Mexicor® (Capsules, Solution) Instructions for Use
ATC Codes
C01EB (Other cardiac preparations)
N07XX (Other nervous system drugs)
Active Substance
Ethylmethylhydroxypyridine succinate (Grouping name)
Clinical-Pharmacological Group
Antioxidant drug
Pharmacotherapeutic Group
Antioxidant agent
Pharmacological Action
An inhibitor of free radical processes – a membrane protector that also has antihypoxic, stress-protective, nootropic, antiepileptic, and anxiolytic effects. It belongs to the class of 3-oxypyridines.
The mechanism of action is due to its antioxidant and membrane-protective properties. It suppresses lipid peroxidation, increases superoxide dismutase activity, improves the lipid-protein ratio, and enhances the structure and function of cell membranes.
It modulates the activity of membrane-bound enzymes (Ca2+-independent PDE, adenylate cyclase, acetylcholinesterase) and receptor complexes (benzodiazepine, GABA, acetylcholine), which promotes their binding to ligands, preserves the structural and functional organization of biomembranes, neurotransmitter transport, and improves synaptic transmission. It increases the concentration of dopamine in the brain.
It enhances the compensatory activation of aerobic glycolysis and reduces the degree of inhibition of oxidative processes in the Krebs cycle under hypoxic conditions, with an increase in ATP and creatine phosphate, and activates the energy-synthesizing function of mitochondria.
It increases the body’s resistance to the effects of various damaging factors in pathological conditions (shock, hypoxia and ischemia, cerebrovascular accidents, ethanol intoxication, and antipsychotic drug intoxication).
It improves the metabolism and blood supply of the brain, microcirculation and rheological properties of blood, and reduces platelet aggregation. It stabilizes the membranes of blood cells (erythrocytes and platelets), reducing the likelihood of hemolysis.
It has a hypolipidemic effect, reducing the content of total cholesterol and LDL.
It improves the functional state of the ischemic myocardium in myocardial infarction, the contractile function of the heart, and also reduces the manifestations of systolic and diastolic dysfunction of the left ventricle.
Under conditions of a critical decrease in coronary blood flow, it helps preserve the structural and functional organization of cardiomyocyte membranes, stimulates the activity of membrane enzymes – PDE, adenylate cyclase, acetylcholinesterase.
It maintains the activation of aerobic glycolysis that develops during acute ischemia and promotes the restoration of mitochondrial redox processes under hypoxic conditions, increasing the synthesis of ATP and creatine phosphate. It ensures the integrity of the morphological structures and physiological functions of the ischemic myocardium.
It improves the clinical course of myocardial infarction, increases the effectiveness of the therapy, accelerates the recovery of the functional activity of the left ventricular myocardium, and reduces the frequency of arrhythmias and intracardiac conduction disturbances.
It normalizes metabolic processes in the ischemic myocardium, reduces the area of necrosis, restores and/or improves the electrical activity and contractility of the myocardium, increases coronary blood flow in the ischemic area, enhances the antianginal activity of nitro drugs, improves the rheological properties of blood, and reduces the consequences of reperfusion syndrome in acute coronary insufficiency.
It reduces enzymatic toxemia and endogenous intoxication in acute pancreatitis.
Pharmacokinetics
It is rapidly absorbed after oral administration (half-absorption period – 0.08-1 h). Tmax after IM administration – 0.3-0.58 h, after oral administration – 0.46-0.5 h. Cmax after IM administration at a dose of 400-500 mg – 2.5-4 µg/ml, after oral administration – 50-100 ng/ml.
It is rapidly distributed in organs and tissues. The mean residence time of the drug in the body after IM administration is 0.7-1.3 h, after oral administration – 4.9-5.2 h.
It is metabolized in the liver by glucuronidation. Five metabolites have been identified: 3-oxypyridine phosphate – formed in the liver and, with the participation of alkaline phosphatase, breaks down into phosphoric acid and 3-oxypyridine; the 2nd metabolite is pharmacologically active, formed in large quantities and detected in urine 1-2 days after administration; the 3rd is excreted in large quantities in the urine; the 4th and 5th are glucuronide conjugates.
T1/2 after oral administration – 4.7-5 h. It is rapidly excreted in the urine mainly as metabolites (50% within 12 h) and in small amounts – unchanged (0.3% within 12 h). It is most intensively excreted within the first 4 hours after taking the drug. The excretion parameters of the unchanged drug and metabolites in the urine have significant individual variability.
Indications
Anxiety disorders in neurotic and neurosis-like conditions; vegetative-vascular dystonia; dyscirculatory encephalopathy; mild cognitive disorders of atherosclerotic origin.
Acute cerebrovascular accidents (as part of combination therapy).
Withdrawal syndrome in alcoholism with a predominance of neurosis-like and vegetative-vascular disorders; acute intoxication with antipsychotic drugs.
Acute purulent-inflammatory processes in the abdominal cavity (including acute necrotizing pancreatitis, peritonitis (as part of complex therapy));
Acute myocardial infarction from the first days (parenterally); Coronary artery disease; complex therapy of ischemic stroke (orally) – as part of complex therapy.
ICD codes
| ICD-10 code | Indication |
| F07 | Personality and behavioral disorders due to disease, damage or dysfunction of the brain |
| F10.3 | Withdrawal state |
| F45.3 | Somatoform dysfunction of the autonomic nervous system |
| F48.0 | Neurasthenia |
| F48.9 | Unspecified neurotic disorder |
| G93.4 | Unspecified encephalopathy |
| I20 | Angina pectoris |
| I21 | Acute myocardial infarction |
| I61 | Intracerebral hemorrhage (cerebrovascular accident of hemorrhagic type) |
| I63 | Cerebral infarction |
| I67.2 | Cerebral atherosclerosis |
| K65.0 | Acute peritonitis (including abscess) |
| K85 | Acute pancreatitis |
| T43 | Poisoning by psychotropic drugs, not elsewhere classified |
| ICD-11 code | Indication |
| 6A8Z | Affective disorders, unspecified |
| 6B6Z | Dissociative disorders, unspecified |
| 6C20.Z | Bodily distress disorder, unspecified |
| 6C40.4Z | Alcohol withdrawal syndrome, unspecified |
| 6E68 | Secondary emotionally labile personality disorder |
| 6E6Z | Unspecified secondary mental or behavioral syndromes |
| 8B00.Z | Intracerebral hemorrhage of unspecified site, unspecified |
| 8B11 | Cerebral ischemic stroke |
| 8E47 | Encephalopathy, not elsewhere classified |
| 8E4A.0 | Paraneoplastic or autoimmune disorders of the central nervous system, including brain and spinal cord |
| 8E63 | Post-cardiopulmonary bypass encephalopathy |
| BA40.Z | Angina pectoris, unspecified |
| BA41.Z | Acute myocardial infarction, unspecified |
| BD55 | Asymptomatic stenosis of intracranial or extracranial artery |
| DC31.Z | Acute pancreatitis, unspecified |
| DC50.0 | Primary peritonitis |
| DC50.2 | Peritoneal abscess |
| DC50.Z | Peritonitis, unspecified |
| NE60 | Poisoning by drugs, medicaments or biological substances, not elsewhere classified |
Dosage Regimen
| The method of application and dosage regimen for a specific drug depend on its form of release and other factors. The optimal dosage regimen is determined by the doctor. It is necessary to strictly adhere to the compliance of the dosage form of a specific drug with the indications for use and dosage regimen. |
Determine the dose, route of administration, and treatment duration individually based on the specific indication and clinical presentation.
For oral administration, administer a total daily dose of 250-500 mg. Divide this dose into two or three separate administrations. Do not exceed the maximum daily dose of 600-800 mg.
For parenteral administration (intramuscular or intravenous), administer a single dose of 50-400 mg. The maximum daily dose for parenteral use is 1200 mg.
For intravenous bolus injection, administer the dose slowly over several minutes to avoid adverse reactions such as taste disturbances or throat discomfort.
For intravenous drip infusion, dilute the required dose in an appropriate volume of infusion solution.
In acute myocardial infarction, initiate therapy with parenteral administration from the first day.
For cerebrovascular accidents and acute pancreatitis, use the drug as part of a combination therapy regimen.
For anxiety disorders and withdrawal syndrome, the oral route is typically indicated. Adjust the dose based on the severity of symptoms.
The standard course of treatment lasts from two to six weeks, depending on the condition being treated and the patient’s response. Repeat courses are possible after a break, as determined by the physician.
Adverse Reactions
When taken orally nausea, dry mouth, diarrhea, drowsiness, allergic reactions.
With parenteral administration (especially IV bolus) dryness, “metallic” taste in the mouth, sensations of “spreading warmth” throughout the body, unpleasant odor, sore throat and discomfort in the chest, feeling of lack of air (usually associated with an excessively high rate of administration and are short-term in nature); with prolonged use – nausea, flatulence; sleep disorders (drowsiness or difficulty falling asleep).
Contraindications
Hypersensitivity; acute hepatic and/or renal failure; pregnancy; lactation period; childhood.
Use in Pregnancy and Lactation
Contraindicated for use during pregnancy and breastfeeding.
Use in Hepatic Impairment
Contraindication: acute hepatic failure.
Use in Renal Impairment
Contraindication: acute renal failure.
Pediatric Use
The drug is contraindicated for use in children and adolescents under 18 years of age.
Special Precautions
Use with caution in patients with a history of allergic diseases.
During treatment, caution should be exercised when driving vehicles and engaging in other potentially hazardous activities that require increased concentration and speed of psychomotor reactions.
Drug Interactions
It enhances the effect of benzodiazepine anxiolytics, antiepileptic (carbamazepine), antiparkinsonian (levodopa) drugs, and nitrates.
It reduces the toxic effects of ethanol.
Storage Conditions
Store at 2°C (36°F) to 25°C (77°F). Keep in original packaging, protected from light. Keep out of reach of children.
Dispensing Status
Rx Only
Important Safety Information
This information is for educational purposes only and does not replace professional medical advice. Always consult your doctor before use. Dosage and side effects may vary. Use only as prescribed.
Medical DisclaimerBrand (or Active Substance), Marketing Authorisation Holder, Dosage Form
Capsules 100 mg: 20, 30 or 60 pcs.
Marketing Authorization Holder
EcoPharmInvest, LLC (Russia)
Manufactured By
MiraxBioPharma JSC (Russia)
Or
AVZ S-P. LLC (Russia)
Dosage Form
 |
Mexicor® | Capsules 100 mg: 20, 30 or 60 pcs. |
Dosage Form, Packaging, and Composition
Capsules hard gelatin, size No. 2, yellow; the contents of the capsules are a granulate containing granules and powder of white or white with a yellowish tint.
| 1 caps. | |
| Ethylmethylhydroxypyridine succinate | 100 mg |
Excipients : potato starch – 54.5 mg, lactose (milk sugar) – 40 mg, povidone K17 (low molecular weight medical polyvinylpyrrolidone) – 4 mg, microcrystalline cellulose – 1 mg, magnesium stearate – 0.5 mg; hard gelatin capsules No. 2 (gelatin – up to 100%, purified water – 14-15%, titanium dioxide (E171) – 1.22 mg, dye sunset yellow (E110) – 0.0036 mg, dye quinoline yellow (E104) – 0.4575 mg).
10 pcs. – blister packs (2) – cardboard packs.
10 pcs. – blister packs (3) – cardboard packs.
10 pcs. – blister packs (6) – cardboard packs.
Solution for intravenous and intramuscular administration 50 mg/1 ml: 2 ml ampoules, 10 pcs.; 5 ml ampoules, 5, 10, or 20 pcs.
Marketing Authorization Holder
EcoPharmInvest, LLC (Russia)
Manufactured By
Ferment Firm, LLC (Russia)
Or
State Institute of Medical and Biological Problems, FSUE (Russia)
Or
RKNPC MZ RF – EPMBP FSBI (Russia)
Dosage Form
|
Mexicor® | Solution for intravenous and intramuscular administration 50 mg/1 ml: 2 ml ampoules, 10 pcs.; 5 ml ampoules, 5, 10, or 20 pcs. |
Dosage Form, Packaging, and Composition
Solution for IV and IM administration transparent, colorless or slightly colored.
| 1 ml | |
| Ethylmethylhydroxypyridine succinate | 50 mg |
Excipients : succinic acid – 5 mg, disodium edetate – 0.1 mg, water for injection – up to 1 ml.
2 ml – dark glass ampoules (5) – blister packs (2) – cardboard packs.
5 ml – dark glass ampoules (5) – blister packs (1) – cardboard packs.
5 ml – dark glass ampoules (5) – blister packs (2) – cardboard packs.
5 ml – dark glass ampoules (5) – blister packs (4) – cardboard packs.
Capsules 100 mg: 20, 30 or 60 pcs.
Marketing Authorization Holder
EcoPharmInvest, LLC (Russia)
Manufactured By
N.A. Semashko Moscow Chemical Pharmaceutical Preparations, JSC (Russia)
Dosage Form
|
Mexicor® | Capsules 100 mg: 20, 30 or 60 pcs. |
Dosage Form, Packaging, and Composition
Capsules hard gelatin, size No. 2, yellow; the contents of the capsules are a granulate containing granules and powder of white or white with a yellowish tint.
| 1 caps. | |
| Ethylmethylhydroxypyridine succinate | 100 mg |
Excipients : potato starch – 54.5 mg, povidone (low molecular weight medical polyvinylpyrrolidone 12600±2700) – 4 mg, lactose (milk sugar) – 40 mg, magnesium stearate – 0.5 mg, microcrystalline cellulose – 1 mg.
Composition of hard gelatin capsule No. 2 gelatin – 59.3189 mg, titanium dioxide (E171) – 1.22 mg, dye sunset yellow (E110) – 0.0036 mg, dye quinoline yellow (E104) – 0.4575 mg.
10 pcs. – blister packs (2) – cardboard packs.
10 pcs. – blister packs (3) – cardboard packs.
10 pcs. – blister packs (6) – cardboard packs.
![Mexicor® [Capsules, Solution] 1](https://www.medixlife.com/wp-content/uploads/Medixlife_favi_512.png "Mexicor® [Capsules, Solution] 2")