A Molecular Analysis of Neural Olfactory Placode Differentiation in Human Pluripotent Stem Cells.

IF 2.5 3区 医学 Q3 CELL & TISSUE ENGINEERING
Rebecca L Bricker, Uchit Bhaskar, Rossella Titone, Melanie A Carless, Tiziano Barberi
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引用次数: 1

Abstract

During embryonic development, the olfactory sensory neurons (OSNs) and the gonadotropic-releasing hormone neurons (GNRHNs) migrate from the early nasal cavity, known as the olfactory placode, to the brain. Defects in the development of OSNs and GNRHNs result in neurodevelopmental disorders such as anosmia and congenital hypogonadotropic hypogonadism, respectively. Treatments do not restore the defective neurons in these disorders, and as a result, patients have a diminished sense of smell or a gonadotropin hormone deficiency. Human pluripotent stem cells (hPSCs) can produce any cell type in the body; therefore, they are an invaluable tool for cell replacement therapies. Transplantation of olfactory placode progenitors, derived from hPSCs, is a promising therapeutic to replace OSNs and GNRHNs and restore tissue function. Protocols to generate olfactory placode progenitors are limited, and thus, we describe, in this study, a novel in vitro model for olfactory placode differentiation in hPSCs, which is capable of producing both OSNs and GNRHNs. Our study investigates the major developmental signaling factors that recapitulate the embryonic development of the olfactory tissue. We demonstrate that induction of olfactory placode in hPSCs requires bone morphogenetic protein inhibition, wingless/integrated protein inhibition, retinoic acid inhibition, transforming growth factor alpha activation, and fibroblast growth factor 8 activation. We further show that the protocol transitions hPSCs through the anterior pan-placode ectoderm and neural ectoderm regions in early development while preventing neural crest and non-neural ectoderm regions. Finally, we demonstrate production of OSNs and GNRHNs by day 30 of differentiation. Our study is the first to report on OSN differentiation in hPSCs.

人多能干细胞神经嗅觉基块分化的分子分析。
在胚胎发育过程中,嗅觉感觉神经元(OSNs)和促性腺释放激素神经元(GNRHNs)从早期鼻腔迁移到大脑。OSNs和gnrhn发育缺陷分别导致嗅觉缺失和先天性促性腺功能低下等神经发育障碍。治疗不能恢复这些疾病中有缺陷的神经元,因此,患者的嗅觉减弱或促性腺激素缺乏。人多能干细胞(hPSCs)可以在体内产生任何类型的细胞;因此,它们是细胞替代疗法的宝贵工具。来源于人造血干细胞的嗅基祖细胞移植是一种很有前景的替代osn和GNRHNs并恢复组织功能的治疗方法。产生嗅觉基板祖细胞的方法是有限的,因此,在本研究中,我们描述了一种新的体外模型,用于hPSCs的嗅觉基板分化,该模型能够产生OSNs和GNRHNs。本研究探讨了反映嗅觉组织胚胎发育的主要发育信号因子。我们证明,在人乳头状细胞中诱导嗅觉位点需要骨形态发生蛋白抑制、无翼/整合蛋白抑制、视黄酸抑制、转化生长因子α激活和成纤维细胞生长因子8激活。我们进一步表明,在发育早期,该方案通过前泛位外胚层和神经外胚层区域转移hPSCs,同时阻止神经嵴和非神经外胚层区域。最后,我们证明在分化的第30天产生了OSNs和GNRHNs。我们的研究首次报道了造血干细胞中OSN的分化。
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来源期刊
Stem cells and development
Stem cells and development 医学-细胞与组织工程
CiteScore
7.80
自引率
2.50%
发文量
69
审稿时长
3 months
期刊介绍: Stem Cells and Development is globally recognized as the trusted source for critical, even controversial coverage of emerging hypotheses and novel findings. With a focus on stem cells of all tissue types and their potential therapeutic applications, the Journal provides clinical, basic, and translational scientists with cutting-edge research and findings. Stem Cells and Development coverage includes: Embryogenesis and adult counterparts of this process Physical processes linking stem cells, primary cell function, and structural development Hypotheses exploring the relationship between genotype and phenotype Development of vasculature, CNS, and other germ layer development and defects Pluripotentiality of embryonic and somatic stem cells The role of genetic and epigenetic factors in development
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