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孤雌胚胎干细胞的体内和体外分化为造血和神经细胞类型。

In vivo and in vitro differentiation of uniparental embryonic stem cells into hematopoietic and neural cell types.

机构信息

Center for Animal Transgenesis and Germ Cell Research; New Bolton Center; University of Pennsylvania; Kennett Square, Pennsylvania USA.

出版信息

Organogenesis. 2008 Jan;4(1):33-41. doi: 10.4161/org.6123.

Abstract

The biological role of genomic imprinting in adult tissue is central to the consideration of transplanting uniparental embryonic stem (ES) cell-derived tissues. We have recently shown that both maternal (parthenogenetic/gynogenetic) and paternal (androgenetic) uniparental ES cells can differentiate, both in vivo in chimeras and in vitro, into adult-repopulating hematopoietic stem and progenitor cells. This suggests that, at least in some tissues, the presence of two maternal or two paternal genomes does not interfere with stem cell function and tissue homeostasis in the adult. Here, we consider implications of the contribution of uniparental cells to hematopoiesis and to development of other organ systems, notably neural tissue for which consequences of genomic imprinting are associated with a known bias in development and behavioral disorders. Our findings so far indicate that there is little or no limit to the differentiation potential of uniparental ES cells outside the normal developmental paradigm. As a potentially donor MHC-matching source of tissue, uniparental transplants may provide not only a clinical resource but also a unique tool to investigate aspects of genomic imprinting in adults.

摘要

基因组印记在成体组织中的生物学作用是考虑将单亲胚胎干细胞(ES)细胞衍生组织移植的核心。我们最近表明,母系(孤雌生殖/卵核生殖)和父系(雄核生殖)单亲 ES 细胞都可以在体内嵌合体和体外分化为具有成人造血干细胞和祖细胞再生能力的细胞。这表明,至少在某些组织中,两个母系或两个父系基因组的存在并不干扰成体中的干细胞功能和组织内稳态。在这里,我们考虑单亲细胞对造血和其他器官系统发育的贡献,特别是神经组织,其基因组印记的后果与已知的发育和行为障碍偏倚有关。到目前为止,我们的发现表明,单亲 ES 细胞在正常发育范例之外的分化潜力很小或没有限制。作为组织的潜在 MHC 匹配供体,单亲移植不仅可以提供临床资源,还可以提供一个独特的工具来研究成人基因组印记的各个方面。

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