Astaxanthin / TumCI Cancer Research Results

ASTX, Astaxanthin: Click to Expand ⟱
Features:

Astaxanthin — a lipophilic xanthophyll carotenoid antioxidant (often sourced from Haematococcus pluvialis microalgae and also present in salmon/crustaceans) used as a nutraceutical with prominent redox and inflammation-modulating biology. It is formally classified as a small-molecule dietary carotenoid (natural product / nutraceutical). Common abbreviations include ASTX and AXT. In oncology-context literature it is primarily discussed as a chemopreventive/cytoprotective redox modulator with context-dependent direct antitumor effects, and with theoretical concern for antagonizing ROS-mediated chemo/radiation mechanisms in some settings.
The European Commission considers natural astaxanthin as a food dye

Primary mechanisms (ranked):

  1. NRF2 pathway activation with downstream antioxidant/phase-II enzyme program (context-dependent; often cytoprotective)
  2. Suppression of inflammatory signaling including NF-κB axis with downstream COX-2/iNOS and cytokine modulation
  3. Growth/survival signaling modulation (context-dependent), commonly reported on PI3K–AKT, ERK/MAPK, STAT3
  4. Mitochondria-linked apoptosis induction and cell-cycle perturbation in select tumor models (dose/model-dependent)
  5. Anti-migration/anti-EMT phenotype (e.g., MMPs, cadherin switch; model-dependent)
  6. Ferroptosis/redox-lethal interactions reported in limited models (model-dependent)

Bioavailability / PK relevance: Poor aqueous solubility and variable oral absorption (fat/formulation-dependent). Plasma exposure is typically low with standard oral supplements; engineered formulations (micellar/nanoemulsion) can increase Cmax and shorten Tmax. Reported terminal half-life in healthy volunteers is on the order of ~1–2 days in at least one human PK study.

In-vitro vs systemic exposure relevance: Many mechanistic cancer studies use micromolar astaxanthin concentrations that can exceed typical human plasma levels after supplementation; therefore, mechanistic claims are frequently concentration- and formulation-limited for systemic antitumor translation.

Clinical evidence status: Predominantly preclinical (cell/animal) for direct anticancer claims. Human evidence is stronger for oxidative stress/inflammation biomarker modulation than for anticancer efficacy endpoints; not an approved anticancer drug. Practical oncology use is mainly adjunctive/chemopreventive framing, with caution discussed around concurrent ROS-dependent chemo/radiation.

Astaxanthin is a xanthophyll carotenoid with exceptionally strong antioxidant capacity. In cancer biology, it shows context-dependent effects—largely chemopreventive and cytoprotective, with limited evidence as a direct antineoplastic agent.
Astaxanthin significantly promotes the proliferation of Akkermansia, a microorganism with enhanced anti-tumor immune effects.
Anti-inflammatory signaling, Astaxanthin can inhibit: NF-κB, COX-2, iNOS
Astaxanthin commonly Activates NRF2: Upregulates antioxidant enzymes (GSH, SOD, CAT, GPX)
-Protective in normal tissues
-Potentially tumor-protective in established cancers

Often discouraged during active chemotherapy or radiation
It may:
-Protect tumor cells from ROS-mediated killing
-Reduce lipid peroxidation-based therapies
This concern is similar to:
-Vitamin E
-Trolox
-High-dose carotenoids

Astaxanthin is less likely to be pro-oxidant than lycopene or β-carotene.
Some reports indicate a pro-oxidant effect, but at concentrations that are not achievable for in vito.

Astaxanthin — mechanistic pathway map (cancer-context)

Rank Pathway / Axis Cancer Cells Normal Cells TSF Primary Effect Notes / Interpretation
1 NRF2 antioxidant response ↑ NRF2 (context-dependent) → ↓ ROS injury; may blunt ROS-lethal therapies ↑ NRF2 → ↑ GSH/SOD/CAT/GPx; cytoprotection R/G Redox buffering and stress tolerance Often positioned as protective; in established tumors this can be tumor-supportive depending on therapy and redox state.
2 NF-κB inflammatory signaling ↓ NF-κB → ↓ pro-survival inflammation (model-dependent) ↓ inflammatory cytokine signaling R/G Anti-inflammatory microenvironment shift Commonly linked to ↓ COX-2/iNOS and reduced inflammatory tone.
3 PI3K–AKT survival signaling ↓ PI3K/AKT (model-dependent) → ↑ apoptosis, ↓ proliferation ↔ / mild cytoprotective bias (context-dependent) R/G Survival pathway suppression in select tumors Directionality is model- and dose-dependent; some datasets show mixed AKT effects.
4 ERK/MAPK signaling ↓ ERK/MAPK (model-dependent) → ↓ proliferation/EMT ↔ / ↓ stress-activated signaling (context-dependent) R/G Anti-growth signaling modulation Often reported alongside PI3K/AKT changes; may converge on apoptosis/cell-cycle effects.
5 STAT3 axis ↓ STAT3 → ↓ proliferation, ↓ immune-evasion programs (model-dependent) G Reduced oncogenic transcription signaling Reported in prostate and other models; typically framed as anti-tumor signaling.
6 Mitochondria-mediated apoptosis ↑ intrinsic apoptosis (BAX↑, Bcl-2↓, caspases↑; model-dependent) ↓ stress-induced apoptosis (cytoprotection) R Cell death modulation Key “anti-tumor” readout in many studies; may require higher concentrations than typical systemic exposure.
7 Cell cycle control ↑ p21/p27 and/or arrest signatures (model-dependent) G Proliferation braking Often co-occurs with apoptosis; direction varies with cell line and dosing.
8 EMT and matrix remodeling ↓ EMT; ↓ MMPs; ↑ E-cadherin (model-dependent) G Anti-migration / anti-metastatic phenotype Reported via miRNA and cadherin/MMP changes in some colon/breast models.
9 Angiogenesis signaling ↓ VEGF/EGFR signaling (limited, model-dependent) G Reduced pro-angiogenic drive Less consistently central than NRF2/NF-κB/PI3K–AKT in the literature.
10 Ferroptosis and lipid peroxidation balance ↔ / ↑ ferroptosis (limited models) but also ↓ lipid peroxidation (context-dependent) ↓ lipid peroxidation injury R Redox-lethal interaction or protection (context-dependent) Net effect depends strongly on baseline oxidative state and whether therapy relies on lipid peroxidation.
11 Clinical Translation Constraint Low/variable oral exposure; many in-vitro effects are high-concentration. Antioxidant/NRF2 biology raises a plausible antagonism risk for ROS-dependent chemo/radiation (context-dependent). Formulation and dosing strategy strongly influence exposure. Translational ceiling Best-supported human domain is oxidative stress/inflammation biomarkers rather than anticancer efficacy endpoints.

TSF legend: P: 0–30 min    R: 30 min–3 hr    G: >3 hr
TumCI, Tumor Cell invasion: Click to Expand ⟱
Source:
Type:
Tumor cell invasion is a critical process in cancer progression and metastasis, where cancer cells spread from the primary tumor to surrounding tissues and distant organs. This process involves several key steps and mechanisms:

1.Epithelial-Mesenchymal Transition (EMT): Many tumors originate from epithelial cells, which are typically organized in layers. During EMT, these cells lose their epithelial characteristics (such as cell-cell adhesion) and gain mesenchymal traits (such as increased motility). This transition is crucial for invasion.

2.Degradation of Extracellular Matrix (ECM): Tumor cells secrete enzymes, such as matrix metalloproteinases (MMPs), that degrade the ECM, allowing cancer cells to invade surrounding tissues. This degradation facilitates the movement of cancer cells through the tissue.

3.Cell Migration: Once the ECM is degraded, cancer cells can migrate. They often use various mechanisms, including amoeboid movement and mesenchymal migration, to move through the tissue. This migration is influenced by various signaling pathways and the tumor microenvironment.

4.Angiogenesis: As tumors grow, they require a blood supply to provide nutrients and oxygen. Tumor cells can stimulate the formation of new blood vessels (angiogenesis) through the release of growth factors like vascular endothelial growth factor (VEGF). This not only supports tumor growth but also provides a route for cancer cells to enter the bloodstream.

5.Invasion into Blood Vessels (Intravasation): Cancer cells can invade nearby blood vessels, allowing them to enter the circulatory system. This step is crucial for metastasis, as it enables cancer cells to travel to distant sites in the body.

6.Survival in Circulation: Once in the bloodstream, cancer cells must survive the immune response and the shear stress of blood flow. They can form clusters with platelets or other cells to evade detection.

7.Extravasation and Colonization: After traveling through the bloodstream, cancer cells can exit the circulation (extravasation) and invade new tissues. They may then establish secondary tumors (metastases) in distant organs.

8.Tumor Microenvironment: The surrounding microenvironment plays a significant role in tumor invasion. Factors such as immune cells, fibroblasts, and signaling molecules can either promote or inhibit invasion and metastasis.
Scientific Papers found: Click to Expand⟱
4820- ASTX,    Astaxanthin suppresses the malignant behaviors of nasopharyngeal carcinoma cells by blocking PI3K/AKT and NF-κB pathways via miR-29a-3p
- in-vitro, NPC, NA
TumCP↓, TumCI↓, Apoptosis↑, TumCCA↑, cycD1/CCND1↓, Bcl-2↓, P21↑, BAX↑, PI3K↓, Akt↓, NF-kB↓, miR-29b↑,
4808- ASTX,    Anti-Tumor Effects of Astaxanthin by Inhibition of the Expression of STAT3 in Prostate Cancer
- in-vitro, Pca, DU145 - in-vivo, NA, NA
TumCP↓, STAT3↓, Apoptosis↑, TumCMig↓, TumCI↓,

Showing Research Papers: 1 to 2 of 2

* indicates research on normal cells as opposed to diseased cells
Total Research Paper Matches: 2

Pathway results for Effect on Cancer / Diseased Cells:


Cell Death

Akt↓, 1,   Apoptosis↑, 2,   BAX↑, 1,   Bcl-2↓, 1,  

Cell Cycle & Senescence

cycD1/CCND1↓, 1,   P21↑, 1,   TumCCA↑, 1,  

Proliferation, Differentiation & Cell State

PI3K↓, 1,   STAT3↓, 1,  

Migration

miR-29b↑, 1,   TumCI↓, 2,   TumCMig↓, 1,   TumCP↓, 2,  

Immune & Inflammatory Signaling

NF-kB↓, 1,  
Total Targets: 14

Pathway results for Effect on Normal Cells:


Total Targets: 0

Scientific Paper Hit Count for: TumCI, Tumor Cell invasion
Query results interpretion may depend on "conditions" listed in the research papers.
Such Conditions may include : 
  -low or high Dose
  -format for product, such as nano of lipid formations
  -different cell line effects
  -synergies with other products 
  -if effect was for normal or cancerous cells

Filter Conditions: Pro/AntiFlg:%  IllCat:%  CanType:%  Cells:%  prod#:382  Target#:324  State#:%  Dir#:1
  wNotes=0  sortOrder:rid,rpid

 

Home Page