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Drug target identification for neuronal apoptosis through a genome scale screening.

机译:通过基因组规模筛选来确定神经元凋亡的药物靶标。

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During normal nervous system development, physiologically appropriate neuronal apoptosis contributes to a sculpting process that removes approximately one-half of all neurons born during neurogenesis. However, neuronal apoptosis subsequent to this developmental window is physiologically inappropriate for most systems and can contribute to neurodegenerative diseases. Neuronal apoptosis is characterized by specific morphological events and requires the activation of an intrinsic transcriptional program. With the completion of genome sequencing in humans and model organisms, and the advent of DNA microarray technology, the transcriptional cascades and networks regulating neuronal apoptosis are being elucidated providing new potential pharmacological targets. This review will introduce the reader to this genomic approach and illustrate with a few examples a methodological strategy for the rational selection of pharmacological targets and the development of neuroprotective agents.
机译:在正常的神经系统发育过程中,生理上适当的神经元凋亡有助于雕刻过程,该过程可消除神经发生过程中出生的所有神经元的大约一半。但是,此发育窗口后的神经元凋亡在生理上对于大多数系统而言是不合适的,并且可能导致神经退行性疾病。神经元凋亡的特征是特定的形态学事件,需要激活内在的转录程序。随着人类和模型生物体内基因组测序的完成,以及DNA微阵列技术的出现,人们正在阐明调控神经元凋亡的转录级联和网络,从而提供了新的潜在药理学靶标。这篇综述将向读者介绍这种基因组方法,并通过一些例子说明合理选择药理靶标和开发神经保护剂的方法策略。

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