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通过神经嵴成黑素细胞的逆转录病毒标记在白化小鼠中产生色素条纹。

Generation of pigmented stripes in albino mice by retroviral marking of neural crest melanoblasts.

作者信息

Huszar D, Sharpe A, Hashmi S, Bouchard B, Houghton A, Jaenisch R

机构信息

Whitehead Institute for Biomedical Research, Massachusetts Institute of Technology, Cambridge 02142.

出版信息

Development. 1991 Oct;113(2):653-60. doi: 10.1242/dev.113.2.653.

Abstract

The pigment cells of the skin are derived from melanoblasts which originate in the neural crest. The dorsoventral migration of melanoblasts has been visualized in pigment stripes seen in aggregation chimeras, and the width of these bands has suggested that the entire pigmentation of the coat is derived from a small number of founder cells. We have generated mosaic mice by marking single melanoblasts in utero to gain information on the clonal history of pigment-forming cells. A retroviral vector carrying the human tyrosinase gene was constructed and microinjected into neurulating albino mouse embryos. Albino mice are devoid of pigmentation due to deficiency of tyrosinase. Thus, transduction of the wild-type gene into the otherwise normal melanoblasts should rescue the mutant phenotype, giving rise to patches of pigmentation, which correspond to the area colonized by the mitotic progeny of a marked clone. Mosaic animals derived from the injected embryos indeed showed pigmented bands with a width strikingly similar to the 'standard' stripes seen in aggregation chimeras. These results are consistent with the notion that the unit width bands seen in aggregation chimeras represent the clonal progeny of a single melanoblast and verify Mintz's (1967) conclusion that a few founder melanoblasts give rise to coat pigmentation. The pigment cells of the eye are of dual origin: the melanocytes in choroid and outer layer of the iris are derived from the neural crest and those in the pigment layer of the retina from the neuroepithelium of the optic cup. Marked clones in both lineages were observed in the eyes of many mosaic animals.

摘要

皮肤的色素细胞源自神经嵴中的成黑素细胞。成黑素细胞的背腹迁移已在聚集嵌合体中所见的色素条纹中显现出来,这些条带的宽度表明被毛的整个色素沉着源自少数祖细胞。我们通过在子宫内标记单个成黑素细胞来生成嵌合小鼠,以获取有关色素形成细胞克隆历史的信息。构建了携带人酪氨酸酶基因的逆转录病毒载体,并将其显微注射到正在神经管形成的白化病小鼠胚胎中。白化病小鼠由于酪氨酸酶缺乏而没有色素沉着。因此,将野生型基因转导到原本正常的成黑素细胞中应该可以挽救突变表型,产生色素沉着斑块,这与由标记克隆的有丝分裂后代定殖的区域相对应。来自注射胚胎的嵌合动物确实显示出色素带,其宽度与聚集嵌合体中所见的“标准”条纹惊人地相似。这些结果与以下观点一致,即聚集嵌合体中所见的单位宽度条带代表单个成黑素细胞的克隆后代,并验证了明茨(1967年)的结论,即少数祖成黑素细胞产生被毛色素沉着。眼睛的色素细胞有双重起源:脉络膜和虹膜外层的黑素细胞源自神经嵴,视网膜色素层的黑素细胞源自视杯的神经上皮。在许多嵌合动物的眼睛中都观察到了这两个谱系中的标记克隆。

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