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嗅觉上皮中纯化的移植球状基底细胞的多能性。

Multipotency of purified, transplanted globose basal cells in olfactory epithelium.

作者信息

Chen Xueyan, Fang Hengsheng, Schwob James E

机构信息

Department of Anatomy and Cellular Biology, Tufts University School of Medicine, Boston, Massachusetts 02111, USA.

出版信息

J Comp Neurol. 2004 Feb 16;469(4):457-74. doi: 10.1002/cne.11031.

Abstract

By comparison with the rest of the nervous system, the olfactory epithelium has an unparalleled ability to renew and repair itself throughout life. However, the identity and capacity of the various types of progenitor cells that underlie that ability are not well established. We used selective isolation, transplantation, and engraftment of various types of marker-labeled cells into the epithelium of methyl bromide-lesioned, unmarked host mice to dissect progenitor cell capacity. Globose basal cells were purified from other potential progenitors using the monoclonal antibody GBC-2 (GBC, globose basal cell) and fluorescence activated cell sorting. Transplanted globose basal cells engraft and, in aggregate, give rise to globose basal cells, neurons, sustentacular cells, and several other kinds of non-neuronal cells. Individual clones, derived from single engrafted globose basal cells, can consist of a mixture of neurons and non-neuronal cells, only neurons, or only non-neuronal cells. Neurons that arise after transplantation mature to the point of expressing odorant receptors and olfactory marker protein and of projecting axons to the olfactory bulb. In contrast, other kinds of epithelial cells are neither neurogenic nor multipotent. For example, sustentacular and duct cells give rise only to themselves after transplantation. Furthermore, horizontal basal cells do not engraft in mice, in which the endogenous population is spared after lesion. Thus, some subtype(s) of GBC is a multipotent progenitor cell, whose multipotency is activated after destruction of both neurons and non-neuronal cells. The results suggest that progenitor cell transplantation may prove useful as a therapeutic modality as well as an analytical tool.

摘要

与神经系统的其他部分相比,嗅觉上皮在其整个生命周期中具有无与伦比的自我更新和修复能力。然而,构成这种能力基础的各种祖细胞的特性和能力尚未完全明确。我们通过将各种标记细胞选择性分离、移植并植入经溴甲烷损伤且未标记的宿主小鼠的上皮组织中,来剖析祖细胞的能力。利用单克隆抗体GBC - 2(GBC,球状基底细胞)和荧光激活细胞分选技术从其他潜在祖细胞中纯化出球状基底细胞。移植的球状基底细胞能够植入,并聚集形成球状基底细胞、神经元、支持细胞以及其他几种非神经元细胞。源自单个植入的球状基底细胞的单个克隆可以由神经元和非神经元细胞的混合物、仅神经元或仅非神经元细胞组成。移植后产生的神经元会成熟到表达气味受体和嗅觉标记蛋白,并将轴突投射到嗅球的程度。相比之下,其他类型的上皮细胞既不是神经源性的,也不是多能的。例如,支持细胞和导管细胞在移植后仅产生自身类型的细胞。此外,水平基底细胞在小鼠中不能植入,在溴甲烷损伤后内源性水平基底细胞群体得以保留。因此,球状基底细胞的某些亚型是多能祖细胞,其多能性在神经元和非神经元细胞均被破坏后被激活。这些结果表明,祖细胞移植可能被证明是一种有用的治疗方式以及分析工具。

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