Hermetica Superfood Encyclopedia
The Short Answer
Caryocar villosum pulp contains phenolic compounds—most notably gallic acid at 182.4 µg/g—alongside flavonoids, carotenoids, and a lipid profile dominated by palmitic acid (44.63–44.84%) and oleic acid (33.62–43.66%), which collectively drive its antioxidant and antifungal bioactivity. In vitro studies demonstrate that its ethanolic extracts inhibit mycelial growth of phytopathogens such as Fusarium spp. and Bipolaris oryzae at concentrations as low as 3.75 µL/mL of expressed oil, with antifungal activity linked to β-sitosterol and reactive unsaturated aldehydes including (Z)-9,17-octadecadienal (19.7% of oil).
CategoryFruit
GroupAmazonian
Evidence LevelPreliminary
Primary KeywordCaryocar villosum benefits
Piquia — botanical close-up
Health Benefits
**Antioxidant Activity**: Phenolic compounds, particularly gallic acid (182
4 µg/g pulp), and flavonoids in the aqueous and hydroalcoholic extracts of piquia pulp scavenge free radicals as measured by ABTS and related assays, providing meaningful in vitro antioxidant capacity comparable to other Amazonian fruits.
**Antifungal Properties**
The expressed oil and ethanolic extracts exhibit broad-spectrum antifungal activity against agricultural pathogens—Fusarium spp., Pestalotiopsis sp., and Bipolaris oryzae—at experimentally effective concentrations of 3.75–10 µL/mL, mediated by β-sitosterol and cytotoxic unsaturated aldehydes that disrupt fungal membrane integrity.
**Anti-inflammatory Potential (Traditional)**
Traditional use among Amazonian communities attributes topical anti-inflammatory properties to piquia preparations; while unconfirmed by controlled studies, this is plausibly linked to the phytosterol β-sitosterol and the high oleic acid content of the mesocarp oil, both associated with modulation of pro-inflammatory mediators in related research contexts.
**Cardiovascular Lipid Support (Theoretical)**
The oil's high oleic acid content (33.62–43.66%), a monounsaturated fatty acid well-characterized in other plant oils, suggests a theoretical capacity to favorably modulate LDL oxidation and endothelial function, though this has not been investigated in C. villosum specifically.
**Phytosterol Contribution**: β-Sitosterol, comprising approximately 14
2% of the industrialized oil's identified components, is a well-documented competitive inhibitor of intestinal cholesterol absorption; piquia oil's β-sitosterol content positions it as a plausible dietary contributor to phytosterol intake in Amazonian populations.
**Nutritional Density from Carotenoids and Ascorbic Acid**
The pulp contains carotenoids and ascorbic acid, micronutrients supporting immune function and acting as lipid-soluble and water-soluble antioxidants respectively, though precise quantitative data for C. villosum remain unreported beyond phenolic measures.
Origin & History
Natural habitat
Caryocar villosum, commonly called piquia, is native to the Guianas and the Central Amazon basin, thriving in humid tropical rainforest ecosystems at low to mid elevations. The tree is a large, slow-growing canopy species adapted to nutrient-poor Amazonian soils, producing large drupes with a fibrous, oil-rich mesocarp. Its cultivation remains largely non-commercial, with fruits harvested from wild or semi-domesticated trees by indigenous and riverside communities across Brazil, Guyana, Suriname, and French Guiana.
“Caryocar villosum has been a subsistence food and folk medicine resource for indigenous Amazonian and Guianese peoples for centuries, with the large, aromatic fruits valued for their calorie-dense, oil-rich mesocarp consumed fresh, boiled, or rendered into cooking fats. Riverside and forest-dwelling communities in Brazil's Pará and Amazonas states, as well as in Suriname and French Guiana, have traditionally used topical preparations of the oil for skin conditions and inflammatory complaints, a practice that has passed largely undocumented in formal ethnobotanical literature compared to its congener C. brasiliense. The fruit's local name 'piquia' (also spelled piqui or piquiá depending on region) encompasses several Caryocar species in vernacular usage, which creates taxonomic ambiguity in historical records. Artisanal extraction of oil from the fibrous mesocarp using manual pressing or boiling-and-skimming methods represents the primary traditional preparation, with no documented role in formal Amazonian healing rituals comparable to other regionally significant plants.”Traditional Medicine
Scientific Research
The scientific evidence base for Caryocar villosum is sparse and exclusively preclinical, comprising a small number of in vitro phytochemical characterization studies and antifungal bioassays; no animal studies or human trials have been published as of available literature. Antifungal efficacy was demonstrated in plate-based mycelial growth inhibition assays using dilution series of ethanolic extracts (10–50% in PDA medium) and expressed oils (2.5–10 µL/mL), establishing minimum inhibitory activity thresholds but not formal MIC values by CLSI standards. Phytochemical profiling has quantified gallic acid at 182.4 µg/g in the pulp and characterized the oil's fatty acid and volatile aldehyde profile by GC-MS, while TLC confirmed flavonoid presence in leaf extracts at 1000 ppm; total phenolic content and antioxidant capacity have been assessed by colorimetric and radical-scavenging assays in at least one comparative study of Caryocar species. Evidence quality is rated low: all data derive from small-scale in vitro work with no replication across independent research groups, and extrapolation to human health outcomes is not scientifically warranted at this stage.
Preparation & Dosage
Traditional preparation
**Traditional Pulp Consumption**
Eaten fresh or processed into artisanal oils by Amazonian communities; no standardized serving size is documented for health purposes.
**Artisanal Oil (Cold-Pressed)**
Extracted from the mesocarp and used topically or as a culinary fat in regional cuisine; no therapeutic dose established.
**Industrialized Oil**
Commercially filtered oil (0.45 µm membrane) has been tested in antifungal assays at 2.5–10 µL/mL in vitro; these concentrations are experimental and not translatable to human supplemental doses.
**Ethanolic/Hydroalcoholic Extract**
Research preparations use 10–50% dilutions in growth media for antifungal testing and 1000 ppm methanolic extracts for TLC phytochemical screening; no human oral dose equivalent exists.
**Standardization**
No commercial standardized extract, capsule, or nutraceutical formulation of C. villosum has been documented; no minimum gallic acid or flavonoid threshold for supplemental use has been established.
**Timing and Administration**
Insufficient data to make any evidence-based timing recommendations.
Nutritional Profile
The mesocarp (pulp) of Caryocar villosum is lipid-rich, with fatty acids dominated by palmitic acid (44.63–44.84%) and oleic acid (33.62–43.66%), giving the oil a semi-solid consistency at room temperature and a saturated-to-monounsaturated fatty acid ratio broadly similar to palm oil. Phenolic content is anchored by gallic acid at a quantified 182.4 µg/g fresh pulp, with additional unquantified flavonoids contributing to total polyphenol load. The industrialized oil contains (Z)-9,17-octadecadienal (19.7%), (Z)-octadecadienal (15.5%), and β-sitosterol (14.2%) among identified non-triglyceride components by GC-MS. Carotenoids and ascorbic acid are reported present in the pulp but have not been quantified specifically for C. villosum; bioavailability of oil-soluble carotenoids from the high-fat matrix is expected to be enhanced by the lipid content based on co-ingestion principles established for other carotenoid-rich tropical fruits. Protein and carbohydrate fractions of the pulp have not been detailed in available literature.
How It Works
Mechanism of Action
The antioxidant activity of Caryocar villosum is primarily attributed to gallic acid and related polyphenols in the pulp, which donate hydrogen atoms or electrons to neutralize reactive oxygen species (ROS) through non-enzymatic radical-chain termination, a mechanism well-characterized for hydrolyzable tannins and gallates in the broader phytochemical literature. Antifungal bioactivity is mechanistically linked to two classes of oil constituents: β-sitosterol, which intercalates into fungal cell membranes to disrupt sterol organization and membrane permeability, and long-chain unsaturated aldehydes—(Z)-9,17-octadecadienal and (Z)-octadecadienal—which are electrophilic species capable of alkylating fungal membrane proteins and interfering with cell wall biosynthesis. The phytosterol β-sitosterol also competitively inhibits intestinal Niemann-Pick C1-Like 1 (NPC1L1) cholesterol transporter activity by structural mimicry of cholesterol, a pathway extrapolated from extensive research on plant sterols rather than C. villosum-specific studies. No specific receptor binding, kinase inhibition, or transcription factor modulation data have been reported for C. villosum extracts, representing a major gap in molecular characterization.
Clinical Evidence
No human clinical trials have been conducted on Caryocar villosum in any form—whole fruit, extract, or oil—as a nutritional supplement or therapeutic agent. The existing research landscape consists entirely of in vitro antifungal assays and phytochemical profiling studies, with no controlled animal pharmacology experiments reported either. Consequently, no clinical outcomes, effect sizes, dose-response relationships, or safety signals can be described from trial data. Confidence in human health applications is very low and any purported benefits remain hypothesis-generating rather than evidence-based; the related species Caryocar brasiliense has a modestly deeper phytochemical literature that may provide directional hypotheses for future C. villosum research.
Safety & Interactions
No formal safety studies, toxicology data, or adverse event reports exist for Caryocar villosum in any preparation, making a complete safety profile impossible to establish at this time. The high palmitic acid content (44.63–44.84%) of the oil warrants consideration in the context of saturated fat intake for individuals managing cardiovascular risk, consistent with general dietary guidance rather than any C. villosum-specific finding. No drug interactions have been identified or studied; however, the β-sitosterol content theoretically warrants caution in individuals on cholesterol-modifying medications (statins, ezetimibe) due to additive cholesterol absorption inhibition, though clinical interaction data are absent. No contraindication data, pregnancy or lactation safety assessments, or maximum tolerable dose thresholds have been reported, and the ingredient should be treated as having an uncharacterized safety profile pending formal toxicological evaluation.
Synergy Stack
Hermetica Formulation Heuristic
Also Known As
Caryocar villosumPiquiaPiquiáPiqui (regional variant)Souari nut (family common name)
Frequently Asked Questions
What are the main bioactive compounds in Caryocar villosum?
The pulp of Caryocar villosum contains gallic acid as its primary quantified phenolic compound at 182.4 µg/g, along with flavonoids, carotenoids, and ascorbic acid. The expressed oil is characterized by palmitic acid (44.63–44.84%), oleic acid (33.62–43.66%), β-sitosterol (14.2%), and reactive unsaturated aldehydes including (Z)-9,17-octadecadienal (19.7%), which collectively underpin its antioxidant and antifungal properties.
Does piquia have antifungal properties?
Yes, in vitro studies demonstrate that both ethanolic extracts (at 40% concentration in culture medium) and expressed oils (as low as 3.75 µL/mL) of Caryocar villosum inhibit mycelial growth of agricultural pathogens including Fusarium spp., Pestalotiopsis sp., and Bipolaris oryzae. This activity is attributed to β-sitosterol, which disrupts fungal membrane sterol organization, and long-chain unsaturated aldehydes that alkylate fungal proteins; however, these findings are exclusively preclinical and have not been tested in humans.
Are there any clinical trials on Caryocar villosum for human health?
No human clinical trials have been conducted on Caryocar villosum in any form as of currently available scientific literature. All research is limited to in vitro phytochemical characterization and antifungal bioassays; there are no animal pharmacology studies or human safety or efficacy trials. Any health claims beyond traditional use therefore lack clinical validation.
What is the recommended dosage of piquia extract or oil?
No evidence-based supplemental dose has been established for Caryocar villosum extract, oil, or any standardized preparation because no human or animal pharmacokinetic or dose-ranging studies have been published. Experimental concentrations used in antifungal assays (2.5–10 µL/mL oil; 10–50% extracts in media) are in vitro values not translatable to human intake recommendations. Traditional consumption involves eating the fresh fruit or using the oil culinarily, with no documented therapeutic dosing protocol.
Is piquia oil safe to consume?
Formal toxicological studies on Caryocar villosum oil or extracts have not been published, so a rigorous safety profile cannot be provided. The oil has a high saturated fat content from palmitic acid (≈44%), which may be relevant for individuals monitoring cardiovascular risk factors. Traditional Amazonian use suggests general tolerability as a food, but drug interactions, contraindications in pregnancy, and maximum safe doses remain entirely unstudied and uncharacterized.
How does piquia oil compare to other Amazonian fruit oils for antioxidant protection?
Piquia oil contains phenolic compounds including gallic acid at concentrations of approximately 182.4 µg/g pulp, delivering antioxidant capacity comparable to other Amazonian fruits as demonstrated by ABTS assay measurements. Its antioxidant potency makes it competitive with established tropical fruit oils, though direct head-to-head studies with specific competitors remain limited in published literature. The combination of gallic acid and flavonoids in piquia provides a broader polyphenol profile than some single-source Amazonian oils.
What forms of piquia are most effective—expressed oil, extract, or whole pulp?
Both expressed oil and ethanolic extracts of piquia demonstrate bioactive properties, with the ethanolic extract showing particularly strong antifungal activity across broad fungal species. The expressed oil preserves fat-soluble antioxidants and bioactive lipids, while ethanolic extracts concentrate water-soluble phenolics and flavonoids. Whole pulp consumption captures both lipid and polyphenol fractions, though concentrated extracts or oils provide more standardized dosing for therapeutic applications.
Is piquia suitable for people with fungal infections or candida concerns?
Piquia's ethanolic extracts and expressed oil exhibit broad-spectrum antifungal properties, making it potentially relevant for individuals concerned with fungal overgrowth, though human clinical evidence remains limited. The antifungal activity has been demonstrated in vitro, suggesting potential application as a complementary approach, but it should not replace conventional antifungal treatment without medical supervision. Those with active fungal infections should consult a healthcare provider before using piquia as part of their treatment strategy.
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