Fasting: The Foundation of Cancer Recovery
An Essay on the First Intervention
The Body Is Its Own Surgeon
Herbert Shelton supervised more than thirty thousand fasts at his Natural Hygiene centers across four decades of clinical practice. What he documented across those decades has no place in conventional oncology and is therefore not discussed in oncology offices. When a person stops eating, the body selectively dismantles its own tissue, and it begins with the tissue it does not need. Fat reserves are consumed first. The body then begins to clear what it has been carrying without anatomical purpose: cysts, fibroids, tumors, arterial deposits, scar accumulations. Vital organs are protected until the very end. The body, given no food, performs surgery on itself, and the surgery is more precise than any external scalpel because the body knows what to keep.¹
Shelton called the process autolysis, meaning enzymatic self-digestion under conditions of voluntary food abstention. He observed fibroid tumors dissolve while the uterus housing them remained intact. He watched arthritic deposits clear while bone and muscle stayed strong. He documented hearts that grew stronger, not weaker, across fasts of two and three weeks. The dismantling was not indiscriminate. It followed a sequence that made anatomical sense, sparing what was useful and clearing what was not.
This is the most paradigm-coherent fact in the entire cancer literature, and almost no patient diagnosed with cancer is ever told about it.
The implications run in one direction. If the body, given no food, dissolves diseased tissue and protects healthy tissue, then the body is not the cause of its own disease but the agent of its own repair. What is needed is an intervention that creates the conditions under which that intelligence can operate, not one that overrides it. Fasting creates those conditions more completely than any other modality available.
Cancer is the test case because cancer is the diagnosis that most thoroughly removes the body’s authority from the conversation. The patient is told, often within hours of diagnosis, that they have a disease their body cannot heal, requiring treatments their body cannot survive without medical management, and that anything else they might try is at best a complement to those treatments and at worst a dangerous delay. The framework is closed before the patient can ask what cancer actually is.
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What Cancer Actually Is
Cancer is a metabolic condition arising from damaged mitochondria in toxically burdened tissue. The framework was established by Otto Warburg in 1924, when he observed that cancer cells generate energy through fermentation of glucose rather than through oxygen-based respiration in the mitochondria.² Normal cells generate energy by respiring; cancer cells generate energy by fermenting glucose, even when oxygen is available. The shift to fermentation is not a quirk of cancer cells. It is the defining feature.
Thomas Seyfried’s nuclear transfer experiments, the culmination of decades of careful work, settled the question of where cancer originates.³ When researchers placed a healthy nucleus into cancerous cytoplasm, the resulting cell became cancerous roughly 97 percent of the time. The reverse experiment, placing a cancerous nucleus into healthy cytoplasm, produced a normal cell. The cause sits in the cytoplasm. The cellular environment determines whether a cell remains healthy, and the so-called genetic blueprint follows from it rather than driving it.
Travis Christofferson chronicles in Tripping over the Truth how this finding overturned half a century of investment in the somatic mutation theory.⁴ The cancer genome projects yielded disappointing results despite billions in funding because they were looking in the wrong place. The mutations that appear in cancer tissue are downstream consequences of metabolic dysfunction, not its cause.
Thomas Cowan extends the framework one step further. Cancer cells are damaged cells running on fermented glucose because their mitochondria can no longer use oxygen to extract energy efficiently. Cowan asks what the tumor itself represents, and his answer, developed across his cancer work, is that tumors function as emergency waste containment.⁵ When normal elimination pathways are overwhelmed, the body builds a structure to sequester toxins that cannot be excreted. The tumor is not the disease itself but the body’s response to a deeper problem it cannot otherwise resolve. The image often used to capture this is a lily pad forming on a polluted pond: a localized holding area for accumulated burden that has nowhere else to go.
This reframing determines what counts as recovery. If the tumor is the disease, recovery means cutting, irradiating, or poisoning it out by any available means. If the tumor is the body’s response to toxic burden in damaged tissue, recovery means restoring the conditions under which the body can resolve the burden itself.
The Verdict on the Dominant Approach
Cancer mortality in the United States fell approximately 5 percent between 1950 and 2005. The War on Cancer was launched in 1971, hundreds of billions of dollars have since been spent on research, and an industry now valued in the hundreds of billions of dollars annually has grown up around the diagnosis. The result remains 5 percent.⁶
The deadliest cancers are pancreatic (12.5 percent five-year survival), glioblastoma (6.8 percent), and small cell lung cancer (7 percent), which happen to be the cancers with the most pronounced Warburg metabolism.⁷
Hardin Jones, a Berkeley biostatistician, completed a twenty-five-year study comparing treated and untreated cancer patients. His finding, presented at the American Cancer Society Science Writers’ Seminar in 1969 and never seriously refuted, was that untreated patients lived on average four times longer than those who accepted conventional treatment.⁸
The screening apparatus that funnels patients into this system has produced overdiagnosis at industrial scale. An estimated 1.3 million American women have been overdiagnosed with breast cancer over thirty years. Roughly 31 percent of 2008 breast cancer diagnoses were tumors that would never have caused symptoms.⁹ About 85 percent of prostate cancer diagnoses fall into the same category: indolent cellular abnormalities that would have remained indolent if no one had looked for them.¹⁰
These figures are not in dispute among researchers who have examined the data. They simply do not penetrate the oncology office, where the patient sits in front of a practitioner whose training and livelihood depend on the framework remaining unquestioned.
How Fasting Addresses the Actual Mechanism
Fasting acts on the metabolic foundation of cancer along four convergent pathways that operate simultaneously.
The fuel switch. Cancer cells depend on glucose (blood sugar) because their damaged mitochondria cannot efficiently use ketones (the alternative fuel the body produces from fat). Normal cells use both. When food is removed, blood glucose drops, the body’s glycogen reserves (stored glucose in the liver and muscles) deplete within twenty-four to thirty-six hours, and the liver begins producing ketones from fat. The rest of the body transitions to ketone metabolism. The brain participates in this transition, drawing the majority of its energy from ketones once adapted, with the liver covering the residual glucose requirement through gluconeogenesis. The notion that the brain requires a constant supply of dietary glucose does not survive examination of the clinical record. Angus Barbieri fasted for 382 days under medical supervision in Scotland between 1965 and 1966, taking only water, tea, coffee, and vitamin supplementation; he lost 276 pounds and remained mentally intact throughout. The case is published in the Postgraduate Medical Journal.²³ Cancer cells struggle, because the fuel they require has been withdrawn and the alternative fuel the body now runs on is one they cannot efficiently use. This is the foundation of the press-pulse strategy that Seyfried developed and that Paul Marik documents in his cancer care protocol.¹¹
Autolysis. Shelton’s clinical observation, confirmed across thousands of supervised cases at multiple institutions, is that the body during extended fasting dismantles its own tissue in order of dispensability. Fat reserves are consumed first. Next come accumulations the body has been carrying without need: cysts, fibroids, tumors, scar tissue, arterial plaques. Vital organs are dismantled last, only under conditions of true starvation. The body becomes its own surgeon, knowing the order of operations because it has been performing this kind of housekeeping continuously since birth. Fasting simply removes the competing demands that ordinarily keep the housekeeping at low intensity.
Autophagy. Yoshinori Ohsumi was awarded the 2016 Nobel Prize in Physiology or Medicine for elucidating the cellular cleanup process called autophagy, which translates literally as self-eating.¹² At the cellular level, autophagy is the mechanism by which cells dismantle and recycle damaged proteins, dysfunctional organelles, and accumulated debris. When insulin drops and the cellular signals that drive growth fall quiet during fasting, cells switch from growth mode to maintenance mode and clear what would otherwise accumulate. Autophagy operates nightly at low levels during sleep. Extended fasting activates it at a depth nothing else approaches, including the most expensive pharmaceutical interventions available.
Stem cell renewal. Around the third day of fasting, when glucose is depleted and insulin production in the pancreas approaches zero, Protein Kinase A levels collapse. PKA normally functions as a brake on stem cell proliferation. With the brake released, dormant stem cells throughout the body begin dividing, with each division producing both a replacement stem cell and a new cell to repair damaged tissue. August Dunning’s research identifies day five of an extended fast as the point at which stem cell proliferation reaches what he describes as a flood.¹³ The body that completes such a fast is not the body that began it. Healthy cells are protected by this state; cancer cells are not. Valter Longo's lab at USC has documented across two decades of peer-reviewed work what he calls differential stress resistance: healthy cells respond to fasting by downregulating growth signaling and entering a protected quiescent state, while cancer cells, whose growth signaling is constitutively activated and cannot be turned down, continue trying to grow in conditions that no longer support it.²⁴ The PKA brake release activates dormant healthy stem cells. It does not activate cancer cells, because cancer cells were already past every brake before fasting began.
The four mechanisms operate together. The body withdraws fuel from cancer cells while it dismantles damaged tissue, clears cellular debris, and builds new cells from its activated reserves. No external intervention is required, and no external intervention could coordinate four processes of this depth simultaneously. The body coordinates them itself, once given the conditions to do so.
What Has Happened When People Have Tried This
Dale Atkinson was given an 11.5-month prognosis for his cancer. Under Dr. Amanda King’s direction, he pursued a metabolic protocol that included ketogenic eating, high-dose cholecalciferol, fasting cycles, and repurposed compounds with documented metabolic effects. His tumors were completely eliminated, without chemotherapy or radiation.¹⁴
Robert Milligan was diagnosed with stage 4 metastatic melanoma, with tumors throughout his organs, broken bones from skeletal metastases, and a prognosis measured in months. He pursued an integrative protocol grounded in metabolic intervention. Four months later he was cancer-free. He subsequently established the Holistic Cancer Care Foundation so that other patients would not have to search for the information he had to assemble himself.¹⁵
Ben was diagnosed with stage IV pancreatic cancer, the deadliest common cancer, with single-digit five-year survival under conventional treatment. He combined conventional treatment with an adjunctive protocol that included fasting, ketogenic eating, and metabolic compounds. He achieved no evidence of disease.¹⁶
Leslie Dennis Taylor’s friend’s husband presented with stage 4 colon cancer metastatic to the liver. His oncologist judged him terminal. His cancer blood marker stood in the 800s. After six months of ketogenic eating and intermittent fasting, alongside a single chemotherapy drug (reduced from the original two-drug regimen), his marker had dropped to 30. Remission is defined as below 5. His oncologist asked him to write down what he had been eating.¹⁷
These cases are not isolated. The Gerson protocol, which incorporates juice fasting alongside whole-food nutrition, has documented 42 percent remission rates in cancers considered terminal by conventional standards, compared with chemotherapy’s approximately 12 percent five-year survival across all cancers combined.¹⁸ German integrative clinics using metabolic interventions report remission rates as high as 88 percent in cancers American oncology categorizes as untreatable.¹⁹
The Russian clinical fasting tradition, largely unknown in the West, has been continuously developed since the 1950s, most recently under Dr. Sergey Filonov at his clinic in Siberia.²⁰ The Russian model uses extended dry fasting, with no food and no water, for periods that would be considered impossible in mainstream Western medicine. The clinic operates because the results obtained are not obtainable through other means.
The standard objection to all of this is that these are anecdotes rather than randomized controlled trials. The reply is straightforward. No one has funded such trials and no one will, because no patentable molecule is involved and no industry stands to gain from the result. The absence of the trials is itself the evidence of which results would be inconvenient to produce. The Gerson outcomes, the German clinic outcomes, and the Russian clinical outcomes were not produced by anecdote; they were produced by clinical practice over decades. They are missing from the literature for the same reason fasting is missing from oncology offices.
None of these cases requires the curious skeptic to accept a complete framework upfront. They require only that the skeptic examine what has happened when patients have tried this, and ask why the option is never presented in an oncology office.
The Range of Approaches
Fasting is not a single intervention but a graduated series.
Time-restricted feeding involves a daily cycle of sixteen hours fasting and eight hours eating. This is the most accessible entry point, activating mild autophagy and supporting metabolic flexibility. It suits prevention and maintenance, and serves as preparation for deeper protocols.
The 24-hour fast, performed two or three times weekly, pushes glycogen depletion and produces meaningful autophagy without requiring extended downtime.
The three-day fast crosses the threshold beyond which ketosis is fully established, autophagy reaches significant depth, and stem cell mobilization begins. Many practitioners consider three days the minimum useful interval for therapeutic effect.
The extended water fast, lasting seven to fourteen days, is the protocol Shelton used at his centers. It produces deep autolysis, profound autophagy, and full stem cell activation. It requires supervision or substantial prior fasting experience. The protocol is not for those on multiple medications, with kidney disease, with a history of gallstones, or who are underweight, except under medical guidance.
The seven-day dry fast, called the Phoenix protocol by August Dunning, is the most intensive option. Performed once or twice yearly with substantial rest, it requires preparation that includes senolytic compounds (which clear senescent cells before the fast begins). The body produces its own water from fat metabolism, accelerating every mechanism that water fasting activates. This is not a beginner’s protocol and carries risks that water fasting does not.
The protocols form a ladder. Most patients begin at the lower rungs and ascend as their experience and condition allow. The literature is clear that supervision matters at the upper end. Blood pressure typically falls, medications need adjustment, refeeding must be done carefully, and individual judgment matters more than rigid protocol adherence.
Why This Sits Under Everything Else
Every other intervention available to a cancer patient adds something to the body. Chemotherapy delivers cytotoxic chemicals into the bloodstream. Radiation deposits ionizing damage in tissue. Surgery cuts away both tumor and surrounding flesh, removing structures the body built for reasons the procedure does not address. Even the better alternative protocols, including ketogenic eating, repurposed compounds, intravenous ascorbic acid, and hyperbaric oxygen, add inputs the body must process before it can use them.
Fasting is the only major modality that operates by subtraction. Nothing is added; the inputs are removed. The body is given a period during which the digestive and detoxification systems that normally run at full capacity from the moment of waking can redirect their energy to repair. The toxic burden that drove the disease begins to clear, damaged cells are dismantled, cellular machinery is reset, and new cells are built from the body’s own activated reserves.
This is why fasting sits under everything else. The four causes of disease in the terrain framework (toxic exposure, nutritional depletion, electromagnetic strain, and psychological stress) are addressed by fasting more directly than by any other intervention. Toxic input falls to whatever the body itself releases during autolysis. Mineral and cofactor reserves are spared because the digestive apparatus stops drawing on them. The metabolic burden of continuous digestion lifts. The patient who fasts is not adding to the burden while attempting to recover from it.
A patient who begins recovery without fasting is attempting to heal in a body that has not stopped accumulating. A patient who incorporates fasting from the start gives every subsequent intervention, whether nutritional, environmental, or biochemical, a cleaner substrate on which to work. The other modalities all amplify when fasting comes first. Ketogenic eating builds on a body that has already transitioned to fat metabolism. Metabolic compounds reach cancer cells more directly in a fasted state. Detoxification protocols work in tissue that has already begun selective dismantling. Fasting is not one option among several; it is the foundation on which the others stand.
This is also why fasting has been suppressed. There is nothing to sell. Fasting cannot be patented, licensed, or billed in any sustainable way. The 1910 Flexner Report restructured American medical education around interventions that could be standardized and scaled, reducing the number of medical schools in the United States from 162 to 66 and eliminating those that taught approaches inconsistent with the new paradigm.²¹ Fasting cannot be scaled. It requires no drug, no device, and no clinical infrastructure beyond rest, water, and supervision where appropriate. An industry that derives its revenue from intervention cannot accommodate a modality whose value lies in cessation.
The 1946 Senate hearings at which Max Gerson presented documented cures of terminal cancer patients followed the same pattern. The hearings were attended and the cases were reviewed, but the pharmaceutical lobby ensured nothing came of them.²² Gerson’s findings were buried institutionally rather than refuted scientifically. Fasting has met the same response across the same period, for the same reason.
What the Body Does
Shelton documented his thirty thousand fasts across forty years. The work was not hidden. His findings were published in books still in print and replicated at the centers he established and at others modeled on his approach. Filonov’s clinic operates today. The Gerson protocol has been continuously refined since the 1940s. The metabolic theory of cancer has been substantially confirmed in peer-reviewed work across the last twenty years. None of this is fringe knowledge. It is not even contested. The metabolic mechanism is not disputed by mainstream biochemistry. What is disputed is whether the patient ever hears about it.
The fact that remains, after every objection and counter-claim has been considered, is the one Shelton documented across forty years and thirty thousand cases. When a person stops eating, the body selectively dismantles diseased tissue and protects vital tissue. It dissolves tumors, clears arterial deposits, breaks down accumulated burdens, builds new cells, and emerges from the process with a measurable shift in function across organ systems. The capacity is present in every human body and has been the entire time. Its operation does not require permission from the medical system that has so far failed to make use of it.
The body, given no food, performs surgery on itself, and it has been doing the work the establishment has not been able to do in seventy-five years of trying. The first intervention is the one the patient has always had and has almost never been told about. Nothing needs to be added to the body for it to operate, and nothing needs to be purchased or approved for its use. The willingness to stop eating, for long enough that the body can do what it has been waiting to do, is the entire protocol.
How to Explain This to a Six-Year-Old
Your body knows how to clean itself, but only when it isn’t busy with other things. Eating is one of the biggest jobs your body does every day. When you stop eating for a while, your body finally has time to look around inside and tidy up.
Little workers inside you go around and find the parts that aren’t working right anymore. They take them apart and use the pieces to build new healthy parts. They start with the things your body doesn’t need: old lumps, bumps that shouldn’t be there, things that got worn out. They leave the important parts alone.
Cancer is what happens when some of your cells get tired and broken. Instead of running on oxygen the way healthy cells do, they start running on sugar, and they need lots of it to keep going. When you stop eating, the sugar goes away. The broken cells run out of food. The healthy cells switch to a different fuel that comes from your body’s stored fat, and they keep working just fine. The body finally has time to take apart what isn’t working and build new healthy things in their place.
So if someone has cancer, one of the most helpful things they can do is give their body a rest from eating. The body knows how. It just needs quiet time to do the work.
The full body of work this essay draws on is gathered in The Unbekoming Cancer Compendium and The Fasting Cure*.*
References
Shelton, Herbert M. Fasting Can Save Your Life. American Natural Hygiene Society Press, 1964.
Warburg, Otto. “Über den Stoffwechsel der Carcinomzelle.” Biochemische Zeitschrift 152 (1924): 309–344. Subsequently published in English as “On the Origin of Cancer Cells.” Science 123, no. 3191 (1956): 309–314.
Seyfried, Thomas N. Cancer as a Metabolic Disease: On the Origin, Management, and Prevention of Cancer. Hoboken: Wiley, 2012.
Christofferson, Travis. Tripping over the Truth: How the Metabolic Theory of Cancer Is Overturning One of Medicine’s Most Entrenched Paradigms. White River Junction: Chelsea Green Publishing, 2017.
Cowan, Thomas. Cancer and the New Biology of Water. White River Junction: Chelsea Green Publishing, 2019.
National Cancer Institute, SEER cancer mortality data. Long-term trend analyses discussed in Christofferson (2017) and Cowan (2019).
National Cancer Institute SEER five-year survival statistics. Correlation between Warburg metabolism and survival discussed in Seyfried (2012).
Jones, Hardin B. “A Report on Cancer.” Address to the American Cancer Society Science Writers’ Seminar, 1969. Discussed in Sloan, Mark. The Cancer Industry: Crimes, Conspiracy and the Death of My Mother, 2018.
Bleyer, Archie, and Welch, H. Gilbert. “Effect of Three Decades of Screening Mammography on Breast-Cancer Incidence.” New England Journal of Medicine 367, no. 21 (2012): 1998–2005.
Welch, H. Gilbert. Should I Be Tested for Cancer? Maybe Not and Here’s Why. Berkeley: University of California Press, 2004; Ablin, Richard, and Piana, Ronald. The Great Prostate Hoax. New York: Palgrave Macmillan, 2014.
Marik, Paul E. Cancer Care. FLCCC Alliance protocol document.
Nobel Assembly at Karolinska Institutet. “The Nobel Prize in Physiology or Medicine 2016: Yoshinori Ohsumi for discoveries of mechanisms for autophagy.”
Dunning, August. The Phoenix Protocol: Dry Fasting for Rapid Healing and Radical Life Extension, 2020.
King, Amanda. Interview with Unbekoming, “A Naturopathic Approach: How Metabolic Interventions Are Changing Cancer Outcomes.” Unbekoming Substack.
Milligan, Robert. Holistic Cancer Care Foundation. Interview, Unbekoming Substack.
“The Space Between: Stage IV Cancer and No Evidence of Disease.” Case study, Unbekoming Substack.
Taylor, Leslie Dennis. Interview with Unbekoming, “On Diabetes, Fasting, Migraines, Autophagy, Diets, Cancer and Much More.” Unbekoming Substack.
Gerson, Charlotte, and Walker, Morton. The Gerson Therapy: The Proven Nutritional Program for Cancer and Other Illnesses. New York: Kensington Publishing, 2001.
Walker, Morton. German Cancer Therapies: Natural and Conventional Medicines That Offer Hope and Healing. New York: Kensington Publishing, 2003.
Slater, Michelle. Starving to Heal in Siberia. 2019. Documenting Dr. Sergey Filonov’s extended dry-fasting clinic.
Flexner, Abraham. Medical Education in the United States and Canada: A Report to the Carnegie Foundation for the Advancement of Teaching. New York: Carnegie Foundation, 1910.
United States Senate hearings on the Pepper-Neely Anticancer Bill (S. 1875), July 1946. Testimony of Dr. Max Gerson on cancer treatment outcomes.
Stewart, W.K., and Fleming, L.W. "Features of a successful therapeutic fast of 382 days' duration." Postgraduate Medical Journal 49, no. 569 (1973): 203–209.
Raffaghello, Lizzia, et al. "Starvation-dependent differential stress resistance protects normal but not cancer cells against high-dose chemotherapy." Proceedings of the National Academy of Sciences 105, no. 24 (2008): 8215–8220.



Author's Note
The comments produced four points worth addressing directly. Two prompted additions to the essay since publication; two require a longer response here.
The brain-glucose objection. KoalaPower raised the common concern that fasting deprives the brain of glucose. Garth Mando responded with the case of Angus Barbieri, the Scottish man who fasted for 382 days under medical supervision at Maryfield Hospital between 1965 and 1966. He took only water, tea, coffee, and vitamin supplementation. He lost 276 pounds and remained mentally intact throughout. The case is published in the Postgraduate Medical Journal (1973). I've added the Barbieri case to the fuel-switch section, along with the underlying mechanism: once metabolically adapted, the brain draws the majority of its energy from ketones, with the liver covering the residual glucose requirement through gluconeogenesis. The notion that the brain requires constant dietary glucose does not survive examination of the clinical record.
The cancer stem cell question. GailDR identified an apparent contradiction in the mechanism section. If the PKA brake is released during fasting and stem cells start dividing, what stops cancer cells from benefiting? The answer is differential stress resistance, documented across two decades of peer-reviewed work by Valter Longo's lab at USC. Healthy cells respond to fasting by downregulating growth signaling and entering a protected quiescent state. Cancer cells, whose growth signaling is constitutively activated and cannot be turned down, continue trying to grow in conditions that no longer support it. The PKA brake release activates dormant healthy stem cells. It does not activate cancer cells, because cancer cells were already past every brake before fasting began. I've added this to the mechanism section.
On fasting as the primary modality. GailDR also asked whether there are documented cases of patients using prolonged water fasting as the primary modality and achieving complete remission. The honest answer is that the cases I cited are all combined protocols. The cases that come closest to fasting as primary modality come from Filonov's Siberian clinic and the broader Russian clinical fasting tradition, where the documentation takes the form of clinical case files rather than published case series in the Western format. The essay's thesis is that fasting is foundational, meaning it sits under and supports every other intervention, rather than that fasting alone is sufficient. The combined-protocol cases support that thesis. A case for fasting as sole modality would require different evidence than I have assembled here, and I am not making that case.
On honey and the apparent contradiction. Big E asked how the fasting-and-cancer argument squares with my previous writing on honey. The cancer context specifically changes the calculus on any glucose-bearing food. Honey is approximately 80 percent sugar. For a healthy person managing terrain factors, honey has real medicinal use, particularly in unprocessed forms with their enzymes and trace minerals intact. When active cancer is present and cells are running the Warburg metabolism, that same honey feeds the disease. The prior posts on honey were not written with active cancer in mind. The dietary framework that applies when cancer is present is ketogenic, not honey-inclusive. The fasting protocol described in this essay takes precedence over any standing nutritional advice from elsewhere in the body of work.
Thanks to everyone who engaged substantively. The work is better for it.
— Unbekoming
This is why fasting has always been frowned upon by the medical establishment. If sickness is your business, you don’t promote wellness, and you do everything you can to put people in search of wellness - off the scent… hence the “3 square meals a day” model, constant focus on food, fast food, and addictive food. And you certainly don’t talk about the cellular cleanup process involved in autophagy/fasting. So many elements have been employed to put people ‘off the scent’ of wellness, instead promoting a dominant establishment of credentialed “know-it-alls”, who actually know very little.