The Energy Code

Dr. Mike Belkowski
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The Energy Code is your blueprint for unlocking limitless vitality at the cellular level. Hosted by Dr. Mike Belkowski, this podcast dives deep into the science of your mitochondria—the true engines of health and energy. From light, water, and magnetism to groundbreaking molecules and lifestyle upgrades, each episode decodes the most effective strategies to strengthen your “Mitochondrial Matrix.” If you’re seeking cutting-edge science, practical tools, and proven methods to optimize your body and mind, you’ve just cracked the code. Check out these sources: www.biolight.shop – Instagram @biolight.shop – YouTube BioLight

  1. -5 H

    The “Hidden” Mitochondria Guardian in Pomegranates: Why Your Microbiome Decides If It Works (Ellagic Acid → Urolithin A)

    In this Energy Code Deep Dive, we go back to the foundation: why you feel energized and resilient—or wrecked and inflamed—often comes down to mitochondrial function. Using a comprehensive review on ellagic acid, we unpack the mitochondria’s central dilemma: they’re power plants that produce ATP… but they also produce reactive oxygen species (ROS)—their own “exhaust.” When ROS outpaces your internal cleanup systems, mitochondria enter a vicious cycle (“ROS-induced ROS release”), fragment, lose membrane potential, and can trigger apoptosis via cytochrome c—an early domino in organ stress and failure. Then comes the twist: ellagic acid from pomegranates, berries, and walnuts is poorly bioavailable—until your gut microbiome upgrades it into urolithins (A–D). Those urolithins act as both antioxidants and signaling molecules that flip key defense and longevity switches (NRF2, SIRT1/SIRT3), while activating mitophagy—the cell’s “quality control” that removes broken mitochondria and helps rebuild healthy ones. Finally, we go organ-by-organ through what the review suggests in models: mitochondrial protection in the liver(acetaminophen, methotrexate), kidneys (gentamicin), heart (doxorubicin, diabetic cardiomyopathy), and brain(Parkinson’s rotenone model, Alzheimer’s clearance systems)—and end with a sobering insight: antibiotics may both damage mitochondria and wipe out the very bacteria you need to make urolithins. (Educational content only, not medical advice.) - Articles Discussed in Episode: The Protective Effect of Ellagic Acid and Its Metabolites Against Organ Injuries: A Mitochondrial Perspective - Key Quotes From Dr. Mike: “When you peel back all the layers of health and longevity… you end up at the mitochondria.” “Gut health is mitochondrial health.” “The mitochondria basically pull the pin on a grenade and tell the cell to self-destruct.” “You aren’t the one processing (ellagic acid [Urolithin A])—your bacteria are.” “Mitophagy is a quality-control team—it takes out the trash.” “By wiping out gut diversity, we might be locking ourselves out of our own energy code.” - Key points The “energy code” starts at the mitochondria: not just energy production, but cell survival decisions. Mitochondria create ATP via the electron transport chain, but it “leaks,” generating ROS/free radicals. When ROS overwhelms cleanup capacity, a vicious cycle begins: ROS-induced ROS release. Damaged mitochondria swell, fragment, lose membrane potential, and can release cytochrome c → apoptosis. Ellagic acid is found in pomegranates, berries, walnuts; but has poor bioavailability on its own. The microbiome is the real refinery: gut bacteria convert ellagic acid into urolithins (A–D) that are highly bioavailable. The episode’s core reframing: “You aren’t what you eat—you’re what your bacteria do with what you eat.” Urolithins do more than “antioxidant mop-up”: they act as signaling molecules that activate NRF2 (endogenous defenses). Urolithins also activate SIRT1/SIRT3, which are longevity-linked efficiency and stress-resilience pathways. The star mechanism: mitophagy (removing broken mitochondria) + mitochondrial renewal/biogenesis (“fleet maintenance”). The review’s models suggest protective effects across organs under chemical/drug stress (liver, kidney, heart, brain). Antibiotics create a double hit: mitochondrial stress + microbiome depletion → locking you out of the urolithin pathway. Practical takeaway: mitochondrial health is a systems problem—diet + microbiome + stress/toxin exposure. - Episode timeline  0:00 – 0:33 — Framing: ditch fads; go microscopic; why you feel “conquer the world” vs “hit by a truck” 0:33 – 1:33 — Mitochondria as “masters of destiny”; intro to ellagic acid as a potential guardian 1:46 – 4:12 — The problem: mitochondrial “exhaust” (ROS), leakage, ROS-induced ROS release, swelling/fragmentation, membrane potential collapse, cytochrome c → apoptosis 4:19 – 5:03 — Where ellagic acid is found + the catch: hydrophobic → poor bioavailability 5:08 – 6:13 — The twist: microbiome as chemical refinery → urolithins A–D; “you are what your bacteria do” 6:19 – 8:49 — What urolithins do: antioxidant + signaling (NRF2), sirtuins (SIRT1/SIRT3), mitophagy + renewal 9:00 – 10:07 — Liver protection models: acetaminophen/Tylenol; methotrexate; preserving ATP and blocking cytochrome c leak 10:09 – 10:46 — Kidney protection model: gentamicin nephrotoxicity; maintaining membrane potential 10:49 – 12:08 — Heart protection: doxorubicin “red devil,” mitochondrial fission/fragmentation; diabetic cardiomyopathy via NRF2 12:14 – 13:33 — Brain: crosses BBB; Parkinson’s rotenone model (complex I); Alzheimer’s waste clearance/lysosomes 13:47 – 14:33 — Zoom out: “universal body armor” + microbiome partnership; feeding the “garden” (prebiotics/fiber) 14:45 – 15:41 — Double-edged sword of antibiotics: mitochondrial damage + microbiome wipeout; closing takeaway 15:43 – 15:59 — Wrap + call to action: “everything you do is a signal — send the right ones” - Dr. Mike's #1 recommendations: Deuterium depleted water: Litewater (code: DRMIKE) EMF-mitigating products: Somavedic (code: BIOLIGHT) Blue light blocking glasses: Ra Optics (code: BIOLIGHT) Grounding products: Earthing.com - Stay up-to-date on social media: Dr. Mike Belkowski: Instagram LinkedIn   BioLight: Website Instagram YouTube Facebook

    16 min

  2. -1 J

    Cancer Isn’t “Bad Luck” — It’s a Mitochondrial Energy Failure

    In this The Energy Code Deep Dives episode, we challenge the standard “cancer is a genetic lottery” narrative and explore a different frame: cancer as a metabolic disease rooted in mitochondrial respiratory failure. Using a 2025 mini-review from Journal of Bioenergetics and Biomembranes led by Thomas Seyfried, we revisit Otto Warburg’s original two-step hypothesis: damaged respiration (OXPHOS) → compensation via fermentation (even in oxygen). Then we unpack why a mid-century “oxygen consumption = healthy mitochondria” assumption derailed the field, and how modern data reframes that as a measurement trap. From there, the episode explains cancer’s dual-fuel reality (glucose + glutamine), why growth requires rerouting carbon “building blocks,” and the “smoking gun” nuclear transfer experiments that suggest the core defect is mitochondrial/cytoplasmic, with DNA mutations as downstream damage. Finally, we get practical with Seyfried’s press-pulse approach: a sustained “press” on glucose via ketogenic metabolic therapy, and a rhythmic “pulse” targeting glutamine—measured using the glucose-ketone index (GKI)—all aiming to starve the tumor while fueling healthy cells. (Educational content only, not medical advice.) - Articles Discussed in Episode: The Warburg hypothesis and the emergence of the mitochondrial metabolic theory of cancer - Key Quotes From Dr. Mike: “If we treat cancer as a metabolic disease… it changes everything.” “Oxygen consumption is not a reliable marker for energy production.” “Cancer is a dual-fuel disease.” “You’re starving the enemy while fueling your own army.” “Energy is what creates order… it’s what maintains your cellular identity.” - Key points The episode’s core premise: cancer may be better understood as a metabolic/energy disease than a purely genetic one. Warburg’s two-step model: respiratory damage → persistent fermentation (aerobic fermentation) for survival. Why the field pivoted: mid-century findings that some cancer cells consumed lots of oxygen led to the assumption mitochondria must be fine. The “logic trap”: oxygen consumption ≠ efficient ATP production (a “revving engine in neutral”). When mitochondria are “uncoupled,” oxygen use can rise while ATP output is impaired, producing more ROS “exhaust.” Cancer’s “missing math”: glucose fermentation alone can’t explain rapid growth → second backup source: glutamine-driven mitochondrial substrate-level phosphorylation (MSLP). Cancer becomes a dual-fuel fermentation system, producing “toxic exhaust” (lactate + succinate). Growth logic: PKM2 creates a metabolic bottleneck so carbon building blocks accumulate for biomass (membranes/DNA), not just “burned for heat.” The somatic mutation theory is challenged: mutations may be smoke damage, not the fire. Nuclear transfer experiments (as described): “bad nucleus + healthy mitochondria” stays normal; “healthy nucleus + damaged mitochondria” trends cancerous → hardware over software framing. “Oncogenic paradox” solved metabolically: diverse carcinogens share a common effect—they damage respiration. Treatment implication: press-pulse = chronic glucose restriction + intermittent glutamine inhibition, tracked via GKI. Metastasis idea discussed: fusion-hybridization with macrophage-like traits enabling movement, powered by fermentation → press-pulse could, in theory, pressure those cells too. Closing theme: energy maintains cellular order and identity; without efficient respiration, cells revert toward chaos/growth mode. - Episode timeline  0:19 – 1:13 — Hook: cancer as “bad luck” vs energy code failure; why metabolic framing changes prevention/treatment 1:17 – 1:59 — Source setup: 2025 mini-review; Warburg → Seyfried → “press-pulse” teased 2:00 – 3:24 — Warburg’s 2-step model: OXPHOS damage → aerobic fermentation (lactate with oxygen present) 3:31 – 4:31 — Why it became controversial: oxygen-consumption argument shifts field toward genetics 4:35 – 5:21 — Aha: oxygen use can be misleading; “engine revving in neutral” → ROS “exhaust,” uncoupling 5:24 – 6:57 — The “missing energy” solved: second backup generator MSLP using glutamine; succinate as waste 7:03 – 7:58 — PKM2 bottleneck: rerouting fuel into building blocks (growth materials) 8:02 – 10:23 — Genetics challenged: somatic mutation theory reframed; nuclear transfer experiments; mutations as downstream 10:35 – 12:33 — “Oncogenic paradox”: many causes share one commonality—mitochondrial respiratory damage; microscopy visuals (cristae loss) + lipid droplets as fuel pile-up 12:55 – 14:59 — Treatment payoff: press-pulse (KMT press on glucose + pulsed glutamine inhibition); GKI tracking 15:05 – 15:58 — Metastasis concept: fusion-hybridization with immune cells; fermentation-fueled spread; why press-pulse could matter 16:02 – 17:34 — Final recap + philosophy: respiration maintains differentiation; energy = order/identity - Dr. Mike's #1 recommendations: Deuterium depleted water: Litewater (code: DRMIKE) EMF-mitigating products: Somavedic (code: BIOLIGHT) Blue light blocking glasses: Ra Optics (code: BIOLIGHT) Grounding products: Earthing.com - Stay up-to-date on social media: Dr. Mike Belkowski: Instagram LinkedIn   BioLight: Website Instagram YouTube Facebook

    18 min

  3. -2 J

    Your Skin Is a Metabolic Engine: The Mitochondria Link to Aging, Weight Gain & Blood Sugar

    Most of us think of skin as a wrapper on our body; something to moisturize, protect, and maybe “anti-age.” But this Deep Dive flips that assumption: your skin is a major metabolic organ, and the mitochondria inside the outer layer (the epidermis) may influence far more than wrinkles. In this episode, we break down research suggesting that epidermal aging is driven primarily by mitochondrial decline(a “battery problem”), not classic senescent “zombie cells.” Then the real shocker: when the skin’s mitochondrial furnace goes offline, the body may burn less fat, store more adipose tissue, and show higher fasting blood glucose—even when everything else looks “normal.” We explore the elegant mouse model that isolated skin mitochondrial failure, the downstream effects (hair thinning, delayed wound healing), and why this research strengthens the case for mitochondrial-support strategies—from targeted nutrients to photobiomodulation principles that aim to stimulate ATP production via cytochrome c oxidase. (Educational content only, not medical advice.) - Articles Discussed in Episode: Aging-Associated Mitochondrial Decline Accelerates Skin Aging and Obesity - Key Quotes From Dr. Mike: “What if what you’re looking at (the skin) is actually a massive metabolic engine?” “The batteries inside those cells might dictate not just how old you look, but how your entire body processes energy.” “It’s not just aesthetics — it’s about keeping the engine running.” “This paper really forces us to rethink what anti-aging actually means.” “It’s not just vanity… it is metabolic healthcare.” - Key points Skin isn’t just a barrier—it’s a metabolic engine that can influence systemic energy handling. The paper reframes anti-aging: it’s not only aesthetics—it’s “keeping the engine running.” Classic skin-aging model focuses on the dermis: collagen/elastin loss + senescent “zombie cells.” New pivot: the epidermis may age differently—not via senescence, but via mitochondrial depletion. Aged epidermis showed no rise in p16INK4A (a common senescence marker), but showed lower mitochondrial DNA content. Causation test: researchers created epidermis-specific TFAM knockout mice (mitochondrial replication “key” removed only in skin cells). Result: mice developed premature aging phenotypes—hair loss, follicle atrophy, and delayed wound healing. Metabolic shock: despite “normal” elsewhere, mice with skin mitochondrial dysfunction gained more fat mass(visceral + subcutaneous) and did worse on a high-fat diet. Proposed mechanism: broken epidermal mitochondria reduce fatty-acid beta oxidation—skin stops acting as a fat-burning “sink,” so energy overflows into storage. System-wide impact: mice showed higher fasting blood glucose, implying skin metabolism may influence glucose regulation. Practical implication: different layers, different strategies—dermis may benefit from senescence-targeting, but epidermis needs energy restoration. Environmental stress (UV, pollution, chronic stress) may accelerate mitochondrial decline, making the “metabolic shield” concept even more relevant. - Episode timeline  0:19 – 1:14 — Hook: skin as “wrapper” vs metabolic engine; big claim (aging + weight + blood sugar) 1:14 – 2:35 — Paper intro (Yamamura et al.); mission: epidermal mitochondria → domino effect across body 2:35 – 3:33 — Classic model: dermis aging = collagen loss + senescent “zombie cells” 3:33 – 4:30 — Key finding: epidermis isn’t senescent (p16INK4A not elevated); instead mitochondrial decline 4:30 – 5:10 — “Energy crisis” framing; correlation vs causation question 5:10 – 6:09 — Causation experiment: epidermis-specific TFAM knockout (“ignition key” removed only in skin) 6:09 – 7:51 — Phenotypes: hair loss, follicle atrophy, delayed wound healing; “energy drop comes first” 7:51 – 10:42 — Obesity connection: weight gain on normal diet, more fat mass; mechanism = reduced beta oxidation in skin 10:42 – 11:34 — “Skin as energy sink” model; overflow into adipose storage 11:34 – 12:33 — Blood glucose increase; skin as systemic metabolic regulator 12:33 – 14:22 — Interventions mentioned (e.g., L-carnitine); PBM tie-in via cytochrome c oxidase → ATP 14:22 – 15:56 — Strategic shift: senolytics for dermis vs recharge epidermal mitochondria 15:56 – 17:07 — 3 pillars recap: battery-driven epidermal aging; physical consequences; systemic metabolic shock 17:07 – 18:34 — Environmental stress accelerant (UV, pollution, stress) + “metabolic shield” framing - Dr. Mike's #1 recommendations: Deuterium depleted water: Litewater (code: DRMIKE) EMF-mitigating products: Somavedic (code: BIOLIGHT) Blue light blocking glasses: Ra Optics (code: BIOLIGHT) Grounding products: Earthing.com - Stay up-to-date on social media: Dr. Mike Belkowski: Instagram LinkedIn   BioLight: Website Instagram YouTube Facebook

    19 min

  4. -3 J

    You’re Not What You Eat — You’re What Your Microbiome Makes (The Longevity Energy Code)

    We obsess over inputs — keto vs vegan, organic vs processed — like the body is a simple engine: better fuel in, better performance out. But this Deep Dive flips the model: your body is an ecosystem, and your gut microbes are the mechanics. In this episode, we decode how dysbiosis and leaky gut can trigger inflammaging, suppress mitochondrial function, and create the “energy crisis” that feels like aging. Then we explore the real plot twist: many “healthy” phytochemicals aren’t the magic—their microbial metabolites are. We break down the all-star compounds (urolithin A, sulforaphane, equol, hesperetin, SCFAs like butyrate), why conversion depends on your personal metabotype, and what to do if your internal “factory” is missing key workers; starting with dietary diversity, synbiotics, and (in some cases) direct metabolite supplementation. (Educational content only, not medical advice.) - Articles Discussed in Episode: Promotion of Healthy Aging Through the Nexus of Gut Microbiota and Dietary Phytochemicals - Key Quotes From Dr. Mike: “The road to mitochondrial health is paved through the gut.” “The body isn’t a machine, it’s an ecosystem… and your microbiome? They’re the mechanics.” “If the gut is chaotic, the whole energy system of the body crashes.” “Phytochemicals aren’t the cleaning crew… they’re the managers.” “The future of longevity might be about rehiring the staff we fired.” - Key points The old model is outdated: It’s not just what you eat, it’s who eats it with you (your microbiome). Healthspan > lifespan: More years aren’t the goal, more capable years are. Aging’s silent driver: Dysbiosis → leaky gut → LPS leakage → chronic inflammation (“inflammaging”). Energy code connection: Inflammation pushes mitochondria into “war mode” (less efficient ATP, more free radicals). Phytochemicals aren’t just antioxidants: At real blood levels, they often act more like signaling managers than “free radical sponges.” Two master switches: NF-κB = master inflammatory alarm NRF2 = master cellular defense/antioxidant program The plot twist: Many polyphenols are poorly absorbed; bacteria convert them into more potent metabolites. All-star metabolites: Urolithin A (from ellagitannins) → mitophagy Sulforaphane (from glucoraphanin; needs myrosinase) → NRF2 activation Equol (from daidzein in soy) → SERM-like benefits (skin/bone/cardiometabolic) Butyrate (SCFAs) → strengthens gut barrier + supports gut-cell mitochondria Hesperetin → neuroprotection potential (BBB relevance mentioned) Metabotype reality: Same food, totally different outcome depending on your microbes (A/B/0 patterns). Practical strategy: Build the factory: plant diversity + synbiotics, and when needed bypass the factory via direct metabolite supplements. - Episode timeline  0:19 – 1:12 — Deep Dive intro + the “inputs” obsession (diet as a combustion engine) 1:12 – 2:24 — The paradigm shift: body as ecosystem; microbiome as “mechanics”; healthspan framing 2:24 – 3:14 — Gut as energy control center: it signals mitochondria, not just feeds them 3:14 – 4:18 — Dysbiosis explained + fortress/garden analogy; diversity loss with age/lifestyle 4:18 – 5:42 — Leaky gut → LPS → systemic inflammation (“inflammaging”) → mitochondrial suppression/“war mode” 5:42 – 6:46 — Phytochemicals redefined: not direct antioxidants; signaling molecules 6:46 – 7:56 — The two switches: NF-κB down, NRF2 up (capacity building vs “mopping”) 7:56 – 9:31 — The plot twist: poor absorption; bacteria convert phytochemicals into potent metabolites 9:31 – 10:54 — Urolithin A: ellagitannins → bacterial conversion → mitophagy 10:55 – 12:08 — Sulforaphane: myrosinase + cooking caveat; gut conversion if enzyme is destroyed 12:08 – 12:58 — Equol: soy controversy reframed; SERM-like benefits 12:58 – 13:38 — Hesperetin + SCFAs (butyrate): BBB relevance + gut barrier fuel 13:38 – 15:26 — Metabotypes: why “superfoods” work for some and not others (A/B/0; equol producers 20–30% in West) 15:26 – 16:44 — Fixing the factory: Mediterranean-style diversity; prebiotics; synbiotics (“worker + lunchbox”) 16:44 – 17:26 — Bypassing the factory: direct metabolite supplementation (urolithin A; equol likely next) - Dr. Mike's #1 recommendations: Deuterium depleted water: Litewater (code: DRMIKE) EMF-mitigating products: Somavedic (code: BIOLIGHT) Blue light blocking glasses: Ra Optics (code: BIOLIGHT) Grounding products: Earthing.com - Stay up-to-date on social media: Dr. Mike Belkowski: Instagram LinkedIn   BioLight: Website Instagram YouTube Facebook

    20 min

  5. -4 J

    The End of the Dental Drill? How Red & Infrared Light Can Kill Pain, Speed Healing, and (Maybe) Regrow Teeth

    The dental drill may be the most iconic sound in healthcare—but this deep dive argues it doesn’t have to be the future. Drawing from a 2026 review paper (“Photobiomodulation in Dentistry”) in the International Journal of Advanced Research, we break down how “cold” red and near-infrared light (PBM) can donate energy to oral tissue, boost ATP production via mitochondrial cytochrome-c oxidase, and trigger repair signaling—without heat, cutting, or drugs. We explore why a temporary ROS spike can be helpful (hormesis), how PBM can reduce pain by calming nerve excitability and inflammation, and why this matters for real dental problems: TMJ pain, post-extraction soreness, dry socket, sensitivity, whitening discomfort, faster implant integration, and even orthodontic discomfort. Finally, we talk home devices—why wavelength + dose accuracy matters—and the wild frontier: PBM-assisted regenerative endodontics that could someday bring a tooth “back to life.” (Educational content only, not medical advice.) - Articles Discussed in Episode: PHOTOBIOMODULATION IN DENTISTRY: CURRENT EVIDENCE AND FUTURE DIRECTIONS - Key Quotes From Dr. Mike: “What if the future of oral health isn’t about cold steel drills or chemical drugs—what if it’s light?” “PBM is the polar opposite of hot lasers. It doesn’t cut. It donates energy to tissue.” “PBM isn’t a painkiller that masks the problem—it changes the tissue environment so the problem resolves.” “Inflammation is the fire in the gums—and PBM turns the fire down.” “The body wants to heal—sometimes it just needs the right signal to get started.” - Key points Dentistry is shifting from “repair after breakdown” (drill/fill) to bioenergetic healing (signal the tissue to regenerate). PBM = “cold laser / LED therapy,” not the hot surgical lasers that cut or vaporize tissue. Typical therapeutic wavelengths discussed: red + near-infrared (~650–1000 nm). Core mechanism: light is absorbed by cytochrome-c oxidase (mitochondrial “solar panel”) → faster electron transport → ATP spike. PBM can create a brief low-level ROS increase that acts as repair signaling (like exercise stress). PBM may shift cells from glycolysis (low efficiency) toward oxidative phosphorylation (high efficiency)—from “survival mode” to “repair mode.” Pain benefits: PBM can modulate nerve transmission, reduce neural excitability, and lower pain signaling locally. Inflammation benefits: PBM can lower pro-inflammatory cytokines (e.g., IL-1, TNF-α) and increase anti-inflammatory signaling (e.g., IL-10). TMJ: PBM is highlighted as a strong non-drug option that can reduce muscle sensitivity and improve jaw movement. Implants: PBM may help osseointegration by stimulating osteoblasts and angiogenesis—faster stabilization, shorter “danger zone.” Dry socket: PBM may beat “patch” approaches by accelerating real closure via immune cell migration and repair. Sensitivity + whitening: PBM may reduce dentin hypersensitivity via neural hyperpolarization and can be used prophylactically before bleaching to reduce pulp irritation. Home PBM is rising, but dosimetry matters: wrong wavelength/power = pretty red glow, weak biology. Future frontier: PBM may stimulate dental pulp stem cells—regenerative endodontics rather than “dead tooth root canals.” - Episode timeline  0:00–0:54 — The dental fear hook Drill sound, antiseptic smell, the “universal phobia,” and why the paradigm may change. 0:54–1:24 — The promise “What if the most powerful tool is light?” + introduce the 2026 dentistry PBM review paper. 1:24–2:19 — PBM basics (what it is / isn’t) PBM vs “hot” surgical lasers; cold laser / LED therapy; wavelength range. 2:19–3:36 — Big reframing Teeth aren’t rocks—mouth is living tissue that can be optimized. 3:36–6:20 — Core mechanism: mitochondria → ATP Cytochrome-c oxidase as chromophore; electron transport chain; “fast charger” analogy; universal mechanism (oral tissue = same engine). 6:20–8:53 — ROS nuance + metabolic upgrade Temporary ROS spike as signaling; hormesis; glycolysis → oxidative phosphorylation (“scooter to Ferrari”). 8:53–11:47 — Pain + inflammation + TMJ Local nerve modulation, cytokines, “blanket over alarm bell”; TMJ outcomes (movement + muscle sensitivity). 11:49–13:13 — Bone + implants Osseointegration; osteoblasts + angiogenesis; faster stabilization. 13:13–14:31 — Dry socket Why it hurts; conventional paste vs PBM-driven repair acceleration. 14:31–15:16 — Ortho angle Reduced tightening pain; possible speed-up of tooth movement (noted variability). 15:16–17:52 — Sensitivity + whitening preconditioning Dentin hypersensitivity; neural hyperpolarization; PBM before bleaching to reduce pulpal pain. 18:00–20:10 — Home devices + dose accuracy warning Trend toward home PBM; dosimetry, irradiance, wavelength precision; “right key opens the lock.” 20:10–21:23 — Stem cells + regenerative endodontics Dental pulp stem cells; proliferate/differentiate; “bring it back to life” future. 21:23–23:15 — Wrap + big question Bioenergetic vs chemical paradigm; “medicine cabinet of light” + call-to-action for listeners. - Dr. Mike's #1 recommendations: Deuterium depleted water: Litewater (code: DRMIKE) EMF-mitigating products: Somavedic (code: BIOLIGHT) Blue light blocking glasses: Ra Optics (code: BIOLIGHT) Grounding products: Earthing.com - Stay up-to-date on social media: Dr. Mike Belkowski: Instagram LinkedIn   BioLight: Website Instagram YouTube Facebook

    23 min

  6. -5 J

    The “Brain Energy” Formula That Isn’t a Stimulant

    In this solo episode of The Energy Code, Dr. Mike Belkowski introduces BioElixir, a new supplement line built around one core idea: focus is not a personality trait, it’s brain energy as biology. You’ll get a transparent, ingredient-by-ingredient breakdown of BioElixir MIND: what each compound is, why it’s in the formula, what human research does (and doesn’t) support, and how to think about dosing evidence in multi-ingredient stacks. Mike frames “brain energy” as a full chain: mitochondrial ATP output, membrane integrity, neurotransmitter signaling, stress chemistry, hydration, blood flow, and waste clearance. From cholinergics (Citicoline + Alpha-GPC) and membrane support (phosphatidylserine), to mitochondrial throughput (ALCAR + creatine/cregaatine + PQQ), stress resilience (tyrosine, rhodiola, ginseng, saffron), neuro-supportive mushrooms (lion’s mane, ergothioneine), and foundations like shilajit and Litewater deuterium-depleted water, this episode is designed to be education-first, hype-last. Mike closes with practical use cases (morning, cognitively intensive work, avoiding “caffeine train”), why he kept the formula natural (no methylene blue), packaging details (Miron violet glass), flavoring notes (pomegranate to mask bitterness), and the launch promo (first-week discount + subscription stacking). Key Quotes From Dr. Mike “If the brain cannot generate ATP efficiently… you’ll feel like you’re driving a sports car with no fuel.” “A brain-energy stack has to reduce the drain, not just push the gas pedal.” “Creatine is in the BioElixir MINDmore or less as a brain battery buffer. It’s not a stimulant; think of it as a reserve tank.” “Focus isn’t willpower. It’s mitochondrial throughput plus clean signaling.” “You don’t need jitters. You need stable voltage.” Key Points Framework: a real brain-energy formula must support mitochondrial output + signaling efficiency + protection from age-related wear and tear, not just stimulation. Evidence honesty: many studies use higher single-ingredient doses than multi-ingredient blends; that doesn’t make blends “bad,” it changes how we interpret results. Cholinergic stack: Citicoline (CDP-choline) supports acetylcholine + membrane substrates; Alpha-GPC is highly bioavailable and often studied in impairment contexts. Together = “messaging + hardware.” Membrane integrity matters: Phosphatidylserine framed as a key but overlooked lever for clean signaling. Mitochondrial throughput: Acetyl-L-carnitine supports fatty acid transport into mitochondria and is positioned as fatigue-to-clarity support. ATP buffer: Creatine (and the formula’s “cregaatine” variant) positioned as a reserve tank for high-demand or sleep-deprived cognition. Stress cognition: L-tyrosine is framed as “best when stress depletes catecholamines,” not a “more dopamine = genius” hack. Long-game neuro support: Lion’s mane and ergothioneine positioned as supportive while used, not instant “20-minute” stimulants. Cognitive outcomes ingredient: PQQ and “PQQ disodium salt” discussed as having controlled cognitive data in aging-adjacent groups (as presented in the transcript). Adaptogens with nuance: Rhodiola and red Korean ginseng described as stamina/resilience supports; results can be mixed depending on extract + population. Mood-cognition link: Saffron included because mood and cognition are inseparable. Taurine realism: human evidence is mixed for dementia protection; taurine framed as stability + calcium handling more than “main driver.” Foundation ingredients: Shilajit (fulvic acids, energy/fatigue signals) + Litewater DDW (lower deuterium to support enzyme kinetics/mitochondrial efficiency) form the “base layer.” Product usage: 10–12 pumps per serving; stable/smooth energy without jitters; flexible timing (morning or before deep work). Launch details: first-week promo + subscription stacking; flavor is pomegranate to mask bitter herbs. Episode Timeline 1:55–2:58 | Disclaimers + brain-energy framework Education only; dosing vs studies; how to interpret evidence. Brain energy chain: ATP, water/hydration, blood flow, glymphatic waste, stress chemistry. 3:34–7:49 | Cholinergics + membrane ‘hardware’ Citicoline (CDP-choline): acetylcholine + phospholipid substrates; memory trial mentioned. Alpha-GPC: bioavailable; more evidence in impairment/dementia contexts; why both together. 7:49–9:31 | Phosphatidylserine Membrane integrity + signaling; trial in MCI blend noted. 9:31–11:03 | Mitochondrial throughput: ALCAR Fatty acid transport + fatigue/cognition signals in older adults. 11:03–12:07 | BioLight bundles promo segment Bundles, what’s in each, 20% off + shipping discount. 12:26–15:07 | Creatine + Tyrosine Creatine as ATP buffer under stress/sleep deprivation. Tyrosine as stress-performance support (not “dopamine genius”). 15:07–17:29 | Lion’s mane + PQQ (as presented) Lion’s mane MCI trial pattern: benefits reduce after stopping. PQQ described as memory/attention support in aging-adjacent studies. 18:13–22:55 | Adaptogens + longevity antioxidants + mood Rhodiola: fatigue/stress cognition (mixed evidence acknowledged). Red Korean ginseng: cognitive tone/stamina, mixed evidence. Ergothioneine: long-game neuroprotection signals. Saffron: mood + emerging cognitive decline relevance. 23:34–26:17 | Theacrine + taurine nuance Theacrine: gentler spark vs aggressive stimulant. Taurine: mixed human dementia findings; emphasized calcium handling/resilience. 26:17–28:14 | Systems-level summary “Not superheroes” individually; brain runs on systems. Stack summary in one paragraph: signaling, membranes, ATP, stress resilience, long-term support. 28:14–33:14 | Shilajit deep dive Fulvic acids, “carrier” concept, fatigue/oxidative stress/energy signals; evidence framed as emerging. 33:14–39:22 | Litewater DDW deep dive Deuterium rationale, ATP synthase kinetics, early evidence caveats, “foundation” role. 39:22–42:52 | How to use + why no methylene blue Pumps, timing, stable energy, avoiding caffeine train. Natural positioning; methylene blue intentionally excluded. 43:21–47:49 | Full ingredient list + flavor rationale Runs through supplement facts; notes bitter herbs; pomegranate flavor + monk fruit/stevia to mask bitterness. - ⚡ NEW PRODUCT RELEASE: BioElixir MIND ⚡ We’re excited to introduce BioElixir MIND — our precision-formulated liquid nootropic designed to support mental clarity, sustained focus, and clean brain energy   Built with a mitochondria-first philosophy, BioElixir MIND combines Alpha-GPC + Citicoline, PQQ, Acetyl-L-Carnitine, adaptogens like Rhodiola and Korean Ginseng, and powerful cellular protectors like L-Ergothioneine and Shilajit. The result? Smooth cognitive performance without the harsh spikes and crashes.   Whether you’re building, creating, training, or simply demanding more from your brain, BioElixir MIND was designed to help you think sharper, stay steady under pressure, and support long-term neural resilience.   Clarity isn’t accidental. It’s engineered.   BioElixir MIND is now live!     🚨 LIMITED TIME OFFER! 🚨   For the next week, get 20% off your order of BioElixir MIND...   Which CAN be combined with subscription discounts!   This ends up being a total of 30% off...You maintain this discount as long as you keep your subscription active! Discount code: BIOELIXIR20Expires on 2/19, midnight PST *Must use "Single" quantity option; code will not work for 2-, 4- or 10-pack quantity options.   Shop BioElixir MIND! - Dr. Mike's #1 recommendations: Deuterium depleted water: Litewater (code: DRMIKE) EMF-mitigating products: Somavedic (code: BIOLIGHT) Blue light blocking glasses: Ra Optics (code: BIOLIGHT) Grounding products: Earthing.com - Stay up-to-date on social media: Dr. Mike Belkowski: Instagram LinkedIn   BioLight: Website Instagram YouTube Facebook

    52 min

  7. -6 J

    Is Long COVID a Mitochondrial Crash? The “Energy Code” Hidden in Your Genes

    For years, we obsessed over the invader: spikes, variants, antibodies, immune escape. But this deep dive flips the lens to the terrain, the battlefield inside the body, and the batteries powering it. Using a 2025 paper from the Journal of Medical Virology on genetic landscape + mitochondrial metabolic dysregulation in severe long COVID, we unpack a provocative idea: long COVID can look like a metabolic crash in people with hidden, common genetic weak links in their energy chain. These aren’t obvious rare childhood disorders. Many patients appear healthy until the virus hits like a stress test. The infection forces a cellular shift from efficient oxygen-based energy (OXPHOS) to quick-and-dirty sugar burning (glycolysis). Most people switch back. In severe long COVID, the system can get stuck. We walk through the study’s patient profile (brain fog, hypersomnia, myopathy), the genetics (dozens of mitochondria-related variants, including hits like POLG, MIPEP, ACOT9), and the functional data (Seahorse XF “live engine audit” showing either crashed ATP production or hypermetabolic redlining). Then we connect the dots to oxidative stress signals like SOD2 roaring like fire trucks that never leave. Bottom line: this frames long COVID as physically real, bioenergetic, and potentially predictable — shifting medicine’s focus from “invader only” to metabolic resilience. (Educational content only, not medical advice.) - Articles Discussed in Episode: Genetic Landscape and Mitochondrial Metabolic Dysregulation in Patients Suffering From Severe Long COVID - Key Quotes From Dr. Mike: “We’ve been completely obsessed with the invader… but we’ve largely ignored the terrain.” “The battlefield is our own bodies… the actual batteries that power that battlefield.” “The difference between bouncing back in a week versus suffering for years… isn’t random.” “Long COVID might actually be a metabolic crash in someone who is genetically susceptible.” “The virus acts as a stress test… a pressure cooker that exposes the weak link.” - Key points The pandemic lens has been invader-first; this episode is terrain-first (the host battlefield). Severe long COVID symptoms cluster in brain + muscle — the body’s top energy consumers. SARS-CoV-2 can interact with mitochondrial proteins and push metabolism toward glycolysis. The study profiled 13 severe long COVID patients with primarily neuro-muscular symptoms. Whole-genome sequencing found many mitochondrial-related variants (not one “smoking gun”). Key idea: heterozygous variants can be silent until a major stressor hits. The episode’s core concept: synergistic heterozygosity = multiple small weak links that fail together under stress. Example genes discussed: POLG (mtDNA replication), MIPEP (mitochondrial protein maturation), ACOT9 (fatty acid metabolism). Seahorse XF bioenergetics showed two failure modes: Crash: ATP production “on the floor” (dead batteries). Redline: hypermetabolism (engine revving itself to burnout). Proteomics showed SOD2 upregulation — a loud signal of ongoing oxidative stress. Some patients showed downregulation of electron transport chain proteins (mechanical breakdown). Clinical implication: standard labs can look normal while the real issue is mitochondrial function. Provocation: in some cases, metabolic resilience may matter as much as (or more than) antibodies for recovery trajectory. - Episode timeline  0:00 – 0:48 | The pivot: invader → terrain Shift from tracking the virus to examining the battlefield and energy capacity. 0:48 – 1:58 | The paper + the thesis 2025 Journal of Medical Virology paper. Long COVID framed as a metabolic crash with genetic susceptibility. 1:58 – 3:10 | Who the patients are (severe profile) 13 patients, severe neuro-muscular symptoms: fatigue, brain fog, hypersomnia, myopathy. Why brain + muscle crash first: energy demand. 3:10 – 5:12 | Viral metabolism hijack SARS-CoV-2 binds mitochondrial proteins, suppresses mitochondrial function. OXPHOS → glycolysis shift; for some, the switch never resets. 5:12 – 6:42 | Genetics: not one gene, many weak links Whole genome sequencing. Many variants in mitochondrial-related genes; some classified pathogenic/likely pathogenic. Why they weren’t sick before: heterozygous “backup power.” 6:42 – 8:37 | Core concept: synergistic heterozygosity Car/Indy 500 analogy. Example genes: POLG, ACOT9, MIPEP. 8:37 – 10:35 | Functional testing: Seahorse XF “Live engine audit” of oxygen consumption/ATP. Patient P4 “double hit” with very low ATP. Others show hypermetabolism (“redlining”). 10:35 – 12:38 | Proteomics + oxidative stress signals SOD2 upregulation = fire trucks outside the building. Downregulation of electron transport chain proteins in some patients. 12:38 – 15:05 | Clinical blind spot + big provocation Why routine labs miss it; fatigue dismissed. Terrain/resilience framing and implications for future medicine. - Dr. Mike's #1 recommendations: Deuterium depleted water: Litewater (code: DRMIKE) EMF-mitigating products: Somavedic (code: BIOLIGHT) Blue light blocking glasses: Ra Optics (code: BIOLIGHT) Grounding products: Earthing.com - Stay up-to-date on social media: Dr. Mike Belkowski: Instagram LinkedIn   BioLight: Website Instagram YouTube Facebook

    15 min

  8. 10 FÉVR.

    Is Your Heart Failing… or Just Running Out of Energy?

    Most heart conversations start and end with plumbing: clogged arteries, cholesterol, blood pressure. This one doesn’t. In this Energy Code Deep Dive, we go straight to the true engine of the heart: mitochondria. Why do heart cells devote nearly a third of their space to these “power plants”? Because your heart never stops, and energy is the real limiting factor. When mitochondria lose their ability to fuse, split, and recycle damage, the heart’s power grid becomes clogged with broken “zombie engines.” Then the real plot twist hits: damaged mitochondria leak DNA that looks bacterial, triggering the immune system to panic and ignite chronic inflammation. That sterile inflammation hardens the heart, disrupts rhythm, and accelerates aging from the inside out. And the best part: if cardiac aging is an energy-maintenance problem, you have leverage. We unpack the two-front strategy: improve mitochondrial efficiency and restore cellular cleanup. This is the why behind tools like photobiomodulation and lifestyle levers that re-balance mTOR and AMPK — so the janitor can come back to work. (Educational content only, not medical advice.) - Articles Discussed in Episode: Heart of the matter: Mitochondrial dynamics and genome alterations in cardiac aging - Key Quotes From Dr. Mike: “Mitochondria are the government, the waste management system, and the power grid all rolled into one.” “When mitochondria start to fail, the heart doesn’t just run out of gas — the control system starts to glitch.” “As we age, the sanitation department goes on strike.” (Alluding to decreased mitophagy activation) “The heart is attacking itself because its own engines are leaking parts that look like an enemy.” “If we can seal the leak and clean the engine… how much of aging is actually reversible?” - Key points We’ve been treating symptoms, not root cause: heart aging isn’t just “pipes and pumps,” it’s an energy failure problem. The heart is an ATP monster: it beats ~100,000 times/day and is heavily mitochondrial by design. Mitochondria aren’t static beans: they’re a dynamic network constantly fusing and splitting (fusion/fission) to stay resilient. Fusion = resource sharing: mitochondria merge to dilute damage and stabilize function. Fission = quality control: mitochondria split to isolate damaged segments for removal. Aging breaks the rhythm: too much fusion or too much fission both impair output and resilience. Mitophagy is the sanitation system: damaged mitochondria must be recycled; aging slows this cleanup. Why cleanup fails: mTOR runs too “build-mode,” AMPK runs too low, so the janitor gets sent home. mtDNA is fragile: mitochondrial DNA sits next to the furnace and accumulates errors, creating a mosaic of function (heteroplasmy). “Blue cells” become conduction roadblocks: a small number of defective cells can disrupt the heart’s electrical wave. The big twist — inflammaging: damaged mitochondria leak DNA that looks bacterial → the immune system triggers sterile inflammation. Inflammation fuels fibrosis + senescence: stiffening, dysfunction, and “zombie cells” secreting toxic signals. Actionable thesis: protect mitochondrial integrity by boosting efficiency + restoring cleanup (energy + recycling). - Episode timeline  0:19 – 1:30 | The reframe Heart health isn’t plumbing. It’s energy and what happens when that currency gets devalued. 1:30 – 3:25 | Why the heart is a mitochondrial machine The heart’s nonstop workload and massive ATP demand. Mitochondria as regulators (ATP, calcium handling, survival signals). 3:25 – 5:25 | Mitochondrial dynamics: the “dance” Fusion (share resources, dilute damage) vs fission (isolate damage, multiply). What goes wrong when the rhythm breaks. 5:25 – 7:50 | Mitophagy: taking out the trash How aging slows cleanup. mTOR too high + AMPK too low = “janitor goes home.” 7:50 – 9:40 | The vulnerable blueprints (mtDNA + heteroplasmy) Why mtDNA is more fragile than nuclear DNA. Mosaic tissue function and “blue” defective cells disrupting conduction. 9:40 – 12:40 | The plot twist: inflammaging via mitochondrial leaks Leaky mitochondria release DNA that resembles bacteria. False infection alarm → innate immune activation → chronic sterile inflammation. Fibrosis and senescence (“zombie cells” + toxic secretions). 12:40 – 14:45 | What to do: fix the code Maintain mitochondrial integrity. Boost mitophagy and efficiency (two-front strategy). PBM + fasting/time-restricted eating as examples of “clean + charge.” 14:45 – 16:07 | Closing provocation “Aging as mistaken identity.” If we can seal leaks and restore cleanup, what’s reversible? - Dr. Mike's #1 recommendations: Deuterium depleted water: Litewater (code: DRMIKE) EMF-mitigating products: Somavedic (code: BIOLIGHT) Blue light blocking glasses: Ra Optics (code: BIOLIGHT) Grounding products: Earthing.com - Stay up-to-date on social media: Dr. Mike Belkowski: Instagram LinkedIn   BioLight: Website Instagram YouTube Facebook

    16 min
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À propos

The Energy Code is your blueprint for unlocking limitless vitality at the cellular level. Hosted by Dr. Mike Belkowski, this podcast dives deep into the science of your mitochondria—the true engines of health and energy. From light, water, and magnetism to groundbreaking molecules and lifestyle upgrades, each episode decodes the most effective strategies to strengthen your “Mitochondrial Matrix.” If you’re seeking cutting-edge science, practical tools, and proven methods to optimize your body and mind, you’ve just cracked the code. Check out these sources: www.biolight.shop – Instagram @biolight.shop – YouTube BioLight

Informations

  • Création
    Dr. Mike Belkowski
  • Années d’activité
    2021 - 2026
  • Épisodes
    268
  • Classification
    Tous publics
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    © Copyright 2021 All rights reserved.
  • Site web de l’émission
    The Energy Code

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