# Lycium shawii (Lycium shawii Roem. & Schult.)

**Canonical URL:** https://ingredients.hermeticasuperfoods.com/ingredients/lycium-shawii-lycium-shawii-roem-schult
**Data Source:** Hermetica Superfoods Ingredient Encyclopedia
**Updated:** 2026-04-02
**Evidence Score:** 1 / 10
**Category:** Middle Eastern
**Also Known As:** Lycium shawii Roem. & Schult., Shaw's boxthorn, Arabian boxthorn, Desert wolfberry

## Overview

Lycium shawii contains phenolics, flavonoids, quinoline alkaloids, sesquiterpene lactones, and triterpenoids whose primary mechanisms include [COX-2](/ingredients/condition/inflammation) enzyme inhibition, heme polymerization disruption, and free-radical scavenging via DPPH-active polyphenols. The fruit ethyl acetate extract demonstrated strong in vitro COX-2 inhibition surpassing aspirin as a reference standard, while the water extract inhibited β-hematin formation at an absorbance of 0.140 ± 0.027 at 1 mg/mL, indicating meaningful antimalarial potential in preclinical models.

## Health Benefits

- **[Anti-inflammatory](/ingredients/condition/inflammation) Activity**: The ethyl acetate fruit extract inhibits COX-2 enzyme in vitro at levels reported to exceed aspirin's reference inhibition, attributed to phenolics including quercetin, p-coumaric acid, and ferulic acid that suppress arachidonic acid cascade signaling.
- **Antimalarial Potential**: Water extracts rich in quinoline alkaloids disrupt heme polymerization in Plasmodium parasites, producing β-hematin inhibition (absorbance 0.140 ± 0.027 at 1 mg/mL), mirroring the mechanism of chloroquine-class antimalarials.
- **[Antioxidant](/ingredients/condition/antioxidant) Capacity**: High total phenolic content (0.67 mg/mL gallic acid equivalents in ethyl acetate fruit extract) correlates with strong DPPH radical scavenging, with identified contributors including gallic acid, rutin, quercetin 3-O-β-glucoside, and quercetin 3,7-diglucoside.
- **[Antimicrobial](/ingredients/condition/immune-support) Effects**: Solvent extracts produce inhibition zones of 13–21 mm against clinical pathogens; the ethyl acetate extract achieves the largest zone (21 mm) against both Staphylococcus epidermidis and Escherichia coli, while hexane extract inhibits S. epidermidis at 10 mm.
- **Cytotoxic/Anticancer Properties**: The essential oil fraction exhibits cytotoxicity against MCF-7 human breast cancer cells with an IC50 of 4.66 mg/L in vitro, suggesting terpenoid and volatile constituents as candidate anticancer agents warranting further mechanistic study.
- **Hypoglycemic Use in Folk Medicine**: Arabian traditional practitioners employ decoctions of Lycium shawii for blood glucose management, consistent with the presence of flavonoid glycosides such as rutin and quercetin derivatives that modulate [glucose metabolism](/ingredients/condition/weight-management) enzymes in related Lycium species.
- **Mineral Nutrient Contribution**: The plant contains biologically relevant concentrations of zinc (15.1 g/dL) and copper (5.9 g/dL) in extracts, trace minerals that support enzymatic antioxidant systems including superoxide dismutase and ceruloplasmin, though heavy metal co-contamination warrants extraction-method scrutiny.

## Mechanism of Action

Quinoline alkaloids concentrated in the water extract intercalate with ferriprotoporphyrin IX (heme) released during hemoglobin [digestion](/ingredients/condition/gut-health) in malaria parasites, preventing its polymerization into non-toxic hemozoin and generating toxic free heme that kills the parasite—a mechanism analogous to chloroquine. Phenolic acids and flavonoids (quercetin, gallic acid, rutin, ferulic acid, p-coumaric acid) competitively inhibit cyclooxygenase-2 (COX-2) enzyme, reducing prostaglandin E2 biosynthesis from arachidonic acid, which underlies both [anti-inflammatory](/ingredients/condition/inflammation) and potential anticarcinogenic effects observed in vitro. Free-radical scavenging proceeds through hydrogen atom transfer and single-electron transfer from hydroxyl groups on the phenolic backbone of gallic acid, quercetin glycosides, and coumarins, neutralizing DPPH, superoxide, and lipid peroxy radicals and protecting cellular macromolecules from oxidative damage. Cytotoxic activity of the essential oil against MCF-7 cells likely involves terpenoid-mediated [mitochondrial](/ingredients/condition/energy) membrane disruption and [reactive oxygen species](/ingredients/condition/antioxidant) induction, though the exact molecular targets—whether Bcl-2 family proteins, caspase cascades, or cell cycle arrest checkpoints—have not yet been elucidated in published studies.

## Clinical Summary

No human clinical trials examining Lycium shawii for any indication have been identified in published literature. The entirety of efficacy data originates from cell-free enzymatic assays ([COX-2](/ingredients/condition/inflammation), β-hematin inhibition), microbial zone-of-inhibition experiments, DPPH [antioxidant](/ingredients/condition/antioxidant) assays, and a single cell-line cytotoxicity study using MCF-7 breast cancer cells. While these in vitro signals are mechanistically coherent and warrant progression to animal pharmacology studies, effect sizes from cell-culture models cannot be extrapolated to human therapeutic doses or outcomes with confidence. Traditional hypoglycemic use in Arabian folk medicine remains entirely evidence-free in controlled settings, representing an important research gap.

## Nutritional Profile

The fruit ethyl acetate extract contains phenolics at 0.67 mg/mL gallic acid equivalents, with identified polyphenols including gallic acid, quercetin, rutin, p-coumaric acid, ferulic acid, quercetin 3-methoxy glucoside, quercetin 3,7-diglucoside, and quercetin 3-O-β-glucoside. Fatty acid components identified by GC-MS include oleic acid, vaccenic acid, and linoleate, indicating unsaturated lipid content consistent with other Lycium fruits. Mineral analysis of extracts reveals zinc (15.1 g/dL), copper (5.9 g/dL), lead (4.2 g/dL), cadmium (0.11 g/dL), chromium (0.08 g/dL), nickel (0.009 g/dL), and manganese (0.006 g/dL); the reported units likely reflect extract-specific analytical concentrations rather than whole-plant content, and the presence of lead and cadmium signals potential heavy metal accumulation from desert soil. Sesquiterpene lactones, triterpenoids, steroids (14 characterized via NMR), and volatile terpenes constitute additional phytochemical classes; bioavailability of all constituents in humans remains entirely unstudied.

## Dosage & Preparation

- **Traditional Water Decoction**: Aerial parts (stems, leaves) simmered in water to produce a tea; the most culturally established form used in Arabian folk medicine for hypoglycemic and general health purposes; no standardized dose established.
- **Ethyl Acetate Extract (Research Use)**: Tested in vitro at concentrations yielding 0.67 mg/mL gallic acid equivalents total phenolics; no human-equivalent dose can be derived from available data.
- **Antimalarial Research Concentration**: Water extract tested at 1 mg/mL for β-hematin inhibition; translational dosing to humans has not been studied.
- **Essential Oil**: Demonstrated MCF-7 cytotoxicity at IC50 4.66 mg/L in vitro; no supplemental or therapeutic dosing guidance exists.
- **Standardization**: No commercial standardized extracts are currently available; no marker compounds have been officially designated for quality control purposes.
- **Timing and Duration**: No pharmacokinetic data available; traditional use patterns are unquantified in published literature.

## Safety & Drug Interactions

No formal human safety studies, toxicological assessments, or established maximum tolerated doses have been published for Lycium shawii in any form. A significant safety concern is the documented presence of lead (4.2 g/dL) and cadmium (0.11 g/dL) in plant extracts; while the analytical units suggest extract-matrix concentrations, chronic consumption of wild-harvested material from potentially contaminated desert soils could pose cumulative heavy metal toxicity risks that have not been quantified or risk-assessed. No drug interaction data exist, but the in vitro [COX-2](/ingredients/condition/inflammation) inhibitory potency exceeding aspirin theoretically raises the possibility of pharmacodynamic interactions with anticoagulants, NSAIDs, and antiplatelet agents if translated to human use. Pregnancy, lactation, and pediatric use cannot be recommended given the complete absence of safety data, the presence of alkaloids, and uncharacterized heavy metal burden; individuals with renal impairment should exercise particular caution given cadmium and lead nephrotoxicity potential.

## Scientific Research

All available evidence for Lycium shawii derives exclusively from in vitro bioassays and phytochemical characterization studies; no human clinical trials or animal pharmacological studies have been published as of the most recent available data. Metabolomics profiling identified 148 metabolites across four solvent extracts, and GC-MS analysis of the fruit ethyl acetate fraction confirmed 13 bioactive volatile compounds, providing strong phytochemical characterization but no efficacy data in biological systems beyond cell-free and cell-culture assays. [Antimicrobial](/ingredients/condition/immune-support) disc-diffusion assays, DPPH [antioxidant](/ingredients/condition/antioxidant) assays, [COX-2](/ingredients/condition/inflammation) enzymatic inhibition assays, β-hematin inhibition assays, and MCF-7 cytotoxicity assays collectively demonstrate biologically plausible activity, but in vitro-to-human translation is unestablished. The evidence base is rated as preliminary, representing an early-stage research plant requiring in vivo pharmacokinetic studies, toxicological profiling, and eventually randomized controlled trials before any therapeutic claims can be substantiated.

## Historical & Cultural Context

Lycium shawii holds a recognized place in Arabian folk medicine across the Arabian Peninsula, Egypt, and adjacent North African regions, where it has been used as a decoction for managing blood sugar, treating fevers, and addressing general [inflammatory](/ingredients/condition/inflammation) conditions for generations. The plant's name honors Richard Shaw, a nineteenth-century botanist, while its Arabic folk names reflect regional variation across Saudi, Emirati, and Egyptian vernaculars. Preparation traditionally involves boiling the woody stems and leaves in water, consistent with the aqueous extraction method confirmed by modern phytochemical studies to yield the highest quinoline content. Egyptian ethnobotanical surveys have documented its use among rural communities, and its inclusion in traditional pharmacopoeias of the region situates it within the broader Lycium genus—which also includes the widely researched L. barbarum (goji berry)—lending ethnobotanical credibility to the current scientific investigation of its bioactivity.

## Synergistic Combinations

Within the Lycium genus, quercetin glycosides and gallic acid commonly exhibit synergistic [antioxidant activity](/ingredients/condition/antioxidant) when combined with vitamin C (ascorbic acid), as ascorbate regenerates oxidized quercetin radicals back to their active form, amplifying total radical scavenging capacity. The quinoline-rich water extract of Lycium shawii may theoretically complement iron chelation strategies used in antimalarial protocols, as heme-binding quinolines and iron-chelating polyphenols (gallic acid, quercetin) could act on complementary targets in Plasmodium heme [metabolism](/ingredients/condition/weight-management). No empirically validated synergistic combinations specific to Lycium shawii have been studied; extrapolation from related polyphenol-rich botanicals such as L. barbarum or green tea catechins combined with quercetin sources represents a plausible research direction.

## Frequently Asked Questions

### What is Lycium shawii used for in traditional medicine?

Lycium shawii is used in Arabian folk medicine primarily as a water decoction for managing blood sugar levels (hypoglycemic use), treating fevers, and addressing inflammatory conditions. Traditional preparation involves boiling the stems and leaves in water, and modern phytochemical analysis confirms this aqueous extraction yields the highest concentration of quinoline alkaloids among all tested solvents.

### Does Lycium shawii have antimalarial properties?

In vitro studies show the water extract of Lycium shawii inhibits β-hematin formation—a key step in malaria parasite survival—with an absorbance reading of 0.140 ± 0.027 at 1 mg/mL, attributed to quinoline alkaloids disrupting heme polymerization in a mechanism similar to chloroquine. However, no animal studies or human clinical trials have confirmed this activity in living systems, and it should not be used as a substitute for established antimalarial treatments.

### Is Lycium shawii safe to consume?

No formal human safety or toxicology studies have been conducted on Lycium shawii. A notable concern is the detection of lead (4.2 g/dL) and cadmium (0.11 g/dL) in plant extracts, which raises potential heavy metal toxicity risks with chronic use, particularly for individuals with kidney disease. Until comprehensive safety data are available, use should be approached with caution and consumption of wild-harvested material from potentially contaminated soils is not advisable.

### What bioactive compounds are found in Lycium shawii?

Metabolomics profiling has identified 148 metabolites across solvent extracts of Lycium shawii, including quinoline alkaloids, phenylpropanoids, sesquiterpene lactones, triterpenoids, steroids, and flavonoids such as quercetin, rutin, gallic acid, p-coumaric acid, ferulic acid, and multiple quercetin glycosides. The fruit ethyl acetate extract also contains fatty acids including oleic acid, vaccenic acid, and linoleate, identified by GC-MS analysis.

### How does Lycium shawii compare to Lycium barbarum (goji berry)?

Both species belong to the Lycium genus and share some polyphenolic constituents including quercetin and rutin, but they differ substantially in research depth: Lycium barbarum has been studied in dozens of human clinical trials for antioxidant, vision-protective, and immunomodulatory effects, while Lycium shawii research is limited entirely to in vitro and phytochemical studies. Lycium shawii's unique quinoline alkaloid content and documented in vitro COX-2 inhibition exceeding aspirin differentiate it pharmacologically, but its therapeutic utility in humans remains unestablished.

### What is the difference between Lycium shawii fruit extract and leaf extract in terms of anti-inflammatory effects?

Lycium shawii fruit extract, particularly the ethyl acetate fraction, demonstrates superior anti-inflammatory potency by inhibiting COX-2 enzyme activity at levels exceeding aspirin's reference inhibition. The fruit's phenolic compounds—including quercetin, p-coumaric acid, and ferulic acid—directly suppress the arachidonic acid cascade that drives inflammation. Leaf extracts have not been reported to achieve comparable COX-2 inhibition levels, making the fruit the preferred source for anti-inflammatory applications.

### Does Lycium shawii contain the same beneficial compounds as common goji berries, and if not, what makes it unique?

While Lycium shawii and Lycium barbarum (goji) are related species sharing some polyphenolic content, Lycium shawii is notable for its distinct quinoline alkaloid profile, particularly in water extracts used for antimalarial applications. Lycium shawii's ethyl acetate fruit extract also demonstrates exceptionally potent COX-2 inhibition that appears to exceed typical goji berry preparations. This makes Lycium shawii potentially more valuable for specific anti-inflammatory and antimalarial applications despite being less commercially available than goji berries.

### What extraction method should be used to obtain the most bioactive form of Lycium shawii for anti-inflammatory benefits?

Ethyl acetate extraction of Lycium shawii fruit yields the highest anti-inflammatory potency by concentrating phenolic compounds responsible for COX-2 inhibition. Water extraction, while effective for isolating quinoline alkaloids with antimalarial potential, does not maximize anti-inflammatory activity compared to ethyl acetate processing. The choice of extraction solvent significantly impacts which bioactive compounds are concentrated, making ethyl acetate the preferred method when anti-inflammatory effects are the primary therapeutic goal.

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