Before reading the following article, read this first.  It’s crucial to understand that Gates and Farrar had their hands all over everything related to COVID – including but not limited to the research being done and the global messaging about it.

The BMJ writes about how the Wellcome Trust’s investments overlap with its research efforts.  At the very bottom of the page it also lists the competing interests and that the BMJ publishes work by research groups and academics funded by the Bill and Melinda Gates Foundation and the Wellcome Trust.

So there’s that……read on….

https://childrenshealthdefense.org/defender/the-bmj-public-health-commonwealth-fund-debate-mary-holland-rapid-response/?

The BMJ and Commonwealth Fund: All Hat, No Cattle?

On Jan. 29, The BMJ published an op-ed by Lucinda Hiam of the Commonwealth Fund: “Public health must bridge the divide with groups who mistrust science.” Using the online “Rapid Response” form provided by The BMJ, I replied to Ms. Hiam’s call to “bridge the divide.” I said I agreed and invited her to engage with CHD. We have received no response from her, and The BMJ has not published our response.

On Jan. 29, The BMJ published an op-ed by Lucinda Hiam of the Commonwealth Fund. The op-ed — “Public health must bridge the divide with groups who mistrust science” — specifically referenced Children’s Health Defense (CHD).

Using the online “Rapid Response” form provided by The BMJ, I replied to Ms. Hiam’s call to “bridge the divide.” I said I agreed and invited her to engage with CHD.

In my response, submitted Feb. 3, I wrote:

“Let’s have an adult conversation about science, vaccination, informed consent, vaccine injury, and civil rights. I invite Ms. Hiam to engage in a public dialogue on CHD’s public platform CHD.TV, or anywhere else, to debate these critical issues.”

Despite Ms. Hiam’s stated goal to “bridge the divide,” we have received no response from her, and The BMJ has not published our “Rapid Response” to her op-ed.

As a result, The BMJ and the Commonwealth Fund have only driven the divide deeper — by failing even to afford the courtesy of a reply.  (See link for article)

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**Comment**

And this is where ‘science’ stands…..in a vice-grip of investors who are running the show.

Those without an agenda are willing to debate those with differing opinions.  Remaining silent shows propaganda politics, not science.

Examples:

By contrast, U.S. Health Secretary Robert F. Kennedy Jr. has agreed for years to debate anyone on vaccines.

For more:

https://childrenshealthdefense.org/defender/jeffrey-epstein-bill-gates-financed-researchgate-control-scientific-discourse/

‘Muzzled and Muted’: Epstein, Gates Financed Research Portal to Control Scientific Discourse

In a series of posts on X, ScienceGuardians revealed that Jeffrey Epstein, Bill Gates and others linked to the Gates Foundation were instrumental in financing ResearchGate, an online scientific research portal. According to ScienceGuardians, the platform was actually developed “as a for-profit business to make big money from science” — with the intent to “control the flow of scientific ideas.”

epstein, gates and money

Jeffrey Epstein and Bill Gates sought to profit from — and exert influence over — scientific publishing and online discourse, according to information in the “Epstein Files” released last month by the U.S. Department of Justice…..

The summary listed ResearchGate, noting that Gates provided $10 million in funding to ResearchGate in 2013. This was part of a Gates-led funding round that attracted $35 million in investments to ResearchGate.

But according to ScienceGuardians, the platform was actually developed “as a for-profit business to make big money from science” — with the intent to “control the flow of scientific ideas” and exert influence over scientific discourse.  (See link for article)

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Important Excerpts:

Investors included Goldman Sachs and the Wellcome Trust, led by Jeremy Farrar, Ph.D., architect of key COVID-19 pandemic-era policies and now assistant director-general of the World Health Organization.

Gates and Epstein also helped secure partnerships with the publishers of major scientific journals, including Nature. Published by Springer Nature, it is widely considered one of the “giants” of medical and scientific publishing.

Other Springer publications include Politico, Springer Health, Nature, BioMedCentral, Scientific American and Nature Medicine — publisher of the infamous “Proximal Origin” paper in 2020, used to support the claim that SARS-CoV-2 had a natural origin.

Hopefully by now it’s clear why COVID messaging was so tyrannically one-sided.  Voices were simply drowned out.  This article shares how sensitive government information has been shared with Epstein.  The Biden administration and corporate media used the “Disinformation Dozen” list to discredit figures like Robert F. Kennedy Jr. and Sayer Ji. Social media platforms deplatformed those included on the list.

According to Ji, the same dark-money infrastructure they used to destroy political opponents were redeployed the identical playbook against U.S.-based health publishers and independent media.”

Internal documents leaked in 2024 showed that CCDH sought to launch “Black Ops” against Kennedy and “kill Musk’s Twitter” — now known as X. “Black ops” refers to secret operations carried out by governments or other organizations that hide their involvement.

Never trust these agencies again.  Ever.  Remain vigilant and do your own research. Whatever the CDC/FDA/NIH are peddling – do the exact opposite!

For more:

During Covid-19, one member of this small group of unaccountable actors, British medical researcher who was previously the director of the Wellcome Trust, Jeremy Farrar, has been given almost absolute power over designing the WHO’s global response to the pandemic.

“There is no peacetime any more…Preparedness and readiness is a constant and needs to be part of the fabric of society… My preference would be to streamline the architecture of global health with the WHO in the middle of the web, convening, advising, guiding and providing an emergency response… Crumbs from the table will not cut it in the era of pandemics.” ~ Jeremy Farrar (2021)  [4]

 

 

https://www.independent.co.uk/life-style/health-and-families/features/lyme-disease-symptoms-bella-hadid-justin-timberlake-

‘Lyme disease ruined my life – I was misdiagnosed with hypochondria and depression for over 20 years’

Frédéric Roscop, 49, contracted Lyme disease aged five years old but wasn’t diagnosed with it until his mid-thirties. He tells Charlotte Cripps about his lifelong battle with the disease, along with co-infections and associated mental health challenges, and how he found his way to a normal life

As a child, I was raised in the French countryside in the Dordogne. From around the age of five, I’d help local farmers by collecting eggs and herding cows in the fields. I was also naturally curious and adventurous and would go exploring in the bushes. I’d often end up covered in ticks and an old lady at the farm would put me in an iron bath and brush them off me. This is not the right way of removing them, which is to pull them out of the skin, as soon as possible, to prevent the transmission of disease. It should often befollowed by a course of antibiotics.

The next day, I’d be covered in bruising and red marks, which we now call a “bullmark”, or the “bulls-eye” rash, medically known as Erythema migrans, a hallmark symptom of Lyme disease. My mum was always horrified and took me to the doctor, who thought it was an allergic reaction to a bite and prescribed me an antihistamine. But due to a lack of awareness years ago, nobody ever mentioned Lyme disease.

Looking back, I suffered years of mild symptoms. I had a delayed puberty because my body was not functioning properly; weight gain due to factors known to be caused by Lyme disease, such as gastrointestinal issues and hormonal imbalances; and I craved sugar because my body was stressed.

As much as I was exhausted, I was also hyper – Lyme disease can cause symptoms that mimic or contribute to ADHD – and I was also hyper-sensitive. I couldn’t switch off. By the age of eight, I was already seeing a psychotherapist who recommended more exercise to exhaust me.  (See link for article)

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**Comment**

A very dismissive article & video on Lyme disease appeared recently dissing celebrities who have the courage to share their battle with it.  Yet, because of these celebrities speaking out, more have become aware of Lyme/MSIDS.

You know it’s bad when you have to learn about a severe medical condition from a celebrity.  But, there it is…..  The truth is, it’s easier to get medical assisted death than treatment for chronic Lyme disease, which is what the man in this article had.

Whenever I see articles on how ‘things are getting better’ in Lymeland, I remember that probably every day someone just like the man in this article is being misdiagnosed and sent on a wild goose chase – maybe for years. 

No, my friends – it ain’t getting better.  Not by a long shot.  To date, the best chance a patient has is to bump into someone who will educate them about this, OR read an article about a celebrity who shares their story.

And this is where we’ve been for a long, long time.

For more:

The stories are endless and continue.  These stories touch people and like it or not, are for some the only way they will learn about this dreadful illness.  The medical and research establishments haven’t helped one iota.

I’ve always said, and I stand by it, the only way this needle is going to move is when enough people are infected with it.

More on the ‘virus,’ ‘no virus,’ debate…..

https://jonfleetwood.substack.com/p/niaid-funded-scientists-tried-to?

NIAID-Funded Scientists Tried to Make Influenza Spread—They Couldn’t Despite 80+ Hours of Close Human Exposure: Journal ‘PLOS Pathogens’

Researchers engineered real-world transmission conditions using infected volunteers and sealed indoor exposure sessions, but no secondary infections were detected.

A new peer-reviewed study reports that researchers were unable to produce a single confirmed case of influenza transmission in a controlled human exposure experiment, despite prolonged close contact between infected individuals and healthy volunteers.

The study, published last month in PLOS Pathogens, tested whether naturally infected people could transmit influenza to others under tightly controlled indoor conditions designed to facilitate spread.

Transmission did not occur.

“[N]o transmission was observed in this study,” the authors confirm.

Researchers recruited individuals with confirmed influenza infection and placed them in repeated exposure sessions with healthy participants inside a sealed hotel-based quarantine environment.

Volunteers interacted face-to-face, shared objects, and spent hours together in a room with intentionally low ventilation—conditions chosen to support transmission.

Even under these circumstances, no recipient developed influenza-like illness, tested PCR-positive, or showed serological evidence of infection.  (See link for article)

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**Comment**

Even the most hardened skeptic must scratch his head on this one.

Authors give possible reasons for the unexpected outcome:

  • the sick weren’t coughing enough
  • people had immune protection
  • airflow quickly diluted exhaled breath, reducing exposure

Fleetwood points out the exact same thing was found with COVID challenge studies. In other words, exposed volunteers failed to produce sustained infections.

This experiment has been repeated numerous times now showing the same result: nadda.  Going all the way back to the 1918 influenza pandemic, an experiment was conducted on 62 prisoners:

injected with infected lung tissue from sick or deceased patients, have infected tissue dropped in their eyes, and sprayed in the nose and mouth with infectious aerosols. Others would see mucus taken from critically ill patients and put it into the noses and throats of prisoners. In other parts of the trials, experimenters would take the blood of the sick and inject it into the healthy, to see if it was spread through infectious microorganisms in the blood.

Not one got ill or died.

What nobody is saying here is that viruses don’t exist.  But, there is a camp that asserts just that.  Go here for the history of this camp.  I would say these challenge studies don’t help the virus camp.

One thing is sure: exposure alone is not enough to make someone sick.

Which makes you wonder about the purpose of this……

https://jonfleetwood.substack.com/p/niaid-funded-scientists-engineer?

NIAID-Funded Scientists Engineer Mutant Influenza Virus and ‘Expand its Host Range’: Journal ‘Nature Communications’

Gain-of-function flu pathogen acquires new cell entry function, expands infection capability.

Scientists funded by the National Institute of Allergy and Infectious Diseases (NIAID) engineered influenza viruses and introduced mutations that expanded the virus’s host range—an outcome that the National Institutes of Health (NIH) itself formally defines as gain-of-function research under a 2025 Executive Order implementation notice.

The study, published in Nature Communicationslast week, confirms the work was funded through a NIAID influenza research center.

The authors state:

“Funding was also provided, in part, by … CRIPT (Center for Research on Influenza Pathogenesis and Transmission), a National Institute of Allergy and Infectious Diseases (NIAID) funded Center for Influenza Research and Response (CEIRR, contract 75N93021C00014…).”

The CEIRR network is one of NIAID’s primary federally funded influenza research programs.

The current Director of NIAID—allowing such risky influenza lab engineering—is Dr. Jeffery Taubenberger, who holds a patent on the technology behind the Trump administration’s $500 million influenza vaccine platform.

The same federal agency funding the creation of mutated influenza viruses is led by the man who helped invent—and could profit from—the vaccine meant to fight them.

Moreover, the study comes as Congress and President Donald Trump have enacted a new law allocating more than $5.5 billion in taxpayer funding for pandemic preparedness, with influenza—the same pathogen engineered in these experiments—named as the only virus explicitly identified in the statute.

Funding for the experiment also came from the U.S. Department of Agriculture (USDA).

(See link for article)

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**Comment**

According to attorney Tom Renz, the scuttle that dangerous ‘gain of function’ research was recently banned due to an Executive Order, is false.  Rather, it’s codified and allowed under new regulation.  It’s all good if you are compliant with current regulation.

“Gain of Function” has now been legitimized and sanctioned.  Far from being banned.

The ‘no virus’ camp rolls their eyes at all of this because according to them, none of this exists.

Something exists and something is making people sicker than dogs. How about we find out what is causing these illnesses killing people and STOP funding research making pathogens deadlier?

For more:

Regarding Wisconsin:

 

 

https://www.globallymealliance.org/blog/understanding-alpha-gal-syndrome-and-its-growing-geographic-overlap-with-lyme-disease?

Learn about alpha-gal syndrome, a tickborne allergy to red meat, its causes, symptoms, testing, and relation to Lyme disease- as well as prevention tips and current research insights.

The Basics 

Alpha-gal syndrome is a more recently identified (c. 2009) tickborne disease. It differs from Lyme disease, babesiosis, anaplasmosis and ehrlichiosis in that it is not a tickborne infection – it is a tickborne allergy. Alpha-gal syndrome is an allergy to red meat and other products containing alpha-gal, including dairy and gelatin for those with more sensitive allergy.

Alpha-gal syndrome’s best recognized cause is tick bites, and it has been described on 6 continents, with the culprit tick species varying across the globe. Lone star tick (Amblyomma americanum) bites are the primary cause of alpha-gal syndrome in the United States. Recently, rare cases linked to blacklegged and western blacklegged ticks (Ixodes scapularis and I. pacificus) have been reported in Maine, Washington state, and the upper Midwest, well outside of the lone star tick range (Thompson et al. 2023). Despite this early evidence that blacklegged ticks and western blacklegged ticks can cause alpha-gal syndrome, they are thought to be an uncommon cause given how few cases have been recognized in high-incidence Lyme regions, particularly of the northeastern United States.

The Timeline: tick bite to food allergy

It is not intuitive to connect how a tick bite can cause food allergy.

To begin with, a typical timeline of the development of allergy is as follows: a tick of a culprit species bites a human. (It is not yet known why some bites do and others do not cause alpha-gal syndrome.) Sometimes the tick bite that preceded new allergy is described as leaving an erythematous, inflamed, and itchy “bite site” lasting weeks. Many tick bites go unnoticed.

Weeks to months after the tick bite, a person who previously ate meat without incident has a meal containing red meat, such as a steak. However, they do not react right away. The allergic symptoms – which can include a combination of hives, facial and throat swelling, wheezing and difficulty breathing, vomiting and other gastrointestinal distress, and anaphylaxis – occur 2-6 hours after eating red meat.

The “classic” story of an initial reaction is someone who eats red meat for dinner, and then wakes up itching in the middle of the night, looks in the mirror, and is surprised to see hives and sometimes facial swelling. There are also less classic clinical presentations, such as people with isolated gastrointestinal distress who eat red meat frequently and may have a hard time connecting the two. Vegetarians and vegans who consume or are exposed to mammalian products may also manifest symptoms of alpha-gal syndrome. Tragically, the first case report of a death from alpha-gal syndrome has been recorded (Platts-Mills 2025).

The alpha-gal molecule and delayed reaction

Alpha-gal syndrome is an allergy to alpha-gal, which is a carbohydrate molecule. (Most food allergies are to proteins.) Human ancestors lost the ability synthesize alpha-gal tens of millions of years ago, but most mammals other than humans – including those that humans eat – do produce alpha-gal. Therefore, “red meat” – or meat from cows, pigs, sheep, deer, and other game – contains alpha-gal. (Fish and birds do not produce alpha-gal.) The alpha-gal carbohydrate in meat is attached to both fats and proteins. The fatty form, glycolipids, take time to be metabolized and enter the bloodstream. That’s why allergic symptoms often appear 2–6 hours after eating, rather than immediately.

In addition to mammals, ticks also have alpha-gal in their saliva, without ever biting a mammal. Why? One compelling explanation is molecular mimicry. Ticks have many ways of trying to disguise their bite to avoid being detected, so expressing alpha-gal may be one additional way to look like their hosts (deer, mice, and other mammals whose cells express alpha-gal). Of tick species in the United States, lone star ticks, blacklegged ticks, brown dog ticks (Rhipicephalus sanguineus) and the invasive Asian longhorned tick (Haemaphysalis longicornis) have been shown to have alpha-gal in their saliva.

Testing for alpha-gal syndrome

Only if you have allergic symptoms, or unexplained gastrointestinal symptoms, should you be tested for alpha-gal syndrome. The test for alpha-gal syndrome is a serum test for alpha-gal IgE. IgE is a type of antibody that the immune system produces in response to allergens. A positive does not necessarily mean you have the allergy. Instead, it shows that your body has made IgE antibodies against alpha-gal, a state called being “sensitized” to an allergen, in allergy terminology.

A high percentage of adult populations screened for alpha-gal IgE in areas with lone star ticks are sensitized to alpha-gal, in the realm of 20-30% and even higher in heavily tick-exposed populations such as forestry and outdoor workers. However, most sensitized individuals in groups that have been screened are “sensitized only” and do not report allergy symptoms.

Alpha-gal syndrome and Lyme disease

There is no established connection between alpha-gal syndrome and Lyme disease in the United States. That’s partly because lone star ticks are the primary cause of alpha-gal syndrome whereas blacklegged ticks transmit the Lyme bacteria. It is important to note that western Europe is different: there, a single tick species—Ixodes ricinus—can both trigger alpha-gal syndrome and transmit Lyme bacteria. Even there, however, being bitten by one of these ticks doesn’t mean a person will develop both conditions. A Swedish study (Tjernberg et al. 2017) found no link between Lyme disease history and having alpha-gal antibodies.

[Ixodes ricinus is commonly known as the castor bean tick or the sheep tick]

Considerations for Lyme-endemic regions of the United States

It is important to recognize that the lone star tick range is expanding, particularly northward and eastward, and prominently along the northeastern coastline. Lone star ticks are now well-established in eastern Long Island, where there are also blacklegged ticks and Lyme disease. Lone star ticks are also increasingly found on Martha’s Vineyard. They are considered an aggressive human-biting tick. Deer are an important host for lone star ticks, whereas white-footed mice (Peromyscus leucopus) are not.  EPA-registered insect repellents such as DEET and picaridin for skin and clothing and permethrin for clothing and gear remain important for lone star tick bite prevention, as for blacklegged and other tick bites. An important distinction from Lyme disease is that alpha-gal syndrome can likely be caused by a tick attached for as little as a few hours. The metric of removing a tick within 24 hours, while good advice for Lyme disease, should therefore not be considered protective for alpha-gal syndrome.

Tick bite avoidance

Not only is avoiding tick bites important to avoid developing alpha-gal syndrome, but it remains important for those who have the allergy. Over time (years), some patients with alpha-gal syndrome who avoid tick bites have declining alpha-gal IgE levels that correspond to a remission of their allergy and the ability to reintroduce red meat into their diets. Reintroducing red meat is a very individualized decision to be made with a knowledgeable healthcare provider and incorporating safety considerations. If a patient returns to eating red meat, new tick bites could cause allergic symptoms to return.

Current unknowns and research questions

Much of what is currently understood about alpha-gal syndrome, outlined above, comes from excellent, collaborative research. Yet important questions remain:

  • What percentage of people bitten by lone star ticks develop alpha-gal syndrome?
  • What percentage of people sensitized to alpha-gal go on to develop alpha-gal syndrome?
  • What genetic and immunologic factors determine whether someone sensitized to alpha-gal develops alpha-gal syndrome?
  • Why are some ticks (i.e., lone star ticks) more effective in sensitizing to alpha-gal and causing alpha-gal syndrome than others (i.e., blacklegged ticks)?
  • What compounds in tick saliva along with alpha-gal provoke the human immune system to produce allergic antibodies (IgE)?
  • What aside from ticks (and possibly chiggers, and Ascaris roundworms) can sensitize a person to alpha-gal? (Stoltz et al. 2019, Murangi et al. 2022)

There has been differing evidence about whether the molecule alpha-gal is produced by the tick itself or is synthesized by bacteria that are part of the tick microbiome. In either case, scientists have asked whether bacteria living in ticks could affect the amount of alpha-gal produced in tick saliva (Kumar et al. 2022, Cabezas-Cruz et al. 2018).

New treatments and future directions

For patients suffering from alpha-gal syndrome, the mainstay of management is avoiding red meat and—for some—dairy and other ingredients containing alpha-gal. For those patients sensitive even to minor exposures to alpha-gal, there also now exists a medication called omalizumab that has been effective in decreasing symptoms. It is an anti-IgE monoclonal antibody, and so works not only for alpha-gal syndrome but for IgE-mediated food allergy more broadly. Omalizumab may also be appropriate for those with unavoidable occupational exposures, such as those working in kitchens with skin and fume exposures to meat, and those who birth animals or dress deer and may be exposed to large amounts of body fluids containing alpha-gal (Nuñez-Orjales et al. 2017).

For patients who crave red meat but are allergic, GalSafe® pork is made from a genetically modified pig that doesn’t express alpha-gal, and so can be consumed by patients with alpha-gal syndrome. The technology of gene-editing mammals could also lead to medical products like gelatin and heparin (a blood thinner) being made without alpha-gal. Although reactions to these products are rare, concerns about alpha-gal have complicated medical care for some patients.

Tick control strategies

New strategies to control lone star tick populations are needed, both environmental controls and interventions under study such as a universal tick vaccine. Alpha-gal syndrome has reanimated some of these goals, both through the threat of people no longer being able to eat meat and dairy; through a growing understanding of how ticks interface with the human immune system; and through geography, which unites a growing swath of the United States population in a campaign against ticks and tickborne disease.

Short and sweet

A simple way to explain alpha-gal syndrome to others is double delay, double avoidance. There is a delay of weeks to months from tick bite to the first allergic reaction, and there is a delay of hours from eating red meat to when allergic symptoms appear. The treatment for alpha-gal syndrome is to avoid red meat and avoid further tick bites.

References:

Cabezas-Cruz A, Espinosa PJ, Alberdi P, Šimo L, Valdés JJ, Mateos-Hernández L, Contreras M, Rayo MV, de la Fuente J. Tick galactosyltransferases are involved in α-Gal synthesis and play a role during Anaplasma phagocytophilum infection and Ixodes Ixodes scapularis tick vector development. Sci Rep. 2018 Sep 21;8(1):14224.

Kumar D, Sharma SR, Adegoke A, Kennedy A, Tuten HC, Li AY, Karim S. Recently Evolved Francisella-Like Endosymbiont Outcompetes an Ancient and Evolutionarily Associated Coxiella-Like Endosymbiont in the Lone Star Tick (Amblyomma americanum) Linked to the Alpha-Gal Syndrome. Front Cell Infect Microbiol. 2022 Apr 12;12:787209.

Maldonado-Ruiz LP, Reif KE, Ghosh A, Foré S, Johnson RL, Park Y. High levels of alpha-gal with large variation in the salivary glands of lone star ticks fed on human blood. Sci Rep. 2023 Dec 4;13(1):21409. 

Murangi T, Prakash P, Moreira BP, Basera W, Botha M, Cunningham S, Facey-Thomas H, Halajian A, Joshi L, Ramjith J, Falcone FH, Horsnell W, Levin ME. Ascaris lumbricoides and ticks associated with sensitization to galactose α1,3-galactose and elicitation of the alpha-gal syndrome. J Allergy Clin Immunol. 2022 Feb;149(2):698-707.e3.

Nuñez-Orjales R, Martin-Lazaro J, Lopez-Freire S, Galan-Nieto A, Lombardero-Vega M, Carballada-Gonzalez F. Bovine Amniotic Fluid: A New and Occupational Source of Galactose-α-1,3-Galactose. J Investig Allergol Clin Immunol. 2017;27(5):313-314.

Platts-Mills TAE, Workman LJ, Richards NE, Wilson JM, McFeely EM. Implications of a fatal anaphylactic reaction occurring 4 hours after eating beef in a young man with IgE antibodies to galactose-α-1,3-galactose. The Journal of Allergy and Clinical Immunology In Practice. 2025 Nov.

Stoltz LP, Cristiano LM, Dowling APG, Wilson JM, Platts-Mills TAE, Traister RS. Could chiggers be contributing to the prevalence of galactose-alpha-1,3-galactose sensitization and mammalian meat allergy? J Allergy Clin Immunol Pract. 2019 Feb;7(2):664-666

Thompson JM, Carpenter A, Kersh GJ, Wachs T, Commins SP, Salzer JS. Geographic Distribution of Suspected Alpha-gal Syndrome Cases – United States, January 2017-December 2022. MMWR Morb Mortal Wkly Rep. 2023 Jul 28;72(30):815-820. 

Tjernberg I, Hamsten C, Apostolovic D, van Hage M. IgE reactivity to α-Gal in relation to Lyme borreliosis. PLoS One. 2017 Sep 27;12(9):e0185723. 

Guest Writer

Dr. Eleanor Saunders

Guest Writer

Opinions expressed by contributors are their own. Dr. Eleanor Saunders is an Infectious Diseases physician at the University of North Carolina at Chapel Hill. Dr. Saunders received her MD & MPH from the UNC School of Medicine and UNC Gillings School of Global Public Health, completed residency in Internal Medicine at Bellevue Hospital/NYU Langone Health, and completed fellowship training in Infectious Diseases at UNC. Dr. Saunders works on the epidemiology of alpha-gal syndrome with Dr. Scott Commins, one of the foremost experts on AGS.

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For more: