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具有强大体外神经保护作用的小分子抗惊厥药物。

Small molecule anticonvulsant agents with potent in vitro neuroprotection.

机构信息

Advanced Neural Dynamics, Inc., Pennsylvania Biotechnology Center, Doylestown, PA 18902, USA.

出版信息

J Mol Neurosci. 2012 Jun;47(2):368-79. doi: 10.1007/s12031-012-9765-x. Epub 2012 Apr 26.

Abstract

Severe seizure activity is associated with recurring cycles of excitotoxicity and oxidative stress that result in progressive neuronal damage and death. Intervention to halt these pathological processes is a compelling disease-modifying strategy for the treatment of seizure disorders. In the present study, a core small molecule with anticonvulsant activity has been structurally optimized for neuroprotection. Phenotypic screening of rat hippocampal cultures with nutrient medium depleted of antioxidants was utilized as a disease model. Increased cell death and decreased neuronal viability produced by acute treatment with glutamate or hydrogen peroxide were prevented by our novel molecules. The neuroprotection associated with this chemical series has marked structure activity relationships that focus on modification of the benzylic position of a 2-phenyl-2-hydroxyethyl sulfamide core structure. Complete separation between anticonvulsant activity and neuroprotective action was dependent on substitution at the benzylic carbon. Chiral selectivity was evident in that the S-enantiomer of the benzylic hydroxy group had neither neuroprotective nor anticonvulsant activity, while the R-enantiomer of the lead compound had full neuroprotective action at <40 nM and antiseizure activity in three animal models. These studies indicate that potent, multifunctional neuroprotective anticonvulsants are feasible within a single molecular entity.

摘要

严重的癫痫发作活动与兴奋性毒性和氧化应激的反复循环有关,导致进行性神经元损伤和死亡。干预这些病理过程是治疗癫痫发作障碍的一种引人注目的疾病修饰策略。在本研究中,针对神经保护作用对具有抗惊厥活性的核心小分子进行了结构优化。利用抗氧化剂耗尽的营养培养基中的大鼠海马培养物进行表型筛选,作为疾病模型。通过急性处理谷氨酸或过氧化氢,我们的新分子可预防细胞死亡增加和神经元活力降低。该化学系列的神经保护作用具有明显的构效关系,主要集中在 2-苯基-2-羟乙基磺酰胺核心结构的苄基位置的修饰上。抗惊厥活性和神经保护作用的完全分离取决于苄基碳的取代。手性选择性明显,即苄基羟基的 S-对映体既没有神经保护作用也没有抗惊厥作用,而先导化合物的 R-对映体在<40 nM 时具有完全的神经保护作用,并且在三种动物模型中具有抗惊厥作用。这些研究表明,在单个分子实体中可以实现有效的、多功能的神经保护抗惊厥药物。

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