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Indispensable function for embryogenesis, expression and regulation of the nonspecific form of the 5-aminolevulinate synthase gene in mouse

机译:小鼠胚胎发生,表达和调节5-氨基乙酰丙酸合酶基因非特异性形式的必不可少的功能

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摘要

The first step of heme biosynthesis in animals is catalyzed by 5-aminolevulinate synthase (ALAS), which controls heme supply in various tissues. To clarify the roles that the nonspecific isoform of ALAS (ALAS-N) plays in vivo, we prepared a green fluorescent protein (GFP) knock-in mouse line in which the Alas1 gene (encoding ALAS-N) is replaced with a gfp gene. We found that mice bearing a homozygous knock-in allele (Alas1GFP/GFP) were lethal by embryonic day 8.5, demonstrating that ALAS-N is essential for early embryogenesis. Fluorescence microscopic and flow cytometric analyses of heterozygous mouse (Alas1+/GFP) tissues showed that the Alas1 expression level differs substantially in tissues; Alas1 is highly expressed in testis Leydig cells, exocrine glands (including submandibular and parotid glands), endocrine glands (such as adrenal and thyroid glands) and hematopoietic lineage cells (including neutrophils and eosinophils). Quantitative analyses of GFP mRNA and ALAS-N mRNA in various tissues of Alas1+/GFP mice suggested that the destabilization of ALAS-N mRNA was not uniform in the various tissues. These results thus lay bare that elaborate control of the endogenous heme supply operates in various mouse tissues through regulation of the ALAS-N expression level and that this control is essential for heme homeostasis in animals.
机译:动物中血红素生物合成的第一步是由5-氨基乙酰丙酸合酶(ALAS)催化,该酶控制各种组织中的血红素供应。为了阐明ALAS(ALAS-N)的非特异性同种型在体内的作用,我们制备了绿色荧光蛋白(GFP)敲入小鼠品系,其中Alas1基因(编码ALAS-N)被gfp基因取代。我们发现携带纯合敲入等位基因(Alas1GFP / GFP)的小鼠在胚胎第8.5天时已致死,表明ALAS-N对早期胚胎发生至关重要。杂合小鼠(Alas1 + / GFP)组织的荧光显微镜和流式细胞仪分析表明,Alas1表达水平在组织中存在显着差异。 Alas1在睾丸Leydig细胞,外分泌腺(包括颌下腺和腮腺),内分泌腺(例如肾上腺和甲状腺)和造血谱系细胞(包括中性粒细胞和嗜酸性粒细胞)中高表达。对Alas1 + / GFP小鼠各种组织中GFP mRNA和ALAS-N mRNA的定量分析表明,在各种组织中ALAS-N mRNA的去稳定作用并不均匀。因此,这些结果揭示了对内源性血红素供应的精细控制通过调节ALAS-N表达水平而在各种小鼠组织中起作用,并且这种控制对于动物体内的血红素稳态是必不可少的。

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