Metabolic Health · Liver · Thyroid · Blood Sugar

The Metabolic Cascade
How Fatty Liver Becomes Diabetes

Fatty liver, thyroid dysfunction, kidney stress, and type 2 diabetes are not separate diagnoses. They are one cascade — each organ failing in sequence as the liver loses its ability to do the jobs it was designed for. The root cause is not sugar. It's what replaced animal fat in your food after 1900.

The Cascade Nobody Told You About

In 2024, roughly 1 in 3 Americans has non-alcoholic fatty liver disease. About 1 in 10 has type 2 diabetes. Thyroid dysfunction affects an estimated 20 million Americans, most of them undiagnosed. Chronic kidney disease affects 37 million more. These statistics are usually presented as four separate epidemics with four separate causes and four separate treatment tracks.

They are not. They are one cascade.

The liver is the metabolic hub of the human body. It converts thyroid hormone into its active form. It clears excess insulin. It synthesizes the proteins that regulate kidney filtration. It processes every fat you eat. When the liver becomes overloaded — clogged with a type of fat it was never designed to store — every downstream organ pays the price. The sequence is predictable. The timeline is measurable. And for most people, it began decades before the first blood panel flagged anything.

Seed Oil Accumulation
Fatty Liver (NAFLD)
T4→T3 Disruption
Kidney Stress
Type 2 Diabetes

Understanding this cascade is not about fear. It's about sequence. If you know which domino falls first, you know where to intervene — and the intervention is not a medication for each organ. It's removing what started the chain reaction.

What this article covers

This article draws on independent researchers who have been studying metabolic disease from outside the pharmaceutical framework — including Zane Griggs, Isaac Pohlman, Ray Peat, and Morley Robbins. Their findings are presented here as perspectives, not as prescriptions. What they have in common: all four locate the root cause upstream of where conventional medicine looks.

Root Cause

The Pre-1900 Question

In 1900, type 2 diabetes was rare enough that Elliott Joslin — who began his diabetic patient ledger in 1893 and became the most prolific early documenter of the disease — could account for most known American cases in a single clinical record. Fatty liver disease did not exist as a clinical entity. Obesity, while present, was uncommon. Then, over the following 80 years, rates of metabolic disease climbed in a pattern that tracked almost exactly with one dietary change: the introduction and mass adoption of industrially processed vegetable oils.

Joslin EP. "The treatment of diabetes mellitus." Can Med Assoc J. 1916;6(8):673–684. PMID 20310820.

Before 1900, Americans cooked in butter, lard, and tallow — saturated fats that had been part of the human food supply for millennia. After 1900, the rise of Crisco (1911), commercial margarine, and eventually a cascade of seed oils — soybean, safflower, sunflower, corn, cottonseed, canola, grapeseed, rice bran — fundamentally changed the fatty acid composition of the Western diet.

The critical distinction, as researcher and author Zane Griggs documents in his Fit Over 40 framework, is the difference between the fats these oils contain. Saturated fats are chemically stable. The polyunsaturated fatty acids (PUFAs) dominant in seed oils — particularly linoleic acid, an omega-6 fat — are highly reactive. They oxidize under heat, light, and oxygen. Once incorporated into cell membranes and organ tissue, they continue to oxidize, generating inflammatory byproducts called oxidized lipids and 4-hydroxynonenal (4-HNE), a compound directly associated with liver cell injury.

What Zane Griggs observes

In his Fit Over 40 framework, Griggs notes that pre-1900 humans ate fruit, potatoes, rice, bread, and honey with essentially zero metabolic disease. The variable that changed was not carbohydrates — it was the type of fat. His protocol removes all seed oils completely and does not restrict whole-food carbohydrates, instead focusing on protein as the anchor and letting carbs come from single-ingredient whole foods.

His macronutrient framework for fat loss and insulin resistance reversal: protein 0.6–0.8g per pound of ideal body weight across 3 meals; fat 10–15% of calories (primarily from whole foods, not added oils); carbohydrates approximately 65% — all from single-ingredient sources.

Griggs Z. The Fit Over 40 Framework. Self-published protocol. | DiNicolantonio JJ, O'Keefe JH. "Omega-6 vegetable oils as a driver of coronary heart disease: the oxidized linoleic acid hypothesis." Open Heart. 2018;5(2):e000898. | Ramsden CE et al. "Re-evaluation of the traditional diet-heart hypothesis: analysis of recovered data from Minnesota Coronary Experiment (1968–73)." BMJ. 2016;353:i1246. | Seike T et al. "Hydroxynonenal causes hepatocyte death by disrupting lysosomal integrity in nonalcoholic steatohepatitis." Cell Mol Gastroenterol Hepatol. 2022;14(4):925–944. PMID 35787976.
The Hub Organ

The Liver Does Not Lie

The liver is where seed oil damage lands first. It is the organ responsible for processing dietary fat, and it is not equipped to handle the oxidation byproducts that come with industrially processed polyunsaturated oils. Over time — often over years or decades of daily exposure — oxidized lipids accumulate in liver cells, triggering inflammation. Fat deposits build up. The liver, which should be 5% fat by weight, moves toward 10%, 20%, 30%. This is non-alcoholic fatty liver disease (NAFLD), and it currently affects approximately one-third of the adult U.S. population.

Petäjä EM, Yki-Järvinen H. "Definitions of normal liver fat and the association of insulin sensitivity with acquired and genetic NAFLD — a systematic review." Int J Mol Sci. 2016;17(5):633. PMID 27128911.

The liver's functions are not aesthetic. It is the conversion factory for nearly every critical hormone and nutrient in the body. When it is inflamed and fatty, these conversions fail — quietly, without a dedicated lab flag, while the patient is told their labs are normal.

~33% of U.S. adults estimated to have NAFLD — most undiagnosed
60% of circulating T3 (active thyroid hormone) is converted in the liver
~80% of NAFLD patients who develop T2DM have significant liver involvement

The liver is also the primary site of T4-to-T3 conversion. Thyroxine (T4), the storage form of thyroid hormone produced by the thyroid gland, is biologically inactive. The liver must convert it to triiodothyronine (T3) — the form that actually runs your metabolism. A fatty, inflamed liver converts less T4. The result is functional hypothyroidism that the standard TSH test cannot detect.

The liver is also the organ that clears excess insulin from the bloodstream. When liver function is impaired, insulin clearance slows. Circulating insulin rises. Cells that were never designed to tolerate constant insulin exposure begin to resist it. Blood sugar rises in response. The pancreas produces more insulin to compensate. The liver gets worse. The thyroid gets worse. The kidneys, forced to filter an increasingly dysregulated bloodstream, come under chronic pressure.

What Ray Peat documented

Bioenergetics researcher Ray Peat spent decades arguing that PUFA accumulation in tissues is the primary driver of metabolic suppression — not carbohydrates, not thyroid disease per se, but the stored oxidative load of decades of seed oil consumption. Peat's position was that PUFAs suppress the activity of enzymes required for thyroid hormone conversion and mitochondrial energy production. His framework prioritized restoring metabolism through nourishing, easily oxidizable foods — not restriction. He was largely ignored by mainstream nutrition science until the oxidized linoleic acid hypothesis began generating independent confirmation after 2015.

Peat R. "Unsaturated fatty acids: nutritionally essential, or toxic?" Ray Peat's Newsletter. 2007. | Buzzetti E et al. "The multiple-hit pathogenesis of non-alcoholic fatty liver disease (NAFLD)." Metabolism. 2016;65(8):1038–1048. | Jian-Gao F. "A national workshop on nonalcoholic fatty liver disease." Chinese Journal of Hepatology. 2003. | Lonardo A et al. "Nonalcoholic fatty liver disease and thyroid." International Journal of Molecular Sciences. 2019;20(11):2875.
The Conversion Problem

Your Thyroid Labs Are Normal. Your Thyroid Isn't.

Most people with sluggish metabolism, persistent fatigue, cold hands and feet, hair loss, constipation, and low body temperature are told their thyroid is fine because their TSH falls within the reference range. The TSH measures the signal sent to the thyroid — not what the thyroid actually produces, and certainly not how well the liver is converting that production into active hormone.

When T4-to-T3 conversion is impaired, the body often shunts T4 into reverse T3 (rT3) instead. Reverse T3 is biologically inert — it occupies the same cellular receptors as active T3, blocking the receptors without activating them. The thyroid is technically working. The signal is there. Nothing downstream is receiving it. This is a liver problem being diagnosed as a thyroid problem.

"The thyroid gland produces a storage hormone. The liver converts it into the active form that runs your metabolism. A fatty liver converts less. Your energy follows."

Morley Robbins, founder of the Root Cause Protocol and author of Cu-RE Your Fatigue, maps this disruption along a different axis — the mineral triad of magnesium, copper, and iron. His argument: unbound iron accumulates in the liver when ceruloplasmin (a copper-dependent protein) is low. This unbound iron drives oxidative stress directly in the liver — compounding PUFA-driven injury — and simultaneously disrupts the enzyme pathways required for thyroid hormone synthesis and conversion.

The standard metabolic panel does not include ceruloplasmin. It does not include a free copper assay. It does not include serum magnesium (as distinct from the plasma magnesium that standard labs measure, which is regulated independently of intracellular magnesium levels). The connections between mineral dysregulation, liver function, and thyroid conversion are real, measurable, and almost universally untested in clinical practice.

Body temperature and hydration — what Matt Stone observes

Author Matt Stone, in his book Eat for Heat, argues that core body temperature is the most honest indicator of metabolic rate — and one that most practitioners never measure. A normal waking oral temperature is generally cited as 97.8–98.6°F. Stone's position: chronic undereating, restriction, low-carb diets, and cold exposure all drive body temperature down over time, signaling cellular hypothyroidism even when labs appear normal. The intervention is not a supplement — it is nourishing the body at a level that allows temperature to normalize. Restriction, he argues, is what caused the suppression; more restriction cannot reverse it.

Urine color as a hydration guide

One of Stone's more counterintuitive observations — and one backed by nephrology research — is that the conventional advice to "drink until your urine is clear" is a sign of overhydration, not optimal health. Stone uses urine color as a simple hydration marker:

Clear

Overhydrated — dilutes electrolytes, lowers body temperature, stresses kidneys

Pale Yellow

Well hydrated — the observed sweet spot

Dark Amber

Underhydrated — drink to thirst, prioritize mineral-rich fluids

Stone's argument: chronic overhydration — driven by the "eight glasses a day" rule — dilutes sodium and electrolytes in the blood, triggering a compensatory stress response (elevated cortisol, ADH) that suppresses metabolism and lowers body temperature. Drinking to thirst rather than to a quota, and avoiding large amounts of plain water with meals (which dilutes stomach acid and digestive enzymes), are consistent observations in his framework. Mineral-rich fluids — broths, water from mineral-dense springs — are preferable to large volumes of plain water.

Robbins M. Cu-RE Your Fatigue: The Root Cause and How to Fix It on Your Own. Morley Robbins. 2021. | Stone M. Eat for Heat: The Metabolic Approach to Food and Drink. CreateSpace. 2012. | Abdalla SM, Bianco AC. "Defending plasma T3 is a biological priority." Clinical Endocrinology. 2014;81(5):633–641. | Iwen KA et al. "Thyroid hormones and the metabolic syndrome." European Thyroid Journal. 2013;2(2):83–92.
Downstream Damage

When the Kidneys Pay the Price

The kidneys are meticulous filtration organs. They rely on precise signals — from the liver, from the endocrine system, from blood pressure regulators — to determine how aggressively to filter, what to retain, and what to excrete. When those upstream signals are disrupted by a failing liver and a sluggish thyroid, kidney function degrades in predictable ways.

Fatty liver disease and chronic kidney disease (CKD) share a striking epidemiological overlap. Studies consistently find that NAFLD patients have significantly higher rates of CKD than matched controls — independent of diabetes, hypertension, or obesity. The mechanisms include reduced hepatic production of angiotensinogen (affecting blood pressure regulation at the kidney), lipid accumulation in kidney tubules, and the chronic inflammatory milieu created by an overtaxed liver that the kidneys must filter.

Thyroid hormone, for its part, directly regulates kidney filtration rate (GFR). Hypothyroid states — including subclinical, conversion-level hypothyroidism — are associated with reduced renal plasma flow and reduced GFR. The kidney is doing less with more pressure. Proteinuria, the leakage of protein into urine that marks early kidney damage, is more prevalent in patients with low-normal T3.

Ix JH, Sharma K. "Mechanisms linking obesity, chronic kidney disease, and fatty liver disease: the roles of fetuin-A, adiponectin, and AMPK." Journal of the American Society of Nephrology. 2010;21(3):406–412. | Speeckaert MM et al. "The thyroid and the kidney: a complex interplay." Frontiers in Endocrinology. 2020;11:496. | Mikolasevic I et al. "Nonalcoholic fatty liver disease and chronic kidney disease: is there a link?" World Journal of Nephrology. 2016;5(3):215–225. | Chaker L et al. "Subclinical and overt hypothyroidism is associated with reduced glomerular filtration rate and proteinuria: a large cross-sectional population study." Sci Rep. 2018;8:10852. PMID 29666509.
The End of the Cascade

Blood Sugar Is Not the Beginning. It's the Alarm.

The standard medical narrative frames type 2 diabetes as a blood sugar problem — the result of eating too many carbohydrates over a lifetime, leading to insulin resistance. The intervention is therefore to reduce carbohydrates, add metformin, and eventually insulin. The problem with this framework is not that blood sugar is irrelevant — it is that treating blood sugar without addressing the liver, the thyroid, and the accumulated PUFA load is treating the alarm, not the fire.

Insulin resistance begins in the liver, not in the muscle. A fatty liver's inability to clear circulating insulin is what creates the hyperinsulinemic state that eventually exhausts the pancreatic beta cells. By the time blood sugar is flagged on a routine panel, insulin has already been elevated for years. HbA1c, the standard 3-month blood sugar average, becomes elevated only after the liver has been compromised long enough that it can no longer compensate.

Isaac Pohlman and the Carb Sweet Spot

Isaac Pohlman of The Pohlman Institute has developed what he calls the "Carb Sweet Spot" — an individualized approach to carbohydrate intake based on the recognition that glucose tolerance is not fixed. It changes with activity level, time of day, season, mineral status, and the metabolic capacity of the individual. His framework categorizes carbohydrates by their impact profile:

Green — Lowest Impact

Fruit — whole, ripe, in season. Natural sugars with fiber, minerals, and enzymatic cofactors intact. Well tolerated by most metabolic types.

Yellow — Moderate Impact

Winter squash, pumpkin, butternut — starchy vegetables with good mineral density. Generally well tolerated with protein.

Orange — Higher Starch

Root vegetables — potatoes, sweet potatoes, carrots, beets. Higher glucose impact; timing matters more here. Best at midday when metabolic rate is highest.

Red — Highest Starch

Grains — rice, oats, bread, corn. Highest glucose impact per gram; most appropriate for higher-activity individuals or those with established carb tolerance.

Pohlman's key insight: the goal is not to eliminate carbohydrates but to find the individual's tolerance window — and work within it while rebuilding the metabolic infrastructure (minerals, liver health, circadian rhythm) that allows that window to expand over time. His recommended testing: HTMA (Hair Tissue Mineral Analysis) for intracellular mineral status, blood sugar panel (fasting glucose + 2-hour post-meal), and Full Monty lab panel for a complete hormonal and metabolic picture.

Two variables that worsen insulin resistance — and are rarely discussed

High dietary fat and insulin resistance: The relationship between fat intake and insulin sensitivity is more nuanced than the saturated-fat narrative suggests. Research on what's called the Randle cycle (the glucose-fatty acid cycle) documents that excess fat in circulation — regardless of source — competes with glucose for cellular uptake, directly impairing insulin sensitivity. This is part of the reasoning behind Griggs's 10–15% dietary fat target during the phase of active insulin resistance reversal: lower fat intake allows cells to oxidize glucose more freely. This does not mean fat is the enemy long-term — it means that during active metabolic dysfunction, a high-fat dietary approach may compound the insulin signaling problem rather than resolve it.

Low sodium intake and insulin resistance: The push to reduce dietary salt has a metabolic consequence that is rarely disclosed. When sodium intake drops below what the body needs, the renin-angiotensin-aldosterone system (RAAS) activates to conserve sodium. Aldosterone — the hormone released in this process — directly promotes insulin resistance at the cellular level. Research by James DiNicolantonio and others documents that low-sodium diets are associated with elevated insulin levels, elevated triglycerides, and increased cardiovascular risk. Adequate salt from whole food sources appears to support insulin sensitivity, not impair it. The salt-heart disease link was built on flawed epidemiology; the insulin-salt connection is mechanistic and documented.

This is a critical distinction for women specifically. Carbohydrate metabolism in women is not the same as in men. Keto and extended fasting studies have been conducted overwhelmingly in male subjects. The female hormonal system — particularly progesterone and estrogen — requires glucose as a co-substrate. Long-term carbohydrate restriction in women frequently produces elevated cortisol, disrupted menstrual cycling, impaired T4-to-T3 conversion, and the metabolic symptoms of hypothyroidism. Restriction causes the suppression it claims to fix.

Pohlman I. The Carb Sweet Spot Masterclass. The Pohlman Institute. thepohlmaninstitute.com. | Lustig RH et al. "Isocaloric fructose restriction and metabolic improvement in children with obesity and metabolic syndrome." Obesity. 2016;24(2):453–460. | Samuel VT, Shulman GI. "Mechanisms for insulin resistance: common threads and missing links." Cell. 2012;148(5):852–871. | Kelley DE et al. "Dysfunction of mitochondria in human skeletal muscle in type 2 diabetes." Diabetes. 2002;51(10):2944–2950. | DiNicolantonio JJ, O'Keefe JH. "The wrong white crystals: not salt but sugar as aetiological in hypertension and cardiometabolic disease." Open Heart. 2014;1(1):e000167. | Kackley ML et al. "Self-reported menses physiology is positively modulated by a well-formulated ketogenic diet vs. low fat diet in women of reproductive age." PLOS ONE. 2024;19(4):e0293670.
The Root Cause Underneath the Root Cause

Light, EMF, and the Circadian Layer

In clinical practice, there is a pattern that does not show up in the standard seed oil or carbohydrate narratives: patients who change their diet dramatically and still cannot move the needle on weight, blood sugar, or thyroid function. The missing variable — consistently — is the circadian environment.

The liver runs on a clock. Every metabolic function — bile acid synthesis, glycogen storage, insulin sensitivity, T4-to-T3 conversion — is regulated by circadian timing signals. Those signals originate in the brain's suprachiasmatic nucleus, which sets the master clock based on light input through the retina. When the light environment is disrupted — by artificial blue light at night, by lack of morning sunlight, by sleeping in a room bathed in electronic devices — the liver's clock desynchronizes from the master clock. Metabolic function degrades even when food choices are good.

The timeline of metabolic disease correlates not only with the introduction of seed oils (post-1900) but also with the introduction of artificial light (electric lighting, post-1880), television (1950s), and 24-hour backlit screens (2007 onward). These are not coincidences. They are overlapping circadian disruptions with additive effects on liver and metabolic function.

Modern Metabolic Timeline

What Changed — and When

1880s

Electric lighting introduced — first circadian disruption at scale. Humans no longer follow sunset. Artificial light at night suppresses melatonin and begins desynchronizing the liver clock from the light/dark cycle.

1911

Crisco launched — the first mass-market industrial seed oil (partially hydrogenated cottonseed oil). Animal fat begins its century-long replacement in the American kitchen.

1950s

Television in the living room — the first nightly blue-light emitter at eye level. Sedentary evening behavior plus artificial blue light begins compounding melatonin suppression for the whole household, every night.

1970s – 80s

Seed oil consumption surges — "low-fat" dietary guidelines direct the population toward a combination of refined carbohydrates and vegetable oil. Animal fat is officially demonized. PUFA intake reaches historically unprecedented levels.

2007

iPhone launched — a backlit touchscreen carried constantly, including into the bedroom. Average sleep duration begins declining in population-level data. The circadian light signal is now disrupted around the clock, not just in the evening.

2010 – Present

Smart TVs, streaming, LED lighting — artificial blue-spectrum light now in every room, at the highest output levels in human history. Non-native EMF from Wi-Fi, smart devices, and wireless infrastructure reaches saturation in most developed-world homes and workplaces.

The non-native electromagnetic field (EMF) burden adds another layer. Preliminary research suggests that RF/microwave radiation — from Wi-Fi routers, smartphones, and wireless devices — disrupts melanopsin signaling and melatonin production. Melanopsin photoreceptors are not limited to the retina: they are also present in the skin and subcutaneous fat, making the body's light-sensing apparatus broadly vulnerable to electromagnetic interference. If the circadian signal is corrupted by both artificial light and RF exposure simultaneously, the liver's metabolic timing is doubly disrupted.

Balmori A. "Electromagnetic pollution from phone masts. Effects on wildlife." Pathophysiology. 2009;16(2–3):191–199. | Halgamuge MN. "Pineal melatonin level disruption in humans due to electromagnetic fields and ICNIRP limits." Radiat Prot Dosimetry. 2013;154(4):405–416. PMID 23051584.

A bed with a smartphone charging 18 inches from the head, a smart TV opposite, a Wi-Fi router in the hall, and no morning sunlight is not a food problem. No dietary intervention will fully overcome a chronically dysregulated circadian environment. This is why sequencing matters.

Figueiro MG et al. "Light at night and measures of urinary melatonin and estrogen metabolites in female night shift workers." Cancer Epidemiology, Biomarkers and Prevention. 2012. | Morris CJ et al. "Circadian misalignment increases cardiovascular disease risk factors in humans." Proceedings of the National Academy of Sciences. 2016;113(10):E1402–E1411. | Fonken LK et al. "Light at night increases body mass by shifting the time of food intake." Proceedings of the National Academy of Sciences. 2010;107(43):18664–18669. | Panda S. The Circadian Code. Rodale Books. 2019.
The Intervention

Protect the Liver First

If the liver is the hub where the cascade begins, then liver recovery is where the cascade ends. This does not require a supplement protocol or a detox cleanse. It requires removing what is injuring the liver — seed oils, chemical personal care products, and circadian disruption — and nourishing it with what allows it to repair: dense whole foods, minerals, movement, and light.

The liver is under chemical pressure from more than just food. Personal care products — conventional shampoos, lotions, deodorants, and fragrances — contain compounds (phthalates, parabens, synthetic musks) that are absorbed transdermally and processed by the liver. In a liver that is already inflamed and fatty, this added processing burden is not trivial. Cleaning up personal care is not aesthetics. It is liver load.

What researchers and practitioners in this space observe supports liver recovery

  • Removing seed oils — the primary source of PUFA-driven liver injury; practitioners in this space consistently prioritize this above all other dietary changes
  • Adequate dietary protein — supports liver cell repair and albumin synthesis; individual requirements vary and are best determined with practitioner support
  • Dense whole-food carbohydrates — real food glucose is liver fuel; the research suggests restriction without adequate nourishment does not support recovery
  • Mineral status — magnesium, copper, and iron regulation; Morley Robbins's work identifies this as foundational to liver oxidative capacity
  • Bile flow — beets, dandelion greens, and bitter foods are commonly cited for supporting bile production; bile is how the liver exports damaged lipids and metabolic waste
  • Morning sunlight — the circadian liver clock depends on retinal light input; this is documented in published circadian biology research
  • Evening darkness — melatonin onset signals the liver's overnight repair cycle; artificial blue light delays that signal
  • Reduced chemical load in personal care — phthalates, parabens, and synthetic fragrance are hepatically processed; lower daily exposure reduces the liver's processing burden

What the clinical and research literature does not support is restriction for its own sake. Practitioners working in this space consistently observe that patients directed to eat less, restrict carbohydrates, and fast often end up with lower body temperatures, worse thyroid conversion, and more metabolic suppression than before. The body does not repair a damaged liver by starving it.

"You can't restrict a fatty liver into a healthy one. You can only remove what caused the damage, and give the body what it needs to rebuild."

The timeline for recovery is not weeks. Seed oil half-life in human adipose tissue has been measured at approximately two years. Full PUFA tissue turnover takes closer to four to six years of consistent change. Body temperature, thyroid conversion, and blood sugar regulation typically begin improving within 3–6 months of consistent intervention — but the depth of recovery is determined by time and consistency, not intensity.

Guyenet SJ, Carlson SE. "Increase in adipose tissue linoleic acid of US adults in the last half century." Adv Nutr. 2015;6(6):660–664. PMID 26567191. (Half-life of linoleic acid incorporation into adipose tissue: ~680 days.)

What the Research Points To

The researchers and practitioners cited in this article tend to address the cascade in a consistent sequence — because the order matters. Changing food without addressing the circadian environment produces partial results. Addressing circadian without removing seed oils produces partial results. What follows is a distillation of what that body of work consistently points toward — not a treatment plan, and not a substitute for working with a practitioner who can assess your individual situation.

A tool researchers and practitioners use: waking body temperature

Matt Stone, in Eat for Heat, and practitioners working in the bioenergetics tradition use waking oral temperature as a proxy for metabolic rate — measuring it for several consecutive mornings before getting out of bed and averaging the readings. A normal waking oral temperature is generally cited as 97.8–98.6°F. Stone and others observe that readings consistently lower than this range correlate with metabolic suppression. This is not a diagnostic tool — it is a pattern-tracking data point that some practitioners find useful for gauging metabolic trend over time.

Layer 1 — Remove the Primary Injury

1

Seed oil removal: why it comes first

Zane Griggs and others in this space treat seed oil removal as the non-negotiable starting point — not a reduction, but a full removal of soybean, canola, safflower, sunflower, corn, cottonseed, grapeseed, and rice bran oils. The reasoning: these are the direct source of oxidized linoleic acid that accumulates in liver tissue. Stable animal fats (butter, ghee, tallow, lard) and coconut oil are what practitioners in this tradition cook with instead. Hidden sources are the main obstacle — most packaged foods, restaurant cooking, and pre-made dressings use industrial seed oils. Label reading matters here.

2

Restaurant food: the hidden seed oil problem

Virtually all restaurant cooking — including high-end restaurants — uses industrial seed oils. This is not a judgment; it is an economic and shelf-life reality. Practitioners working with this framework note that meaningful seed oil reduction is difficult to achieve while eating most restaurant food regularly. Cooking at home from whole ingredients eliminates the guesswork. Where restaurants are unavoidable, asking specifically about cooking fats — and choosing places that use butter or animal fats — is the practical workaround.

3

Clean up personal care

Replace conventional products containing synthetic fragrance ("parfum"), parabens, and phthalates with alternatives using EWG Skin Deep or the Think Dirty app. Priority items: deodorant, shampoo/conditioner, lotion, and any fragrance sprays. These compounds are processed by the liver every day — removing them reduces liver processing load immediately.

Layer 2 — Nourish

4

Protein as the dietary anchor

Griggs's framework emphasizes protein as the structural anchor of every meal — whole food sources like eggs, beef, lamb, poultry, fish, and organ meats. He and others in this space observe that adequate protein intake supports liver cell repair, albumin synthesis, and satiety in ways that reduce the drive toward processed foods. Circadian research also notes that eating a substantial first meal early in the day — rather than skipping breakfast — appears to signal the liver's metabolic clock to activate. Exact requirements vary by individual and are best determined with a qualified practitioner who can assess body composition and metabolic status.

5

Understand carbohydrate tolerance — it is not fixed

Research and practitioners in this space consistently observe that carbohydrate tolerance is not a static trait — it shifts with mineral status, activity level, circadian rhythm, and the overall health of the liver. Isaac Pohlman's framework notes that whole-food carbohydrates — fruit, squash, root vegetables — tend to be tolerated differently than grain-based starches, and that pairing carbohydrates with protein appears to affect the glycemic response. Ray Peat's work documents that very low carbohydrate intake suppresses T4-to-T3 conversion in the liver; published research supports a threshold below which thyroid conversion begins to decline. How an individual responds to different carbohydrate sources, quantities, and timing is something a qualified practitioner working with you directly — and your own lab work — can help clarify. This is not an area for self-prescription.

6

Prioritize dense whole foods at every meal

Whole food means one ingredient. Beef is a whole food. Beef jerky made with dextrose and soybean oil is not. Potato is a whole food. Potato chips fried in canola oil are not. Butter is a whole food. Margarine is not. The guiding question is always: is this food as close to its natural state as possible, with nothing added that wouldn't have been in a kitchen before 1900?

7

Hydration: urine color over fluid quotas

The conventional advice to drink eight glasses of water daily and aim for clear urine is contradicted by both nephrology research and the observations of practitioners like Matt Stone. Stone documents that chronic overhydration — drinking beyond thirst, especially plain water — dilutes blood sodium and electrolytes, triggering a cortisol and antidiuretic hormone response that suppresses metabolism and lowers body temperature. Clear urine is a sign of overhydration, not optimal health. The observed markers: pale yellow indicates appropriate hydration; clear indicates excess; dark amber indicates genuine dehydration. Stone recommends drinking to thirst rather than to a quota, and avoiding large amounts of plain water immediately before or during meals, which dilutes stomach acid and digestive enzymes. Mineral-rich fluids — bone broth, spring water, water with adequate natural minerals — are observed to support hydration more effectively than plain water at high volume.

8

Bile flow and why fat restriction backfires

The liver exports damaged lipids and metabolic waste via bile — and bile release from the gallbladder is triggered by dietary fat. This is why very low-fat diets are observed to impair detoxification: without adequate fat intake, bile stagnates and the compounds the liver was trying to remove recirculate. Bitter foods — arugula, radicchio, dandelion greens, lemon juice — are traditionally used before meals to stimulate bile production. Beets (raw, roasted, or as beet kvass) are commonly cited in liver-support literature. Movement after meals is also observed to support bile flow mechanically.

Layer 3 — Reset the Circadian Environment

9

Morning sunlight within 30 minutes of waking

Direct outdoor light exposure within the first 30 minutes of waking sets the master circadian clock via the retinal melanopsin pathway — which in turn sets the liver's metabolic clock, cortisol rhythm, insulin sensitivity, and thyroid hormone production timing. The quality of this signal depends on two things: eyes and skin. Eyes open to the sky (no sunglasses, no glass window) delivers the retinal signal. Exposed skin — arms, legs, as much surface as is practical — absorbs light photons directly, which research suggests activates additional photoreceptor pathways in skin cells independent of the retinal clock. The more skin exposed, the stronger the signal. Longer is better. A minimum of 10–20 minutes is commonly cited in circadian research; an hour or more, especially in the first half of the day, compounds the metabolic benefit. On overcast days, exposure time increases because cloud cover reduces lux — 45–60 minutes accomplishes what 15 minutes of direct sun does. A window does not substitute; glass filters the UV and near-infrared frequencies that carry the biological signal.

10

Protect the evening light environment

After sunset, eliminate or dramatically reduce blue-spectrum light. Options in order of effectiveness: no screens after sunset; blue-blocking glasses (must filter to 550nm — orange or red lens, not the yellow "computer glasses"); dim warm-toned lighting only; Iris or f.lux software on all screens if screens are unavoidable. The goal is to allow melatonin onset to occur at its natural time — typically 2–3 hours after sunset. Melatonin is not a sleep supplement. It is the liver's nighttime repair signal.

Sasseville A et al. "Blue blocker glasses impede the capacity of bright light to suppress melatonin production." J Pineal Res. 2006;41(1):73–78. PMID 16842544. | West KE et al. "Blue light from light-emitting diodes elicits a dose-dependent suppression of melatonin in humans." J Appl Physiol. 2011;110(3):619–626. PMID 21164152.
11

Reduce EMF burden in the sleeping space

The bedroom is where the body spends 7–9 hours in its deepest repair state. Phone charging in another room (or on airplane mode). Router on a timer to power off at bedtime — but a router timer only works if every device that talks to it is also off. A smart TV in standby mode continues transmitting Wi-Fi and Bluetooth signals even when the screen is dark; it needs to be fully unplugged, not just turned off, for the router shutoff to actually reduce RF in the room. The same applies to streaming sticks, smart speakers, and cable boxes with wireless radios. Minimize electric field exposure from bedside lamps and cords — unplug what isn't in use. A low-EMF sleep environment is not about fear — it is about giving the liver and nervous system the undisturbed quiet they need to run overnight metabolic repair.

12

Meal timing and the liver's overnight repair window

Circadian biology research consistently shows that eating in the hours immediately before sleep shifts the liver's metabolic clock and impairs overnight repair. The liver's peak detoxification and regeneration activity occurs during sleep — and that activity is suppressed when it is still processing a recent meal. Practitioners in this space observe that front-loading calories earlier in the day and allowing a gap between the last meal and sleep appears to support this repair window. This is a timing observation, not a restriction — total nourishment during waking hours is the goal.

Layer 4 — Track and Test

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Waking body temperature as a trend marker

Practitioners using the bioenergetics framework observe that waking body temperature tends to trend upward as metabolic function improves — and that it tends to remain suppressed when seed oil exposure continues (often hidden in restaurant meals or packaged foods), mineral deficiency is significant, or the circadian environment hasn't changed. Stone and others use temperature trending over weeks or months — not a single reading — as a pattern indicator. A trend upward is generally read as a positive metabolic signal; a flat or declining trend points back to unresolved upstream factors. This is not a diagnostic measure and should be considered alongside other clinical assessments.

Use our printable basal body temperature chart to track your waking readings over time.

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HTMA mineral testing — one tool among several

Hair Tissue Mineral Analysis (HTMA) measures mineral levels deposited in hair over the previous 3 months — in theory offering a window into intracellular mineral status that blood serum testing doesn't capture well (serum minerals are tightly regulated independently of cellular stores). Morley Robbins and practitioners trained in the Root Cause Protocol use it specifically to assess the magnesium/copper/iron relationship. That said, HTMA has real limitations: hair products, dyes, bleach, and chemical treatments all affect results and can render a sample unreliable. It is one data point among several — useful for pattern recognition when interpreted by a practitioner who understands its limitations, not a standalone diagnostic. Some practitioners use it as a starting reference and retest periodically; others weight it more lightly and rely on it only alongside blood work and symptom picture.

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Lab panels worth requesting

For a fuller metabolic picture: fasting insulin (not just fasting glucose — insulin rises first); 2-hour post-meal glucose; Free T3 and Reverse T3 (not just TSH); ALT and AST (liver enzymes); GGT; ferritin; serum ceruloplasmin; RBC magnesium (not standard serum magnesium); uric acid. Bring these requests to your provider — many are standard panels that simply aren't ordered routinely.

Studies & Resources

These sources represent a range of frameworks and methodologies. They are presented as perspectives worth examining, not as unified consensus. Read them yourself. Consider who funded them and who didn't. Form your own conclusions.

Frameworks & Independent Researchers

Zane Griggs — Fit Over 40

The Fit Over 40 Framework

Griggs's framework documents the parallel rise of seed oil consumption and metabolic disease incidence, and argues that the removal of saturated fat from the food supply — replaced with polyunsaturated vegetable oils — is the primary driver. His protocol is protein-anchored, carbohydrate-permissive (whole food sources), and explicitly anti-seed oil. Available through his website and coaching programs.

Isaac Pohlman — The Pohlman Institute

The Carb Sweet Spot Masterclass & The Pohlman Method

Pohlman's work focuses on individualized carbohydrate tolerance as a function of mineral status, metabolic health, and circadian timing. His carb-typing system (fruit → squash → root veg → grains) provides a practical framework for reintroducing carbohydrates without triggering blood sugar dysregulation. Pairs with HTMA testing for mineral assessment. thepohlmaninstitute.com

Ray Peat — Bioenergetics

Unsaturated Fatty Acids and Metabolic Suppression

Peat's extensive newsletter archive covers PUFA accumulation in tissue, thyroid hormone activation, mitochondrial function, and the relationship between oxidized linoleic acid and degenerative disease. His work is dense, referenced, and largely unpublished in peer-reviewed form — but it preceded much of the seed oil research now appearing in mainstream journals. raypeat.com (archive)

Morley Robbins — Root Cause Protocol

Cu-RE Your Fatigue: The Root Cause and How to Fix It on Your Own (2021)

Robbins maps metabolic dysfunction along the magnesium-copper-iron triad. His argument: unbound (non-ceruloplasmin-bound) iron accumulates in the liver when copper metabolism is disrupted, driving oxidative damage that compounds PUFA injury. The Root Cause Protocol focuses on restoring ceruloplasmin function through whole-food copper sources, liver (the food), and magnesium. RootCauseProtocol.com

Matt Stone — 180 Degree Health

Eat for Heat: The Metabolic Approach to Food and Drink (2012)

Stone's argument is that body temperature is the most honest available signal of metabolic rate, and that chronic restriction — including low-carb diets, fasting, and undereating — drives temperature down and suppresses metabolism. His intervention is nourishment, not restriction. 180degreehealth.com

Peer-Reviewed Research

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DiNicolantonio JJ, O'Keefe JH. "Omega-6 vegetable oils as a driver of coronary heart disease: the oxidized linoleic acid hypothesis." Open Heart. 2018;5(2):e000898. Proposes that oxidized linoleic acid — the primary PUFA in seed oils — is the actual mediator of cardiovascular and metabolic disease; reviews mechanistic and epidemiological evidence.
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Ramsden CE et al. "Re-evaluation of the traditional diet-heart hypothesis: analysis of recovered data from Minnesota Coronary Experiment (1968–73)." BMJ. 2016;353:i1246. Recovery of suppressed RCT data showing that replacing saturated fat with linoleic acid (from vegetable oil) increased mortality — findings that were never published in the original trial.
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Lonardo A et al. "Nonalcoholic fatty liver disease and thyroid." International Journal of Molecular Sciences. 2019;20(11):2875. Systematic review of the NAFLD–thyroid connection, including evidence that low-normal thyroid function impairs hepatic fat metabolism and that NAFLD impairs T4-to-T3 conversion.
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Buzzetti E et al. "The multiple-hit pathogenesis of non-alcoholic fatty liver disease (NAFLD)." Metabolism. 2016;65(8):1038–1048. Reviews the mechanisms by which NAFLD progresses from simple steatosis to NASH to cirrhosis, including the role of dietary fat quality, gut microbiome disruption, and oxidative stress.
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Ix JH, Sharma K. "Mechanisms linking obesity, chronic kidney disease, and fatty liver disease: the roles of fetuin-A, adiponectin, and AMPK." Journal of the American Society of Nephrology. 2010;21(3):406–412. Documents the shared mechanisms by which NAFLD drives CKD progression, including hepatic protein synthesis disruption and inflammatory signaling.
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Morris CJ et al. "Circadian misalignment increases cardiovascular disease risk factors in humans." Proceedings of the National Academy of Sciences. 2016;113(10):E1402–E1411. Controlled study showing that circadian misalignment (shifted sleep/light schedule) impairs insulin sensitivity, blood pressure, and inflammatory markers within days.
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Fonken LK et al. "Light at night increases body mass by shifting the time of food intake." Proceedings of the National Academy of Sciences. 2010;107(43):18664–18669. Animal study demonstrating that exposure to light at night increases body mass even when total caloric intake is unchanged — through circadian timing disruption of metabolic signaling.
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Speeckaert MM et al. "The thyroid and the kidney: a complex interplay." Frontiers in Endocrinology. 2020;11:496. Reviews bidirectional thyroid-kidney relationships, including evidence that hypothyroid states — even subclinical — reduce GFR and increase proteinuria risk.
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Samuel VT, Shulman GI. "Mechanisms for insulin resistance: common threads and missing links." Cell. 2012;148(5):852–871. Landmark review establishing that hepatic insulin resistance — not peripheral muscle resistance — is the primary initiating event in T2DM pathogenesis.
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Abdalla SM, Bianco AC. "Defending plasma T3 is a biological priority." Clinical Endocrinology. 2014;81(5):633–641. Explains how the body prioritizes maintaining circulating T3 even at the expense of tissue T3, why TSH does not reflect tissue thyroid status, and why T3/rT3 ratio matters more than TSH in clinical practice.

Prescription Drugs & Metabolic Terrain

Research documenting how commonly prescribed drug classes interrupt mitochondrial function, deplete essential nutrients, disrupt the gut microbiome, and suppress metabolic rate — mechanisms rarely disclosed at the point of prescription.

Statins — CoQ10 depletion and cardiac consequences

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Folkers K et al. "Lovastatin decreases coenzyme Q levels in humans." Proc Natl Acad Sci USA. 1990;87(22):8931–8934. PMID 2247468 Lovastatin significantly depleted blood and tissue CoQ10 in patients; in those with class IV cardiomyopathy the depletion was life-threatening until CoQ10 was supplemented. The first published documentation of statin-induced CoQ10 depletion in humans.
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Rundek T et al. "Atorvastatin decreases the coenzyme Q10 level in the blood of patients at risk for cardiovascular disease and stroke." Arch Neurol. 2004;61(6):889–892. PMID 15210526 Thirty days of atorvastatin reduced mean blood CoQ10 by approximately 50% (from 1.26 to 0.62 µg/mL). Authors suggest CoQ10 depletion underlies statin-associated muscle side effects including myalgia and rhabdomyolysis.
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Langsjoen PH et al. "Statin-Associated Cardiomyopathy Responds to Statin Withdrawal and Administration of Coenzyme Q10." Perm J. 2019;23:18–257. PMID 31496499 In 142 patients with heart failure that developed during long-term statin therapy, statin discontinuation plus CoQ10 supplementation raised mean ejection fraction from 35% to 47% and improved NYHA Class I status from 8% to 79% — suggesting statin-induced CoQ10 depletion drove the cardiomyopathy.

Metformin — Complex I inhibition and B12 depletion

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El-Mir MY et al. "Dimethylbiguanide inhibits cell respiration via an indirect effect targeted on the respiratory chain complex I." J Biol Chem. 2000;275(1):223–228. PMID 10617608 Metformin selectively inhibited mitochondrial respiratory chain Complex I in intact hepatocytes and in vivo in rats, providing the first mechanistic explanation for metformin's glucose-lowering effect — and for the lactic acidosis risk in patients with impaired mitochondrial reserve.
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Owen MR et al. "Evidence that metformin exerts its anti-diabetic effects through inhibition of complex 1 of the mitochondrial respiratory chain." Biochem J. 2000;348(Pt 3):607–614. PMID 10839993 Confirmed that metformin's primary mechanism is time- and concentration-dependent inhibition of Complex I, suppressing hepatic gluconeogenesis — and identifying why the drug carries a contraindication in conditions where mitochondrial function is already compromised.
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de Jager J et al. "Long term treatment with metformin in patients with type 2 diabetes and risk of vitamin B-12 deficiency: randomised placebo controlled trial." BMJ. 2010;340:c2181. PMID 19593117 In a 4.3-year RCT, metformin-treated patients showed a progressive 19% reduction in serum B12 levels and a significantly higher rate of clinical B12 deficiency than placebo; the authors conclude that B12 monitoring is indicated for all patients on long-term metformin therapy.

SSRIs — peripheral serotonin and metabolic disruption

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Yano JM et al. "Indigenous bacteria from the gut microbiota regulate host serotonin biosynthesis." Cell. 2015;161(2):264–276. PMID 25860609 Gut bacteria directly stimulate colonic enterochromaffin cells to produce serotonin — establishing that roughly 95% of the body's serotonin is manufactured in the gut, not the brain, where it regulates GI motility, platelet aggregation, and metabolic signaling rather than mood.
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Chen X et al. "Reduced serotonin reuptake transporter (SERT) function causes insulin resistance and hepatic steatosis independent of food intake." PLoS One. 2012;7(3):e32511. PMID 22412882 SERT-deficient mice (pharmacologically equivalent to SSRI-treated animals) developed insulin resistance, glucose intolerance, and fatty liver despite eating less than controls — demonstrating that blocking peripheral serotonin reuptake produces metabolic dysfunction through mechanisms independent of appetite.
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Crane JD et al. "Inhibiting peripheral serotonin synthesis reduces obesity and metabolic dysfunction by promoting brown adipose tissue thermogenesis." Nat Med. 2015;21(2):166–172. PMID 25485911 Blocking peripheral serotonin synthesis protected mice from high-fat-diet-induced obesity and insulin resistance by disinhibiting thermogenesis in brown adipose tissue — demonstrating that elevated peripheral serotonin (as with chronic SSRI use) actively suppresses fat burning.

Corticosteroids — mitochondrial suppression and tissue destruction

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Du J et al. "Dynamic regulation of mitochondrial function by glucocorticoids." Proc Natl Acad Sci USA. 2009;106(9):3543–3548. PMID 19202080 Glucocorticoids regulate mitochondrial function in a biphasic, dose-dependent manner — low doses enhance mitochondrial activity, while chronic high doses inhibit mitochondrial function and impair neural plasticity; a mechanistic basis for why long-term steroid use damages every organ system that depends on mitochondrial output.
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Hwang JL, Weiss RE. "Steroid-induced diabetes: a clinical and molecular approach to understanding and treatment." Diabetes Metab Res Rev. 2014;30(2):96–102. PMID 24123849 Glucocorticoid therapy causes clinically significant hyperglycemia and steroid-induced diabetes through reduced insulin secretion and peripheral insulin resistance; these drug-induced metabolic effects produce preventable hospitalizations and are frequently attributed to the patient's underlying condition rather than the treatment.
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Canalis E. "Mechanisms of glucocorticoid-induced osteoporosis." Curr Opin Rheumatol. 2003;15(4):454–457. PMID 12819474 Glucocorticoids reduce bone formation by suppressing osteoblast number and function while increasing bone resorption — producing a net bone loss that begins within months of treatment onset and persists for the duration of exposure, causing fractures that are attributed to the treated condition rather than the drug.

Beta-blockers — metabolic rate suppression and insulin resistance

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Lamont LS. "Beta-blockers and their effects on protein metabolism and resting energy expenditure." J Cardiopulm Rehabil. 1995;15(3):183–185. PMID 8542522 Beta-blocker therapy acutely reduces whole-body resting metabolic rate and increases protein oxidation at rest — effects that, without intervention, lead to increased body fat, loss of lean tissue, and the fatigue patients experience as a feature of their condition rather than a consequence of their treatment.
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Pollare T et al. "Sensitivity to insulin during treatment with atenolol and metoprolol: a randomised, double blind study of effects on carbohydrate and lipoprotein metabolism in hypertensive patients." BMJ. 1989;298(6681):1152–1157. PMID 2500169 In a 16-week randomized crossover trial, both atenolol and metoprolol significantly reduced insulin-mediated glucose uptake, raised fasting insulin and blood glucose, increased triglycerides, and decreased HDL cholesterol — metabolic changes that increase diabetes risk and are compounded by the weight gain the drugs also cause.

Proton pump inhibitors — nutrient depletion and gut microbiome disruption

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Lam JR et al. "Proton pump inhibitor and histamine 2 receptor antagonist use and vitamin B12 deficiency." JAMA. 2013;310(22):2435–2442. PMID 24327038 In 25,956 patients, two or more years of PPI use was associated with a 65% increased odds of vitamin B12 deficiency (OR 1.65), with dose-dependent effect — establishing that acid suppression prevents the proteolysis required to free food-bound B12 for absorption.
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Hoorn EJ et al. "A case series of proton pump inhibitor-induced hypomagnesemia." Am J Kidney Dis. 2010;56(1):112–116. PMID 20189276 Four patients on long-term PPI therapy developed severe hypomagnesemia with dangerous secondary electrolyte disturbances — hypokalemia, hypocalcemia, cardiac arrhythmias, and prolonged QT intervals; a class effect seen across all PPI agents, with magnesium deficiency compounding virtually every aspect of metabolic dysfunction.
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Imhann F et al. "Proton pump inhibitors affect the gut microbiome." Gut. 2016;65(5):740–748. PMID 26657899 Across 1,815 individuals, PPI use was associated with changes in 20% of gut bacterial taxa, reduced microbial diversity, and overgrowth of oral bacteria and opportunistic pathogens including Enterococcus, Streptococcus, and E. coli — with an effect size at the population level larger than that of antibiotics.
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Gomm W et al. "Association of Proton Pump Inhibitors With Risk of Dementia: A Pharmacoepidemiological Claims Data Analysis." JAMA Neurol. 2016;73(4):410–416. PMID 26882076 In a prospective cohort of 73,679 adults aged 75 and older, regular PPI use was associated with a significantly elevated dementia risk (adjusted HR 1.44) — consistent with PPI-driven B12, magnesium, and gut microbiome disruptions that collectively impair neurological function.

Testing Resources

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Hair Tissue Mineral Analysis (HTMA) Measures intracellular mineral levels over a 3-month window. Look for labs using the Analytical Research Labs (ARL) or Trace Elements Inc. methodology. Interpret with a practitioner trained in HTMA — raw numbers without context are not clinically useful.
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Full Monty Blood Panel (via Ulta Lab Tests or similar) Comprehensive self-pay panel including: fasting insulin, Free T3, Free T4, Reverse T3, ferritin, ceruloplasmin, RBC magnesium, uric acid, ALT, AST, GGT, homocysteine, and a standard metabolic panel. Self-pay options available without a doctor order in most states.

Books

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Robbins M. Cu-RE Your Fatigue. (2021) The Root Cause Protocol in book form — covers the magnesium/copper/iron triad, ceruloplasmin, and how to assess and restore mineral status without pharmaceutical intervention.
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Stone M. Eat for Heat. (2012) Body temperature as metabolic signal; nourishment over restriction; why undereating drives the metabolic suppression it claims to fix.
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Panda S. The Circadian Code. Rodale Books (2019) Accessible overview of circadian biology by a Salk Institute researcher — covers light, food timing, liver clock, and practical interventions. More mainstream than Peat or Robbins, but a solid entry point.
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DiNicolantonio JJ. The Salt Fix. Harmony Books (2017) Though focused on salt, provides critical context for understanding how low-sodium guidelines interact with aldosterone, kidney function, and the downstream mineral dysregulation that drives the metabolic cascade.