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Id蛋白与碱性螺旋-环-螺旋转录因子的差异相互作用。

Differential interactions of Id proteins with basic-helix-loop-helix transcription factors.

作者信息

Langlands K, Yin X, Anand G, Prochownik E V

机构信息

Section of Hematology/Oncology, Children's Hospital of Pittsburgh, The, Pittsburgh, Pennsylvania 15213, USA.

出版信息

J Biol Chem. 1997 Aug 8;272(32):19785-93. doi: 10.1074/jbc.272.32.19785.

Abstract

Dimerization of three Id proteins (Id1, Id2, and Id3) with the four class A E proteins (E12, E47, E2-2, and HEB) and two groups of class B proteins, the myogenic regulatory factors (MRFs: MyoD, myogenin, Myf-5 and MRF4/Myf-6), and the hematopoietic factors (Scl/Tal-1, Tal-2, and Lyl-1) were tested in a quantitative yeast 2-hybrid assay. All three Ids bound with high affinity to E proteins, but a much broader range of interactions was observed between Ids and the class B factors. Id1 and Id2 interacted strongly with MyoD and Myf-5 and weakly with myogenin and MRF4/Myf-6, whereas Id3 interacted weakly with all four MRFs. Similar specificities were observed in co-immunoprecipitation and mammalian 2-hybrid analyses. No interactions were found between the Ids and any of the hematopoietic factors. Each Id was able to disrupt the ability of E protein-MyoD complexes to transactivate from a muscle creatine kinase reporter construct in vivo. Finally, mutagenesis experiments showed that the differences between Id1 and Id3 binding map to three amino acids in the first helix and to a small cluster of upstream residues. The Id proteins thus display a signature range of interactions with all of their potential dimerization partners and may play a role in myogenesis which is distinct from that in hematopoiesis.

摘要

在定量酵母双杂交试验中,检测了三种Id蛋白(Id1、Id2和Id3)与四种A类E蛋白(E12、E47、E2-2和HEB)以及两组B类蛋白,即生肌调节因子(MRFs:MyoD、肌细胞生成素、Myf-5和MRF4/Myf-6)和造血因子(Scl/Tal-1、Tal-2和Lyl-1)的二聚化情况。所有三种Id蛋白都与E蛋白高亲和力结合,但在Id蛋白与B类因子之间观察到了更广泛的相互作用。Id1和Id2与MyoD和Myf-5强烈相互作用,与肌细胞生成素和MRF4/Myf-6弱相互作用,而Id3与所有四种MRF弱相互作用。在共免疫沉淀和哺乳动物双杂交分析中也观察到了类似的特异性。未发现Id蛋白与任何造血因子之间存在相互作用。每种Id蛋白都能够在体内破坏E蛋白-MyoD复合物从肌肉肌酸激酶报告基因构建体中转录激活的能力。最后,诱变实验表明,Id1和Id3结合的差异映射到第一个螺旋中的三个氨基酸以及一小簇上游残基。因此,Id蛋白与其所有潜在二聚化伙伴之间呈现出一系列独特的相互作用,并且可能在成肌过程中发挥与造血过程不同的作用。

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