# Dammarane (Dammarane-type Triterpenoids)

**Canonical URL:** https://ingredients.hermeticasuperfoods.com/ingredients/dammarane-dammarane-type-triterpenoids
**Data Source:** Hermetica Superfoods Ingredient Encyclopedia
**Updated:** 2026-04-02
**Evidence Score:** 1 / 10
**Category:** Compound
**Also Known As:** Dammarane Triterpenoid Saponins (Panax spp. and Ziziphus spina-christi), Dammarane-type triterpenoids, Dammarane saponins, PNS (Panax notoginseng saponins), Dammarane (tetracyclic triterpene skeleton from Panax spp.), Tetracyclic triterpenes, Protopanaxadiol-type ginsenosides

## Overview

Dammarane-type triterpenoids exert [anti-inflammatory](/ingredients/condition/inflammation) effects by inhibiting nitric oxide production in macrophages (IC₅₀ 71.85–95.71 μM) and cytotoxic effects through molecular mechanisms involving microtubule disruption via tubulin binding (docking energy −9.7 kcal/mol) and apoptosis induction via BCL-2 inhibition (−9.1 kcal/mol). In vitro cytotoxicity against cancer cell lines including HepG2, NCI-H460, and MCF-7 has been demonstrated, with the most potent isolated compound achieving IC₅₀ values of 10.65–14.28 μM against A549, HepG2, and MCF-7 cells, though no human clinical trial data currently exists to confirm these effects in vivo.

## Health Benefits

- **[Anti-Inflammatory](/ingredients/condition/inflammation) Activity**: Dammarane compounds 3, 7, and 8 suppress nitric oxide production in RAW 264.7 macrophages with IC₅₀ values of 71.85–95.71 μM, suggesting modulation of the inflammatory signaling cascade downstream of LPS stimulation.
- **Cytotoxic and Antitumor Potential**: Isolated dammarane saponin 2 from Panax notoginseng inhibits HepG2 hepatocellular carcinoma cells (IC₅₀ 4.49 μg/mL), NCI-H460 lung cancer cells (8.06 μg/mL), and MCF-7 breast cancer cells (7.38 μg/mL) in vitro, representing among the most potent anti-proliferative activities recorded for this compound class.
- **Microtubule Disruption**: Molecular docking studies indicate compounds 7 and 11 bind tubulin with energies of −9.7 and −9.4 kcal/mol respectively, suggesting a colchicine-like mechanism of cytoskeletal interference that could arrest cancer cell division.
- **BCL-2-Mediated Apoptosis Induction**: Compound 15 demonstrates dual binding to tubulin (−8.7 kcal/mol) and the anti-apoptotic protein BCL-2 (−9.1 kcal/mol), indicating a potential multi-target mechanism that simultaneously disrupts mitosis and promotes programmed cell death.
- **Hypoglycemic Properties**: Dammarane saponins derived from Panax species have been investigated for [blood glucose](/ingredients/condition/weight-management) regulation, consistent with the broader ethnopharmacological use of ginseng in traditional Chinese medicine for metabolic support, though mechanistic data at the molecular level requires further elucidation.
- **Virucidal and Antifungal Activity**: Certain dammarane-type compounds have been attributed virucidal and antifungal properties, contributing to their broad bioactivity profile, though these effects require rigorous controlled experimental validation beyond preliminary observations.
- **Structural Basis for Diverse Bioactivity**: The tetracyclic dammarane scaffold provides a rigid hydrophobic core amenable to diverse glycosylation and hydroxylation patterns, enabling interactions with multiple protein targets and explaining the compound class's wide range of reported pharmacological activities across cancer, inflammation, and metabolic pathways.

## Mechanism of Action

Dammarane-type triterpenoids act through multiple molecular pathways depending on their specific substitution patterns. [Anti-inflammatory](/ingredients/condition/inflammation) activity is mediated by suppression of inducible nitric oxide synthase (iNOS) expression or activity in activated macrophages, reducing NO production triggered by lipopolysaccharide stimulation in RAW 264.7 cells (IC₅₀ 71.85–95.71 μM for compounds 3, 7, and 8). Cytotoxic activity is driven by tubulin polymerization disruption — compound 7 binds the tubulin colchicine-binding site with a docking energy of −9.7 kcal/mol — and by BCL-2 inhibition; compound 15 binds BCL-2 at −9.1 kcal/mol, relieving its suppression of pro-apoptotic BAX and BIM proteins to trigger the intrinsic apoptotic cascade. Glycosylated dammarane saponins from Panax notoginseng (e.g., compound 1, C₃₆H₆₀O₉, HR-ESI-MS m/z 659.4130 [M+Na]⁺) and Panax ginseng (compound 1, C₄₀H₆₆O₁₂, m/z 761.4446 [M+Na]⁺) likely interact with membrane-associated receptors and transporters due to their amphiphilic character, potentially modulating glucose transport and cellular signaling cascades relevant to metabolic regulation.

## Clinical Summary

No clinical trials specifically investigating isolated dammarane-type triterpenoids as defined in recent phytochemical isolation studies have been identified in the available literature. While the parent plants Panax ginseng and Panax notoginseng have been subjects of numerous randomized controlled trials examining cognition, fatigue, [immune function](/ingredients/condition/immune-support), and hemostasis, the pharmacological contributions of individual dammarane compounds cannot be attributed from these whole-extract studies. The most clinically relevant in vitro finding is cytotoxicity against HepG2 at IC₅₀ 4.49 μg/mL (Panax notoginseng saponin 2), which warrants progression to animal tumor model studies before any clinical extrapolation. Confidence in the clinical utility of isolated dammarane compounds as therapeutic agents is currently very low, and all benefit claims remain preliminary hypotheses generated from cell culture and computational chemistry data.

## Nutritional Profile

Dammarane is a pure phytochemical compound class, not a food ingredient, and therefore possesses no conventional macronutrient or micronutrient profile. As triterpenoids, dammarane compounds are lipophilic secondary metabolites biosynthesized from the mevalonate pathway via squalene and 2,3-oxidosqualene precursors, with molecular formulas typically in the range of C₃₆H₆₀O₉ to C₄₀H₆₆O₁₂ and molecular weights of approximately 637–739 g/mol for aglycone and glycoside forms respectively. In Panax species, dammarane saponins (ginsenosides) constitute the major class of bioactive phytochemicals, representing 2–3% of dried root weight in standardized preparations. Bioavailability of intact dammarane saponins is generally low due to poor intestinal absorption of their glycosidic forms; gut microbiota-mediated deglycosylation to compound K and other metabolites is considered essential for systemic activity, though this conversion efficiency varies substantially between individuals.

## Dosage & Preparation

- **Isolation Research Form**: Pure dammarane compounds are isolated via multi-step chromatography including reversed-phase RP-18 columns with acetone-water gradients, silica gel with n-hexane-acetone systems, and Sephadex LH-20 with CH₂Cl₂-MeOH; isolation yields range from 10 mg (compound 9) to 235 mg (compound 12) per extraction batch.
- **Traditional Ginseng Root Decoction**: Panax ginseng root, the primary natural source of dammarane saponins, is traditionally prepared as a water decoction using 3–9 g of dried root per day in traditional Chinese medicine practice.
- **Standardized Ginsenoside Extracts**: Commercial Panax ginseng supplements are typically standardized to 4–7% total ginsenosides (protopanaxadiol and protopanaxatriol dammarane saponins), with common daily doses of 200–400 mg standardized extract used in clinical research on ginseng broadly.
- **No Established Dose for Isolated Dammaranes**: No standardized supplemental dose, bioavailability data, or pharmacokinetic profile has been established for isolated dammarane compounds outside of their source plant extracts; dosing recommendations cannot be provided based on current evidence.
- **Quality Control**: HPLC fingerprinting of Panax notoginseng saponins (PNS) is employed for quality standardization of source plant extracts, serving as an indirect proxy for dammarane content.

## Safety & Drug Interactions

Safety data specifically for isolated dammarane-type triterpenoids are absent from the available literature; in vitro cytotoxicity studies have not assessed effects on normal (non-cancerous) human cell lines, leaving the therapeutic index and selectivity of these compounds entirely undefined. No drug interaction studies, contraindication data, or reproductive toxicology assessments have been reported for isolated dammarane compounds. Extrapolating cautiously from the well-documented safety profile of Panax ginseng whole-root preparations — which contain dammarane saponins as their primary bioactives — common adverse effects at high doses include [insomnia](/ingredients/condition/sleep), headache, gastrointestinal upset, and potential interactions with warfarin, MAO inhibitors, and hypoglycemic agents due to additive effects on coagulation and [blood glucose](/ingredients/condition/weight-management). Pregnant and lactating women are generally advised to avoid concentrated ginseng preparations due to insufficient safety data, and this precautionary guidance extends logically to isolated dammarane compounds until independent toxicological evaluation is conducted.

## Scientific Research

Current evidence for dammarane-type triterpenoids is restricted entirely to in vitro cell-based assays and in silico molecular docking simulations; no animal pharmacokinetic studies, preclinical efficacy models, or human clinical trials have been reported in the available literature. Cytotoxicity data are derived from standard MTT or equivalent cell viability assays using human cancer cell lines (A549, HepG2, MCF-7, HL-60, NCI-H460, MGC80-3) and macrophage lines (RAW 264.7), which provide mechanistic hypotheses but do not predict in vivo efficacy or safety. Molecular docking analyses using AutoDock or comparable platforms report binding energies ranging from −7.4 to −9.7 kcal/mol for tubulin and −7.7 to −9.1 kcal/mol for BCL-2, offering computational rationale for observed cytotoxicity but requiring experimental validation through binding assays and animal models. The compound class broadly benefits from the extensive clinical literature on Panax ginseng ginsenosides — which share the dammarane scaffold — but isolated dammarane compounds as defined in the recent phytochemical studies cited have no independent clinical trial record.

## Historical & Cultural Context

Dammarane-type triterpenoids derive their pharmacological relevance largely from the multi-millennium history of Panax ginseng and Panax notoginseng in traditional Chinese medicine (TCM), where ginseng root has been classified as a superior tonic herb for at least 2,000 years and documented in the Shennong Bencao Jing (Divine Farmer's Classic of Materia Medica, circa 200 CE). In TCM, Panax ginseng is prescribed to tonify the yuan qi (source energy), strengthen the spleen and lung, calm the mind, and generate body fluids, functions that are now being investigated through the lens of individual saponin compounds including dammarane derivatives. Panax notoginseng, known in Chinese as Sanqi, has a distinct TCM history focused on hemostasis and blood circulation, referenced extensively in the 16th-century Bencao Gangmu (Compendium of Materia Medica) by Li Shizhen. The chemical identity of dammarane as the structural backbone of ginseng saponins was elucidated through mid-20th-century phytochemical research, translating centuries of empirical medicinal use into a framework of isolable, structurally characterized bioactive compounds.

## Synergistic Combinations

Dammarane saponins in their natural botanical context co-occur with oleanolic acid-type triterpenoids, polysaccharides, and polyacetylenes in Panax species, and whole-plant ginseng extracts demonstrate broader and sometimes superior bioactivity compared to isolated fractions, suggesting synergistic interactions among these compound classes. In the context of [anti-inflammatory](/ingredients/condition/inflammation) stacks, dammarane compounds may complement flavonoids such as quercetin or curcumin through complementary mechanisms — dammaranes targeting iNOS-mediated NO production while flavonoids modulate NF-κB transcriptional activity — though this synergy is hypothetical and not experimentally validated for isolated dammaranes. For potential antitumor applications, the dual tubulin/BCL-2 binding profile of compound 15 theoretically complements paclitaxel-class tubulin stabilizers through distinct binding site interactions, warranting future combination index studies.

## Frequently Asked Questions

### What are dammarane triterpenoids and where do they come from?

Dammarane triterpenoids are a class of tetracyclic triterpene compounds built on a 30-carbon dammarane skeleton, biosynthesized primarily in the roots of Panax ginseng and Panax notoginseng — plants native to mountainous East Asia. They constitute the structural backbone of ginsenosides, the principal bioactive compounds in ginseng, and also occur in select fungal species. Their diverse pharmacological activities arise from variable glycosylation and hydroxylation patterns on the core tetracyclic scaffold.

### What is the evidence for dammarane compounds fighting cancer?

Current evidence is limited to in vitro cell culture studies and computational molecular docking; no animal tumor models or human clinical trials have been conducted. The most potent isolated compound (saponin 2 from Panax notoginseng) inhibited HepG2 liver cancer cells at IC₅₀ 4.49 μg/mL and MCF-7 breast cancer cells at 7.38 μg/mL. Molecular docking suggests tubulin binding (−9.7 kcal/mol) and BCL-2 inhibition (−9.1 kcal/mol) as potential mechanisms, but these findings require extensive further validation before any clinical conclusions can be drawn.

### Are dammarane supplements available and what dose should I take?

Isolated dammarane-type triterpenoids are not currently available as standardized commercial supplements; they exist as research chemicals isolated from plant extracts. Standardized Panax ginseng extracts containing the dammarane scaffold as ginsenosides (typically 4–7% total ginsenosides) are commercially available, with doses of 200–400 mg/day used in clinical ginseng research. No established dose, bioavailability, or pharmacokinetic data exists for isolated dammarane compounds specifically.

### Are dammarane triterpenoids safe to consume?

No dedicated safety or toxicology studies have been published for isolated dammarane compounds, and in vitro studies have not assessed effects on normal human cell lines, leaving the therapeutic index undefined. Cautious extrapolation from the Panax ginseng safety literature — where dammarane saponins are the primary bioactives — suggests potential interactions with warfarin, hypoglycemic drugs, and MAO inhibitors at high doses. Until independent toxicological evaluation is completed, isolated dammarane compounds should be regarded as research-stage substances rather than safe consumer supplements.

### How do dammarane compounds differ from other ginseng saponins like ginsenosides?

Ginsenosides are the specific glycosylated dammarane saponins found in Panax species — meaning all protopanaxadiol and protopanaxatriol ginsenosides (e.g., Rb1, Rg1, Rd) are dammarane-type triterpenoids by structural classification. The term 'dammarane' refers to the parent tetracyclic carbon skeleton shared by this entire subgroup of ginsenosides, distinguishing them from the oleanane-type saponin Ro also found in ginseng. Recent phytochemical research isolates individual novel dammarane compounds with distinct molecular formulas (e.g., C₃₆H₆₀O₉ or C₄₀H₆₆O₁₂) that extend beyond the classical ginsenoside catalog.

### What is the bioavailability of dammarane triterpenoids, and does the source plant affect absorption?

Dammarane bioavailability is influenced by their glycoside structure and the plant matrix they come from; compounds from Panax notoginseng and Panax ginseng may have different absorption profiles due to variations in associated cofactors and processing methods. In vitro studies suggest dammaranes are absorbed in the gastrointestinal tract, but human pharmacokinetic data remain limited, making it difficult to establish definitive bioavailability rates. Extraction method and formulation type (standardized extract vs. whole plant) likely impact the amount of active dammarane reaching systemic circulation.

### Which populations might benefit most from dammarane supplementation based on current research?

Individuals with elevated inflammatory markers or those seeking hepatoprotective support may benefit most from dammarane compounds, given evidence of anti-inflammatory and cytotoxic effects in macrophages and hepatocellular carcinoma cells. People with metabolic conditions or those using ginseng traditionally for immune support could also be candidates, though human clinical trials are limited. Conversely, those with active cancer treatment, liver disease, or taking immunosuppressive medications should consult a healthcare provider before use.

### How do dammarane triterpenoids interact with the gut microbiome, and does this affect their efficacy?

Limited research exists on how dammarane compounds are metabolized by gut bacteria or whether the microbiome influences their bioavailability and anti-inflammatory effects. Since many triterpenoids undergo microbial metabolism in the colon, individual differences in gut flora composition may affect dammarane absorption and activity, potentially explaining variability in supplement efficacy between individuals. This represents a significant gap in dammarane research that could inform personalized supplementation strategies.

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