Copper and Cu NanoParticles / Catalase Cancer Research Results

Cu, Copper and Cu NanoParticles: Click to Expand ⟱

Features:

Copper
Metal
Copper levels are considerably elevated in various malignancies.
Copper [Cu(II)] is a transition and trace element in living organisms. It increases reactive oxygen species (ROS) and free-radical generation that might damage biomolecules like DNA, proteins, and lipids.

Copper (dietary/physiology) ≠ copper-loading therapeutics ≠ copper nanoparticles.
For Cu nanoparticles, the dominant and most reproducible theme is toxicity via ROS → mitochondrial damage/genotoxicity, not clean tumor selectivity.
- Copper acts as a critical cofactor for numerous enzymes involved in redox reactions, energy production, and connective tissue formation.
- Increased copper levels in the tumor microenvironment can enhance angiogenic signaling and thus supply the tumor with necessary oxygen and nutrients, facilitating tumor growth and metastasis.
- Copper can participate in redox cycling reactions, similar to the Fenton reaction, leading to the production of reactive oxygen species (ROS).
- Cancer cells often exhibit altered copper homeostasis, with some studies showing elevated copper levels in tumor tissues relative to normal tissues.

Two main approaches are:
- Copper Chelation: Drugs that bind copper (chelators) can reduce the bioavailability of copper, potentially inhibiting angiogenesis and other copper-dependent tumor processes.
- Copper Ionophores: These agents facilitate the transport of copper into cancer cells to induce cytotoxicity by elevating intracellular copper levels beyond a tolerable threshold, leading to cell death.

- Depletion of glutathione and stimulation of lipid peroxidation, catalase and superoxide dismutase.
- Studies have shown that the level of copper in tumour cells and blood serum from cancer patients is elevated, and the conclusion is that cancer cells need more copper than healthy cells. (but also sometimes depleted).
- Copper is a double-edged sword, maintaining normal cell development and promoting tumor development.
- Tumor tissue has a higher demand for copper and is more susceptible to copper homeostasis, copper may modulate cancer cell survival through reactive oxygen species (ROS) excessive accumulation, proteasome inhibition and anti-angiogenesis.

Natural Product: Cu, Copper (ion biology)

Rank	Pathway / Axis	Cancer / Tumor Context	Normal Tissue Context	TSF	Primary Effect	Notes / Interpretation
1	Cuproptosis (copper-triggered mitochondrial cell death)	Cu accumulation → binding to lipoylated TCA proteins → aggregation; Fe–S proteins ↓; proteotoxic stress ↑	Tight copper homeostasis usually prevents this	R, G	Regulated cell death (mitochondria-linked)	Cuproptosis is a distinct copper-dependent death pathway tied to mitochondrial metabolism and lipoylated TCA components. :contentReference[oaicite:0]{index=0}
2	Copper homeostasis machinery (transport/chaperones)	Copper trafficking affects tumor programs (growth/metastasis; context)	Essential micronutrient; homeostasis prevents toxicity	R, G	Homeostasis / signaling coupling	Copper import/export and chaperones couple copper availability to signaling and phenotype; dysregulation is increasingly discussed in cancer biology. :contentReference[oaicite:1]{index=1}
3	Angiogenesis support (copper-dependent tumor vascularization)	Pro-angiogenic tone supported by copper availability (context)	Physiologic angiogenesis/wound repair support	G	Vascular program modulation	Copper deficiency/chelation has been reported to impair tumor angiogenesis in preclinical/clinical contexts. :contentReference[oaicite:2]{index=2}
4	LOX/LOXL family (ECM remodeling; copper-dependent enzymes)	ECM crosslinking / invasion-metastasis programs ↑ (context)	Normal ECM maturation and tissue repair	G	Microenvironment remodeling	LOX enzymes are copper-dependent and implicated in tumor stroma remodeling and metastatic niche biology. :contentReference[oaicite:3]{index=3}
5	ROS / redox chemistry (Cu redox cycling)	Oxidative stress ↑ (context); DNA/protein damage ↑	Redox enzyme cofactor; excess is toxic	P, R, G	Stress amplification (conditional)	Copper can catalyze redox reactions; whether this is tumor-selective depends on copper handling, antioxidants, and exposure context.
6	Copper ionophores / copper-loading strategies (research/therapy concept)	Intracellular Cu ↑ → stress/death programs ↑ (context)	—	R, G	Therapeutic lever (conceptual)	Reviews discuss copper ionophores as tools to drive copper accumulation and explore cuproptosis/ROS mechanisms; clinical positioning varies. :contentReference[oaicite:4]{index=4}
7	Copper chelation (anti-angiogenic / microenvironment strategy)	Angiogenesis and tumor progression pressure ↓ (context)	Risk of deficiency if excessive	G	Translation/strategy axis	Tetrathiomolybdate and related chelation strategies have been studied clinically as anti-angiogenic approaches. :contentReference[oaicite:5]{index=5}

Time-Scale Flag (TSF): P / R / G

P: 0–30 min (rapid redox interactions)
R: 30 min–3 hr (acute mitochondrial/proteotoxic stress signaling)
G: >3 hr (gene-regulatory adaptation and phenotype outcomes)

Copper Nanoparticles: CuNP / CuO-NP (tox + “anticancer” claims are mostly preclinical)

Rank	Axis	Cell/Tumor Context	Whole-Body / Normal Tissue Context	TSF	Primary Effect	Notes / Interpretation
1	Oxidative stress (ROS generation) + antioxidant depletion	ROS ↑; lipid peroxidation ↑; DNA damage ↑ (reported)	Liver/kidney oxidative injury risk ↑ in animal studies	P, R, G	Primary toxicity driver	CuO nanoparticles are widely reported to cause cytotoxicity primarily via oxidative stress leading to genotoxicity. :contentReference[oaicite:6]{index=6}
2	Mitochondrial dysfunction	ΔΨm ↓; ATP ↓; apoptosis signaling ↑ (reported)	Organ toxicity links include mitochondrial impairment	R, G	Energy failure / apoptosis coupling	Mitochondria-mediated apoptosis has been reported with CuO NPs in cell models (e.g., HepG2). :contentReference[oaicite:7]{index=7}
3	Inflammation / immune activation	Inflammatory signaling ↑ (context)	Inflammation contributes to organ injury in vivo	R, G	Tissue injury amplification	Sub-chronic exposure reviews describe inflammation as part of CuNP/CuO-NP toxicity patterns. :contentReference[oaicite:8]{index=8}
4	Genotoxicity	DNA strand breaks ↑; chromosomal damage ↑ (reported)	Potential long-term risk signal (model-dependent)	R, G	Genome damage	Often downstream of ROS; repeatedly reported across CuO NP toxicity literature. :contentReference[oaicite:9]{index=9}
5	“Anticancer” cytotoxicity claims (preclinical)	Viability ↓ in various cell lines (often at high concentrations)	Translation limited by toxicity and exposure constraints	G	Non-selective cytotoxicity risk	Many studies show tumor cell killing, but often at concentrations that also harm normal cells; selectivity is a major issue. :contentReference[oaicite:10]{index=10}
6	Reproductive/developmental toxicity signals (animal models)	—	Reported reproductive system impacts in animal studies	G	Safety constraint	Recent studies discuss reproductive toxicity and mitochondrial injury in germline cells with CuO NPs. :contentReference[oaicite:11]{index=11}

Time-Scale Flag (TSF): P / R / G

P: 0–30 min (rapid ROS/redox interactions at particle surfaces)
R: 30 min–3 hr (mitochondrial stress + inflammatory signaling)
G: >3 hr (genotoxicity, apoptosis, organ-level outcomes)

Catalase, Catalase: Click to Expand ⟱

Source:

Type:

Caspases are a cysteine protease that speed up a chemical reaction via pointing their target substrates following an aspartic acid residue.1 They are grouped into apoptotic (caspase-2, 3, 6, 7, 8, 9 and 10) and inflammatory (caspase-1, 4, 5, 11 and 12) mediated caspases.
Caspase-1 may have both tumorigenic or antitumorigenic effects on cancer development and progression, but it depends on the type of inflammasome, methodology, and cancer.
Catalase is an enzyme found in nearly all living cells exposed to oxygen. Its primary role is to protect cells from oxidative damage by catalyzing the conversion of hydrogen peroxide (H₂O₂), a potentially damaging byproduct of metabolism, into water (H₂O) and oxygen (O₂). This detoxification process is crucial because excess H₂O₂ can lead to the formation of reactive oxygen species (ROS) that damage proteins, lipids, and DNA.

Catalase and Cancer
Oxidative Stress and Cancer:
Cancer cells often experience increased levels of oxidative stress due to rapid proliferation and metabolic changes. This stress can lead to DNA damage, promoting tumorigenesis.
Catalase helps mitigate oxidative stress, and its expression can influence the survival and proliferation of cancer cells.
Expression Levels in Different Cancers:
Overexpression: In some cancers, such as breast cancer and certain types of leukemia, catalase may be overexpressed. This overexpression can help cancer cells survive in oxidative environments, potentially leading to more aggressive tumor behavior.
Downregulation: Conversely, in other cancers, such as colorectal cancer, reduced catalase expression has been observed. This downregulation can lead to increased oxidative stress, contributing to tumor progression and metastasis.
Prognostic Implications:
Survival Rates: Studies have shown that high levels of catalase expression can be associated with poor prognosis in certain cancers, as it may enable cancer cells to resist apoptosis (programmed cell death) induced by oxidative stress.

Some types of cancer cells have been reported to exhibit lower catalase activity, possibly increasing their vulnerability to oxidative damage under certain conditions. This vulnerability has even been exploited in some therapeutic strategies (for example, approaches that generate excess H₂O₂ or other ROS specifically targeting cancer cells have been researched).

Scientific Papers found: Click to Expand⟱

1570-

Cu,

Development of copper nanoparticles and their prospective uses as antioxidants, antimicrobials, anticancer agents in the pharmaceutical sector

Review,

NA,

selectivity↑, antiOx↑, ROS↑, eff↑, GSH↓, lipid-P↑, Catalase↓, SOD↓, other↑,

Showing Research Papers: 1 to 1 of 1

* indicates research on normal cells as opposed to diseased cells
Total Research Paper Matches: 1

Pathway results for Effect on Cancer / Diseased Cells:

Redox & Oxidative Stress ⓘ

antiOx↑, 1, Catalase↓, 1, GSH↓, 1, lipid-P↑, 1, ROS↑, 1, SOD↓, 1,

Transcription & Epigenetics ⓘ

other↑, 1,

Drug Metabolism & Resistance ⓘ

eff↑, 1, selectivity↑, 1,
Total Targets: 9

Pathway results for Effect on Normal Cells:

Total Targets: 0

Scientific Paper Hit Count for: Catalase, Catalase

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