Quick Comparison
| Emoxypine (Mexidol) | Piracetam | |
|---|---|---|
| Half-Life | 2-2.6 hours | 4-5 hours |
| Typical Dosage | Standard: 125-375 mg daily in 2-3 divided doses. Commonly 125 mg twice daily. Take with food. Effects are noticeable within 30-60 minutes. Russian clinical practice uses 4-6 week courses. | Standard: 1200-4800 mg daily in 2-3 divided doses. Clinical studies commonly use 2400-4800 mg daily. The 'attack dose' protocol uses 4800 mg daily for the first week, then reduces to maintenance. |
| Administration | Oral (tablets). Also available as IV/IM injection in clinical settings. Mexidol is the brand name. | Oral (powder, capsules, tablets). Highly bioavailable orally with nearly 100% absorption. |
| Research Papers | 10 papers | 10 papers |
| Categories |
Mechanism of Action
Emoxypine (Mexidol)
Emoxypine (2-ethyl-6-methyl-3-hydroxypyridine succinate) has a 3-hydroxypyridine structure similar to vitamin B6 (pyridoxine). It is one of the most potent inhibitors of lipid peroxidation in brain tissue — it scavenges hydroxyl radicals and peroxyl radicals, inhibits Fe2+-induced lipid peroxidation, and may chelate transition metals. It modulates the GABA-benzodiazepine receptor complex (GABA-A), enhancing GABAergic transmission through positive allosteric modulation — possibly at a site distinct from the classical benzodiazepine binding site, explaining the lack of sedation and tolerance. It improves mitochondrial function (Complex I protection, membrane stabilization), stabilizes cell membranes (reducing fluidity changes during oxidative stress), and enhances cerebral microcirculation (possibly via nitric oxide or prostaglandin modulation). The anxiolytic mechanism may involve partial agonism or different subunit selectivity.
Piracetam
Piracetam modulates AMPA (α-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid) and NMDA (N-methyl-D-aspartate) glutamate receptors through positive allosteric modulation, enhancing excitatory neurotransmission without direct agonism. It increases membrane fluidity of neuronal phospholipid bilayers by reducing membrane microviscosity, which improves ion channel function and signal transmission. Piracetam enhances acetylcholine receptor density and turnover in the hippocampus, upregulating both muscarinic (M1) and nicotinic receptor expression. It potentiates the cholinergic system through increased high-affinity choline uptake. Additionally, piracetam improves cerebral blood flow via nitric oxide-dependent vasodilation and enhances oxygen utilization (glucose metabolism) in aged or hypoxic brain tissue, supporting mitochondrial function.
Risks & Safety
Emoxypine (Mexidol)
Common
Mild nausea, drowsiness, dry mouth.
Serious
Limited Western safety data. Allergic reactions reported.
Rare
Elevated blood pressure, emotional lability.
Piracetam
Common
Headache (often from insufficient choline intake), insomnia if taken late in the day, gastrointestinal discomfort.
Serious
Very rare — piracetam has an extremely favorable safety profile. May increase the effects of blood thinners.
Rare
Nervousness, agitation, weight gain.
Full Profiles
Emoxypine (Mexidol) →
A vitamin B6 derivative with powerful antioxidant and anxiolytic properties, widely prescribed in Russia and Eastern Europe for anxiety, cognitive impairment, and cerebrovascular disease. Emoxypine inhibits lipid peroxidation, modulates GABA-A and benzodiazepine binding sites, and improves cerebral blood flow. It provides anxiolytic effects similar to benzodiazepines without sedation, tolerance, or addiction.
Piracetam →
The original nootropic, synthesized in 1964 by Corneliu Giurgea who coined the term 'nootropic.' Piracetam modulates glutamate and acetylcholine neurotransmission to enhance memory, learning, and cognitive fluidity. Widely prescribed in Europe for cognitive decline and used globally as a cognitive enhancer. One of the most studied nootropics with decades of clinical data.