Doerenkamp-Zbinden Chair for In Vitro Toxicology and Biomedicine, University of Konstanz, Konstanz D-78457, Germany.
Cell Death Differ. 2011 Mar;18(3):383-95. doi: 10.1038/cdd.2010.109. Epub 2010 Sep 24.
As neuronal differentiation of embryonic stem cells (ESCs) recapitulates embryonic neurogenesis, disturbances of this process may model developmental neurotoxicity (DNT). To identify the relevant steps of in vitro neurodevelopment, we implemented a differentiation protocol yielding neurons with desired electrophysiological properties. Results from focussed transcriptional profiling suggested that detection of non-cytotoxic developmental disturbances triggered by toxicants such as retinoic acid (RA) or cyclopamine was possible. Therefore, a broad transcriptional profile of the 20-day differentiation process was obtained. Cluster analysis of expression kinetics, and bioinformatic identification of overrepresented gene ontologies revealed waves of regulation relevant for DNT testing. We further explored the concept of superimposed waves as descriptor of ordered, but overlapping biological processes. The initial wave of transcripts indicated reorganization of chromatin and epigenetic changes. Then, a transient upregulation of genes involved in the formation and patterning of neuronal precursors followed. Simultaneously, a long wave of ongoing neuronal differentiation started. This was again superseded towards the end of the process by shorter waves of neuronal maturation that yielded information on specification, extracellular matrix formation, disease-associated genes and the generation of glia. Short exposure to lead during the final differentiation phase, disturbed neuronal maturation. Thus, the wave kinetics and the patterns of neuronal specification define the time windows and end points for examination of DNT.
由于胚胎干细胞(ESCs)的神经元分化再现了胚胎神经发生,因此该过程的紊乱可能会模拟发育性神经毒性(DNT)。为了确定体外神经发育的相关步骤,我们实施了一种产生具有所需电生理特性的神经元的分化方案。聚焦转录谱分析的结果表明,检测到有毒物质(如视黄酸(RA)或环巴胺)引发的非细胞毒性发育性干扰是可能的。因此,获得了 20 天分化过程的广泛转录谱。表达动力学的聚类分析和生物信息学鉴定过表达基因的本体论揭示了与 DNT 测试相关的调控波。我们进一步探讨了叠加波的概念,将其作为有序但重叠的生物过程的描述符。最初的转录本波表明染色质的重组和表观遗传变化。然后,参与神经元前体形成和模式形成的基因短暂上调。同时,持续的神经元分化长波开始。在这个过程结束时,神经元成熟的短波再次取代了它,这些短波提供了关于神经元特化、细胞外基质形成、与疾病相关的基因以及神经胶质生成的信息。在最后分化阶段短暂接触铅会干扰神经元成熟。因此,波动力学和神经元特化模式定义了检查 DNT 的时间窗口和终点。