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对人类胚胎干细胞进行药理学操控的潜力。

Potential for pharmacological manipulation of human embryonic stem cells.

作者信息

Atkinson Stuart P, Lako Majlinda, Armstrong Lyle

机构信息

Centro de Investigacion Principe Felipe, Valencia, Spain.

出版信息

Br J Pharmacol. 2013 May;169(2):269-89. doi: 10.1111/j.1476-5381.2012.01978.x.

Abstract

The therapeutic potential of human embryonic stem cells (hESCs) and induced pluripotent stem cells (iPSCs) is vast, allowing disease modelling, drug discovery and testing and perhaps most importantly regenerative therapies. However, problems abound; techniques for cultivating self-renewing hESCs tend to give a heterogeneous population of self-renewing and partially differentiated cells and general include animal-derived products that can be cost-prohibitive for large-scale production, and effective lineage-specific differentiation protocols also still remain relatively undefined and are inefficient at producing large amounts of cells for therapeutic use. Furthermore, the mechanisms and signalling pathways that mediate pluripotency and differentiation are still to be fully appreciated. However, over the recent years, the development/discovery of a range of effective small molecule inhibitors/activators has had a huge impact in hESC biology. Large-scale screening techniques, coupled with greater knowledge of the pathways involved, have generated pharmacological agents that can boost hESC pluripotency/self-renewal and survival and has greatly increased the efficiency of various differentiation protocols, while also aiding the delineation of several important signalling pathways. Within this review, we hope to describe the current uses of small molecule inhibitors/activators in hESC biology and their potential uses in the future.

摘要

人类胚胎干细胞(hESCs)和诱导多能干细胞(iPSCs)具有巨大的治疗潜力,可用于疾病建模、药物发现与测试,或许最重要的是可用于再生疗法。然而,问题也很多;培养自我更新的hESCs的技术往往会产生自我更新和部分分化细胞的异质群体,并且通常包含动物源产品,这对于大规模生产来说成本过高,而且有效的谱系特异性分化方案仍然相对不明确,在大量生产用于治疗的细胞方面效率低下。此外,介导多能性和分化的机制及信号通路仍有待充分了解。然而,近年来,一系列有效的小分子抑制剂/激活剂的开发/发现对hESC生物学产生了巨大影响。大规模筛选技术,加上对相关通路的更多了解,已经产生了能够提高hESC多能性/自我更新和存活率的药物制剂,极大地提高了各种分化方案的效率,同时也有助于阐明几个重要的信号通路。在这篇综述中,我们希望描述小分子抑制剂/激活剂在hESC生物学中的当前用途及其未来的潜在用途。

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