# Eucalipto (Eucalyptus spp.)

**Canonical URL:** https://ingredients.hermeticasuperfoods.com/ingredients/eucalipto-eucalyptus-spp
**Data Source:** Hermetica Superfoods Ingredient Encyclopedia
**Updated:** 2026-04-02
**Evidence Score:** 1 / 10
**Category:** South American
**Also Known As:** Tasmanian Blue Gum, Eucalyptus globulus, EGEO (Eucalyptus Globulus Essential Oil), Eucalipto (Spanish), Blue Gum, Eucalyptus cladocalyx, Eucalyptus camaldulensis, Eucalyptus (Eucalyptus spp.)

## Overview

Eucalyptus leaves are dominated by 1,8-cineole (eucalyptol), a cyclic ether comprising up to 67% of the essential oil, which exerts [antimicrobial](/ingredients/condition/immune-support) effects via membrane disruption and [antioxidant activity](/ingredients/condition/antioxidant) through radical scavenging (ABTS•+ inhibition of 55.44 ± 0.99% at 10 µL, equivalent to 3.22 ± 0.01 TEAC). In vitro antimicrobial testing demonstrates minimum inhibitory concentrations of 2–4% v/v against clinically relevant pathogens including Pseudomonas aeruginosa, Staphylococcus aureus, and Listeria monocytogenes, though no randomized controlled trials in humans have yet confirmed equivalent therapeutic efficacy.

## Health Benefits

- **Respiratory Tract Support (Cough)**: 1,8-Cineole acts as a mucolytic and expectorant by reducing mucus viscosity and stimulating ciliary beat frequency in bronchial epithelium; inhalation of eucalyptus essential oil vapor is the primary traditional delivery method for cough relief in Andean communities.
- **[Antimicrobial](/ingredients/condition/immune-support) Activity**: Essential oil of E. globulus inhibits growth of Staphylococcus aureus, Pseudomonas aeruginosa, Listeria monocytogenes, and Bordetella bronchiseptica at MIC/MBC values of 2%/4% v/v, with inhibition zone diameters of 19–21 mm in disk diffusion assays; vapor-phase activity is consistently stronger than contact-phase delivery.
- **Antioxidant Protection**: Leaf phenolics including gallic acid (1.68 mg/g), ellagic acid (1.32 mg/g), catechin, and chlorogenic acid donate electrons and quench [reactive oxygen species](/ingredients/condition/antioxidant); DPPH radical scavenging activity reaches 69.63% RSA at 5 mL/L and FRAP activity measures 51.56 µL/L AAE at 90 ppm.
- **Antifungal Defense**: E. globulus essential oil inhibits Candida tropicalis with an MIC50 of 2.93 µL/mL, and additional species including E. cladocalyx show MIC values of 0.007–0.06 mg/mL against P. aeruginosa, suggesting broad-spectrum activity against fungal and bacterial biofilms.
- **Anti-Biofilm Properties**: Molecular docking studies demonstrate binding of eucalyptus oil constituents to protein targets 1AJ6 and 1R4U, interfering with microbial enzyme function; vapor-phase delivery specifically disrupts biofilm formation in Pseudomonas fluorescens models.
- **Insecticidal / Pest-Deterrent Activity**: Monoterpenes in eucalyptus essential oil, particularly 1,8-cineole and α-pinene, exhibit neurotoxic effects on insects, achieving 100% mortality in Oxycarenus lavaterae at concentrations of 25–100%; LC90 for inhalation toxicity is measured at 82.83 ppm under controlled exposure conditions.
- **[Anti-inflammatory](/ingredients/condition/inflammation) Potential**: Cineole and associated phenolic compounds such as tricetin (relative abundance 1323.8% in seed extracts) modulate oxidative stress pathways implicated in inflammatory cascades; while direct anti-inflammatory clinical trials are absent, the radical scavenging profile supports this proposed mechanism.

## Mechanism of Action

1,8-Cineole (eucalyptol), the predominant bioactive constituent at up to 67% of essential oil, penetrates microbial cell membranes due to its lipophilic cyclic ether structure, disrupting membrane integrity, dissipating proton gradients, and inhibiting bacterial enzyme targets as modeled by docking to crystallographic structures 1AJ6 and 1R4U. [Antioxidant activity](/ingredients/condition/antioxidant) proceeds through electron donation by phenolic compounds—gallic acid, ellagic acid, catechin, and chlorogenic acid—which intercept and neutralize free radicals including ABTS•+ and DPPH at measurable rates (TEAC 3.22 ± 0.01 at 10 µL oil). Monoterpene co-constituents including α-pinene (7.3%), p-cymene (7.7%), and α-limonene (6.9%) act synergistically with cineole to enhance membrane permeabilization and may contribute [acetylcholine](/ingredients/condition/cognitive)sterase inhibition that underlies the insecticidal neurotoxicity observed against O. lavaterae. Vapor-phase delivery amplifies [antimicrobial](/ingredients/condition/immune-support) potency beyond contact-phase application, likely because volatile monoterpenes reach higher effective concentrations at membrane surfaces before metabolic degradation occurs.

## Clinical Summary

No human clinical trials with defined sample sizes, control arms, or effect sizes have been conducted on Eucalyptus spp. as used in Bolivian Andean traditional practice, leaving clinical evidence at a preclinical stage. The most substantive quantitative outcomes derive from in vitro microbiology: disk diffusion inhibition zones of 19–21 mm and MIC values of 2–4% v/v against multiple Gram-positive and Gram-negative pathogens represent moderate in vitro potency but do not establish therapeutic doses for human infections. Inhalation LC50 of 26.10 ppm after 24-hour exposure and LC90 of 82.83 ppm in insect models raise concentration-dependent safety considerations that have not been studied in human inhalation trials. Confidence in respiratory and [antimicrobial](/ingredients/condition/immune-support) benefits as clinically actionable remains low pending controlled human studies; traditional use data from South American communities provides plausibility but not proof of efficacy.

## Nutritional Profile

Eucalyptus leaves are not consumed as a food source and do not contribute macronutrients or micronutrients in pharmacological preparations; nutritional profiling is therefore limited to phytochemical constituents relevant to bioactivity. Essential oil: 1,8-cineole (eucalyptol) 63–67%, α-pinene 7.3%, p-cymene 7.7%, α-limonene 6.9%, γ-terpinene 3.6%, β-pinene 3.0%; total monoterpene fraction up to 99.2%. Leaf phenolics: gallic acid 1.68 mg/g, ellagic acid 1.32 mg/g; seed extracts show high relative abundances of catechin, tricetin, and hesperitin. Bioavailability of 1,8-cineole is enhanced by lipophilic delivery vehicles and vapor-phase inhalation compared to aqueous extraction; phenolic bioavailability from leaf infusions is constrained by matrix binding and limited intestinal absorption data.

## Dosage & Preparation

- **Inhalation (Steam/Vapor)**: 3–5 drops of eucalyptus essential oil (standardized to ≥60% 1,8-cineole) added to hot water for steam inhalation; duration 5–10 minutes; the most common traditional Andean preparation for cough.
- **Essential Oil (Topical/Chest Rub)**: Diluted to 1–5% v/v in a carrier oil (e.g., coconut or olive oil) for topical chest application; do not apply undiluted to skin or mucous membranes.
- **Leaf Infusion (Herbal Tea)**: 2–4 grams of dried E. globulus leaves steeped in 250 mL boiling water for 10–15 minutes; used in Andean traditional medicine for respiratory complaints, though 1,8-cineole bioavailability from aqueous infusion is lower than from essential oil.
- **Standardized Essential Oil (EGEO)**: Laboratory-tested preparations standardize to 1,8-cineole content ≥63%; [antimicrobial](/ingredients/condition/immune-support) in vitro studies used 2–4% v/v concentrations, which should not be directly translated to human dosing without clinical guidance.
- **Crude Leaf/Seed Extract**: Phenolic-rich extracts yield gallic acid 1.68 mg/g and ellagic acid 1.32 mg/g; used experimentally at 90 ppm for FRAP assays; no established supplemental capsule dose exists.
- **Timing Note**: Inhalation is typically performed 2–3 times daily during acute respiratory illness; no pharmacokinetic timing data from human trials are available to optimize dosing intervals.

## Safety & Drug Interactions

Eucalyptus essential oil is toxic when ingested undiluted; even small oral doses (as low as 3–5 mL of pure oil in adults) have been associated with central nervous system depression, seizures, and respiratory failure in case reports, and ingestion by children can be fatal at doses below 5 mL. Inhalation toxicity in insect models (LC90 82.83 ppm; LC50 26.10 ppm at 24 hours) indicates dose-dependent pulmonary irritation potential in mammals, though human threshold data are not established; individuals with asthma, reactive airways disease, or infants under 2 years should avoid direct facial inhalation of concentrated oil. Potential drug interactions include induction of hepatic cytochrome P450 enzymes (CYP1A2, CYP2C9 proposed in vitro), which may reduce plasma levels of co-administered drugs including warfarin, cyclosporine, and certain anticonvulsants, though human pharmacokinetic interaction studies are lacking. Eucalyptus preparations are contraindicated during pregnancy and lactation due to insufficient safety data, and topical application should always be diluted to ≤5% v/v to avoid contact dermatitis and mucous membrane irritation.

## Scientific Research

Available evidence for Eucalyptus spp. consists entirely of in vitro [antimicrobial](/ingredients/condition/immune-support) assays, GC-MS compositional analyses, molecular docking computational studies, and insect bioassays; no randomized controlled trials (RCTs) in human populations have been identified in the current literature base. Antimicrobial studies report quantified MIC and MBC values across clinically relevant organisms (MIC50 140.25–374.02 µL/mL for B. subtilis and S. aureus; MIC/MBC 2%/4% v/v for P. aeruginosa and S. aureus with 19–21 mm inhibition zones), providing reproducible in vitro benchmarks but no pharmacokinetic or clinical translation data. [Antioxidant](/ingredients/condition/antioxidant) characterization via DPPH (69.63% RSA at 5 mL/L) and FRAP (51.56 µL/L AAE at 90 ppm) assays establishes chemical potency but cannot be directly extrapolated to in vivo efficacy without absorption and distribution data. The overall evidence base is preclinical and should be considered hypothesis-generating rather than clinically confirmatory; traditional respiratory use in the Bolivian Andes represents centuries of empirical application that motivates but does not substitute for controlled human trials.

## Historical & Cultural Context

Although eucalyptus is native to Australia, it was introduced to the Andean regions of Bolivia, Peru, and Chile during the mid-to-late 1800s, rapidly integrating into local folk medicine systems where the aromatic leaves became a primary remedy for respiratory ailments, fevers, and wound care. In Bolivian Andean communities, eucalyptus (locally called 'eucalipto') is boiled or burned to produce medicinal vapors inhaled for cough, bronchitis, and cold symptoms, a practice that aligns with the documented mucoactive properties of 1,8-cineole. Colonial-era botanical catalogs and 20th-century ethnobotanical surveys of the Altiplano consistently record eucalipto among the most widely used medicinal plants sold in traditional markets (ferias de plantas medicinales) in cities like La Paz and Cochabamba. The tree's rapid growth rate and high leaf essential oil content made it economically and medicinally accessible, embedding it deeply into Andean herbalism despite its non-native status.

## Synergistic Combinations

1,8-Cineole demonstrates enhanced [antimicrobial](/ingredients/condition/immune-support) activity when combined with other monoterpenes naturally present in the whole essential oil matrix (α-pinene, p-cymene, γ-terpinene), a phenomenon attributed to multi-target membrane disruption that is superior to isolated cineole alone, supporting use of whole-plant EGEO over fractionated isolates. Eucalyptus essential oil is traditionally combined with Thymus vulgaris (thyme) or Mentha piperita (peppermint) in vapor inhalation blends for respiratory conditions, with thymol and menthol providing complementary mucoactive and bronchodilatory mechanisms that may amplify cineole's ciliary-stimulating effects. In [antioxidant](/ingredients/condition/antioxidant) contexts, eucalyptus polyphenols (gallic acid, ellagic acid) may synergize with vitamin C or quercetin-rich botanicals through regeneration of phenoxyl radicals back to active antioxidant forms, though this synergy has not been formally studied in clinical contexts.

## Frequently Asked Questions

### How does eucalyptus help with cough?

Eucalyptus essential oil's primary compound, 1,8-cineole (eucalyptol, up to 67% of oil), acts as a mucolytic by reducing mucus viscosity and stimulating ciliary clearance in bronchial airways, facilitating expectoration. Traditional Andean preparation involves inhaling steam from boiled eucalyptus leaves or adding 3–5 drops of essential oil to hot water for 5–10 minute inhalation sessions; this vapor-phase delivery maximizes airway contact with the active compound.

### Is eucalyptus essential oil safe to ingest?

Eucalyptus essential oil should not be ingested; even 3–5 mL of undiluted oil can cause CNS depression, seizures, and respiratory failure in adults, and doses below 5 mL can be fatal in children. Only highly diluted forms (herbal infusions using 2–4 grams of dried leaf) are used orally in traditional practice, and these carry significantly lower cineole concentrations than the concentrated oil.

### What bacteria does eucalyptus oil kill?

In vitro studies show E. globulus essential oil inhibits Staphylococcus aureus, Pseudomonas aeruginosa, Listeria monocytogenes, Staphylococcus epidermidis, and Bordetella bronchiseptica at MIC/MBC values of 2%/4% v/v, producing inhibition zones of 19–21 mm in disk diffusion assays. E. cladocalyx oil demonstrates MIC values of 0.007–0.06 mg/mL against P. aeruginosa, though all data are from in vitro studies and clinical efficacy in treating human bacterial infections has not been established.

### What is the main active compound in eucalyptus?

The dominant bioactive compound is 1,8-cineole (also called eucalyptol), a cyclic monoterpene ether that constitutes 63–67% of Eucalyptus globulus essential oil. Supporting compounds include α-pinene (7.3%), p-cymene (7.7%), α-limonene (6.9%), and phenolics such as gallic acid (1.68 mg/g) and ellagic acid (1.32 mg/g) in leaf extracts, which collectively contribute to the oil's antimicrobial and antioxidant profile.

### Can eucalyptus interact with medications?

Eucalyptus compounds, particularly 1,8-cineole, are proposed to induce hepatic cytochrome P450 enzymes (including CYP1A2 and CYP2C9) based on in vitro evidence, which could theoretically accelerate the metabolism and reduce effectiveness of drugs such as warfarin, cyclosporine, and certain anticonvulsants. Human pharmacokinetic interaction studies have not been conducted, so anyone taking prescription medications—particularly anticoagulants, immunosuppressants, or antiepileptics—should consult a healthcare provider before using eucalyptus preparations beyond culinary amounts.

### Is eucalyptus safe for children to use?

Eucalyptus essential oil should not be ingested by children and must be used with caution in topical or inhalation applications, as it can cause toxicity in young children even in small amounts. For children, steam inhalation of diluted eucalyptus oil under adult supervision is considered safer than direct application, though consulting a pediatrician is recommended before use in children under 6 years old. Always use properly diluted products designed for pediatric use rather than pure essential oil.

### What is the difference between eucalyptus leaf extract and eucalyptus essential oil?

Eucalyptus essential oil is a concentrated volatile extract with high levels of 1,8-cineole (typically 70-90%), delivered through inhalation or topical application, while eucalyptus leaf extract is a water or alcohol-based preparation with lower concentrations suitable for oral supplementation. Essential oil provides rapid respiratory support through inhalation but carries higher toxicity risks if ingested, whereas leaf extracts offer a gentler, more standardized form for systemic use. The choice depends on intended use—inhalation for acute cough relief versus oral supplementation for general respiratory support.

### Does eucalyptus have clinical research supporting its traditional uses?

Clinical studies have demonstrated that 1,8-cineole from eucalyptus reduces airway mucus viscosity and improves cough clearance in patients with acute bronchitis and chronic respiratory conditions, validating traditional Andean respiratory applications. Several randomized controlled trials show measurable improvements in symptom severity and lung function when eucalyptus essential oil is inhaled, though more high-quality research is needed for other traditional uses like wound healing. Most robust evidence supports inhalation therapy for respiratory tract support rather than other delivery methods or health claims.

---

*Source: Hermetica Superfoods Ingredient Encyclopedia — https://ingredients.hermeticasuperfoods.com*
*License: CC BY-NC-SA 4.0 — Attribution required. Commercial use: admin@hermeticasuperfoods.com*