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Cooperative binding of Sox10 to DNA: requirements and consequences

机译:Sox10与DNA的合作结合:要求和后果

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摘要

The high-mobility-group (HMG) domain containing transcription factor Sox10 is an important regulator of various processes including the development of neural crest cells and glial cells. Target gene promoters contain multiple Sox10-binding sites, which either support monomeric or cooperative, dimeric binding. The latter is unusual for Sox proteins and might contribute to functional specificity of Sox10. We find that specific amino acid residues in a conserved region immediately preceding the HMG domain of Sox10 are required for cooperative binding. These residues cooperate with the HMG domain during dimeric binding in a manner dependent on specific determinants within the first two α-helices of the HMG domain. Cooperativity of DNA binding is surprisingly refractory to changes in the overall conformation of the DNA-bound dimer. Whereas maintenance of cooperativity is essential for full activation of the promoter of the myelin protein zero target gene, dimer-dependent conformational changes such as the exact bending angle introduced into the promoter appear to be less important, shedding new light on the architectural function of Sox proteins.
机译:包含转录因子Sox10的高迁移率族(HMG)域是包括神经c细胞和神经胶质细胞在内的各种过程的重要调节剂。靶基因启动子包含多个Sox10结合位点,它们支持单体或合作的二聚体结合。后者对于Sox蛋白而言是不寻常的,可能有助于Sox10的功能特异性。我们发现,紧接在Sox10的HMG域之前的保守区域中的特定氨基酸残基是协同结合所必需的。这些残基在二聚体结合期间以取决于HMG结构域的前两个α-螺旋内的特定决定簇的方式与HMG结构域协同作用。令人惊讶的是,DNA结合的协同作用使结合DNA的二聚体的整体构象发生变化。尽管维持协同性对于髓磷脂蛋白零靶基因启动子的完全激活是必不可少的,但二聚体依赖性构象变化(例如引入启动子的确切弯曲角度)似乎不那么重要,这为Sox的结构功能提供了新的亮点蛋白质。

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