Aceclofenac

CLINICAL USE

NSAID and analgesic

DOSE IN NORMAL RENAL FUNCTION

100 mg twice daily

PHARMACOKINETICS

  • Molecular weight                           :354.2
  • %Protein binding                           :>99
  • %Excreted unchanged in urine     : 66 (mainly as metabolites)
  • Volume of distribution (L/kg)       :25 litres
  • half-life – normal/ESRD (hrs)      :4/Unchanged

    DOSE IN RENAL IMPAIRMENT

    GFR (mL/MIN)

  • 20 to 50     : Dose as in normal renal function but use with caution
  • 10 to 20     : Dose as in normal renal function but avoid if possible
  • <10           : Dose as in normal renal function but only if on dialysis

    DOSE IN PATIENTS UNDERGOING RENAL REPLACEMENT THERAPIES

  • CAPD                :Not dialysed. Dose as in normal renal function.
  • HD                             :Not dialysed. Dose as in normal renal function.
  • HDF/high flux   :Unknown dialysability. Dose as in normal renal function.
  • CAV/VVHD      :Not dialysed. Dose as in normal renal function

    IMPORTANT DRUG INTERACTIONS

    Potentially hazardous interactions with other drugs

  • ACE inhibitors and angiotensin-II antagonists: antagonism of hypotensive effect; increased risk of nephrotoxicity and hyperkalaemia
  • Analgesics: avoid concomitant use of 2 or more NSAIDs, including aspirin (increased side effects); avoid with ketorolac (increased risk of side effects and haemorrhage)
  • Antibacterials: possible increased risk of convulsions with quinolones
  • Anticoagulants: effects of coumarins enhanced; possible increased risk of bleeding with heparins and coumarins
  • Antidepressants: increased risk of bleeding with SSRIs and venlafaxine
  • Antidiabetic agents: effects of sulphonylureas enhancedAnti-epileptics: possibly increased phenytoin concentration
  • Antivirals: increased risk of haematological toxicity with zidovudine; concentration possibly increased by ritonavir
  • Ciclosporin: may potentiate nephrotoxicity
  • Cytotoxic agents: reduced excretion of methotrexate; increased risk of bleeding with erlotinib
  • Diuretics: increased risk of nephrotoxicity; antagonism of diuretic effect, hyperkalaemia with potassium-sparing diureticsLithium: excretion decreased
  • Pentoxifylline: increased risk of bleeding
  • Tacrolimus: increased risk of nephrotoxicity

    ADMINISTRATION

    Reconstition

    Route

    Oral

    Rate of Administration

    Comments

    OTHER INFORMATION

  • Use with caution in uraemic patients predisposed to gastrointestinal bleeding or uraemic coagulopathies
  • Inhibition of renal prostaglandin synthesis by NSAIDs may interfere with renal function, especially in the presence of existing renal disease – avoid if possible; if not, check serum creatinine 48–72 hours after starting NSAID therapy – if raised, discontinue NSAID therapy
  • Use normal doses in patients with ESRD on dialysis if they do not pass any urine
  • Use with great caution in renal transplant recipients; it can reduce intrarenal autocoid synthesis
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