# Koprna (Zingiber officinale Roscoe)

**Canonical URL:** https://ingredients.hermeticasuperfoods.com/ingredients/koprna-zingiber-officinale-roscoe
**Data Source:** Hermetica Superfoods Ingredient Encyclopedia
**Updated:** 2026-04-03
**Evidence Score:** 1 / 10
**Category:** Pacific Islands
**Also Known As:** Sheng Jiang (Chinese), Koprna (Zingiber officinale Roscoe, Zingiberaceae), Zingiber officinale Roscoe, Jengibre (Spanish), Koprna (Zingiber zerumbet), Ginger, Ingwer (German), Adrak (Hindi), Koprna (Tok Pisin, Papua New Guinea)

## Overview

Koprna (ginger) contains phenolic compounds—principally 6-gingerol in fresh rhizomes and 6-shogaol in dried preparations—that exert anti-inflammatory and antioxidant effects by inhibiting NF-κB signaling, activating Nrf2/HO-1 transcription, suppressing [pro-inflammatory cytokine](/ingredients/condition/inflammation)s (TNF-α, IL-6, IL-1β), and modulating [reactive oxygen species](/ingredients/condition/antioxidant) (ROS) through upregulation of [glutathione](/ingredients/condition/detox) biosynthesis genes including GCLC, GCLM, and HO-1. Preclinical evidence demonstrates that a 6-gingerol-rich fraction at 50–100 mg/kg in female Wistar rats significantly reduces markers of oxidative stress (H₂O₂, MDA) while elevating glutathione (GSH) levels and antioxidant enzyme activity, supporting its traditional use for inflammation-related and gastrointestinal conditions across Pacific Island cultures.

## Health Benefits

- **Antioxidant Defense**: 6-Shogaol at 20 μM in HCT-116 cells upregulates antioxidant genes including AKR1B10, FTL, HO-1, MT1, GCLC, and GCLM while increasing the GSH/GSSG ratio, significantly reducing cellular oxidative burden and protecting against ROS-mediated tissue damage.
- **Anti-Inflammatory Activity**: Ginger-derived nanoparticles (GDNPs 2, 0.3 mg in murine models) suppress NF-κB activation and reduce [pro-inflammatory cytokine](/ingredients/condition/inflammation)s TNF-α, IL-6, and IL-1β while elevating anti-inflammatory interleukins IL-10 and IL-22, offering multi-cytokine modulation relevant to chronic inflammatory conditions.
- **Gastrointestinal Support**: Gingerols and shogaols stimulate gastric motility, reduce nausea, and inhibit gut inflammatory signaling; these compounds are the basis for ginger's ancient and widespread traditional use for nausea, vomiting, dyspepsia, and bloating across Asian and Pacific Island medical traditions.
- **Anticancer Potential (Preclinical)**: Ginger extract at 2–10 mg/mL in HT29 colorectal cancer cells and 100 mg/kg in murine models promotes apoptosis through caspase-9 upregulation, suppresses proliferative signals cyclin D1, KRAS, ERK, and Bcl-xL, and activates the tumor-suppressive AMPK/p53 pathway.
- **Nrf2 Pathway Activation**: Ginger oleoresin at 100 μg/mL triggers Nrf2 nuclear translocation, upregulating cytoprotective enzymes HO-1 and NQO1, thereby conferring protection against electrophilic and [oxidative stress](/ingredients/condition/antioxidant)ors at the cellular level.
- **Metabolic and Lipid Modulation**: Gingerols and related phenolics modulate PPARγ and AMPK pathways, with preclinical data indicating potential benefits for [insulin sensitivity](/ingredients/condition/weight-management), lipid metabolism, and reduction of hepatic steatosis markers, relevant to metabolic syndrome contexts.
- **[Antimicrobial](/ingredients/condition/immune-support) and Antiviral Properties**: Molecular docking studies demonstrate that gingerols and curcuminoids from the Zingiberaceae family interact with SARS-CoV-2 targets including the main protease, RNA-dependent RNA polymerase (RdRp), furin cleavage site, and ACE2 receptor, as well as cathepsin K, suggesting broad-spectrum antimicrobial and antiviral potential warranting further clinical investigation.

## Mechanism of Action

6-Gingerol and 6-shogaol, the primary phenolic bioactives of Zingiber officinale, inhibit the NF-κB signaling cascade by preventing IκB kinase phosphorylation, thereby blocking nuclear translocation of NF-κB and downstream transcription of pro-[inflammatory](/ingredients/condition/inflammation) mediators including TNF-α, IL-6, IL-1β, iNOS, and COX-2. Simultaneously, these compounds activate Nrf2 (nuclear factor erythroid 2-related factor 2) translocation to the nucleus where it binds [antioxidant](/ingredients/condition/antioxidant) response elements (ARE), inducing expression of cytoprotective enzymes HO-1 (heme oxygenase-1), NQO1 (NAD(P)H quinone oxidoreductase-1), GSTP1, and rate-limiting [glutathione](/ingredients/condition/detox) biosynthesis enzymes GCLC and GCLM, thereby fortifying cellular antioxidant capacity. At the anticancer level, gingerol-rich fractions modulate the PI3K/Akt/mTOR axis, activate AMPK to stabilize p53 tumor suppressor function, suppress anti-apoptotic Bcl-xL expression, and upregulate pro-apoptotic caspase-9, collectively shifting the balance toward programmed cell death in malignant cells. Terpenic constituents of the essential oil—including α-zingiberene, β-bisabolene, geranial, and β-sesquiphellandrene—contribute to [antimicrobial](/ingredients/condition/immune-support) activity and may modulate TRPV1 (transient receptor potential vanilloid 1) receptors, explaining the spasmolytic, analgesic, and thermogenic properties attributed to ginger in traditional Papua New Guinean and broader Pacific healing practices.

## Clinical Summary

Formal clinical trial data directly studying koprna or Zingiber officinale in Papua New Guinean populations is absent from the current evidence base, with available human-relevant data extrapolated from broader international ginger research. Preclinical studies have demonstrated statistically significant [antioxidant](/ingredients/condition/antioxidant) effects (reduced MDA, elevated GSH and superoxide dismutase activity) in rat models at doses of 50–100 mg/kg of 6-gingerol-rich fractions, and [anti-inflammatory](/ingredients/condition/inflammation) suppression of TNF-α in C57BL/6J mice using 50 mg/mL ginger extract; these outcomes are mechanistically plausible but require confirmation in human trials with standardized preparations. The most clinically relevant human evidence for ginger broadly concerns nausea and vomiting (particularly pregnancy-related and chemotherapy-induced), where multiple RCTs have demonstrated benefit, though these studies used standardized Zingiber officinale extracts rather than preparations specifically identified as koprna. Overall confidence in koprna's traditional medicinal applications is moderate from a scientific standpoint, supported by strong mechanistic plausibility and a growing preclinical evidence base, but limited by the absence of human RCTs specific to its Pacific Island use context.

## Nutritional Profile

Fresh ginger rhizome contains approximately 80% water, 2% protein, 0.75% fat, 15–17% total carbohydrates (including 2% dietary fiber), and provides approximately 80 kcal per 100 g. Micronutrient content includes potassium (~415 mg/100 g), magnesium (~43 mg/100 g), phosphorus (~34 mg/100 g), vitamin C (~5 mg/100 g), and B-complex vitamins including niacin and pyridoxine in small quantities. The primary pharmacologically active phytochemicals are phenolic compounds: 6-gingerol (the dominant compound in fresh rhizome, typically 0.5–1.5 mg/g dry weight), 8-gingerol, 10-gingerol, and their dehydration products 6-shogaol, 8-shogaol, and 10-shogaol, which concentrate 5.2-fold in dried preparations; paradols and zingerone are present as minor phenolics. The essential oil fraction (1–3% of dry weight) comprises α-zingiberene (20–30% of oil), β-bisabolene, geranial, neral, β-sesquiphellandrene, and α-curcumene; polysaccharides (galanans), organic acids (cinnamic acid, 5-carboxyvanillic acid), and lipids constitute additional nutritional components. Bioavailability of gingerols is enhanced by lipid co-consumption and may be increased by co-administration with piperine from black pepper, which inhibits glucuronidation and sulfation [metabolism](/ingredients/condition/weight-management).

## Dosage & Preparation

- **Fresh Rhizome (Traditional, Papua New Guinea)**: Rhizomes are crushed, chewed, or prepared as a decoction in hot water; no standardized dose established for traditional use, but typical culinary and medicinal servings range from 1–4 g of fresh rhizome per preparation.
- **Dried Ground Rhizome (Powder)**: Commonly dosed at 1–3 g per day in divided doses for general wellness; dried ginger contains 5.2-fold higher total phenolics than fresh rhizome due to conversion of gingerols to shogaols during dehydration.
- **Standardized Extract (5% Gingerols)**: Typical supplemental doses of 250–500 mg, two to four times daily, totaling 1–2 g/day of extract; standardization to ≥5% total gingerols/shogaols is recommended for consistent bioactive delivery.
- **Ginger Oleoresin**: Used in research at 100 μg/mL for Nrf2/HO-1 activation in cellular models; supplemental oleoresin preparations provide concentrated phenolics and are typically dosed at 100–200 mg/day.
- **Essential Oil (Steam Distilled)**: Prepared by steam distillation of fresh or dried rhizomes; used topically (diluted in carrier oil at 2–5%) or aromatically; not typically consumed orally in high doses due to concentrated terpene content.
- **Hot Water Extract (Tea/Decoction)**: Traditional Papua New Guinean method: 5–10 g fresh rhizome simmered in 200–300 mL water for 10–15 minutes; suitable for gastrointestinal and [anti-inflammatory](/ingredients/condition/inflammation) applications.
- **Timing Note**: Ginger preparations for nausea are most effective when taken 30–60 minutes before anticipated triggers; anti-inflammatory effects appear dose-dependent and require consistent daily administration over 4–8 weeks based on preclinical models.

## Safety & Drug Interactions

Zingiber officinale is generally regarded as safe at conventional culinary and supplemental doses (1–3 g/day dried powder or equivalent); preclinical toxicity studies demonstrate no adverse effects at doses up to 100 mg/kg in rodent models, and related Zingiberaceae compounds show a NOAEL of 1000 mg/kg in 90-day oral studies, suggesting a wide safety margin for human use. The primary clinically relevant drug interactions involve anticoagulant and antiplatelet agents (warfarin, aspirin, clopidogrel), as gingerols inhibit thromboxane synthetase and may augment bleeding risk, warranting caution and INR monitoring in patients on anticoagulation therapy; ginger may also potentiate hypoglycemic agents by modulating AMPK and [insulin sensitivity](/ingredients/condition/weight-management) pathways. Contraindications include active gallstone disease (due to choleretic activity), pre-surgical settings (discontinue ≥2 weeks before surgery due to antiplatelet effects), and caution is advised in individuals with gastroesophageal reflux disease (GERD) as high doses may exacerbate symptoms in sensitive individuals. Pregnancy use at low culinary doses (up to 1 g/day) is generally considered safe and has been studied for morning sickness, but high-dose supplemental use (>2 g/day) during pregnancy is not recommended without medical supervision due to theoretical uterotonic effects at pharmacological doses; no specific koprna-related adverse event data from Papua New Guinea traditional use has been documented in the published literature.

## Scientific Research

The evidence base for Zingiber officinale's bioactive properties rests predominantly on in vitro and preclinical in vivo studies, with robust mechanistic characterization but a relative scarcity of large, well-controlled human randomized controlled trials (RCTs) reported in the available research context. Preclinical models have yielded quantifiable outcomes—such as significant reduction in malondialdehyde (MDA) and H₂O₂ with concurrent GSH elevation at 50–100 mg/kg in female Wistar rats, and tumor growth inhibition in HT29 colorectal cells and C57BL/6J murine models at 50–100 mg/mL ginger extract—providing mechanistically coherent but not directly translatable data. Analytical chemistry studies using UPLC-HRMS and GC-MS have rigorously characterized the phytochemical composition of ginger extracts, identifying 6-gingerol, 6-shogaol, α-zingiberene, and geranial as dominant compounds with confirmed biological activity, lending high credibility to the mechanistic claims. Specific to koprna's use in Papua New Guinea traditional medicine, no published ethnopharmacological RCTs or clinical intervention trials were identified in the available literature, meaning the therapeutic application in Pacific Island contexts remains validated by traditional knowledge and preclinical proxy data rather than regional clinical trial evidence.

## Historical & Cultural Context

Ginger (Zingiber officinale), known as koprna in Papua New Guinea's Tok Pisin linguistic tradition, has been integral to traditional healing systems across the Asia-Pacific region for at least 3,000 years, with documented references in ancient Sanskrit texts, Chinese pharmacopoeia (Shennong Bencao Jing, ~200 CE), and Ayurvedic compendiums such as the Charaka Samhita, where it was described as a universal medicine ('vishwabhesaj'). In Papua New Guinea and broader Melanesian cultures, ginger rhizomes are employed by traditional healers for a wide spectrum of conditions including gastrointestinal distress, fever, pain, and general bodily weakness, often administered as chewed raw rhizome, decoction, or topical poultice applied to inflamed areas. The plant holds cultural significance beyond medicine in many Pacific Island societies, appearing in ritual contexts, as a ceremonial exchange item, and as a protective amulet in some Highlands PNG communities, reflecting the deep integration of medicinal plants into spiritual and social frameworks. Ginger's historical diffusion from Southeast Asian origins throughout the Pacific via Austronesian maritime trade networks means koprna represents both an ancient botanical heritage and an enduring component of living traditional medical knowledge in the region.

## Synergistic Combinations

Koprna (ginger) demonstrates significant pharmacokinetic and pharmacodynamic synergy with Piper nigrum (black pepper), wherein piperine inhibits cytochrome P450 enzymes and phase II conjugation (glucuronidation, sulfation) of gingerols, substantially increasing their systemic bioavailability and prolonging plasma half-life; this combination is reported to enhance overall [anti-inflammatory](/ingredients/condition/inflammation) and [antioxidant activity](/ingredients/condition/antioxidant) beyond the additive effects of either compound alone. Ginger combined with turmeric (Curcuma longa, also Zingiberaceae) produces complementary NF-κB and Nrf2 pathway modulation—gingerols targeting IKK phosphorylation while curcuminoids additionally inhibit NLRP3 inflammasome assembly—creating a broader-spectrum anti-inflammatory effect relevant to musculoskeletal, metabolic, and gastrointestinal indications. In traditional Pacific and Asian medicine, ginger is frequently combined with honey and lemon (citrus flavonoids), where quercetin and hesperidin from citrus may act synergistically with shogaols on antioxidant response element activation, while honey's [antimicrobial](/ingredients/condition/immune-support) compounds complement ginger's direct antimicrobial terpene constituents.

## Frequently Asked Questions

### What is koprna and how is it used in Papua New Guinea traditional medicine?

Koprna is the Tok Pisin (Papua New Guinea Creole) name for ginger (Zingiber officinale Roscoe), a rhizomatous plant from the Zingiberaceae family. In Papua New Guinea, traditional healers use koprna for a broad range of medicinal applications including gastrointestinal complaints, fever, pain, and general bodily weakness, typically preparing it as a chewed raw rhizome, a hot water decoction, or a topical poultice applied to inflamed or painful areas.

### What are the key bioactive compounds in koprna (ginger) and what do they do?

The primary bioactive compounds in koprna are 6-gingerol (dominant in fresh rhizomes), 6-shogaol (enriched up to 5.2-fold in dried preparations), 8-gingerol, 10-gingerol, and terpenes including α-zingiberene and geranial. These compounds exert antioxidant effects by activating the Nrf2/HO-1 pathway and upregulating glutathione biosynthesis genes (GCLC, GCLM), and anti-inflammatory effects by inhibiting NF-κB signaling and reducing cytokines TNF-α, IL-6, and IL-1β at molecular concentrations as low as 20 μM (6-shogaol in cell culture models).

### What is the recommended dosage of koprna (ginger) as a supplement?

For general health and anti-inflammatory purposes, standardized ginger extract (standardized to ≥5% gingerols/shogaols) is typically dosed at 250–500 mg two to four times daily, totaling 1–2 g/day of extract. Dried ginger powder is commonly used at 1–3 g/day in divided doses, while traditional preparations in Papua New Guinea use fresh rhizome decoctions (approximately 5–10 g fresh rhizome in 200–300 mL water); no formal RCT-derived dosing specific to Pacific Island use has been established.

### Is koprna (ginger) safe to take every day, and are there any drug interactions?

Koprna (ginger) is generally considered safe at doses of 1–3 g/day of dried rhizome equivalent, with preclinical studies showing no adverse effects at up to 100 mg/kg in animal models. The most clinically important drug interaction is with anticoagulants and antiplatelet medications (warfarin, aspirin, clopidogrel), as gingerols inhibit thromboxane synthetase and may increase bleeding risk; patients on blood thinners should consult their healthcare provider, and ginger supplementation should be discontinued at least two weeks before surgery.

### How does dried koprna (ginger) differ from fresh ginger in terms of health benefits?

Dried koprna (ginger) contains significantly higher concentrations of shogaols—formed through dehydration-induced conversion of gingerols—with total phenolic content approximately 5.2-fold higher than fresh ginger, resulting in enhanced antioxidant activity as measured by DPPH and FRAP assays. Fresh ginger is richer in gingerols (particularly 6-gingerol), which are more relevant for acute anti-nausea and anti-inflammatory applications, while dried ginger with higher shogaol content may offer more potent antioxidant and anticancer-relevant properties based on current preclinical evidence.

### What is the difference in bioavailability between fresh koprna (ginger) and ginger-derived nanoparticles?

Ginger-derived nanoparticles (GDNPs) are engineered formulations that significantly enhance bioavailability and cellular uptake compared to fresh ginger, allowing active compounds like 6-shogaol to reach target tissues more effectively. While fresh koprna delivers whole-plant compounds through standard digestion, nanoparticle formulations bypass some absorption barriers and enable direct cellular interaction at lower doses. This enhanced delivery system is particularly relevant for achieving the anti-inflammatory and antioxidant benefits documented in research at specific bioactive concentrations.

### Who should consider koprna (ginger) supplementation for antioxidant and anti-inflammatory support?

Individuals with elevated oxidative stress, chronic inflammatory conditions, or those seeking cellular protection from reactive oxygen species (ROS) may benefit most from koprna supplementation. People with age-related cellular aging, autoimmune concerns, or those exposed to environmental stressors can leverage koprna's ability to upregulate antioxidant defense genes like HO-1, GCLC, and GCLM. However, those with bleeding disorders, on anticoagulant medications, or pregnant women should consult a healthcare provider before use.

### How strong is the scientific evidence for koprna's antioxidant effects at the cellular level?

In vitro research demonstrates that 6-shogaol, a key bioactive in koprna, significantly upregulates multiple antioxidant genes and increases the GSH/GSSG ratio in human colon cancer cells (HCT-116), providing robust mechanistic evidence for cellular protection. Murine model studies show that ginger-derived nanoparticles suppress NF-κB activation, a master inflammatory pathway, confirming anti-inflammatory activity at physiologically relevant doses. While these findings are compelling at the cellular and animal model level, human clinical trials translating these benefits to real-world health outcomes remain limited and warrant further investigation.

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