# Cocklebur (Xanthium strumarium)

**Canonical URL:** https://ingredients.hermeticasuperfoods.com/ingredients/cocklebur-xanthium-strumarium
**Data Source:** Hermetica Superfoods Ingredient Encyclopedia
**Updated:** 2026-04-02
**Evidence Score:** 1 / 10
**Category:** South American
**Also Known As:** Xanthium strumarium, Cang Er Zi, Common Cocklebur, Rough Cocklebur, Arishta, Chota Dhatura, Clotbur

## Overview

Xanthium strumarium contains sesquiterpenoids, phenylpropanoids, and flavonoids—including cirsilineol and structurally unique benzofuran-acrylaldehyde derivatives—that exert [antioxidant activity](/ingredients/condition/antioxidant) via free-radical scavenging and cytotoxic effects through probable apoptosis induction. The ethyl acetate leaf fraction (400 mg/kg) reduced fasting [blood glucose](/ingredients/condition/weight-management) by approximately 38% (from 353 ± 10.6 to 220 ± 25.5 mg/dL, p ≤ 0.05) in alloxan-induced diabetic mice over 18 days, representing the most quantitatively substantiated preclinical effect to date.

## Health Benefits

- **Antidiabetic Activity**: The ethyl acetate foliage fraction significantly lowered blood glucose in alloxan-induced diabetic mice at 400 mg/kg over 18 days, likely through phenolic-mediated enhancement of [insulin sensitivity](/ingredients/condition/weight-management) or peripheral glucose uptake; effect size was approximately 38% reduction (p ≤ 0.05).
- **Antioxidant Protection**: Acetone whole-plant extracts demonstrated exceptionally high free-radical scavenging capacity (DPPH: 442.81 ± 5.21 mg Trolox/g; TPC: 454.54 ± 4.32 mg GAE/g), driven by dense phenolic and flavonoid content that neutralizes [reactive oxygen species](/ingredients/condition/antioxidant).
- **Cytotoxic/Anticancer Potential**: Isolated compound 1—a benzofuran-acrylaldehyde sesquilignan—showed IC₅₀ of 10.2 ± 1.2 µM against HepG2 hepatocellular carcinoma cells in vitro, with cirsilineol displaying moderate activity against MCF-7 breast cancer cells, suggesting apoptosis-inducing properties.
- **Antimicrobial Action**: Acetone extracts exhibited the lowest minimum inhibitory concentrations among tested solvent fractions against multiple bacterial and fungal strains, attributed to the combined activity of sesquiterpenoids and phenylpropanoids disrupting microbial membrane integrity.
- **[Anti-inflammatory](/ingredients/condition/inflammation) Effects**: Leaf extracts display membrane-stabilizing activity in preclinical assays—a recognized proxy for anti-inflammatory potential—consistent with traditional use for rheumatic and inflammatory conditions, though the precise molecular targets remain uncharacterized.
- **[Hepatoprotective](/ingredients/condition/detox) Potential**: The cytotoxic selectivity of isolated compounds toward hepatocellular carcinoma lines, combined with high antioxidant indices, suggests possible hepatoprotective properties under oxidative stress conditions, though direct hepatoprotection models have not been formally published.
- **[Immunomodulatory](/ingredients/condition/immune-support) Support**: Polysaccharide and flavonoid fractions are traditionally ascribed immunomodulatory roles, and the presence of over 170 identified phytochemicals—including alkaloids, terpenoids, and lignanoids—provides a phytochemical basis for pleiotropic immune interactions, though controlled mechanistic studies are lacking.

## Mechanism of Action

The [antioxidant activity](/ingredients/condition/antioxidant) of X. strumarium extracts is primarily mediated by electron-donation and hydrogen-atom transfer from phenolic hydroxyl groups of flavonoids (including cirsilineol) and phenylpropanoids, as quantified by DPPH, ABTS, and FRAP assays, with ethyl acetate fractions showing the highest phenolic density (95.25 mg GAE/g) and corresponding radical-scavenging potency. Antidiabetic effects are hypothesized to involve phenolic inhibition of α-glucosidase and α-amylase or direct potentiation of insulin signaling cascades (e.g., GLUT-4 translocation), consistent with the significant [blood glucose](/ingredients/condition/weight-management) reduction observed in alloxan-diabetic mice, though specific enzyme kinetics and receptor binding data have not been published. Cytotoxic compounds such as the benzofuran-acrylaldehyde derivative (compound 1, IC₅₀ 10.2 ± 1.2 µM on HepG2) likely trigger intrinsic apoptotic pathways involving [mitochondrial](/ingredients/condition/energy) membrane depolarization and caspase activation, a mechanism inferred from structural analogy with related sesquilignans rather than direct pathway confirmation. Membrane-stabilizing activity in leaf extracts suggests inhibition of phospholipase A₂ or stabilization of lysosomal membranes as a contributing [anti-inflammatory](/ingredients/condition/inflammation) mechanism, paralleling the action profile of non-steroidal anti-inflammatory scaffolds.

## Clinical Summary

No human clinical trials investigating X. strumarium for any indication—including rheumatism, diabetes, or cancer—have been published or indexed in available literature. The entirety of functional evidence derives from in vitro cytotoxicity assays (cancer cell lines, n = 3 replicates per experiment) and a single-species alloxan-induced diabetic mouse model for antidiabetic activity. The most compelling quantified outcome remains the 38% fasting glucose reduction at 400 mg/kg ethyl acetate fraction in mice, a dose that has no validated human equivalent without allometric scaling and bioavailability data. Confidence in therapeutic extrapolation to humans is very low; the ingredient should be regarded as a research-stage botanical candidate rather than a clinically validated supplement.

## Nutritional Profile

Xanthium strumarium is not consumed as a food ingredient and lacks a conventional macronutrient profile; its nutritional relevance lies in its dense secondary metabolite content. Total phenolic content ranges from 12.20 mg GAE/g (water fraction) to 454.54 mg GAE/g (acetone extract), and total flavonoids reach 78.94 ± 2.25 mg catechin equivalents/g in acetone extract—values indicating extraordinary phenolic richness relative to common dietary botanicals. Characteristic phytochemicals include sesquiterpenoids (xanthatin, xanthinosin, tomentosin), phenylpropanoids, lignanoids (including benzofuran-acrylaldehyde derivatives), flavonoids (cirsilineol, luteolin derivatives), alkaloids, and polysaccharides, totaling over 170 identified compounds. Bioavailability of these constituents is unknown; solvent polarity markedly affects extractable phenolic yield, with ethyl acetate consistently outperforming aqueous fractions for phenolic recovery from foliage, suggesting lipophilic carriers may enhance absorption, though no in vivo pharmacokinetic data exist.

## Dosage & Preparation

- **Ethyl Acetate Leaf Fraction (Research)**: 400 mg/kg body weight orally in mice (sole dose with quantified antidiabetic outcome); no human equivalent dose established.
- **Acetone Whole-Plant Extract**: Used in [antioxidant](/ingredients/condition/antioxidant) and [antimicrobial](/ingredients/condition/immune-support) assays at concentrations yielding TPC of 454.54 ± 4.32 mg GAE/g; not standardized for human use.
- **Ethanol Extract**: 65.14 mg GAE/g total phenolics; used in comparative phytochemical analysis; no clinical dose defined.
- **Traditional Decoction (Folkloric)**: Dried fruits or leaves boiled in water and consumed orally for [anti-inflammatory](/ingredients/condition/inflammation) or rhinitis indications in Asian traditional medicine; quantities are not standardized in any pharmacopeial reference.
- **Methanol Leaf Extract**: Reported richest in total phytoconstituents among commonly used solvents; employed in antimicrobial MIC testing but lacks human dosing guidance.
- **Standardization**: No commercial standardization to specific marker compounds (e.g., cirsilineol or xanthatin) has been established; no certificate-of-analysis benchmarks are published.
- **Timing/Notes**: No pharmacokinetic data exist to guide administration timing; given known toxicity of certain fractions at higher concentrations, unsupervised human use is not recommended.

## Safety & Drug Interactions

Xanthium strumarium contains compounds with demonstrated dose-dependent cytotoxicity in cancer cell lines (extract IC₅₀ values: 180.12–410.23 µg/mL for crude fractions; 10.2–18.3 µM for isolated compounds), raising concern that high-dose or prolonged human exposure could harm normal tissues, particularly hepatocytes—a risk underscored by historical reports of livestock poisoning from seedling ingestion attributed to carboxyatractyloside, a diterpenoid glycoside. No formal drug interaction studies exist; however, given phenolic-mediated modulation of [glucose metabolism](/ingredients/condition/weight-management), concurrent use with antidiabetic medications (metformin, sulfonylureas, insulin) theoretically risks additive hypoglycemia, and anticoagulant interactions cannot be excluded given flavonoid content. The plant is contraindicated in pregnancy in TCM tradition due to its uterotonic potential, and it should be avoided in lactation, pediatric populations, and individuals with hepatic impairment absent safety data; cases of hepatotoxicity in humans have been anecdotally linked to Cang Er Zi overdose in Chinese medical literature. No maximum safe human dose has been established through controlled toxicological studies; human use beyond supervised ethnomedicinal contexts is not currently supportable by the available evidence.

## Scientific Research

The current evidence base for X. strumarium consists entirely of in vitro cell-line studies and small in vivo rodent experiments, with no registered or published human clinical trials identified in any available database as of the current review. Key quantitative findings include a ~38% [blood glucose](/ingredients/condition/weight-management) reduction in alloxan-diabetic mice with ethyl acetate extract at 400 mg/kg over 18 days (n unspecified, p ≤ 0.05), and cytotoxic IC₅₀ values for isolated compounds ranging from 10.2 ± 1.2 µM (compound 1, HepG2) to 18.3 ± 1.6 µM (compound 3), each measured in triplicate. Phytochemical characterization studies are the most robust portion of the literature, with over 170 compounds structurally identified across multiple independent investigations, lending high confidence to compositional claims but not to therapeutic efficacy in humans. The overall evidence level is preliminary, and extrapolation of preclinical dose-response data to human supplementation is not scientifically supported without pharmacokinetic bridging studies and randomized controlled trials.

## Historical & Cultural Context

Xanthium strumarium has a lengthy history of use in Traditional Chinese Medicine (TCM), where the dried ripe fruits—known as Cang Er Zi (苍耳子)—are a classical remedy for rhinitis, sinusitis, headache, and rheumatic pain, appearing in the Shennong Bencao Jing and subsequent materia medica texts spanning over two millennia. In Ayurvedic traditions of the Indian subcontinent, the plant is recognized as Arishta or Chota Dhatura and applied topically and internally for skin diseases, leprosy, and joint inflammation. Indigenous communities in parts of South America and Africa have independently adopted the plant for wound healing and [anti-inflammatory](/ingredients/condition/inflammation) purposes, consistent with its cosmopolitan distribution and the convergent observation of its bioactive phenolic content across cultures. Traditional preparation most commonly involves decoction of dried fruits or leaves, though seed oils and whole-plant pastes have also been documented, with dosing historically governed by empirical tradition rather than measured pharmacology.

## Synergistic Combinations

In TCM formulations, Cang Er Zi (X. strumarium fruit) is classically combined with Xin Yi Hua (Magnolia biondii flower buds) and Bo He (Mentha haplocalyx) to treat nasal congestion and rhinitis, where the [anti-inflammatory](/ingredients/condition/inflammation) and vasoconstrictive properties of magnolol/honokiol and menthol are thought to act synergistically with xanthatin's anti-inflammatory sesquiterpenoid activity. Phenolic-rich extracts of X. strumarium may exhibit additive [antioxidant](/ingredients/condition/antioxidant) synergy when combined with other high-polyphenol botanicals such as green tea (EGCG) or quercetin-containing plants, as multi-pathway radical scavenging via structurally diverse phenolics can outperform single-compound approaches in vitro. No pharmacodynamically validated or clinically tested combination stacks involving X. strumarium have been published in peer-reviewed literature.

## Frequently Asked Questions

### What is Xanthium strumarium used for in traditional medicine?

In Traditional Chinese Medicine, the dried fruits (Cang Er Zi) have been used for over 2,000 years to treat rhinitis, sinusitis, headache, and rheumatic pain. In Ayurvedic medicine, the plant is applied for skin diseases and joint inflammation, while South American and African traditions use it for wound healing and anti-inflammatory purposes. Preparations typically involve decoction of dried fruits or leaves, though no modern standardized dosage form exists.

### Does Xanthium strumarium lower blood sugar?

Preclinical evidence shows that the ethyl acetate leaf fraction of X. strumarium (400 mg/kg orally) reduced fasting blood glucose by approximately 38%—from 353 ± 10.6 to 220 ± 25.5 mg/dL (p ≤ 0.05)—in alloxan-induced diabetic mice over 18 days. The mechanism is hypothesized to involve phenolic inhibition of carbohydrate-digesting enzymes or enhancement of insulin signaling, but no human clinical trials have been conducted to confirm this effect in people.

### Is Xanthium strumarium safe for human consumption?

Human safety data for X. strumarium are very limited; the plant's seeds and seedlings contain carboxyatractyloside, a diterpenoid glycoside associated with hepatotoxicity in livestock and anecdotal cases of liver injury in humans from Cang Er Zi overdose. Isolated compounds show dose-dependent cytotoxicity in cell lines at low micromolar concentrations, and no maximum safe human dose has been established through controlled toxicology studies. Use during pregnancy is contraindicated in TCM tradition, and individuals with liver disease or those taking antidiabetic or anticoagulant medications should avoid unsupervised use.

### What are the main bioactive compounds in Xanthium strumarium?

Over 170 compounds have been identified in X. strumarium, with sesquiterpenoids (xanthatin, xanthinosin, tomentosin), phenylpropanoids, lignanoids (including a benzofuran-acrylaldehyde derivative with IC₅₀ 10.2 µM against HepG2 cells), and flavonoids (cirsilineol, luteolin derivatives) regarded as the primary bioactives. Total phenolic content in the most potent extracts reaches up to 454.54 mg GAE/g (acetone extract) and total flavonoids up to 78.94 mg catechin equivalents/g. The specific phytochemical profile varies significantly by plant part and extraction solvent.

### Are there clinical trials on Xanthium strumarium?

As of the current literature review, no published human clinical trials investigating X. strumarium for any therapeutic indication—including rheumatism, diabetes, or cancer—have been identified in available databases. All existing efficacy data are derived from in vitro cell-line assays and small rodent models, which limits their direct applicability to human health outcomes. Xanthium strumarium should currently be considered a research-stage botanical with promising preclinical signals but unverified clinical benefit.

### What forms of Xanthium strumarium are available, and which is most bioavailable?

Xanthium strumarium is available as dried leaf powder, ethanol/water extracts, and standardized herbal formulations. Research shows that ethyl acetate foliage fractions and acetone whole-plant extracts demonstrate superior bioavailability and antidiabetic/antioxidant activity compared to aqueous preparations. Extract forms appear to concentrate the phenolic and bioactive compounds responsible for the herb's biological effects more effectively than simple dried preparations.

### Is Xanthium strumarium safe to use with diabetes medications?

Xanthium strumarium should not be combined with diabetes medications without medical supervision, as it has demonstrated significant blood glucose-lowering effects (approximately 38% reduction in animal studies). Co-administration with insulin or oral hypoglycemic agents could increase hypoglycemia risk and require dose adjustments. Consult a healthcare provider before using this ingredient alongside any diabetes treatment.

### Who should avoid Xanthium strumarium supplementation?

Pregnant and breastfeeding women should avoid Xanthium strumarium due to insufficient safety data and its known bioactive compounds that may affect fetal development or milk composition. Individuals with existing hypoglycemia, those scheduled for surgery, and people with severe liver or kidney dysfunction should also avoid this herb. Additionally, those with allergies to plants in the Asteraceae family may experience cross-reactivity.

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