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原位杂交显示,在最早的小鼠红细胞祖细胞中,胚胎型和成体型α珠蛋白基因共表达。

In situ hybridization reveals co-expression of embryonic and adult alpha globin genes in the earliest murine erythrocyte progenitors.

作者信息

Leder A, Kuo A, Shen M M, Leder P

机构信息

Department of Genetics, Harvard Medical School, Boston, MA.

出版信息

Development. 1992 Dec;116(4):1041-9. doi: 10.1242/dev.116.4.1041.

Abstract

Murine erythropoiesis begins with the formation of primitive red blood cells in the blood islands of the embryonic yolk sac on day 7.5 of gestation. By analogy to human erythropoiesis, it has been thought that there is a gradual switch from the exclusive expression of the embryonic alpha-like globin (zeta) to the mature adult form (alpha) in these early mouse cells. We have used in situ hybridization to assess expression of these two globin genes during embryonic development. In contrast to what might have been expected, we find that there is simultaneous expression of both zeta and alpha genes from the very onset of erythropoiesis in the yolk sac. At no time could we detect expression of embryonic zeta globin mRNA without concomitant expression of adult alpha globin mRNA. Indeed, adult alpha transcripts exceed those of embryonic zeta in the earliest red cell precursors. Moreover, the pattern of hybridization reveals co-expression of both genes within the same cells. Even in the fetal liver, which supersedes the yolk sac as the major site of murine fetal erythropoiesis, there is a brief co-expression of zeta and alpha genes followed by the exclusive expression of the adult alpha genes. These data indicate an important difference in hematopoietic ontogeny between mouse and that of human, where zeta expression precedes that of alpha. In addition to resolving the embryonic expression of these globin genes, our results suggest that the embryonic alpha-like globin gene zeta may be physiologically redundant, even during the earliest stages of embryonic development.

摘要

小鼠红细胞生成始于妊娠第7.5天胚胎卵黄囊血岛中原始红细胞的形成。类比人类红细胞生成过程,人们一直认为在这些早期小鼠细胞中,会逐渐从仅表达胚胎型α样珠蛋白(ζ)转变为表达成熟的成人型(α)。我们利用原位杂交技术评估了这两种珠蛋白基因在胚胎发育过程中的表达情况。与预期相反,我们发现从卵黄囊中红细胞生成刚开始时,ζ和α基因就同时表达。在任何时候,我们都检测不到仅表达胚胎型ζ珠蛋白mRNA而不伴随成人型α珠蛋白mRNA表达的情况。实际上,在最早的红细胞前体细胞中,成人型α转录本的数量超过胚胎型ζ转录本。此外,杂交模式显示这两个基因在同一细胞中共表达。即使在取代卵黄囊成为小鼠胎儿红细胞生成主要部位的胎儿肝脏中,ζ和α基因也会短暂共表达,随后成人型α基因单独表达。这些数据表明小鼠和人类在造血个体发生上存在重要差异,在人类中ζ的表达先于α。除了解决这些珠蛋白基因的胚胎期表达问题,我们的结果还表明,即使在胚胎发育的最早阶段,胚胎型α样珠蛋白基因ζ在生理上可能也是多余的。

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