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The Energy CodeAuthor: Dr. Mike Belkowski Language: en Genres: Alternative Health, Health & Fitness Contact email: Get it Feed URL: Get it iTunes ID: Get it |
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Is Long COVID a Mitochondrial Crash? The “Energy Code” Hidden in Your Genes
Episode 268
Wednesday, 11 February, 2026
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
