Nordihydroguaiaretic acid (NDGA): The dominant lignan in chaparral, comprising 5-10% of the dry weight of the leaves and approximately 80% of all phenolic compounds in the leaf resin; a potent antioxidant with documented anticancer, antiviral, anti-inflammatory, and antimicrobial activity in laboratory settings, but also the compound most linked to hepatotoxicity concerns

Other lignans: Norisoguaiacin, dihydroguaiaretic acid, partially demethylated dihydroguaiaretic acid, and 3'-demethoxyisoguaiasin

Flavonoids: 19 identified flavonoids in the leaf resin, including kaempferol

Volatile terpenoids: Alpha-pinene, limonene, linalool, and other aromatic compounds

Triterpene saponins: Larreagenin A, larreic acid

Sterols: Beta-sitosterol, campesterol

Wax esters and essential oils: Contributing to the characteristic resinous coating

NDGA and other chaparral compounds demonstrate activity against bacteria, fungi, protozoa, and viruses in laboratory settings

Traditional use for skin infections (including staph infections and impetigo), gut infections, and fungal infections like athlete's foot

Shown to inhibit growth of drug-resistant organisms including certain multidrug-resistant bacteria

Active against Entamoeba histolytica (the protozoan that causes amoebic dysentery) in laboratory studies

Claims of antiviral activity against HPV, HIV, and herpes simplex virus through inhibition of viral gene replication (laboratory data only)

NDGA is one of the most potent naturally occurring antioxidants identified

Inhibits lipid peroxidation (the oxidative damage of fats that leads to cell damage)

Scavenges free radicals and protects cells from oxidative stress

May protect against neurodegenerative damage through antioxidant mechanisms in animal studies

Was formerly used as a food preservative antioxidant before FDA removed its GRAS status

NDGA inhibits lipoxygenase (the 5-LOX enzyme), blocking the production of inflammatory leukotrienes

Also inhibits cyclooxygenase (COX) and phospholipase A2, reducing inflammatory prostaglandins

Traditional use for arthritis, rheumatic conditions, sciatica, joint pain, back pain, and headaches

Rat studies showed improvement in stomach ulcers and arthritis-related inflammation

NDGA inhibits cancer cell growth in numerous laboratory studies across multiple cancer types (breast, prostate, lung, colon, melanoma, lymphoma)

Topical NDGA significantly reduced tumor-promoting agent activity in mouse skin studies

A derivative of NDGA called M4N has shown the ability to stop cancer cell growth in laboratory models

However, a clinical trial in 45 cancer patients found chaparral was not effective as a cancer treatment, with only 4 of 45 patients seeing tumor shrinkage and 41 seeing tumor progression

One report suggested NDGA may actually stimulate tumor growth in some cancer patients

No human clinical evidence supports chaparral as a cancer treatment

Traditional use for wound healing, skin sores, and skin infections

Used topically for chickenpox lesions

Applied as poultices or fomentations for rheumatic and joint pain

Antifungal effects against tinea (athlete's foot, toenail fungus) when used as soaks or topical tincture

Masoprocol (a purified form of NDGA) was formerly available as a prescription topical cream for actinic keratoses (precancerous skin lesions) but was withdrawn from the market in 1996

Digestive support including cramping, dyspepsia, and gas

Respiratory conditions including colds and tuberculosis (traditional only)

Kidney and gallbladder stone treatment (traditional tea)

Dysmenorrhea and premenstrual syndrome

Blood sugar support (traditional use by Pima Indians for diabetes)

Used in sweat lodge ceremonies and saunas for aromatic and purifying purposes

1 teaspoon (approximately 5 grams) of dried leaves and flowers steeped in 1 cup (250 mL) of hot water for 10-15 minutes

Traditional dose: Up to 3 cups per day

Maximum duration: 2 weeks unless under direct supervision of a physician experienced in botanical medicine

Important: Water-based tea extracts very little NDGA compared to capsules or tinctures, which may explain why traditional tea use has far fewer reports of toxicity

Traditional dose: 0.5-1 mL taken three times daily, OR 20 drops up to 3 times daily

One retrospective study found that low-dose tincture (less than 10% Larrea in a complex formula, less than 1 mL total daily) showed no liver damage over a 22-month observation period

Tinctures extract more NDGA than tea due to the alcohol solvent but less than capsules when used at low doses

NOT RECOMMENDED: Almost all reported cases of hepatotoxicity have been associated with capsule use

Documented hepatotoxic doses range from 1.5 to 3.5 grams of crude herb per day in capsule form

Capsules bypass the body's natural taste-based protective mechanism (the extremely bitter, unpleasant taste of chaparral tea naturally limits how much a person can tolerate)

Tea or tincture can be applied to cloths and used as compresses or fomentations on skin

Tincture applied directly to fungal infections (athlete's foot, toenail fungus)

Castor oil-based extracts of chaparral for topical application (shown to be safe in the retrospective study)

Hot chaparral tea soaks for fungal infections of feet and toes

Short-term use ONLY for internal applications (maximum 2 weeks without professional supervision)

Topical use may be continued longer with monitoring

Liver function should be monitored via blood work before, during, and after internal use

For antimicrobial purposes: Divided doses throughout the day (morning, midday, evening) to maintain consistent levels

For digestive support: 30 minutes before meals (traditional approach)

For topical infections: Apply 2-3 times daily, covering the affected area

Tea: Can be consumed on its own or with food; taking with food may help reduce any nausea

Tincture: With food is generally recommended to reduce GI irritation

Topical: Not applicable

NDGA is a strong chelating agent (binds metals), so avoid using metal utensils when preparing chaparral tea; use clay, glass, or ceramic vessels instead

The tea has an extremely strong, bitter, unpleasant taste that most people find disagreeable; this taste actually serves as a natural safety mechanism limiting overconsumption

Traditional preparations were almost exclusively water-based teas, which extract very little NDGA

If making a tea, do not over-steep or boil the herb; a simple hot water infusion for 10-15 minutes is the traditional method

Topical antimicrobial effects: May be noticed within days of consistent application

Internal effects: Traditional use suggests effects may develop over several days to weeks

No clinical data exists on the pharmacokinetics of chaparral in humans

Lipoxygenase inhibition: NDGA powerfully inhibits the 5-lipoxygenase (5-LOX) enzyme, blocking the production of inflammatory leukotrienes; this is one of the primary anti-inflammatory mechanisms

Cyclooxygenase (COX) inhibition: Reduces prostaglandin synthesis, contributing to anti-inflammatory and analgesic effects

Phospholipase A2 inhibition: Blocks an early step in the inflammatory cascade, preventing release of arachidonic acid from cell membranes

Free radical scavenging: NDGA's chemical structure allows it to donate hydrogen atoms to neutralize free radicals, preventing oxidative damage to lipids, proteins, and DNA

Mitochondrial electron transport chain inhibition: NDGA and related lignans can inhibit cellular respiration in pathogens and cancer cells, which may underlie both antimicrobial and anticancer effects

Transcription factor Sp1 blockade: May prevent viral gene replication (proposed mechanism for antiviral effects)

HER2 and IGF-1 receptor inhibition: NDGA can block growth factor signaling in cancer cells, particularly HER2-overexpressing breast cancer cells (laboratory data)

Collagen cross-linking: NDGA can cross-link collagen fibers, which has generated interest in tissue engineering and tendon repair applications

Nitric oxide synthase modulation: NDGA may increase endothelial nitric oxide synthase expression, potentially supporting vascular function

NDGA is metabolized in the liver to an orthoquinone derivative, which may deplete glutathione (the liver's primary detoxification antioxidant)

The idiosyncratic nature of the liver injury (affecting only some individuals) and the finding of eosinophils on liver biopsy suggest an allergic or immunological mechanism in susceptible individuals

Rapid recurrence of liver damage upon re-exposure supports an immune-mediated reaction

CYP450 enzyme inhibition by NDGA may interfere with the liver's normal detoxification processes

Capsule forms deliver much higher NDGA loads than tea, potentially overwhelming the liver's capacity to safely metabolize the compound

The root of the plant contains larreantin, a potential hepatotoxin; contamination of leaf products with root material could contribute to toxicity in some cases

Milk thistle (Silymarin): Liver-protective effects may help mitigate chaparral's hepatotoxicity risk; some commercial chaparral products include silymarin for this reason

Vitamin C (Ascorbic acid): May enhance NDGA's antioxidant effects; one animal study showed NDGA combined with vitamin C had modest anti-tumor activity; also sold in some chaparral combination products

NAC (N-Acetyl Cysteine): Supports glutathione production, which may help protect the liver during chaparral use

Probiotics: General support for gut health and immune function when using antimicrobial herbs

Castor oil: Used as a carrier for topical chaparral applications; studied in the retrospective safety study

Tea tree oil: Complementary antifungal support for topical use on skin infections

Calendula: Traditional combination for wound healing poultices

Any combination with other hepatotoxic herbs or supplements (comfrey, kava, germander, pennyroyal) should be strictly avoided

Do not combine with alcohol, which places additional stress on the liver

Other hepatotoxic herbs: Kava, comfrey, germander, pennyroyal, or any supplement with known liver toxicity risk; combining with chaparral greatly increases the risk of liver damage

Acetaminophen (Tylenol): Additional liver stress; never combine with chaparral

Alcohol: Significantly increases hepatotoxicity risk

Statins and other liver-metabolized medications: NDGA inhibits certain CYP450 enzymes; combining may alter drug metabolism and increase toxicity risk

Blood thinners: Chaparral's anti-inflammatory mechanism may affect platelet function; discuss with healthcare provider

Immunosuppressant drugs: Chaparral's immune-modulating effects may interfere

Diabetes medications: Traditional use for blood sugar support suggests possible additive effects on glucose lowering

Hormonal medications/birth control: Chaparral contains phytoestrogenic compounds; potential for hormonal interference

Any CYP450-metabolized drug: NDGA's enzyme inhibition may affect the metabolism of a wide range of medications

Chaparral has been reported to have abortifacient effects (may cause miscarriage); strictly avoid during pregnancy

NDGA has been shown to block mammary gland synthesis following prolactin stimulation; avoid during breastfeeding

The FDA classifies oral chaparral as "likely unsafe"; discuss any use with your healthcare provider

Individuals working with a trained naturopathic physician or clinical herbalist experienced with Larrea tridentata specifically

People using topical preparations only for skin infections, fungal conditions, or wound care (the safest application)

Those with specific conditions where a knowledgeable practitioner has determined the benefit may outweigh the risk, using low-dose tincture as part of a complex formula (not as a standalone product)

Individuals with no history of liver disease, kidney disease, or current medication use, who have been properly screened

Topical use: The safest and most practical application; good evidence from traditional use for skin infections, fungal conditions, and wound support

Short-term use only: Even for those who choose to use chaparral internally, strict time limits and liver function monitoring are essential

Anyone with liver disease or a history of liver problems: Chaparral can cause serious, potentially irreversible liver damage

Anyone with kidney disease or kidney dysfunction: Cases of renal cysts and renal cell carcinoma have been associated with chaparral use

Pregnant women: Abortifacient effects documented; may induce uterine contractions

Breastfeeding women: NDGA blocks mammary gland function; safety unknown

Children: Higher toxicity risk due to lower body weight and developing liver/kidney function

Anyone taking hepatotoxic medications: The additive liver stress is too dangerous

People using capsule/tablet forms: Almost all reported liver damage cases involved capsule products

Anyone on prescription medications (CYP450 enzyme interactions)

People with autoimmune conditions (immune-modulating effects are unpredictable)

Individuals taking blood thinners

People with hormone-sensitive conditions (phytoestrogenic compounds)

Anyone with a history of allergic reactions to plants (contact dermatitis reported with chaparral)

People who cannot commit to liver function monitoring during use

Those trying to become pregnant (chaparral may prevent ovulation)

Extremely potent antioxidant activity from NDGA, among the strongest known natural antioxidants

Broad-spectrum antimicrobial activity demonstrated in laboratory settings against bacteria, fungi, protozoa, and viruses

Strong anti-inflammatory effects through multiple enzyme pathways (5-LOX, COX, phospholipase A2)

Traditional use spanning centuries among Native American populations without widespread toxicity reports (when used as tea)

One retrospective clinical study showed low-dose tincture use (under 1 mL daily, less than 10% of formula) was safe with no liver damage over 22 months

Topical applications appear safe and effective for skin infections and fungal conditions based on traditional use and practitioner reports

NDGA's collagen cross-linking ability has generated interest in tissue engineering for tendon and musculoskeletal repair

No controlled human clinical trials support any therapeutic use

The only human cancer trial showed chaparral was ineffective and tumors grew in most patients

Potent antioxidant effects in a test tube do not automatically translate to safe or effective use in humans

Safer, better-studied alternatives exist for virtually every condition chaparral is used for (curcumin for inflammation, tea tree oil for skin infections, conventional antimicrobials for infections)

Hepatotoxicity (liver damage): The most significant concern; multiple case reports of acute hepatitis, cholestatic hepatitis, hepatic fibrosis, cirrhosis, and acute liver failure requiring liver transplantation

Kidney damage: Cases of renal cysts and renal cell carcinoma associated with regular chaparral tea consumption

Liver failure: Some cases were severe enough to require liver transplantation; at least some were potentially fatal without intervention

Rapid recurrence on re-exposure: If liver injury occurred previously, re-exposure can cause rapid and severe recurrence

Stomach pain and cramping

Nausea (especially with tea, due to the extremely unpleasant taste)

Diarrhea

Weight loss (with prolonged use)

Fever

Contact dermatitis and skin rash (topical use)

Itching

Liver injury from chaparral appears to be idiosyncratic (affecting only certain susceptible individuals), not dose-dependent in all cases

The finding of eosinophils on liver biopsy in some cases suggests an allergic or immunological mechanism

This means it is impossible to predict who will be affected

Some researchers have questioned whether contaminants, improper preparation, or adulteration of products contributed to reported cases

A review of 18 case reports confirmed chaparral can cause severe, irreversible liver damage and failure

No standardization exists for chaparral products

Product quality varies enormously between manufacturers

Root material (which contains the hepatotoxin larreantin) may contaminate leaf products

Capsule products are particularly risky because they deliver concentrated NDGA and bypass the bitter taste that naturally limits tea consumption

The FDA and Health Canada both advise against oral use of chaparral

Skin infections (bacterial, fungal)

Joint pain and inflammatory conditions (arthritis, rheumatism)

Digestive complaints (cramping, dyspepsia, parasites)

Respiratory infections (colds, bronchitis)

Wound healing (external application)

Kidney and gallbladder stones (traditional tea)

Blood sugar imbalances (traditional use among Pima Indians)

Stubborn fungal skin infections (athlete's foot, toenail fungus) that have not responded to conventional treatment

Minor skin infections or wounds where antimicrobial support is desired

Inflammatory skin conditions where topical anti-inflammatory support may help

For antioxidant support: Green tea, pomegranate, turmeric, resveratrol

For anti-inflammatory effects: Curcumin, boswellia, omega-3 fatty acids, ginger

For antimicrobial support: Oregano oil, garlic, berberine, tea tree oil (topical)

For joint pain: Curcumin, boswellia, SAMe, glucosamine

For digestive parasites: Berberine, wormwood (under professional supervision)

Jaundice (yellowing of the skin and eyes)

Dark-colored urine

Severe fatigue and weakness

Nausea, vomiting, and loss of appetite

Upper right abdominal pain or tenderness

Pale or clay-colored stools

Unexplained itching

Fever

Decreased urine output

Swelling in legs, ankles, or feet

Fatigue and confusion

Pain in the flank or lower back

Stop taking chaparral immediately

Seek emergency medical care

Bring the product with you to the hospital

Request liver function tests (ALT, AST, bilirubin, alkaline phosphatase)

Request kidney function tests (BUN, creatinine)

Inform medical staff of all supplements and medications you are taking

Liver damage has been reported after as few as 3 weeks of use, though some cases occurred after months of regular consumption

Toxicity is idiosyncratic, meaning it can occur unpredictably in susceptible individuals regardless of dose

Re-exposure after initial liver injury causes rapid recurrence

The root, bark, and stems contain larreantin and other potentially toxic alkaloids

Only the leaves and flowering tops should be used, and only in properly prepared forms

Avoid consuming any part of the plant raw or in large quantities

Topical application (safest): Tea compresses, tincture applied to skin, castor oil-based extracts; no reported systemic toxicity from topical use

Traditional water-based tea (moderate risk): Extracts very little NDGA due to poor water solubility; centuries of traditional use with few toxicity reports; taste naturally limits consumption; still carries some risk

Low-dose tincture in complex formula (higher risk): One study showed safety at less than 10% Larrea in formula, under 1 mL daily; should only be used under professional supervision

Capsules/tablets (AVOID): Deliver concentrated NDGA, bypass taste-based safety mechanism; associated with nearly all reported cases of serious liver damage; never recommended

This is perhaps the single most important safety consideration with chaparral

Traditional tea preparation uses hot water, which extracts very little NDGA because it is poorly water-soluble

Capsules contain the powdered dry leaf with ALL of the resinous NDGA intact

Alcoholic tinctures fall somewhere in between, extracting more NDGA than water but less than pure powder

Native American populations used chaparral tea for decades without published evidence of toxicity

The shift to capsule products in health food stores coincided with the emergence of hepatotoxicity reports

Baseline liver function panel before starting (ALT, AST, alkaline phosphatase, bilirubin)

Repeat at 2 weeks

Repeat at 4 weeks (if continuing beyond 2 weeks under supervision)

Stop immediately if any values become elevated

Also monitor kidney function (BUN, creatinine)

NDGA strongly binds metals

Use glass, ceramic, or clay vessels when preparing chaparral tea

Avoid metal teapots, strainers, or cooking utensils

This also means chaparral could theoretically affect mineral absorption if used internally

FDA: Issued public safety warning (1992); NDGA removed from GRAS list (1968); chaparral listed as a poisonous plant

Health Canada: Warning issued in 2005; products banned

Despite these warnings, chaparral remains legally available for sale in the United States

Masoprocol (topical NDGA cream for actinic keratoses) was withdrawn from the US market in 1996

Cancer treatment (the only human cancer trial showed it was ineffective)

Antiviral treatment in humans

Diabetes management in humans

Any internal therapeutic use

Potent antioxidant activity (NDGA is among the strongest known natural antioxidants)

Anticancer effects in cell lines and some animal models (breast, prostate, lung, colon, melanoma, lymphoma)

Anti-inflammatory effects through 5-LOX, COX, and phospholipase A2 inhibition

Antimicrobial activity against bacteria, fungi, protozoa, and viruses

Neuroprotective effects in animal models of ischemic injury

Renoprotective effects against chemical-induced kidney damage in animals

Metabolic protective effects against diet-induced obesity in mice

One retrospective study (13 patients) showing low-dose tincture safety over 22 months

One cancer trial (45 patients) showing ineffectiveness as an anticancer agent

Multiple case reports (18 reviewed) documenting liver damage

No randomized controlled trials for any therapeutic indication

Safety concerns have prevented human clinical trials from being conducted

Most preclinical findings have not been replicated in human studies

The gap between NDGA's powerful laboratory effects and its lack of human efficacy is a fundamental problem

Individual variability in liver metabolism makes it impossible to predict who will experience toxicity

Quality control issues with commercial products make it difficult to draw reliable conclusions from case reports