Stereoselective anticonvulsant and pharmacokinetic analysis of valnoctamide, a CNS-active derivative of valproic acid with low teratogenic potential

被引:24
|
作者
Shekh-Ahmad, Tawfeeq [1 ]
Hen, Naama [1 ]
Yagen, Boris [1 ,2 ]
McDonough, John H. [3 ]
Finnell, Richard H. [4 ]
Wlodarczyk, Bogdan J. [4 ]
Bialer, Meir [1 ,2 ]
机构
[1] Hebrew Univ Jerusalem, Inst Drug Res, Fac Med, Sch Pharm, IL-91120 Jerusalem, Israel
[2] Hebrew Univ Jerusalem, David R Bloom Ctr Pharm, IL-91120 Jerusalem, Israel
[3] US Army Med Res Inst Chem Def, Pharmacol Branch, Div Res, Aberdeen Proving Ground, MD USA
[4] Univ Texas Austin, Dell Pediat Res Inst, Dept Nutr Sci, Austin, TX 78712 USA
关键词
Chiral switch; Strereoselective pharmacokinetic and pharmacodynamics analysis; New antiepileptic drugs; CNS drugs; CHIRAL AMIDE ANALOG; ANTIEPILEPTIC DRUGS; UNIQUE ACTIVITY; ISOMER; PROFILE;
D O I
10.1111/epi.12480
中图分类号
R74 [神经病学与精神病学];
学科分类号
摘要
Objective Valnoctamide (VCD), a central nervous system (CNS)-active chiral constitutional isomer of valpromide, the corresponding amide of valproic acid (VPA), is currently undergoing phase IIb clinical trials in acute mania. VCD exhibits stereoselective pharmacokinetics (PK) in animals and humans. The current study comparatively evaluated the pharmacodynamics (PD; anticonvulsant activity and teratogenicity) and PK of the four individual stereoisomers of VCD. Methods The anticonvulsant activity of VCD individual stereoisomers was evaluated in several rodent anticonvulsant models including maximal electroshock, 6Hz psychomotor, subcutaneous metrazol, and the pilocarpine-induced and soman-induced status epilepticus (SE). The PK-PD (anticonvulsant activity) relationship of VCD stereoisomers was evaluated following intraperitoneal administration (70mg/kg) to rats. Induction of neural tube defects (NTDs) by VCD stereoisomers was evaluated in a mouse strain that was highly susceptible to teratogen-induced NTDs. Results VCD had a stereoselective PK, with (2S,3S)-VCD exhibiting the lowest clearance, and consequently a twice-higher plasma exposure than all other stereoisomers. Nervertheless, there was less stereoselectivity in VCD anticonvulsant activity and each stereoisomer had similar median effective dose (ED)(50) values in most models. VCD stereoisomers (258 or 389mg/kg) did not cause NTDs. These doses are 3-12 times higher than VCD anticonvulsant ED50 values. Significance VCD displayed stereoselective PK that did not lead to significant stereoselective activity in various anticonvulsant rodent models. If VCD exerted its broad-spectrum anticonvulsant activity using a single mechanism of action (MOA), it is likely that it would exhibit a stereoselective PD. The fact that there was no significant difference between racemic VCD and its individual stereoisomers suggests that VCD's anticonvulsant activity is due to multiple MOAs.
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页码:353 / 361
页数:9
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