Betulinic Acid

• Anti-inflammatory
• Antioxidant
• Anti-cancer
• Immunomodulatory

• Hepatoprotective
• Antiviral
• Antimicrobial
• Neuroprotective
• Metabolic regulation

Betulinic acid (BA) exerts its diverse biological effects through multiple molecular pathways and cellular targets. As an anti-cancer agent, BA primarily induces apoptosis through the intrinsic mitochondrial pathway. It directly affects the mitochondrial membrane potential, leading to the release of cytochrome c, activation of caspases, and subsequent cell death. This process is mediated by the generation of reactive oxygen species (ROS) and is independent of the p53 tumor suppressor pathway, making BA effective against both p53 wild-type and p53-deficient cancer cells.

BA also inhibits topoisomerase I, an enzyme essential for DNA replication, further contributing to its anti-cancer properties. Additionally, BA modulates several key signaling pathways involved in cancer progression, including the inhibition of nuclear factor-kappa B (NF-κB), signal transducer and activator of transcription 3 (STAT3), and specificity protein (Sp) transcription factors. By downregulating these pathways, BA reduces the expression of genes involved in cell proliferation, angiogenesis, and metastasis. The anti-inflammatory properties of BA stem from its ability to inhibit NF-κB signaling, a master regulator of inflammation.

By preventing the phosphorylation and degradation of IκB, BA blocks the nuclear translocation of NF-κB and subsequent expression of pro-inflammatory genes. This leads to reduced production of inflammatory cytokines such as tumor necrosis factor-alpha (TNF-α), interleukin-6 (IL-6), and interleukin-1β (IL-1β). BA also inhibits cyclooxygenase-2 (COX-2) and inducible nitric oxide synthase (iNOS), further contributing to its anti-inflammatory effects. The antioxidant properties of BA involve both direct and indirect mechanisms.

It directly scavenges free radicals and indirectly activates nuclear factor erythroid 2-related factor 2 (Nrf2), a master regulator of cellular antioxidant responses. Nrf2 activation leads to increased expression of antioxidant enzymes such as heme oxygenase-1 (HO-1), NAD(P)H:quinone oxidoreductase 1 (NQO1), and glutathione S-transferase (GST). BA’s immunomodulatory effects are mediated through its impact on various immune cells. It enhances the activity of natural killer (NK) cells and cytotoxic T lymphocytes, promoting anti-tumor immunity.

BA also modulates the function of macrophages, shifting them from a pro-inflammatory M1 phenotype to an anti-inflammatory M2 phenotype under certain conditions. In the context of viral infections, BA inhibits viral entry and replication through multiple mechanisms. It interferes with the viral envelope glycoprotein gp41, preventing HIV-1 entry into cells. BA also inhibits HIV-1 maturation by blocking the cleavage of the Gag polyprotein, a critical step in viral assembly.

For hepatitis B and C viruses, BA suppresses viral replication by modulating host cell signaling pathways. BA’s neuroprotective effects are mediated through its anti-inflammatory and antioxidant properties, as well as its ability to inhibit acetylcholinesterase, an enzyme that breaks down the neurotransmitter acetylcholine. By preserving acetylcholine levels, BA may improve cognitive function. BA also protects neurons from excitotoxicity and oxidative stress-induced damage, potentially benefiting neurodegenerative conditions.

In metabolic regulation, BA activates AMP-activated protein kinase (AMPK), a key energy sensor that regulates cellular metabolism. This activation enhances glucose uptake in skeletal muscle, improves insulin sensitivity, and promotes fatty acid oxidation. BA also modulates peroxisome proliferator-activated receptors (PPARs), particularly PPAR-α and PPAR-γ, which further contributes to its beneficial effects on glucose and lipid metabolism. Recent research has identified BA as a potential activator of longevity-related pathways, including sirtuins and FOXO transcription factors, which may contribute to its potential lifespan-extending effects observed in some model organisms.

BA also promotes autophagy, a cellular ‘housekeeping’ process that removes damaged proteins and organelles, which is crucial for cellular health and longevity.

Typical supplemental dosages range from 100-500 mg per day of standardized betulinic acid, though clinical evidence for optimal human dosing is limited. Most studies showing benefits have been conducted in animal models with doses that would translate to this range in humans. Enhanced delivery systems (liposomal, nanoparticle) may allow for lower effective doses.

Starting Dose: 100 mg daily

Adjustment Protocol: May increase by 100 mg every 2-4 weeks if needed and well-tolerated

Maximum Recommended Dose: 500 mg daily for most conditions

Protocol: Some practitioners recommend 8-12 weeks on, followed by 2-4 weeks off

Rationale: May help prevent tolerance development and allow assessment of effects, though clinical evidence for the necessity of cycling is limited

Pregnancy Lactation: Not recommended due to insufficient safety data

Liver Impairment: Use with caution and at reduced doses; monitor liver function

Kidney Impairment: Limited data; use with caution and at reduced doses

Autoimmune Conditions: Consult healthcare provider due to immunomodulatory effects

Cancer Patients: Only use under oncologist supervision due to potential interactions with chemotherapy

Standard Formulations: May require higher doses due to poor bioavailability

Enhanced Delivery Systems: Liposomal, nanoparticle, or phospholipid complex formulations may allow for 30-50% lower doses

Combination Products: When combined with synergistic compounds, lower doses may be effective

HIV Studies: Bevirimat (3-O-(3′,3′-dimethylsuccinyl)betulinic acid) has been studied at doses of 75-250 mg as a single dose in phase I/II trials

Cancer Studies: Preclinical studies have used equivalent human doses of 200-500 mg/day

Topical Applications: 0.5-2% concentrations have been studied for dermatological applications

Most dosing recommendations are extrapolated from animal studies and limited human trials. Individual responses may vary significantly. Clinical trials with standardized preparations are needed to establish optimal therapeutic dosages for specific conditions.

Very low, estimated to be less than 1% for oral administration

Extremely poor water solubility (practically insoluble in water), High lipophilicity, Large molecular size limiting passive diffusion, Extensive first-pass metabolism in the liver, P-glycoprotein efflux in the intestinal epithelium, Extensive enterohepatic circulation

Primary Pathways: Primarily metabolized in the liver through phase I (oxidation, hydroxylation) and phase II (glucuronidation, sulfation) reactions

Major Metabolites: Various hydroxylated derivatives and glucuronide/sulfate conjugates

Half Life: Approximately 8-12 hours in humans based on limited pharmacokinetic studies

Protein Binding: High (>99%) binding to plasma proteins, primarily albumin

Tissue Distribution: Accumulates primarily in the liver, with lower concentrations in adipose tissue; limited blood-brain barrier penetration though some studies show CNS effects

Primary Route: Primarily eliminated through biliary excretion and feces

Secondary Routes: Minor urinary excretion of metabolites

Optimal Timing: Best taken with meals containing some fat to enhance absorption

Frequency: Due to relatively long half-life, once or twice daily dosing is typically sufficient

Special Considerations: Absorption may be reduced when taken with high-fiber meals; spacing from fiber supplements is recommended

Absorption Characteristics: Slow and incomplete absorption from the gastrointestinal tract

Peak Plasma Concentration: Typically reached 2-4 hours after oral administration of standard formulations

Bioavailability Enhancement Factor: Enhanced delivery systems can improve bioavailability by 5-20 fold depending on the specific formulation

Dosing Considerations: Higher doses may be required with standard formulations to achieve therapeutic plasma levels

Formulation Selection: Enhanced delivery systems are strongly recommended for clinical applications

Monitoring Recommendations: Plasma level monitoring may be valuable in research settings but is not typically necessary for supplement use

Most pharmacokinetic data comes from animal studies, with limited human data available. More comprehensive human pharmacokinetic studies are needed to better understand the bioavailability and metabolism of betulinic acid in humans.

LD50: Oral LD50 in mice >2000 mg/kg body weight

Observations: Demonstrates relatively low acute toxicity in animal studies with a wide safety margin

Established UL: No officially established upper limit

Research Observations: Doses up to 500 mg daily appear well-tolerated in limited human studies

Safety Concerns: Doses above 500 mg daily have not been well-studied in humans and should be approached with caution

Chronic Toxicity Data: Limited long-term human data; animal studies suggest good tolerability with chronic administration

Bioaccumulation: No evidence of significant bioaccumulation in tissues

Adaptation Effects: No significant tolerance or adaptation effects reported

Pediatric: Not recommended due to insufficient safety data

Geriatric: Start with lower doses; monitor for drug interactions

Hepatic Impairment: Use with caution; start with lower doses and monitor liver function

Renal Impairment: Limited data; use with caution at reduced doses

Cancer Patients: Only use under oncologist supervision due to potential interactions with cancer treatments

Suggested Tests: Consider baseline and periodic liver function tests with long-term use

Frequency: Before beginning supplementation and every 3-6 months during long-term use

Warning Signs: Persistent gastrointestinal distress, unusual fatigue, jaundice, or signs of allergic reaction

Phase 1 Trials: Limited phase 1 trials with bevirimat (a betulinic acid derivative) showed good tolerability at doses up to 250 mg

Adverse Events: Most reported adverse events were mild and transient

Discontinuation Rates: Low discontinuation rates due to adverse effects in available studies

Skin Irritation: Generally well-tolerated with minimal irritation at concentrations of 0.5-2%

Systemic Absorption: Limited systemic absorption through intact skin

Contraindications: Avoid application to broken or inflamed skin

Classification: Generally recognized as a dietary ingredient in the United States when present in traditional food sources

Approved Claims: No FDA-approved health claims

Structure Function Claims: Limited to general statements about supporting immune health, antioxidant activity, and healthy inflammatory response

Regulatory History: Has not been the subject of significant FDA regulatory actions

New Dietary Ingredient Status: Not formally submitted as a New Dietary Ingredient (NDI) notification for standalone use, though present in many traditional foods and herbs

Approved Drugs: No approved pharmaceutical products containing betulinic acid as the active ingredient

Clinical Trials: Derivatives such as bevirimat have undergone clinical trials for HIV treatment

Orphan Drug Status: No orphan drug designations for betulinic acid itself, though some derivatives have been considered for orphan indications

Investigational Status: Under investigation for multiple conditions but not designated as an Investigational New Drug (IND) in the US

Pharmacopeial Monographs: No official monograph specifically for betulinic acid, though present in monographs for certain plants, No official United States Pharmacopeia monograph, No official European Pharmacopoeia monograph

Industry Standards: Various industry specifications exist for commercial products, typically requiring 60-98% purity depending on intended use

Us: Must be listed as an ingredient; no specific warnings required

Eu: Must be listed as an ingredient; no specific warnings required

Other Regions: Variable requirements; may need traditional use statements in some jurisdictions

Restrictions: No specific restrictions on import/export in most countries

Documentation: Standard documentation for botanical ingredients typically required

Tariff Classifications: Typically classified under botanical extracts or natural products

Increasing Scrutiny: Growing interest from regulatory bodies as research expands, particularly for anti-cancer and antiviral applications

Harmonization Efforts: No specific international harmonization efforts for betulinic acid

Future Outlook: Likely to remain available as a dietary ingredient while pharmaceutical applications continue to be explored

Us: Permitted in cosmetic products; must be listed in ingredients

Eu: Permitted in cosmetic products; must be listed in INCI name

Claims Limitations: Anti-aging and skin health claims must be substantiated and not cross into drug claim territory

Compound Patents: The natural compound itself is not patentable, but various derivatives, formulations, and applications have been patented

Formulation Patents: Multiple patents exist for enhanced delivery systems and specific formulations

Application Patents: Patents exist for specific therapeutic applications, particularly for derivatives

Medium to high

Standard Formulations: $2.00-$5.00 per day for basic extracts (100-200 mg)

Enhanced Formulations: $5.00-$15.00 per day for bioavailability-enhanced formulations

High Purity Formulations: $8.00-$20.00 per day for high-purity (>90%) formulations

Historical Trend: Gradually decreasing over the past decade as extraction and purification methods improve

Future Projections: Likely to continue moderate decrease as production scales increase and more efficient extraction methods are developed

Market Factors: Growing demand for natural anti-cancer and antiviral compounds may offset some price decreases

Cost Benefit Assessment: Moderate value for general health support; potentially high value for specific applications like cancer support

Factors Affecting Value: Poor bioavailability of standard formulations reduces cost-effectiveness, Enhanced formulations offer better value despite higher cost due to improved absorption, Value increases for individuals with specific health concerns addressed by betulinic acid’s mechanisms, Value as an adjunct to conventional treatments may be significant

Optimal Value Approaches: Using birch bark or chaga extracts standardized for betulinic acid content may provide better value than isolated compound, Combination products leveraging synergistic compounds may offer better overall value, Enhanced delivery systems significantly improve value despite higher cost

Affordability Assessment: Moderately accessible for regular use in developed countries; may be cost-prohibitive in developing regions

Insurance Coverage: Generally not covered by health insurance

Cost Reduction Strategies: Bulk purchasing can reduce per-dose cost, Using standardized extracts rather than high-purity isolates, Seasonal purchasing when raw material harvests reduce extraction costs

Environmental Cost Factors: Moderate to high environmental footprint from extraction processes and solvent use

Sustainable Sourcing Impact: Sustainable harvesting practices and cultivation can improve economic and environmental sustainability

Long Term Economic Outlook: Likely to become more economically viable as production scales increase and more efficient extraction methods are developed

Cancer Patients: Potentially high value as an adjunct to conventional treatments

Individuals With Viral Infections: Moderate value for specific viral conditions

General Wellness: Moderate value as part of a comprehensive supplement regimen

Specific Health Conditions: Potentially high value for individuals with specific inflammatory or metabolic conditions

Cost Per Publication: Relatively high research output relative to investment

Translation To Clinical Applications: Moderate success in translating research findings to clinical applications

Future Research Priorities: Enhanced delivery systems and combination therapies offer the best return on research investment

Pure Compound: 3-5 years when stored properly

Standardized Extracts: 2-3 years when stored properly

Formulated Products: 1-3 years depending on formulation and packaging

Temperature: Store at room temperature (15-25°C); avoid exposure to high temperatures

Light: Protect from direct light; amber or opaque containers recommended

Humidity: Store in a dry place; avoid exposure to high humidity

Packaging: Airtight containers preferred; nitrogen-flushed packaging may extend shelf life

Capsules: High compatibility with vegetable or gelatin capsules

Tablets: Moderate compatibility; may require appropriate excipients for proper disintegration

Liquid Formulations: Poor solubility in aqueous systems; requires solubilizers or emulsifiers

Liposomes: Good compatibility; enhances stability and bioavailability

Nanoparticles: Good compatibility with various nanoparticle systems; may enhance stability

Topical Formulations: Excellent compatibility with various dermatological bases; good stability in properly formulated products

Accelerated stability testing (elevated temperature and humidity), Real-time stability testing under recommended storage conditions, Photostability testing according to ICH guidelines, HPLC analysis for quantification and detection of degradation products, Dissolution testing for solid dosage forms

Manufacturing: Minimize exposure to heat during processing; consider inert gas protection for sensitive operations

Transportation: Maintain temperature control; avoid extreme conditions

Reconstitution: For powdered formulations, reconstitute immediately before use in appropriate vehicles

PH Stability Range: Most stable at pH 5-7; avoid strongly acidic or alkaline formulations

Excipient Compatibility: Compatible with most common pharmaceutical excipients; avoid strong oxidizing agents

Solvent Compatibility: Soluble in ethanol, methanol, acetone, and other organic solvents; practically insoluble in water

Bevirimat: 3-O-(3′,3′-dimethylsuccinyl)betulinic acid shows improved stability compared to parent compound

Other Derivatives: Various synthetic derivatives may have different stability profiles; should be evaluated individually

Synthesis Methods

Natural Sources

Extraction Methods

Quality Considerations

Commercial Forms

Industry Trends

Isolation: First isolated and characterized in the early 20th century

Identification In Traditional Remedies: Recognized as an active component in many traditional medicinal plants in the mid-20th century

Pharmacological Characterization: Systematic investigation of biological activities began in the 1970s-1980s

Key Researchers: Pisha E. and Pezzuto J.M. – Pioneering work on anti-cancer properties, Fujioka T. and Kashiwada Y. – Early work on anti-HIV activity, Fulda S. – Extensive research on apoptotic mechanisms

Pre 1950: Used primarily in traditional medicine without knowledge of active compounds

1950s 1970s: Identification as active component in traditional remedies; early pharmacological studies

1980s 1990s: Discovery of anti-cancer and anti-HIV properties; increased research interest

1990s 2000s: Elucidation of mechanisms of action; development of semi-synthetic derivatives

2000s Present: Clinical trials of derivatives; development of enhanced formulations to overcome bioavailability limitations; expanded research into various therapeutic applications

Traditional Use Safety: Generally considered safe based on centuries of traditional use

Documented Adverse Effects: Few historical reports of adverse effects when used in traditional preparations

Historical Contraindications: Limited documentation of specific contraindications in traditional texts

Scientific Validation: Modern research has validated many traditional uses, particularly for anti-inflammatory and antimicrobial effects

Pharmaceutical Development: Development of semi-synthetic derivatives for pharmaceutical applications, particularly for HIV and cancer

Supplement Market Emergence: Increasingly available as a dietary supplement, often as part of birch bark extracts or chaga mushroom preparations

Decoctions: Boiling plant materials in water to extract water-soluble components (though betulinic acid itself is poorly water-soluble)

Tinctures: Extraction in alcohol, which more effectively extracts betulinic acid

Infused Oils: Extraction into oils for topical applications

Poultices: Direct application of crushed or macerated plant materials to affected areas

Cancer Research: Identification of selective cytotoxicity against melanoma cells in the 1990s sparked renewed interest

HIV Research: Discovery of anti-HIV activity led to development of bevirimat and other derivatives

Ethnopharmacological Studies: Scientific investigation of traditional remedies led to identification of betulinic acid as an active component

Rating Rationale: Moderate evidence from numerous preclinical studies and limited human trials. Strong mechanistic understanding but lacks large-scale clinical trials for most applications.

Limited formal meta-analyses exist specifically for betulinic acid interventions due to the heterogeneity of study designs and limited number of clinical trials, Systematic reviews of triterpenes including betulinic acid suggest consistent anti-cancer, anti-inflammatory, and antiviral effects across multiple studies

Clinical evaluation of betulinic acid derivatives for HIV treatment, Investigation of enhanced delivery systems for betulinic acid in cancer therapy, Studies on topical applications for melanoma and other skin cancers, Evaluation of betulinic acid as an adjunct therapy in combination with conventional cancer treatments

Clinical Validation: Large-scale, well-designed clinical trials are needed to validate preclinical findings

Bioavailability: Further research on enhancing bioavailability in humans is critical

Long Term Effects: Studies on long-term safety and efficacy are lacking

Dosing Optimization: Optimal dosing regimens for specific conditions need to be established

Drug Interactions: More comprehensive evaluation of potential drug interactions is needed

Comparative Effectiveness: Studies comparing betulinic acid to established treatments for various conditions

Cancer Effects: While most studies show selective cytotoxicity against cancer cells, some cell types appear resistant to betulinic acid-induced apoptosis

Mechanism Specificity: Some studies suggest p53-independent mechanisms, while others indicate p53 involvement in certain cell types

Bioavailability Impact: Disagreement on the clinical relevance of poor bioavailability, with some researchers suggesting local gastrointestinal effects may be beneficial regardless of systemic absorption

Consensus View: Generally recognized as a promising natural compound with multiple health benefits, particularly for anti-cancer, anti-inflammatory, and antiviral applications

Areas Of Disagreement: Optimal formulations, dosing, and specific clinical applications remain subjects of debate

Future Directions: Focus on enhanced delivery systems and targeted clinical trials is recommended by most experts

Cancer Patients: Strongest evidence for potential benefits in melanoma and other cancer types

HIV Patients: Limited but promising evidence for antiviral effects, particularly with modified derivatives

Inflammatory Conditions: Moderate evidence for benefits in various inflammatory disorders

Metabolic Disorders: Emerging evidence for benefits in metabolic syndrome and related conditions

Success Rate: Limited translation of promising preclinical findings to clinical applications thus far

Barriers: Poor bioavailability, limited funding for natural product research, and regulatory challenges

Promising Areas: Modified derivatives and enhanced delivery systems show the most potential for successful clinical translation