Sachinidis Agapios, Sotiriadou Isaia, Seelig Bianca, Berkessel Albrecht, Hescheler Jürgen
Centre of Physiology and Pathophysiology, Institute of Neurophysiology, Cologne, Germany.
Comb Chem High Throughput Screen. 2008 Jan;11(1):70-82. doi: 10.2174/138620708783398322.
Cell replacement therapy of severe degenerative diseases such as diabetes, myocardial infarction and Parkinson's disease through transplantation of somatic cells generated from embryonic stem (ES) cells is currently receiving considerable attention for the therapeutic applications. ES cells harvested from the inner cell mass (ICM) of the early embryo, can proliferate indefinitely in vitro while retaining the ability to differentiate into all somatic cells thereby providing an unlimited renewable source of somatic cells. In this context, identifying soluble factors, in particular chemically synthesized small molecules, and signal cascades involved in specific differentiation processes toward a defined tissue specific cell type are crucial for optimizing the generation of somatic cells in vitro for therapeutic approaches. However, experimental models are required allowing rapid and "easy-to-handle" parallel screening of chemical libraries to achieve this goal. Recently, the forward chemical genetic screening strategy has been postulated to screen small molecules in cellular systems for a specific desired phenotypic effect. The current review is focused on the progress of ES cell research in the context of the chemical genetics to identify small molecules promoting specific differentiation of ES cells to desired cell phenotype. Chemical genetics in the context of the cell ES-based cell replacement therapy remains a challenge for the near future for several scientific fields including chemistry, molecular biology, medicinal physics and robotic technologies.
通过移植由胚胎干细胞(ES细胞)生成的体细胞来对糖尿病、心肌梗死和帕金森病等严重退行性疾病进行细胞替代治疗,目前在治疗应用方面受到了广泛关注。从早期胚胎的内细胞团(ICM)中获取的ES细胞,能够在体外无限增殖,同时保留分化为所有体细胞的能力,从而提供了一个无限可再生的体细胞来源。在这种情况下,识别可溶性因子,特别是化学合成的小分子,以及参与向特定组织特异性细胞类型进行特定分化过程的信号级联反应,对于优化体外生成用于治疗方法的体细胞至关重要。然而,需要实验模型来实现对化学文库的快速且“易于操作”的平行筛选以达成这一目标。最近,正向化学遗传学筛选策略被提出用于在细胞系统中筛选小分子以获得特定的期望表型效应。当前的综述聚焦于在化学遗传学背景下ES细胞研究的进展,以识别促进ES细胞向期望细胞表型进行特定分化的小分子。在基于ES细胞的细胞替代治疗背景下的化学遗传学,在包括化学、分子生物学、医学物理学和机器人技术等多个科学领域的近期内仍然是一项挑战。