# Butterfly Pea Flower (Clitoria ternatea L.)

**Canonical URL:** https://ingredients.hermeticasuperfoods.com/ingredients/butterfly-pea-flower-clitoria-ternatea-l
**Data Source:** Hermetica Superfoods Ingredient Encyclopedia
**Updated:** 2026-04-05
**Evidence Score:** 1 / 10
**Category:** Southeast Asian
**Also Known As:** Clitoria ternatea L., Aparajita, Asian pigeonwings, Bunga telang, Anchan, Blue pea flower, Darwin pea

## Overview

Clitoria ternatea flowers contain polyacylated anthocyanins called ternatins (delphinidin derivatives A1–D3) alongside phenolics and flavonoids that exert antioxidant, [neuroprotective](/ingredients/condition/cognitive), and enzyme-inhibitory effects through [free radical scaveng](/ingredients/condition/antioxidant)ing, α-glucosidase inhibition, and modulation of [inflammatory](/ingredients/condition/inflammation) signaling. Preclinical data show optimized ethanol extracts yield a total flavonoid content of 187.05 ± 3.18 mg quercetin/g dry sample with DPPH radical inhibition up to 63.53% and a 50% reduction in MCF-7 breast cancer cell migration at sub-IC50 concentrations, though no large human clinical trials yet confirm these effects in vivo.

## Health Benefits

- **[Antioxidant Protection](/ingredients/condition/antioxidant)**: Ternatins and phenolic compounds scavenge DPPH radicals (up to 63.53 ± 0.95% inhibition) and ABTS radicals (84.86 ± 1.52 µM Trolox/g), reducing oxidative stress implicated in neurodegeneration, [cardiovascular](/ingredients/condition/heart-health) disease, and cellular aging.
- **Cognitive and Anxiolytic Support**: Traditional Ayurvedic and Southeast Asian use attributes nootropic and anxiolytic properties to root and flower extracts; animal models suggest [acetylcholine](/ingredients/condition/cognitive)sterase inhibition and modulation of GABAergic pathways contribute to improved memory and reduced anxiety-like behavior.
- **Blood Sugar Regulation**: Phenolic-rich extracts inhibit α-amylase and α-glucosidase activity, slowing postprandial glucose absorption; antidiabetic applications are supported by in vitro enzyme inhibition studies and traditional use in Ayurvedic medicine for metabolic conditions.
- **Anticancer Potential**: Hydrophilic flower extracts reduced HEp-2 laryngeal cancer cell viability by 95% at 1 mg/mL in vitro and inhibited MCF-7 breast cancer cell migration by 50% below the IC50 of 862 µg/mL, suggesting pro-apoptotic and anti-migratory mechanisms mediated by high phenolic content.
- **[Antimicrobial](/ingredients/condition/immune-support) Activity**: Anthocyanin-rich fractions demonstrated stronger inhibitory activity against Bacillus cereus, B. subtilis, Escherichia coli, and Proteus mirabilis compared to crude extracts, indicating that ternatins contribute meaningfully to the plant's antibacterial properties.
- **Antihypertensive Effects**: Phenolic compounds inhibit angiotensin-converting enzyme (ACE-I) in vitro, a mechanism parallel to pharmaceutical antihypertensive drug classes, while also reducing LDL oxidation and DNA damage in cell-based assays.
- **Natural Food Colorant with Functional Benefits**: The pH-responsive blue-to-pink color shift of ternatin anthocyanins (stable at pH 3.2–5.2) enables dual use as a natural colorant and bioactive ingredient in functional foods, with encapsulated forms achieving 76% encapsulation efficiency, 99% solubility, and 71% bioaccessibility.

## Mechanism of Action

Ternatin anthocyanins — polyacylated delphinidin-3,7,3',5'-tetraglucoside derivatives — function as potent [free radical scaveng](/ingredients/condition/antioxidant)ers by donating hydrogen atoms to neutralize DPPH, ABTS, and hydroxyl radicals, with their antioxidant capacity strongly correlated with total phenolic content (FRAP r² > 0.90 across extraction studies). At the enzyme level, phenolic and flavonoid fractions competitively inhibit α-amylase, α-glucosidase, lipase, and ACE-I, reducing starch hydrolysis, glucose absorption, fat [digestion](/ingredients/condition/gut-health), and angiotensin II production respectively. In cancer cell models, high-phenolic hydrophilic extracts block glucose transporter (GLUT) activity and disrupt glycolytic enzyme function, inducing intrinsic apoptotic pathways and reducing cell viability and migratory capacity. [Neuroprotective effect](/ingredients/condition/cognitive)s are attributed partly to inhibition of acetylcholinesterase and, in animal studies, to interaction with GABAergic and serotonergic receptor systems, though the specific receptor binding affinities of individual ternatins remain incompletely characterized.

## Clinical Summary

No published human randomized controlled trials with reported sample sizes and effect sizes specific to standardized Clitoria ternatea extracts were identified in the available literature. The anticancer findings (95% HEp-2 viability reduction at 1 mg/mL; 50% MCF-7 migration inhibition below IC50 of 862 µg/mL) derive entirely from in vitro cell culture experiments, which cannot establish clinically meaningful doses or safety margins for human use. Encapsulation studies have demonstrated promising bioaccessibility (71% intestinal absorption in lyophilized capsule models), suggesting oral delivery is feasible, but absorption in actual human gut physiology has not been formally validated in clinical cohorts. Confidence in all purported benefits remains low-to-moderate pending well-designed Phase I/II human trials; current clinical use should be regarded as evidence-informed traditional practice rather than evidence-based medicine.

## Nutritional Profile

Butterfly pea flowers are low in macronutrients when consumed as a tea infusion but are nutritionally significant for their dense phytochemical profile. Total phenolic content reaches up to 41.60 mg GAE/g dry sample in optimized extracts, with total flavonoid content up to 187.05 mg quercetin equivalents/g dry sample. Anthocyanins — principally polyacylated delphinidin-3,7,3',5'-tetraglucoside ternatins (A1, A2, A3, B1, B2, B3, B4, C1, D1, D2, D3) — are quantified at up to 0.97 ± 0.50 mg malvidin-3-glucoside equivalents/g. Secondary phytochemicals include saponins, triterpenoids (taraxerol, taraxerone), alkaloids, tannins, phlobatannins, and steroids distributed variably across flowers, seeds, roots, and leaves. Bioavailability of anthocyanins is enhanced by encapsulation (71% bioaccessibility in lyophilized ionic gelation capsules) but reduced by thermal degradation above 80°C and photodegradation under UV light; the extracts are stable across pH 3.2–5.2.

## Dosage & Preparation

- **Herbal Tea/Infusion (Traditional)**: 5–10 dried flowers steeped in 200–250 mL hot water at 80°C for 5 minutes; yields approximately 23.91 ± 0.90 mg GAE/g total phenolics per optimized hot-water extraction at 0.008 g/mL ratio.
- **Ethanol/Water Extract (Standardized)**: Optimized 50–70% ethanol extraction yields TPC of 41.17 ± 0.5 mg GAE/g and TFC of 187.05 ± 3.18 mg quercetin/g dry sample; preferred for maximum flavonoid and anthocyanin content.
- **Encapsulated Powder/Capsules**: Lyophilized flower extract encapsulated via ionic gelation achieves 76% encapsulation efficiency, 99% solubility, and 71% bioaccessibility; no standardized human dose established — typical functional food applications use 50–200 mg extract equivalents.
- **Anthocyanin-Standardized Extract**: Commercial extracts standardized to ternatin anthocyanin content (commonly expressed as mg MVE/g or delphinidin equivalents); anthocyanin content in optimized extracts reaches 28.60 ± 0.04 mg/L.
- **Traditional Powder (Root/Seed)**: Ayurvedic preparations use dried root or seed powder (traditionally 1–3 g/day) for [nootropic](/ingredients/condition/cognitive) and antidiabetic applications, though no pharmacokinetically validated dose exists.
- **Timing Note**: No clinical data establish optimal dosing timing; traditional use suggests morning or afternoon tea consumption; photolabile anthocyanins should be stored away from direct light to preserve potency.

## Safety & Drug Interactions

In vitro cytotoxicity has been observed at high concentrations (1–9 mg/mL in cell culture models), but these concentrations are unlikely to be reached with standard dietary or supplemental use, and food-grade applications are generally regarded as safe based on centuries of traditional consumption. No formal human safety trials, established tolerable upper intake levels, or documented adverse event profiles exist in the peer-reviewed literature for standardized Clitoria ternatea extracts, representing a significant evidence gap. Theoretical drug interactions exist with antihyperglycemic agents (additive α-glucosidase inhibition potentiating hypoglycemia risk), antihypertensive medications (additive ACE inhibition), and anticoagulants (flavonoid-mediated platelet effects), though none have been clinically documented. Pregnancy and lactation safety is unestablished; traditional uterotonic use of root preparations in some South Asian systems suggests caution is warranted during pregnancy, and use should be avoided without medical supervision in these populations.

## Scientific Research

The current evidence base for Clitoria ternatea consists predominantly of in vitro phytochemical characterization studies, extraction optimization experiments, and a smaller number of animal model studies, with no published large-scale randomized controlled trials in humans identified in the peer-reviewed literature as of 2024. In vitro studies have rigorously quantified [antioxidant](/ingredients/condition/antioxidant) capacity (DPPH, ABTS, FRAP assays), enzyme inhibition (α-amylase, α-glucosidase, ACE-I), and cytotoxicity (HEp-2 and MCF-7 cell lines), providing mechanistic plausibility but not clinical proof of efficacy. Several animal studies in rodent models support [cognitive enhancement](/ingredients/condition/cognitive), anxiolytic activity, and antidiabetic effects, yet interspecies translation is uncertain. The overall evidence quality is preclinical; human pharmacokinetic data, bioavailability studies in clinical populations, and dose-response trials are critical unmet needs before therapeutic recommendations can be made.

## Historical & Cultural Context

Clitoria ternatea has been documented in Ayurvedic medicine for over two millennia under the Sanskrit name 'Aparajita,' where it was prescribed as a medhya rasayana (brain tonic) for improving intellect, [memory](/ingredients/condition/cognitive), and voice, and for managing epilepsy, anxiety, and [inflammatory](/ingredients/condition/inflammation) conditions. In Southeast Asian traditions — particularly Thailand, Malaysia, and the Philippines — the vivid blue flowers have been used for centuries as a natural food and textile colorant, and the plant features prominently in ceremonial foods such as the Thai blue rice dish 'Khao Yam.' Traditional Malay medicine employed root decoctions as diuretics and uterotonic agents, while in Sri Lanka and India seed and leaf preparations addressed respiratory complaints and skin disorders. The genus name Clitoria references the flower's anatomical resemblance to female reproductive anatomy, a morphological feature historically linked in Doctrine of Signatures-influenced systems to gynecological applications.

## Synergistic Combinations

Clitoria ternatea anthocyanins demonstrate enhanced antioxidant synergy when combined with other polyphenol-rich botanicals such as roselle (Hibiscus sabdariffa), where complementary anthocyanin profiles (cyanidin vs. delphinidin derivatives) broaden free radical scavenging across multiple [reactive oxygen species](/ingredients/condition/antioxidant). Pairing butterfly pea flower extract with piperine (from black pepper) may improve phenolic bioavailability by inhibiting intestinal glucuronidation and efflux transporters, a mechanism well-documented for structurally related flavonoids. For cognitive applications, traditional Ayurvedic stacking with Bacopa monnieri (brahmi) is documented, with both plants proposed to act on cholinergic pathways — Bacopa inhibiting [acetylcholine](/ingredients/condition/cognitive)sterase and Clitoria ternatea supporting neuronal membrane integrity — though no controlled human trial has evaluated this combination.

## Frequently Asked Questions

### What are the main active compounds in butterfly pea flower?

The primary bioactive compounds in Clitoria ternatea flowers are polyacylated anthocyanins called ternatins (A1–D3), which are delphinidin-3,7,3',5'-tetraglucoside derivatives responsible for the characteristic deep blue color. The flowers also contain a broad array of phenolics and flavonoids, with optimized extracts yielding up to 187.05 mg quercetin equivalents/g dry sample, alongside saponins, triterpenoids, alkaloids, and tannins that vary by plant part and extraction method.

### Does butterfly pea flower help with anxiety and brain health?

Traditional Ayurvedic medicine has classified Clitoria ternatea as a medhya rasayana (brain tonic) used for memory, anxiety, and cognitive clarity for centuries. Animal model studies suggest the plant's extracts may inhibit acetylcholinesterase and modulate GABAergic and serotonergic pathways, but no peer-reviewed human clinical trials have confirmed anxiolytic or nootropic effects with measured effect sizes, so these benefits remain supported by preclinical and traditional evidence only.

### How do you prepare butterfly pea flower tea for maximum benefits?

Optimal phenolic extraction for hot water tea occurs at 80°C for 5 minutes using approximately 0.008 g of dried flowers per mL of water, yielding a total phenolic content of approximately 23.91 mg GAE/g. For maximum flavonoid and anthocyanin content, ethanol-water extraction is superior (up to 41.17 mg GAE/g TPC and 187.05 mg quercetin/g TFC), but for everyday consumption, steeping 5–10 dried flowers in hot water for 5 minutes is the practical traditional method and preserves a meaningful phytochemical load.

### Is butterfly pea flower safe to consume daily?

Clitoria ternatea flowers have a long history of safe consumption as a food ingredient and tea across Southeast Asia and South Asia, and food-grade use is generally considered safe based on this traditional record. However, no formal human clinical safety trials or established upper intake limits exist; in vitro cytotoxicity appears at concentrations of 1–9 mg/mL in cell culture, which are not replicated by typical dietary intake. Individuals taking antidiabetic, antihypertensive, or anticoagulant medications should exercise caution due to theoretical additive interactions, and pregnant women should avoid therapeutic doses given traditional uterotonic use of root preparations.

### What is the best supplement form of butterfly pea flower?

Lyophilized encapsulated extracts produced via ionic gelation currently demonstrate the highest bioaccessibility, with 76% encapsulation efficiency, 99% solubility, and 71% intestinal bioaccessibility, making them preferable to raw powder or unprotected liquid extracts for consistent delivery of ternatins and phenolics. Standardized extracts expressing anthocyanin content in malvidin-3-glucoside equivalents or delphinidin equivalents offer the most reproducible dosing, though no clinically validated human dose has been established; commercial products typically provide 50–200 mg of flower extract equivalent per serving.

### Does butterfly pea flower interact with blood thinners or anticoagulant medications?

While butterfly pea flower has mild anticoagulant properties due to its phenolic compounds, clinical interaction data with warfarin, apixaban, or other anticoagulants is limited. If you take prescription blood thinners, consult your healthcare provider before adding butterfly pea flower supplements to avoid potential additive effects. Most dietary use at standard doses is considered safe alongside anticoagulants, but individualized medical guidance is recommended.

### Is butterfly pea flower safe for pregnant or breastfeeding women?

Traditional use in Southeast Asian and Ayurvedic medicine suggests safety, but clinical safety data in pregnancy and lactation is insufficient. Pregnant or breastfeeding women should consult their healthcare provider before using butterfly pea flower supplements, as some compounds may cross placental barriers or appear in breast milk. Whole-food amounts in tea are generally considered lower-risk than concentrated extracts.

### How does butterfly pea flower's antioxidant potency compare to other herbal nootropics like ashwagandha or bacopa?

Butterfly pea flower demonstrates strong ABTS radical scavenging (84.86 ± 1.52 µM Trolox/g), which rivals or exceeds many adaptogens, though direct head-to-head clinical comparisons are limited. Bacopa and ashwagandha have more extensive human cognitive trials, while butterfly pea flower's evidence base is primarily in vitro and traditional use. The combination of all three may offer complementary neuroprotective mechanisms rather than one being definitively superior.

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