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Hyponatremia drug-related

Oxcarbazepine is closely related to carbamazepine and useful in the same seizure types, but it may have an improved toxicity profile. Oxcarbazepine has a half-life of only 1-2 hours. Its activity, therefore, resides almost exclusively in the 10-hydroxy metabolite, to which it is rapidly converted and which has a half-life similar to that of carbamazepine, ie, 8-12 hours. The drug is mostly excreted as the glucuronide of the 10-hydroxy metabolite. Oxcarbazepine is less potent than carbamazepine, both in animal models of epilepsy and in epileptic patients clinical doses of oxcarbazepine may need to be 50% higher than those of carbamazepine to obtain equivalent seizure control. Some studies report fewer hypersensitivity reactions to oxcarbazepine, and cross-reactivity with carbamazepine does not always occur. Furthermore, the drug appears to induce hepatic enzymes to a lesser extent than carbamazepine, minimizing drug interactions. Those adverse effects—such as hyponatremia—that do occur with oxcarbazepine are similar in character to reactions reported with carbamazepine. [Pg.557]

Seizures associated with intravenous use of vinca alkaloids are very rare (60-62). Some cases may have been due to SIADH-associated hyponatremia. Other forms include tumor-related effects, nervous system infections, or cerebral hemorrhage, which often make direct causal relations between drug exposure and nervous system adverse effects very difficult. [Pg.3635]


See other pages where Hyponatremia drug-related is mentioned: [Pg.431]    [Pg.229]    [Pg.21]    [Pg.599]    [Pg.120]    [Pg.35]    [Pg.248]    [Pg.314]    [Pg.431]    [Pg.575]    [Pg.169]    [Pg.293]   
See also in sourсe #XX -- [ Pg.410 ]




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