A woman covered in melanoma tumors was given one injection—into a single tumor.
Weeks later, every tumor across her body vanished.
It wasn’t luck. It was her immune system learning to fight back.
Here’s how researchers re-trained it to destroy cancer on its own. 🧵
A new class of cancer drug in development shrank the tumors in half of 12 advanced cancer patients in a clinical trial, avoiding severe side effects seen with previous versions of this class of drugs, according to a recent report.
The treatment uses CD40 agonist antibodies, a type of immunotherapy that uses the body’s immune system to attack cancer.
While this drug class has shown promise for two decades, development has been hampered by severe side effects, including widespread inflammation, low blood platelet counts, and liver toxicity—even at low doses.
Systemic Response From Local Treatment
The trial included 12 patients with various advanced cancers, including melanoma, kidney cancer, and breast cancer. Six patients experienced tumor shrinkage, and in two of those cases, the tumors disappeared completely.
The drug’s effects were not limited to tumors that were directly injected with the drug; cancer tumors elsewhere in the body also shrank or were completely destroyed.
“Seeing these significant shrinkages and even complete remission in such a small subset of patients is quite remarkable,” Juan Osorio, study first author and a visiting assistant professor at Rockefeller and a medical oncologist at Memorial Sloan Kettering Cancer Center, stated.
One melanoma patient had dozens of tumors on her leg and foot, but after multiple injections into just one tumor, all other tumors vanished.
The breast cancer patient had tumors in her skin, liver, and lung that all disappeared following injection of a single skin tumor.
“This effect—where you inject locally but see a systemic response—that’s not something seen very often in any clinical treatment,” Dr. Jeffrey V. Ravetch, head of the Laboratory of Molecular Genetics and Immunology at Rockefeller University, stated. “It’s another very dramatic and unexpected result from our trial.”
None of the 12 patients experienced the severe side effects typical of previous CD40 therapies.
Tissue analysis confirmed that the drug stimulated immune activity within the tumors.
CD40 is a protein found on immune cells that, when activated, prompts the immune system to fight tumors and develop tumor-specific T cells. The enhanced 2141-V11 drug also engages a specific receptor on immune cells called Fc receptor, amplifying the immune response.
“We were quite surprised to see that the tumors became full of immune cells—including different types of dendritic cells, T cells, and mature B cells—that formed aggregates resembling something like a lymph node,” Osorio stated, emphasizing that these structures are associated with better treatment outcomes.
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Addressing Treatment-Resistant Cancers
Dr. John Oertle, chief medical officer and cancer specialist at Envita Medical Centers, who was not involved in the study, told The Epoch Times that this approach could help treat cancers currently resistant to existing immunotherapies.
He explained that many resistant cancers exhibit “immune exhaustion,” where T cells become dysfunctional and unable to mount an effective attack against cancer despite their presence.
Injecting the CD40 agonist directly into a tumor may help “reprogram” the tumor microenvironment, restore immune vitality, and drive T cell infiltration, to break through treatment resistance, he said.
“However,” he noted, “This is rarely a one-size-fits-all solution. Designing combinations that are tailored to the patient’s specific disease biology and immune profile is critical to sustaining responses and improving overall outcomes.”
Severe Side Effects Had Slowed Development
Developing CD40 antibodies for cancer treatment has taken more than twenty years of research.
While animal trials showed these drugs to be effective in clearing cancer, human trials found they also caused widespread inflammation, low blood platelet counts, and liver toxicity—even at low doses.
However, in 2018, researchers at Rockefeller University’s Laboratory of Molecular Genetics and Immunology made a key breakthrough. Led by Ravetch, the team engineered an enhanced version of the CD40 antibody, 2141-V11, to boost immune system activation while minimizing harmful side effects.
The modified drug binds more tightly to CD40 receptors on human cells and is 10 times more potent at activating anti-cancer immune responses. Rather than administering the drug through traditional intravenous infusion, which often caused toxicity due to widespread CD40 receptors on healthy cells, in the recent clinical trial, published in October, researchers switched to injecting the drug directly into tumors.
Next Steps and Broader Impact
These findings have led to additional clinical trials in collaboration with Memorial Sloan Kettering and Duke University, which are currently in their early phases. These studies are exploring 2141-V11’s effects on cancers such as bladder, prostate, and glioblastoma, an aggressive and deadly brain cancer, with nearly 200 patients enrolled.
Researchers seek to understand why some patients respond to the drug while others do not. For example, the two patients whose cancers disappeared had high levels of T cells, immune cells that kill cancer cells, before treatment.
“This suggests there are some requirements from the immune system in order for this drug to work, and we’re in the process of dissecting these characteristics in more granular detail in these larger studies,” Ravetch stated.
As a broader challenge in cancer immunotherapy, Ravetch noted that only 25 to 30 percent of patients will respond to immunotherapy, so the biggest challenge in the field is to try to determine which patients will benefit from it.
“While this trial is early and the patient number is small, the fact that we’re seeing complete remissions in aggressive cancers from localized injection is a very encouraging sign,” Oertle said.
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The Real Reason 8 Hours of Sleep Still Leaves You Exhausted
Millions wake up drained even after a full night’s rest.
Doctors say your body may be working instead of healing—burning energy when it should be restoring it.
Studies now link this to early dementia and hidden metabolic damage.
What if your “good night’s sleep” is actually wearing you out? 🧵
For years, Patty Schmidt believed she was doing everything right.
She went to bed by 10 p.m., woke up at 6 a.m., avoided coffee after lunch, and stayed off screens before bed. Yet most mornings she woke up exhausted.
“I thought I was disciplined about sleep, but my body told a different story,” said Schmidt. “I would wake up groggy, push through the day, and crash again by midafternoon.”
Her experience points to a reality millions face: meeting the seven-to-nine-hour recommendation for sleep doesn’t guarantee you will feel rested.
Recent research shows the real issue is not only the length of sleep, but its quality, the body’s internal processes during the night, and whether you’re sleeping at the correct biological time.
High-THC Cannabis Products Linked to Immediate Psychosis and Addiction
Cannabis today is far stronger—and far more dangerous—than most people realize.
Just one hit of high-THC vapes or concentrates can trigger psychosis or schizophrenia symptoms within hours, according to a review of 221,000 people.
Hallucinations, paranoia, and delusions can strike almost instantly—and with THC levels pushing 90%, dependence is nearly inevitable.
🧵 THREAD
As marijuana legalization spreads nationwide and young Americans increasingly view cannabis as harmless, new research reveals a paradox: Modern products such as vapes, dabs, and concentrates with high levels of tetrahydrocannabinol or THC, the main psychoactive ingredient, are triggering serious mental health problems at rates far higher than the marijuana of previous generations.
Using cannabis products with high levels of THC is linked with increased risk for psychosis or schizophrenia, especially within 12 hours after use, a new review of 99 studies found.
Michael Hill at Occidental College accidentally used too little current in his experiment—and stumbled upon a discovery that might replace LASIK with a gentler treatment that reshapes corneas without ever cutting the eye.
The discovery may offer hope for the millions of people living with poor vision who want an alternative to glasses and contact lenses but are wary of LASIK’s risks.
While laser eye surgery is generally successful, it involves cutting into the eye and can cause complications including dry eyes, vision problems, and in rare cases, severe side effects.
A Forgotten Antibiotic Just Shook Up the Lyme Disease Debate
In a pair of new studies, one overlooked drug eliminated Lyme bacteria at doses 100x lower than standard antibiotics—without wrecking the gut microbiome.
Even more surprising? It might prevent infection entirely.
And it's already FDA-approved.
Now the question is… why hasn’t this been used all along?
🧵 THREAD
Scientists may be closing in on two major advances in the fight against Lyme disease: an overlooked antibiotic that eliminates the infection at exceptionally low doses and new insights into why symptoms often persist long after treatment.
In a pair of studies published recently in Science Translational Medicine, scientists showed that piperacillin—a Food and Drug Administration-approved antibiotic—cleared Lyme infections in mice at doses up to 100 times lower than those of doxycycline, the current first-line treatment.
Unlike doxycycline, piperacillin targets the Lyme disease bacteria specifically, sparing the gut microbiome from the disruption that typically accompanies doxycycline use.
Researchers Found Unvaccinated Children Healthier Than Vaccinated, Didn’t Publish Findings
A Michigan study of 18,000 children found vaccinated kids were 2.5x more likely to suffer chronic illness.
The findings were so explosive, the researchers never published them.
🧵THREAD
Researchers from a large health care system in Michigan found that vaccinated children were more likely to develop a chronic health condition, but never published the findings, according to a copy of the study obtained by The Epoch Times.
Henry Ford Health System, whose employees carried out the study, said it was deficient.
Dr. Marcus Zervos, an infectious disease specialist at the Henry Ford Health, and colleagues studied 18,468 children born between 2000 and 2016 who were enrolled in the health system’s insurance plan, drawing data from medical, clinical, and payer records and supplementing with information from Michigan’s immunization registry.
The secret to slowing aging may not lie in your genes—but in your kidneys.
For centuries, healers believed every wrinkle, gray hair, and burst of vitality came from one source: your kidney’s vital energy.
Now scientists are confirming two sharp aging spikes—around 44 and 60—that align almost exactly with what ancient medicine predicted.
What if aging isn’t random decay, but a measurable energy loss you can restore naturally? The answer could rewrite everything we know about growing old.
🧵 THREAD
The eastern concept of the kidney extends beyond the anatomical organ. It refers to a broader energy system, where the kidney’s vital energy (qi) and the life’s essence are stored.
Kidney essence is regarded as the foundation of human growth, development, and reproductive function. Meanwhile, vital energy nourishes and warms the body’s internal organs and tissues, supporting overall vitality.
According to Traditional Chinese Medicine (TCM), a decline in the kidneys’ vital energy is seen as the beginning of the aging process. Yet there are practical and simple ways to replenish the kidneys’ vital energy.
How the Kidneys’ Vital Energy Plays a Role in Growth and Aging
The strength or decline of the kidney’s vital energy is believed to play a key role in the processes of growth and aging.
According to the classic text, “The Yellow Emperor’s Classic of Internal Medicine,” human development follows a pattern of “seven- and eight-year cycles.”
Women undergo major developmental changes every seven years, while men undergo them every eight years.