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转换最小Hox反应元件的体内特异性。

Switching the in vivo specificity of a minimal Hox-responsive element.

作者信息

Chan S K, Ryoo H D, Gould A, Krumlauf R, Mann R S

机构信息

Department of Biochemistry and Molecular Biophysics, Center for Neurobiology and Behavior, Columbia University, New York, NY 10032, USA.

出版信息

Development. 1997 May;124(10):2007-14. doi: 10.1242/dev.124.10.2007.

Abstract

The homeodomain proteins encoded by the Hox complex genes do not bind DNA with high specificity. In vitro, Hox specificity can be increased by binding to DNA cooperatively with the homeodomain protein extradenticle or its vertebrate homologs, the pbx proteins (together, the PBC family). Here we show that a two basepair change in a Hox-PBC binding site switches the Hox-dependent expression pattern generated in vivo, from labial to Deformed. The change in vivo correlates with an altered Hox binding specificity in vitro. Further, we identify similar Deformed-PBC binding sites in the Deformed and Hoxb-4 genes and show that they generate Deformed or Hoxb-4 expression patterns in Drosophila and mouse embryos, respectively. These results suggest a model in which Hox-PBC binding sites play an instructive role in Hox specificity by promoting the formation of different Hox-PBC heterodimers in vivo. Thus, the choice of Hox partner, and therefore Hox target genes, depends on subtle differences between Hox-PBC binding sites.

摘要

由Hox复合基因编码的同源结构域蛋白与DNA的结合特异性不高。在体外,通过与同源结构域蛋白额外齿(extradenticle)或其脊椎动物同源物pbx蛋白(统称为PBC家族)协同结合DNA,Hox的特异性可以提高。我们在此表明,Hox-PBC结合位点中的两个碱基对变化会改变体内产生的Hox依赖性表达模式,从唇(labial)模式转变为变形(Deformed)模式。体内的这种变化与体外Hox结合特异性的改变相关。此外,我们在变形基因和Hoxb-4基因中鉴定出类似的变形-PBC结合位点,并表明它们分别在果蝇和小鼠胚胎中产生变形或Hoxb-4表达模式。这些结果提示了一个模型,其中Hox-PBC结合位点通过促进体内不同Hox-PBC异二聚体的形成,在Hox特异性方面发挥指导作用。因此,Hox伴侣的选择以及Hox靶基因的选择,取决于Hox-PBC结合位点之间的细微差异。

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