant properties that binds to toxins and helps usher them out of your system.

Aromatic bitters and bitter herbs are also a smart choice. They activate bitter receptors throughout your GI tract to aid digestion and support healthy blood glucose levels. Bitter herbs such as berberine, gentian, dandelion, and andrographis are also known to support healthy liver function, Dr. Rawls says.

Eat Fruits and Veggies More Than Anything Else

berries, fruits, and vegetables assortment on grey background

The high water content of fruits and vegetables helps flush out toxins, plus they contain antioxidants that tamp down inflammation. Produce is also packed with fiber, which feeds the good bacteria in your gut that helps strengthen the gut barrier and keep toxins from crossing the gut-blood barrier. Aim to load up at least half your plate with fruits and vegetables at every meal.

At the same time, be sure to limit grain-based carbohydrates and packaged foods. Instead, fill the second half of your plate with mostly whole sources of healthy fat and protein, like nuts, legumes, fish, and organic eggs.

Keep Hydrated

two glasses of ice water, filled with cucumber slices and mint

Adequate hydration helps lubricate your lymphatic system and flush out toxins. Sip filtered water throughout the day, or enjoy fruit-infused waters or decaffeinated herbal teas.

Keep Your Body Moving

Mature couple walking with their bike in a park

Exercise is one of the best detoxifying “medicines” for your body, Dr. Rawls says. It helps move along lymphatic fluid and the toxins it carries and strengthens your heart and vascular system. It’s also an effective way to diffuse stress, improve sleep, and sweat — long known as an efficient way to remove some toxins such as heavy metals from your body.

You don’t necessarily need to do intense workouts, although they won’t hurt (if you’re already accustomed to them). Start by simply going for a long, brisk walk every day, taking more activity breaks throughout the day, and trying gentle stretching practices such as yoga or qigong.

Step Up Your Sleep Hygiene

Cannabis oil surrounded by cannabis leaves.

Do all you can to set yourself up for a night of quality sleep and at least 8 hours of shuteye. That means shutting off electronics at least an hour before bedtime, keeping the room cool and dark, and getting on a consistent sleep schedule where you turn in and wake up at the same time each night and morning.

Herbal or natural sleep aids can help in the short term. Try full-spectrum CBD oil (aka cannabidiol), magnesium, tart cherry (a natural source of melatonin) or calming herbs like bacopa, passionflower and motherwort as you get back on track with natural detoxifying habits.

“Ultimately, detoxing shouldn’t be painful or restrictive, nor a punishment for past behavior,” reminds Dr. Rawls. Instead, consider these habits part of a healthy lifestyle that will promote health benefits so you feel your best this spring and beyond!

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References
1. Klein AV and Kiat, H. “Detox diets for toxin elimination and weight management: a critical review of the evidence.” Journal of Human Nutrition and Dietetics. 2015 Dec;28(6):675-86.

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For more:

https://www.medpagetoday.com/infectiousdisease/covid19/92062?xid=nl_covidupdate_2021-04-

CDC, FDA Warn on J&J Vax

The CDC and FDA confirm: six cases of cerebral venous sinus thrombosis with thrombocytopenia have occurred with the Johnson & Johnson COVID vaccine — the same condition connected to the AstraZeneca vaccine — and “we are recommending a pause in the use of this vaccine,” the agencies said early Tuesday in a joint statement. The CDC is calling an emergency meeting of its vaccines advisory committee on Wednesday to discuss the issue. Full story to come on MedPage Today. For more on adverse reactions and deaths.

https://time.com/5952976/astrazeneca-covid-vaccine-rare-clots/

European Regulators Find Possible Link Between AstraZeneca COVID-19 Vaccine and Rare Clotting Disorder

(LONDON) — The European Union’s drug agency said Wednesday that it found a “possible link” between the AstraZeneca coronavirus vaccine and a rare clotting disorder but recommended that vaccinations continue in adults, saying the benefits of the shot still outweigh risks.

https://www.thelancet.com/journals/laninf/article/PIIS1473-3099(21)00170-5/fulltext

Genomic characteristics and clinical effect of the emergent SARS-CoV-2 B.1.1.7 lineage in London, UK: a whole-genome sequencing and hospital-based cohort study

Excerpt:

Emerging evidence exists of increased transmissibility of B.1.1.7, and we found increased virus load by proxy for B.1.1.7 in our data. We did not identify an association of the variant with severe disease in this hospitalised cohort.

For more on this: https://madisonarealymesupportgroup.com/2021/04/05/covid-variants-much-ado-about-nothing/

https://healthimpactnews.com/2021/military-unveils-next-stage-of-covid-vaccines-on-60-minutes-implantable-microchips/

Military Unveils Next Stage of COVID Vaccines on 60 Minutes: Implantable Microchips

Video: DARPA Is Working On COVID Vaccine, Implantable Microchip To Detect Virus

by Steve Watson
Summit News

The Pentagon’s Defense Advanced Research Projects Agency (DARPA) is working on a COVID vaccine that will work on all variants and has developed an implantable microchip that it says will continuously monitor the human body for signs of the virus.

Retired Colonel Matt Hepburn, an army infectious disease physician heading up DARPA’s response to the pandemic, appeared on 60 Minutes to demonstrate the technology.

Holding up a vial of green tissue-like gel, which contains the chip, Hepburn proclaimed:

“You put it underneath your skin and what that tells you is that there are chemical reactions going on inside the body, and that signal means you are going to have symptoms tomorrow.”

“It’s like a ‘check engine’ light,” Hepburn added, noting that those with the chip “would get the signal, then self-administer a blood draw and test themselves on site.”

“We can have that information in three to five minutes,” Hepburn continued, adding “As you truncate that time, as you diagnose and treat, what you do is you stop the infection in its tracks.”

Watch:

Hepburn also declared that DARPA has developed a filter to remove the virus from the blood via a dialysis machine, and that the FDA has approved it, and it has already been used on 300 patients.

The 60 Minitues report also highlights how the pentagon has hundreds of tissue samples from soldiers and sailors infected with pathogens all over the world, including the 1918 Spanish Flu which killed millions globally.

Pentagon scientist Dr Kayvon Modjarrad also highlighted that the military is developing a one size fits all vaccine for COVID, commenting “This is not science fiction, this is science fact.”

“We have the tools, we have the technology, to do this all right now,” he said explaining that the goal is to inoculate people against potentially deadly viruses that have not even appeared yet.

“Killer viruses that we haven’t seen or even imagined, we’ll be protected against,” Modjarrad declared.

It was recently revealed that a third of active duty service members opted out of taking the COVID vaccine, with sources claiming the actual figure is probably closer to half.

The finding prompted the likes of TIME to declare that ‘vaccine hesitancy’ is threatening national security, and that while “These troops may not be co-opted by domestic terrorists, but they are clearly influenced by conspiracy theorists online and they just don’t trust basic science.”

The DARPA announcement of implantable microchip technology tied to the virus and a vaccine will likely only serve to enforce concerns the media continually describes as ‘conspiracy theories.’

Read the full article at Summit News.

https://beta.ctvnews.ca/local/montreal/2021/3/30/1_5369158.html  Video Here

Health Canada says a citizen complaint launched mask recall; other masks under investigation

March 30, 2021 

MONTREAL — An expert says much more needs to be known about a COVID-19 mask recalled last week before it’s clear whether it poses a danger to the thousands of Quebec workers who wore them.

Health Canada says these masks weren’t subject to strict regulation at first, but it’s now taking a much closer look—and it explained that a regular citizen raised the alarm.