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首页> 外文期刊>Histochemistry and cell biology >Use of dual section mRNA in situ hybridisation/immunohistochemistry to clarify gene expression patterns during the early stages of nephron development in the embryo and in the mature nephron of the adult mouse kidney.
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Use of dual section mRNA in situ hybridisation/immunohistochemistry to clarify gene expression patterns during the early stages of nephron development in the embryo and in the mature nephron of the adult mouse kidney.

机译:使用双节mRNA原位杂交/免疫组织化学来阐明在成年小鼠肾脏的胚胎和成熟肾单位中的肾单位发育的早期阶段的基因表达模式。

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摘要

The kidney is the most complex organ within the urogenital system. The adult mouse kidney contains in excess of 8,000 mature nephrons, each of which can be subdivided into a renal corpuscle and 14 distinct tubular segments. The histological complexity of this organ can make the clarification of the site of gene expression by in situ hybridisation difficult. We have defined a panel of seven antibodies capable of identifying the six stages of early nephron development, the tubular nephron segments and the components of the renal corpuscle within the embryonic and adult mouse kidney. We have analysed in detail the protein expression of Wt1, Calb1 Aqp1, Aqp2 and Umod using these antibodies. We have then coupled immunohistochemistry with RNA in situ hybridisation in order to precisely identify the expression pattern of different genes, including Wnt4, Umod and Spp1. This technique will be invaluable for examining at high resolution, the structure of both the developing and mature nephron where standard in situ hybridisation and histological techniques are insufficient. The use of this technique will enhance the expression analyses of genes which may be involved in nephron formation and the function of the mature nephron in the mouse.
机译:肾脏是泌尿生殖系统中最复杂的器官。成年小鼠肾脏包含超过8,000个成熟肾单位,每个成熟肾单位可细分为肾小体和14个不同的肾小管节段。该器官的组织学复杂性使得通过原位杂交难以阐明基因表达的位点。我们定义了一组七种抗体,可以识别早期肾单位发育的六个阶段,肾小管肾节段以及胚胎和成年小鼠肾脏内肾小体的成分。我们已经使用这些抗体详细分析了Wt1,Calb1 Aqp1,Aqp2和Umod的蛋白质表达。然后,我们将免疫组织化学与RNA原位杂交相结合,以精确鉴定包括Wnt4,Umod和Spp1在内的不同基因的表达模式。该技术对于高分辨率检测发育中的和成熟的肾单位的结构将是无价的,而标准的原位杂交和组织学技术不足。该技术的使用将增强可能与肾单位的形成和小鼠中成熟肾单位的功能有关的基因的表达分析。

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