# Pennyroyal (Mentha pulegium)

**Canonical URL:** https://ingredients.hermeticasuperfoods.com/ingredients/pennyroyal-mentha-pulegium
**Data Source:** Hermetica Superfoods Ingredient Encyclopedia
**Updated:** 2026-04-02
**Evidence Score:** 1 / 10
**Category:** Middle Eastern
**Also Known As:** Mentha pulegium, Pennyroyal, European pennyroyal, Fleabane, Pudding grass, Flieh-Minze, Poleo, Fliou (Arabic)

## Overview

Pennyroyal's essential oil is dominated by the monoterpene ketone pulegone (40–61%) and menthone (up to 21%), which exert [antimicrobial](/ingredients/condition/immune-support), antispasmodic, and enzyme-inhibitory effects through membrane disruption and modulation of tyrosinase and elastase activity. In vitro [antioxidant](/ingredients/condition/antioxidant) studies show phenolic extracts achieve DPPH radical scavenging with an IC50 of 18 µg/mL, comparable to ascorbic acid at 15 µg/mL, though no human clinical trials have validated therapeutic doses or confirmed safety for internal use.

## Health Benefits

- **[Antimicrobial](/ingredients/condition/immune-support) Activity**: The essential oil's pulegone and menthone components disrupt microbial cell membranes, demonstrating broad-spectrum activity against bacterial and fungal pathogens in multiple in vitro assays, with synergistic effects when the whole EO is used versus isolated fractions.
- **[Antioxidant Protection](/ingredients/condition/antioxidant)**: Hydroalcoholic extracts rich in ferulic acid (13.19 µg/mL), chrysoeriol (15.36 µg/mL), and kaempferol (11.14 µg/mL) scavenge free radicals with an IC50 of 18 µg/mL across DPPH, PAB, and NO assays, suggesting potential for oxidative stress reduction.
- **Anti-inflammatory Effects**: Phenolic compounds including caffeic acid, p-coumaric acid, and luteolin inhibit pro-[inflammatory pathway](/ingredients/condition/inflammation)s in vitro, with the whole extract demonstrating hemolysis inhibition of 79.8% at 1000 µg/mL, indicating membrane-stabilizing and anti-inflammatory capacity.
- **Respiratory and Antispasmodic Support**: Traditional use for bronchitis and respiratory congestion is supported by the presence of eucalyptol (1,8-cineole, 3.82–5.2%), a known bronchodilatory and mucolytic agent, alongside menthol (up to 5.18%) which activates TRPM8 cold receptors to ease airway perception.
- **Digestive Aid**: Historical use for in[digestion](/ingredients/condition/gut-health) and flatulence is consistent with the carminative properties of menthone and pulegone, which relax gastrointestinal smooth muscle and reduce intestinal spasms, though clinical confirmation is absent.
- **[Anti-aging](/ingredients/condition/longevity) and Dermocosmetic Potential**: Whole EO inhibits tyrosinase at 56 µg/mL and elastase at 90 µg/mL, with molecular synergy exceeding isolated pulegone (217–240 µg/mL) or menthone alone, suggesting topical utility for pigmentation and [skin elasticity](/ingredients/condition/skin-health).
- **Insecticidal and Repellent Properties**: EO monoterpenes demonstrate contact insecticidal activity against aphids with LD50 values of 107–142 µL/mL and historically served as a flea and insect repellent in Mediterranean households, a use supported by modern laboratory data.

## Mechanism of Action

Pulegone, the dominant monoterpene ketone (40–61% of EO), is metabolized hepatically via CYP450 enzymes to the reactive intermediate menthofuran, which depletes [glutathione](/ingredients/condition/detox) and can induce oxidative hepatotoxicity at high doses; at subthreshold concentrations, pulegone and menthone modulate enzyme activity by competitively inhibiting tyrosinase (IC50 ~56 µg/mL for whole EO) and elastase (IC50 ~90 µg/mL), reducing melanin synthesis and extracellular matrix degradation respectively. Phenolic constituents such as ferulic acid, caffeic acid, and chrysoeriol donate hydrogen atoms to neutralize [reactive oxygen species](/ingredients/condition/antioxidant) and chelate transition metals, while flavonoids including kaempferol and luteolin inhibit cyclooxygenase and lipoxygenase pathways to reduce pro-inflammatory eicosanoid production. Molecular docking studies on the related compound piperitenone indicate binding affinities for acetylcholinesterase (−7.4 kcal/mol), DNA gyrase (−6.4 kcal/mol), and peroxiredoxin (−5.3 kcal/mol), suggesting plausible [neuroprotective](/ingredients/condition/cognitive) and [antimicrobial](/ingredients/condition/immune-support) mechanisms that require experimental validation. Eucalyptol (1,8-cineole) present in the EO activates TRPA1 channels and inhibits NF-κB signaling, contributing to both bronchodilatory and [anti-inflammatory](/ingredients/condition/inflammation) effects observed in the respiratory traditional use context.

## Clinical Summary

No formal clinical trials in human subjects have been identified in the peer-reviewed literature for Mentha pulegium across any of its traditional indications including respiratory disease, in[digestion](/ingredients/condition/gut-health), or menstrual disorders. Ex vivo coagulation studies using human plasma demonstrated measurable PT and APTT prolongation at 50 µg/mL extract concentration, signaling a pharmacologically relevant anticoagulant effect that raises drug interaction concerns but does not constitute clinical efficacy evidence. Animal toxicology data consistently highlights hepatotoxic and abortifacient risks from pulegone-containing preparations, which has discouraged the initiation of human dose-escalation or efficacy studies. Confidence in any clinical benefit claim remains very low, and regulatory authorities in the EU and US have issued warnings against internal use of pennyroyal oil, reflecting the unfavorable risk-benefit profile in the absence of positive clinical trial data.

## Nutritional Profile

Dried Mentha pulegium aerial parts provide modest amounts of dietary minerals including calcium, magnesium, and potassium typical of leafy herbs, but are consumed in quantities too small to contribute meaningfully to micronutrient intake. The principal bioactive constituents are concentrated in the essential oil fraction: pulegone (40–61%), menthone (up to 21%), α-terpineol (7.98%), eucalyptol/1,8-cineole (3.82–5.2%), menthol (1.5–5.2%), D-limonene (2.42%), and minor pinene isomers. The phenolic fraction of hydroalcoholic extracts contains ferulic acid (13.19 µg/mL), cinnamic acid (12.69 µg/mL), caffeic acid (11.45 µg/mL), pyrogallol (9.36 µg/mL), and p-coumaric acid (5.06 µg/mL), alongside flavonoids chrysoeriol (15.36 µg/mL), kaempferol (11.14 µg/mL), 7-hydroxyflavone (10.14 µg/mL), and luteolin (2.36 µg/mL). Bioavailability data for these compounds from whole herb preparations is absent; volatile terpenes are expected to be rapidly absorbed via inhalation or gastrointestinal mucosa, while polyphenol bioavailability depends on gut microbiota-mediated biotransformation.

## Dosage & Preparation

- **Herbal Tea (Traditional)**: 1–2 g of dried aerial parts steeped in 150–200 mL boiling water for 5–10 minutes; consumed up to twice daily in folk medicine contexts, though no safe dose has been established clinically.
- **Essential Oil (External/Research Use Only)**: Tested in vitro at concentrations of 0.5–3 mg/mL; not recommended for internal consumption due to pulegone hepatotoxicity; topical application requires significant dilution (≤0.5% in carrier oil) and patch testing.
- **Hydroalcoholic Extract**: Used in laboratory studies at IC50 concentrations of 18 µg/mL for [antioxidant activity](/ingredients/condition/antioxidant); no standardized commercial preparation exists for human supplementation.
- **Standardization**: No pharmacopoeial standardization for pulegone content in supplements exists; raw EO may contain 40–61% pulegone, making dose control critical and internal use hazardous.
- **Timing and Caution**: All preparations should be avoided in pregnancy, during anticoagulant therapy, and in individuals with hepatic impairment; no safe long-term dosing regimen has been validated in humans.

## Safety & Drug Interactions

Mentha pulegium essential oil poses serious hepatotoxicity risk due to high pulegone content (40–61%), which is bioactivated by hepatic CYP2E1 to the reactive intermediate menthofuran, depleting [glutathione](/ingredients/condition/detox) stores and causing centrilobular necrosis; fatal human cases have been documented following ingestion of as little as 10–30 mL of pure EO. Ex vivo data showing PT prolongation to 21.5 s and APTT to 49.5 s at 50 µg/mL extract concentrations indicates clinically relevant anticoagulant activity requiring avoidance alongside warfarin, heparin, aspirin, and other antiplatelet or anticoagulant agents. Pennyroyal is an established abortifacient and is absolutely contraindicated in pregnancy at any dose; it should also be avoided during lactation, in individuals with hepatic disease, renal impairment, or epilepsy, and in children. No maximum safe dose for internal use has been established in humans, and regulatory bodies including the European Medicines Agency and the US FDA advise against the internal consumption of pennyroyal oil; diluted topical use carries lower but non-zero risk of sensitization and systemic absorption.

## Scientific Research

The current evidence base for Mentha pulegium consists almost entirely of in vitro and ex vivo studies, with no published human randomized controlled trials reporting specific sample sizes, effect sizes, or clinical endpoints for any therapeutic indication. In vitro studies have quantified [antioxidant](/ingredients/condition/antioxidant) capacity (DPPH IC50 18 µg/mL), anticoagulant effects (PT prolongation to 21.5 s and APTT to 49.5 s at 50 µg/mL), and enzyme inhibition for tyrosinase and elastase using isolated compounds and whole EO fractions, providing mechanistic plausibility but no translational clinical data. Insecticidal activity has been characterized with LD50 values of 107–142 µL/mL against aphid models, representing one of the more quantitatively robust datasets available for this plant. Given the hepatotoxic risk of pulegone and the complete absence of controlled human trials, the overall evidence quality is classified as preliminary, and no therapeutic dose recommendations can be responsibly derived from current literature.

## Historical & Cultural Context

Mentha pulegium has one of the longest documented histories of any Mediterranean herb, referenced by ancient Greek physicians including Dioscorides and by Roman writers such as Pliny the Elder, who noted its use for digestive complaints, respiratory ailments, and menstrual regulation. In Middle Eastern and North African folk medicine, pennyroyal tea remains a common household remedy for bloating, colds, and bronchitis, and dried bunches are traditionally hung in homes and food stores as insect repellents, particularly against fleas — a practice that gave rise to the common name 'pennyroyal' (from the Latin pulegium, linked to pulex meaning flea). Medieval European herbalists classified it as an emmenagogue and used it to stimulate delayed menstruation, a practice that persisted through the 19th century and contributed to dangerous self-administration attempts. Its dual role as a culinary flavoring in some Mediterranean cuisines and as a medicinal herb underscores the cultural normalization of its use, contrasting sharply with modern toxicological assessments that classify the pure essential oil as potentially lethal in doses as low as 10 mL in adults.

## Synergistic Combinations

The whole essential oil of Mentha pulegium demonstrates synergistic enzyme inhibition compared to isolated compounds: combined pulegone and menthone show tyrosinase inhibition at 56 µg/mL versus 217–240 µg/mL for individual components, and elastase inhibition at 90 µg/mL versus 118–133 µg/mL, indicating a matrix synergy effect typical of complex botanical EOs. In traditional Middle Eastern formulations, pennyroyal is frequently paired with other aromatic herbs such as thyme (Thymus vulgaris) or oregano (Origanum compactum), combinations that may produce additive or synergistic [antimicrobial](/ingredients/condition/immune-support) effects through complementary membrane-disrupting terpene profiles including thymol and carvacrol acting alongside pulegone. Topical [anti-aging](/ingredients/condition/longevity) applications could theoretically benefit from pairing pennyroyal EO (for tyrosinase and elastase inhibition) with ascorbic acid or niacinamide, which address complementary oxidative and pigmentation pathways, though no combined formulation studies have been conducted.

## Frequently Asked Questions

### Is pennyroyal safe to drink as a tea?

Pennyroyal tea made from small amounts of dried herb (1–2 g) has a long history of traditional use, but carries real risk because even dilute preparations contain pulegone, a compound metabolized to the hepatotoxic intermediate menthofuran. No safe human dose has been established clinically, and the herb is absolutely contraindicated in pregnancy due to its abortifacient properties; individuals with liver conditions or on anticoagulant medications should avoid it entirely.

### What is pulegone and why is it dangerous?

Pulegone is a monoterpene ketone comprising 40–61% of pennyroyal essential oil and is the compound primarily responsible for both its biological activity and toxicity. It is bioactivated by hepatic CYP2E1 enzymes into menthofuran, a reactive metabolite that depletes hepatic glutathione and induces centrilobular liver necrosis; fatal human poisonings have occurred following ingestion of as little as 10–30 mL of pure pennyroyal essential oil.

### Can pennyroyal be used as an insect repellent?

Yes, pennyroyal has one of the best-documented insecticidal and repellent applications among Mediterranean herbs, with essential oil LD50 values of 107–142 µL/mL demonstrated against aphids in laboratory studies and centuries of traditional use against fleas — which is the etymological origin of its Latin name pulegium, from pulex (flea). Topical or environmental use of diluted EO is considered lower risk than internal consumption, though skin sensitization is possible and significant dilution in a carrier oil is necessary for direct skin application.

### Does pennyroyal help with respiratory problems?

Traditional use of pennyroyal tea for coughs, bronchitis, and nasal congestion is pharmacologically plausible given the presence of eucalyptol (1,8-cineole, 3.82–5.2%) and menthol (up to 5.18%) in the essential oil, both of which have established bronchodilatory and mucolytic mechanisms in other clinical contexts. However, no human clinical trials have evaluated pennyroyal specifically for respiratory outcomes, so evidence remains anecdotal and preclinical; safer, better-studied alternatives such as eucalyptus or peppermint oil are preferable for respiratory support.

### What drugs does pennyroyal interact with?

Pennyroyal extracts have demonstrated significant anticoagulant activity in ex vivo human plasma studies, prolonging prothrombin time (PT) to 21.5 seconds and activated partial thromboplastin time (APTT) to 49.5 seconds at 50 µg/mL, indicating a meaningful risk of bleeding potentiation when combined with warfarin, heparin, aspirin, clopidogrel, or other anticoagulant and antiplatelet agents. Additionally, its pulegone content may induce or compete with CYP2E1 and other hepatic enzymes, potentially altering the metabolism of drugs processed by these pathways; individuals on any prescription medication should consult a healthcare provider before use.

### What is the difference between pennyroyal essential oil and pennyroyal extract for antimicrobial purposes?

Pennyroyal essential oil demonstrates broader antimicrobial activity than isolated extracts because its pulegone and menthone components work synergistically to disrupt bacterial and fungal cell membranes. While the whole essential oil shows superior broad-spectrum activity in laboratory assays, the concentrated pulegone content in pure oil also carries higher toxicity risks, making diluted or whole-plant extracts potentially safer alternatives for topical antimicrobial applications.

### Is pennyroyal safe for pregnant women or breastfeeding mothers?

Pennyroyal is not recommended during pregnancy or breastfeeding due to pulegone's hepatotoxic and abortifacient properties, which have been associated with miscarriage and severe liver damage. The herb's toxicity profile makes it unsuitable for any reproductive or lactation phases when maternal and fetal safety must be prioritized.

### What clinical evidence supports pennyroyal's antioxidant benefits compared to other herbal antioxidants?

Pennyroyal's hydroalcoholic extracts contain significant antioxidant compounds like ferulic acid (13.19 µg/mL) and chrysoeriol, demonstrating free-radical scavenging capacity in laboratory studies. However, most clinical evidence remains limited to in vitro assays; robust human clinical trials comparing pennyroyal's antioxidant efficacy to established herbal antioxidants like green tea or turmeric extract are lacking, limiting definitive claims about its practical therapeutic benefit.

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*Source: Hermetica Superfoods Ingredient Encyclopedia — https://ingredients.hermeticasuperfoods.com*
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