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发育控制基因和疾病基因在胚胎表达模式上的人与小鼠差异。

Human-mouse differences in the embryonic expression patterns of developmental control genes and disease genes.

作者信息

Fougerousse F, Bullen P, Herasse M, Lindsay S, Richard I, Wilson D, Suel L, Durand M, Robson S, Abitbol M, Beckmann J S, Strachan T

机构信息

URA-CNRS 1922-Généthon, 1 rue de l'Internationale, BP 60, 91002 Evry, France.

出版信息

Hum Mol Genet. 2000 Jan 22;9(2):165-73. doi: 10.1093/hmg/9.2.165.

Abstract

Our understanding of early human development has been impeded by the general difficulty in obtaining suitable samples for study. As a result, and because of the extraordinarily high degree of evolutionary conservation of many developmentally important genes and developmental pathways, great reliance has been placed on extrapolation from animal models of development, principally the mouse. However, the strong evolutionary conservation of coding sequence for developmentally important genes does not necessarily mean that their expression patterns are as highly conserved. The very recent availability of human embryonic samples for gene expression studies has now permitted for the first time an assessment of the degree to which we can confidently extrapolate from studies of rodent gene expression patterns. We have found significant human-mouse differences in embryonic expression patterns for a variety of genes. We present detailed data for two illustrative examples. Wnt7a, a very highly conserved gene known to be important in early development, shows significant differences in spatial and temporal expression patterns in the developing brain (midbrain, telencephalon) of man and mice. CAPN3, the locus for LGMD2A limb girdle muscular dystrophy, and its mouse orthologue differ extensively in expression in embryonic heart, lens and smooth muscle. Our study also shows how molecular analyses, while providing explanations for the observed differences, can be important in providing insights into mammalian evolution.

摘要

获取合适的研究样本存在普遍困难,这阻碍了我们对人类早期发育的理解。因此,由于许多对发育至关重要的基因和发育途径具有高度的进化保守性,人们高度依赖从发育动物模型(主要是小鼠)进行推断。然而,对发育重要基因的编码序列具有强烈的进化保守性,并不一定意味着它们的表达模式也高度保守。最近人类胚胎样本可用于基因表达研究,这首次使得我们能够评估从啮齿动物基因表达模式研究中进行可靠推断的程度。我们发现多种基因在胚胎表达模式上存在显著的人类 - 小鼠差异。我们给出两个说明性例子的详细数据。Wnt7a是一个在早期发育中非常重要的高度保守基因,在人类和小鼠发育中的大脑(中脑、端脑)的空间和时间表达模式上存在显著差异。CAPN3是肢带型肌营养不良2A型(LGMD2A)的基因座,其在胚胎心脏、晶状体和平滑肌中的表达与小鼠直系同源基因有很大差异。我们的研究还表明,分子分析在为观察到的差异提供解释的同时,对于深入了解哺乳动物进化也很重要。

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