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Title: Rilmenidine  
Author: World Heritage Encyclopedia
Language: English
Subject: Clonidine, Imidazoline receptor, Sympatholytic, Bethanidine, Deserpidine
Publisher: World Heritage Encyclopedia


Systematic (IUPAC) name
Clinical data
Trade names Albarel
Legal status
  • (Prescription only)
Routes of
Pharmacokinetic data
Protein binding 7%
Metabolism Minimal
Biological half-life 8 hours
Excretion Renal, unchanged
CAS Registry Number  N
ATC code C02
PubChem CID:
ChemSpider  Y
Chemical data
Formula C10H16N2O
Molecular mass 180.247 g/mol

Rilmenidine is a prescription medication for the treatment of hypertension.[1] It is marketed under the brand names Albarel, Hyperium, Iterium and Tenaxum.


  • Form and composition 1
  • Mode of action 2
  • Indications 3
  • Contraindications 4
  • Warning 5
  • Precautions 6
  • Drug interactions 7
  • Side effects 8
  • Dosage and route of administration 9
  • Overdosage 10
  • References 11

Form and composition

Each tablet contains 1.544 mg rilmenidine dihydrogen phosphate, an amount equivalent to 1 mg of rilmenidine base.

Mode of action

Rilmenidine, an oxazoline compound with antihypertensive properties, acts on both medullary and peripheral vasomotor structures. Rilmenidine shows greater selectivity for imidazoline receptors than for cerebral alpha2-adrenergic receptors, distinguishing it from reference alpha2-agonists.




Severe depression, severe renal failure (creatinine clearance <15 ml/min), as a precaution in the absence of currently available studies.


Therapy should never be interrupted suddenly; the dosage should be reduced gradually.


  • As with all antihypertensive agents, regular medical monitoring is required when rilmenidine is administered to patients with a recent history of cardiovascular disease (stroke, myocardial infarction).
  • Alcohol consumption should be avoided during treatment.
  • In patients with renal failure, no dosage adjustment is necessary if creatinine clearance is greater than 15 mL/min.
  • In the absence of documented experiments in this area, rilmenidine is not recommended for prescription to children.
  • Pregnancy: as with all new molecules, administration of rilmenidine should be avoided in pregnant women, although no teratogenic or embryotoxic effects have been observed in animal studies.
  • Lactation: rilmenidine is excreted in breast milk, and its use is therefore not recommended during lactation.
  • Effects on the ability to drive motor vehicles or operate machinery: double-blind, placebo-controlled studies have not shown rilmenidine to have any effect on alertness at therapeutic doses (1or 2 daily administrations of 1 mg). If these doses are exceeded, or if rilmenidine is combined with other drugs capable of reducing alertness, vehicle drivers or machine operators should be warned of the possibility of drowsiness.

Drug interactions

Combinations not recommended: combination with MAOIs is not recommended; combination with tricyclic antidepressants requires prudence, as the antihypertensive activity of rilmenidine may be partly antagonized.

Side effects

  • At a dose of 1 mg given as a single daily administration during controlled trials, the incidence of side effects was comparable to that observed with placebo.
  • At a dose of 2 mg per day of rilmenidine, controlled comparative studies versus clonidine (0.15 to 0.30 mg/day) or alpha2-methyldopa (500 to 1000 mg/day) demonstrated that the incidence of side effects was significantly lower with rilmenidine than with either clonidine or a-methyldopa.

Side-effects are rare, non-severe, and transient at therapeutic doses: asthenia, palpitations, insomnia, drowsiness, fatigue on exercise, epigastric pain, dryness of the mouth, diarrhea, skin rash; and exceptionally, cold extremities, postural hypotension, sexual disorders, anxiety, depression, pruritus, edema, cramps, nausea, constipation, hot flushes.

Dosage and route of administration

The recommended dosage is 1 tablet per day as a single morning administration. If results are not adequate after 1 month of treatment, the dosage may be increased to 2 tablets per day, given in divided doses (1 tablet morning and evening) before meals. As a result of its good clinical and biological acceptability, rilmenidine may be administered to both elderly and diabetic hypertensive patients. In patients with renal failure, no dosage adjustment is necessary in principle when the creatinine clearance is greater than 15 mL/min.

Treatment may be continued indefinitely.


No cases of massive absorption have been reported. Likely symptoms in such an eventuality would be marked hypotension and lowered alertness. In addition to gastric lavage, sympathomimetic agents may also required. Rilmenidine is only slightly dialysable.


  1. ^ Remková A, Kratochvíl'ová H (August 2002). "Effect of the new centrally acting antihypertensive agent rilmenidine on endothelial and platelet function in essential hypertension". J Hum Hypertens 16 (8): 549–55.  

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