CONDITIONS WE TREAT

Longevity, Cellular Health & Anti-Aging Medicine

Longevity medicine focuses on extending healthspan — the years of healthy, functional life — not just lifespan. SynergyO3 targets the upstream biological drivers of accelerated aging: mitochondrial decline, oxidative damage, cellular senescence, and chronic inflammation — to help you function at your peak for longer.

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CLINICAL PRESENTATION

Recognizing Longevity & Anti-Aging Symptoms

Biological aging accelerates when cellular repair and regeneration can no longer keep pace with damage accumulation. Many people experience accelerated biological aging years before it becomes clinically apparent. Dr. Volpp evaluates your biological age markers to identify areas most responsive to intervention.

Biological Aging Markers We Evaluate

SynergyO3 evaluates biological age indicators including telomere length, mitochondrial function markers, oxidative stress biomarkers (8-OHdG, isoprostanes), advanced glycation end-products, inflammatory age markers (inflammaging), NAD+ levels, and functional capacity assessments.

Measurable Abnormalities

Key longevity biomarkers include NAD+ levels, oxidative stress markers (8-OHdG, isoprostanes), advanced glycation end-products (AGEs), inflammatory indices (CRP, IL-6), telomere length assessment, mitochondrial respiratory function, HRV, and VO₂ max.

Primary Symptoms · Most Common

Declining Energy & Vitality — Reduced ATP production from aging mitochondria
Cognitive Changes — Memory, processing speed, and focus declining with age
Reduced Physical Performance — Sarcopenia, reduced strength, slower recovery
Metabolic Slowdown — Increasing insulin resistance, weight gain, reduced metabolic rate
Immune Decline — Immunosenescence reducing resistance to infection and cancer surveillance
Skin & Connective Tissue Aging — Reduced collagen synthesis, wound healing, and tissue repair

Secondary Symptoms · Also Reported

Sleep Quality Decline — Reduced deep sleep, lower HGH release, circadian disruption
Hormonal Decline — Testosterone, estrogen, DHEA, growth hormone, and melatonin decline
Cardiovascular Changes — Arterial stiffening, endothelial dysfunction, reduced cardiac reserve
Chronic Musculoskeletal Pain — Reduced cartilage, increased systemic inflammation
Vision & Hearing Changes — Mitochondria-dependent sensory cell decline
Mood & Motivation Changes — Dopaminergic and serotonergic changes with neurological aging

COMMONLY OVERLAPPING CONDITIONS

Mitochondrial DysfunctionCardiovascular Disease RiskHormonal DeclineMetabolic SyndromeNeurodegeneration RiskChronic Inflammation / Inflammaging

CLINICAL EDUCATION

The Biology of Longevity & Anti-Aging

Biological aging is driven by the gradual accumulation of cellular damage that exceeds repair capacity. The hallmarks of aging include mitochondrial dysfunction, oxidative DNA damage, cellular senescence, telomere attrition, epigenetic dysregulation, and chronic low-grade inflammation ('inflammaging'). These mechanisms are interconnected and mutually reinforcing.

Mitochondrial Decline & NAD+ Depletion

Mitochondrial function declines with age due to accumulating oxidative damage to mitochondrial DNA and electron transport chain components. NAD+ — critical for mitochondrial energy production and sirtuin activation — falls dramatically with age, accelerating virtually every hallmark of aging.

Cellular Senescence & SASP

Senescent cells have stopped dividing but remain metabolically active, secreting a pro-inflammatory cocktail called the Senescence-Associated Secretory Phenotype (SASP). Accumulating senescent cells drive tissue dysfunction, chronic inflammation, and accelerated aging in neighboring cells.

Oxidative DNA Damage & Telomere Attrition

Reactive oxygen species accumulating with age damage nuclear and mitochondrial DNA, causing telomere shortening with each cell division. Short telomeres trigger cell senescence or apoptosis, reducing tissue regenerative capacity and driving organ function decline.

KEY STATISTICS

Longevity & Anti-Aging at a Glance

50%

Decline in NAD+ levels between age 40–60

10%

Decline in VO₂ max per decade after 30 without intervention

Variation in biological age vs. chronological age

6–12

Typical longevity protocol sessions

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PHASE 1

Evaluation & Testing (Wks 1–2)

Comprehensive intake, targeted labs, and biomarker assessment to map biological drivers.

PHASE 2

Active Treatment Protocol (Wks 3–10)

Physician-designed sequenced protocol combining EBOO, HOCATT, and IV nutrients.

PHASE 3

Monitoring & Optimization

Follow-up labs, functional benchmarks, and protocol refinement based on response.

ROOT CAUSE INVESTIGATION

Biological Drivers We Investigate

Dr. Volpp evaluates each patient's complete picture — identifying which biological mechanisms are most active — before any protocol is designed. Individual results vary.

NAD+ & Sirtuin Pathway Activation

NAD+ is required for sirtuin enzymes (SIRT1-7) that regulate DNA repair, mitochondrial biogenesis, inflammation, and metabolic efficiency. Declining NAD+ with age disables these longevity pathways — accelerating mitochondrial dysfunction and cellular aging.

Inflammaging & Chronic Cytokine Elevation

Chronic low-grade inflammation ('inflammaging') accumulates with age from senescent cells, microbiome changes, oxidative burden, and accumulated damage signals. Elevated IL-6, TNF-α, and CRP are independent predictors of biological aging rate and mortality.

Mitochondrial Biogenesis Reduction

With aging, the signaling pathways that trigger mitochondrial biogenesis (PGC-1α, AMPK) become less responsive. Fewer new mitochondria are produced while damaged ones accumulate, reducing cellular energy capacity and stress resilience.

TREATMENT APPROACH

Therapies Used in Longevity & Anti-Aging Protocols

All protocols are physician-designed and supervised by Dr. Heather Volpp, MD. Therapies are selected based on each patient's evaluation. Results may vary.

PRIMARY PROTOCOL

EBOO Ozone Therapy

EBOO ozone therapy may activate key longevity signaling pathways including Nrf2 (antioxidant response), support mitochondrial biogenesis, reduce the oxidative burden that accelerates cellular aging, and improve tissue oxygen delivery.

Activates Nrf2 — master regulator of antioxidant and cellular repair response
May support mitochondrial function and biogenesis signaling
Reduces oxidative burden that drives cellular senescence
Supports microvascular oxygen delivery to all tissues

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SUPPORTIVE PROTOCOL

HOCATT Sauna Therapy

The HOCATT's combination of ozone, far-infrared, and carbonic acid activates multiple longevity pathways — stimulating heat shock proteins, improving circulation, reducing systemic oxidative burden, and supporting autonomic balance.

Far-infrared activates heat shock proteins (HSP70, HSP90) supporting protein homeostasis
Ozone steam supports mitochondrial biogenesis signaling
Carbonic acid simulates altitude adaptation — stimulating cardiovascular efficiency
Autonomic modulation supports heart rate variability and nervous system resilience

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YOUR PATH FORWARD

The SynergyO3 Patient Journey

Every patient begins with a comprehensive physician evaluation. No protocol begins before Dr. Volpp has reviewed your complete clinical picture.

WEEKS 1–2

Consultation & Evaluation

A comprehensive intake with Dr. Volpp reviewing your symptom timeline, prior lab work, medications, and functional status. Targeted lab panels are ordered to identify active biological drivers.

WEEKS 3–10

Physician-Designed Protocol

Based on your evaluation findings, Dr. Volpp designs a sequenced treatment protocol — typically combining EBOO sessions, HOCATT therapy, and IV nutrient support at clinically appropriate intervals.

ONGOING

Monitoring & Optimization

Functional benchmarks and symptom tracking guide protocol adjustments. Follow-up labs assess inflammatory markers and key biomarkers. Treatment frequency is adjusted as you progress toward your goals.

COMMON QUESTIONS

Frequently Asked Questions

WHAT IS BIOLOGICAL AGE AND HOW IS IT DIFFERENT FROM CHRONOLOGICAL AGE?

Chronological age is simply time elapsed since birth. Biological age reflects the functional state of your cells and tissues — how well your body is actually performing relative to its years. Biological age can be 10–20 years younger or older than chronological age depending on lifestyle, genetics, and accumulated damage.

HOW DOES OZONE THERAPY SUPPORT LONGEVITY?

Research suggests ozone therapy may activate the Nrf2 antioxidant pathway, support mitochondrial biogenesis, reduce the inflammatory burden that accelerates cellular aging (inflammaging), and improve oxygen delivery to tissues. All protocols are physician-designed based on your specific biomarker profile.

WHAT IS NAD+ AND WHY IS IT IMPORTANT FOR AGING?

NAD+ (nicotinamide adenine dinucleotide) is a coenzyme essential for mitochondrial energy production and sirtuin enzyme activation. Sirtuins regulate DNA repair, mitochondrial biogenesis, inflammation, and cellular stress response. NAD+ levels fall by approximately 50% between ages 40 and 60, accelerating virtually every hallmark of aging.

HOW IS SYNERGYO3'S LONGEVITY APPROACH DIFFERENT FROM CONVENTIONAL MEDICINE?

Conventional medicine typically addresses aging-related disease after symptoms develop. SynergyO3 proactively evaluates biological aging markers and addresses the upstream cellular mechanisms driving accelerated aging — mitochondrial decline, oxidative damage, inflammaging, and NAD+ depletion — before they manifest as clinical disease.

TAKE THE NEXT STEP

Ready to Investigate the Root Cause?

Begin with a comprehensive consultation with Dr. Heather Volpp, MD — Board-Certified Internal Medicine. Your evaluation will review your full clinical picture and identify which biological mechanisms may be driving your symptoms.

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Physician-Supervised · SynergyO3 Medical · Encinitas, CA · (760) 450-4602

Individual results vary. Consult with Dr. Volpp during your evaluation.