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通过X连锁酶组织化学法显示体细胞突变和结肠隐窝克隆性

Demonstration of somatic mutation and colonic crypt clonality by X-linked enzyme histochemistry.

作者信息

Griffiths D F, Davies S J, Williams D, Williams G T, Williams E D

机构信息

Department of Pathology, University of Wales College of Medicine, Heath Park, Cardiff, UK.

出版信息

Nature. 1988 Jun 2;333(6172):461-3. doi: 10.1038/333461a0.

Abstract

Cellular mosaicism resulting from X-chromosome inactivation in heterozygous females can be shown histochemically; using this approach we have demonstrated age-related gene reactivation and tumour clonality. We now show in female mice heterozygous for reduced expression of glucose-6-phosphate dehydrogenase (G6PD) activity that colonic epithelial cells express either normal or low enzyme activity, and form patches composed of multiple crypts of uniform phenotype. We also show that a low-enzyme colonic epithelial cell phenotype can be induced in normal mice by carcinogen treatment, these cells again occur in patches, but are restricted to scattered single crypts, the frequency of which is related to treatment. A small proportion of colonic tumours in carcinogen treated normal mice are also of low-enzyme phenotype. We conclude that we have visualized the effects of a sporadic carcinogen induced somatic mutation in the G6PD gene of crypt stem cells and that a single stem cell maintains each colonic crypt. This inducible defective activity of a ubiquitous 'housekeeping' enzyme provides a somatic clonal marker system of wide potential application.

摘要

杂合子雌性中因X染色体失活导致的细胞镶嵌现象可通过组织化学方法显示;利用这种方法,我们已经证明了与年龄相关的基因重新激活和肿瘤克隆性。我们现在在葡萄糖-6-磷酸脱氢酶(G6PD)活性表达降低的杂合雌性小鼠中发现,结肠上皮细胞要么表达正常酶活性,要么表达低酶活性,并形成由多个具有统一表型的隐窝组成的斑块。我们还表明,通过致癌物处理可在正常小鼠中诱导出低酶活性的结肠上皮细胞表型,这些细胞同样以斑块形式出现,但局限于散在的单个隐窝,其频率与处理有关。在致癌物处理的正常小鼠中,一小部分结肠肿瘤也具有低酶活性表型。我们得出结论,我们已经观察到致癌物诱导的隐窝干细胞G6PD基因散发性体细胞突变的影响,并且单个干细胞维持每个结肠隐窝。这种普遍存在的“管家”酶的可诱导缺陷活性提供了一个具有广泛潜在应用的体细胞克隆标记系统。

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