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在子宫内将人类神经嵴细胞注射到小鼠胚胎后,其对种间嵌合体的皮毛色素沉着有贡献。

Human neural crest cells contribute to coat pigmentation in interspecies chimeras after in utero injection into mouse embryos.

作者信息

Cohen Malkiel A, Wert Katherine J, Goldmann Johanna, Markoulaki Styliani, Buganim Yosef, Fu Dongdong, Jaenisch Rudolf

机构信息

Whitehead Institute for Biomedical Research, Cambridge, MA 02142;

Whitehead Institute for Biomedical Research, Cambridge, MA 02142; Department of Biology, Massachusetts Institute of Technology, Cambridge, MA 02142

出版信息

Proc Natl Acad Sci U S A. 2016 Feb 9;113(6):1570-5. doi: 10.1073/pnas.1525518113. Epub 2016 Jan 25.

Abstract

The neural crest (NC) represents multipotent cells that arise at the interphase between ectoderm and prospective epidermis of the neurulating embryo. The NC has major clinical relevance because it is involved in both inherited and acquired developmental abnormalities. The aim of this study was to establish an experimental platform that would allow for the integration of human NC cells (hNCCs) into the gastrulating mouse embryo. NCCs were derived from pluripotent mouse, rat, and human cells and microinjected into embryonic-day-8.5 embryos. To facilitate integration of the NCCs, we used recipient embryos that carried a c-Kit mutation (W(sh)/W(sh)), which leads to a loss of melanoblasts and thus eliminates competition from the endogenous host cells. The donor NCCs migrated along the dorsolateral migration routes in the recipient embryos. Postnatal mice derived from injected embryos displayed pigmented hair, demonstrating differentiation of the NCCs into functional melanocytes. Although the contribution of human cells to pigmentation in the host was lower than that of mouse or rat donor cells, our results indicate that hNCCs, injected in utero, can integrate into the embryo and form mature functional cells in the animal. This mouse-human chimeric platform allows for a new approach to study NC development and diseases.

摘要

神经嵴(NC)代表多能细胞,这些细胞产生于神经胚形成期胚胎的外胚层和预期表皮之间的间期。神经嵴具有重要的临床意义,因为它与遗传性和获得性发育异常均有关。本研究的目的是建立一个实验平台,该平台能够将人类神经嵴细胞(hNCCs)整合到原肠胚形成期的小鼠胚胎中。神经嵴细胞源自多能性小鼠、大鼠和人类细胞,并显微注射到胚胎第8.5天的胚胎中。为了促进神经嵴细胞的整合,我们使用了携带c-Kit突变(W(sh)/W(sh))的受体胚胎,该突变导致成黑素细胞缺失,从而消除了内源性宿主细胞的竞争。供体神经嵴细胞在受体胚胎中沿着背外侧迁移路径迁移。注射胚胎出生后的小鼠出现了有色素的毛发,这表明神经嵴细胞分化为功能性黑素细胞。尽管人类细胞对宿主色素沉着的贡献低于小鼠或大鼠供体细胞,但我们的结果表明,子宫内注射的hNCCs能够整合到胚胎中,并在动物体内形成成熟的功能细胞。这个小鼠-人类嵌合平台为研究神经嵴发育和疾病提供了一种新方法。

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