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四种人类肌肉调节性螺旋-环-螺旋蛋白Myf3-Myf6表现出相似的异源二聚化和DNA结合特性。

The four human muscle regulatory helix-loop-helix proteins Myf3-Myf6 exhibit similar hetero-dimerization and DNA binding properties.

作者信息

Braun T, Arnold H H

机构信息

Department of Toxicology, Medical School, University of Hamburg, FRG.

出版信息

Nucleic Acids Res. 1991 Oct 25;19(20):5645-51. doi: 10.1093/nar/19.20.5645.

Abstract

The muscle regulatory proteins Myf3, Myf4, Myf5, and Myf6 share a highly conserved DNA binding and dimerization domain consisting of a cluster of basic amino acids and a potential helix-loop-helix structure. Here we demonstrate that the four human muscle-specific HLH proteins have similar DNA binding and dimerization properties. The members of this family form protein complexes of comparable stability with the ubiquitously expressed HLH proteins E12, E2-2, and E2-5 and bind to the conserved DNA sequence CANNTG designated as E-box with similar efficiency in vitro. The binding affinities of the various complexes are greatly influenced by the variable internal and flanking nucleotides of the consensus motif. Combinations of Myf proteins with one another and with lyl-1, and HLH protein from human T cells, do not bind to DNA in vitro. Our results suggest that combinatorial associations of the various tissue-specific and more widely expressed HLH factors do not result in differential recognition of DNA sequences by Myf proteins.

摘要

肌肉调节蛋白Myf3、Myf4、Myf5和Myf6共享一个高度保守的DNA结合和二聚化结构域,该结构域由一簇碱性氨基酸和一个潜在的螺旋-环-螺旋结构组成。在此我们证明,这四种人类肌肉特异性HLH蛋白具有相似的DNA结合和二聚化特性。该家族成员与普遍表达的HLH蛋白E12、E2-2和E2-5形成稳定性相当的蛋白复合物,并在体外以相似的效率结合到保守的DNA序列CANNTG(称为E盒)上。各种复合物的结合亲和力受到共有基序可变的内部和侧翼核苷酸的极大影响。Myf蛋白彼此之间以及与lyl-1(一种来自人类T细胞的HLH蛋白)的组合在体外不与DNA结合。我们的结果表明,各种组织特异性和更广泛表达的HLH因子的组合关联不会导致Myf蛋白对DNA序列的差异识别。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4479/328970/fd66982bff1a/nar00100-0168-a.jpg

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