AI Article Synopsis

  • OM-TMCD is a new drug designed as a methoxyamide derivative of a cyclopropyl analogue of valproic acid (VPA) to improve anticonvulsant effectiveness while reducing VPA's harmful side effects, specifically neural tube defects and liver toxicity.
  • When tested on rats, OM-TMCD showed greater potency in preventing seizures compared to VPA, although it was ineffective in a specific mouse seizure test.
  • Safety assessments indicated that OM-TMCD has similar fetal toxicity to VPA but is more effective as an anticonvulsant, along with favorable pharmacokinetic properties, warranting further research on its therapeutic potential.

Article Abstract

N-methoxy-2,2,3,3-tetramethylcyclopropane carboxamide (OM-TMCD) is a methoxyamide derivative of a cyclopropyl analogue of valproic acid (VPA). The structural considerations used in the design of OM-TMCD were aimed to enhance OM-TMCD anticonvulsant potency (compared to VPA) and to prevent VPA's two life-threatening side effects, i.e., induction of neural tube defects (NTDs) and hepatotoxicity. Following i.p. administration to rats OM-TMCD demonstrated a broad spectrum of anticonvulsant activity and showed better potency than VPA in the maximal electroshock seizure and subcutaneous pentylenetetrazole tests as well as in the hippocampal kindling model. OM-TMCD was inactive in the mouse 6-Hz test at 100 mg/kg dose. Teratogenicity studies performed in a SWV/Fnn-mouse model for VPA-induced-exencephaly showed that on the equimolar basis OM-TMCD possesses the same fetal toxicity and ability to induce NTDs as VPA, but since OM-TMCD is a much more potent anticonvulsant its activity/exencephaly formation ratio appears to be much more beneficial than that of VPA. OM-TMCD was found to be non-mutagenic and non-pro-mutagenic in the Ames test. It showed a beneficial pharmacokinetic profile in rats, having a high oral bioavailability of 75% and satisfactory values of clearance and volume of distribution. These results support further studies to fully characterize the therapeutic potential of OM-TMCD.

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Source
http://dx.doi.org/10.1016/j.eplepsyres.2006.08.004DOI Listing

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