Copper (as Copper Bisglycinate) vs Molybdenum

Side-by-side comparison of mechanisms, dosing, interactions, and stacking potential.

✅ Stacking Partners — These compounds are commonly used together and may have synergistic effects.

⚠️ Known Interaction

MEDIUM High molybdenum (>500 mcg) can induce copper deficiency by forming insoluble copper-thiomolybdate complexes

	Copper (as Copper Bisglycinate)	Molybdenum
Category	Minerals	Minerals
Standard Dose	1-2mg elemental copper daily (when supplementing zinc >25mg)	75-250 mcg daily
Timing	With food. Separate from zinc by 2+ hours for optimal absorption of both.	With meals. Often included in multimineral formulas.
Cycle Duration	ongoing when zinc supplementation is ongoing	ongoing (via multimineral)
Evidence Level	strong_human	moderate_human

Copper (as Copper Bisglycinate)

Minerals

Mechanism

Copper is a cofactor for critical cuproenzymes: cytochrome c oxidase (Complex IV, mitochondrial respiration), Cu/Zn-SOD (superoxide dismutation), ceruloplasmin (ferroxidase — converts Fe2+ to Fe3+ for transferrin loading; essential for iron metabolism), lysyl oxidase (collagen and elastin cross-linking), dopamine beta-hydroxylase (dopamine to norepinephrine conversion), tyrosinase (melanin synthesis), and peptidyl-glycine alpha-amidating monooxygenase (neuropeptide processing). Copper is transported by ATP7A/B (Menkes/Wilson proteins) and regulated by metallothionein and glutathione.

Standard Dosing

1-2mg elemental copper daily (when supplementing zinc >25mg)

Timing

With food. Separate from zinc by 2+ hours for optimal absorption of both.

Cycle Duration

ongoing when zinc supplementation is ongoing

Side Effects

Nausea (on empty stomach)
GI upset
Metallic taste
Copper toxicity at high doses (hepatotoxicity, hemolytic anemia)

Contraindications

Wilson's disease (genetic copper overload)
Copper storage disorders
Copper excess states

Best Stacking Partners

Zinc (1:15 Cu:Zn ratio)Vitamin C (low dose — high-dose C reduces Cu absorption)Iron

Molybdenum

Minerals

Mechanism

Molybdenum is the essential cofactor for three human enzymes: sulfite oxidase (converts toxic sulfite to sulfate — critical for sulfur amino acid metabolism), xanthine oxidase (purine catabolism to uric acid), and aldehyde oxidase (aldehyde detoxification, drug metabolism). The molybdenum cofactor (Moco) requires molybdopterin as a carrier. Sulfite oxidase is the most clinically significant — sulfite accumulation is neurotoxic. Molybdenum also plays a role in the metabolism of sulfur-containing amino acids and may support phase I/II detoxification pathways.

Standard Dosing

75-250 mcg daily

Timing

With meals. Often included in multimineral formulas.

Cycle Duration

ongoing (via multimineral)

Side Effects

Generally very well tolerated
Gout flares at high doses (increased uric acid production)
Copper depletion at very high doses
Joint pain (rare)

Contraindications

Gout (xanthine oxidase is the uric acid-producing enzyme — molybdenum supports this enzyme)
Copper deficiency

Best Stacking Partners

B-ComplexNACCopper (molybdenum can reduce copper)

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Copper (as Copper Bisglycinate)

Mechanism

Standard Dosing

Timing

Cycle Duration

Side Effects

Contraindications

Best Stacking Partners

Molybdenum

Mechanism

Standard Dosing

Timing

Cycle Duration

Side Effects

Contraindications

Best Stacking Partners

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