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Transcriptional activation by mitochondrial transcription factor A involves preferential distortion of promoter DNA

机译:线粒体转录因子A的转录激活涉及启动子DNA的优先变形

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Mitochondrial transcription factor A (mtTFA/TFAM) is a nucleus-encoded, high-mobility-group-box (HMG-box) protein that regulates transcription of the mitochondrial genome by specifically recognizing light-strand and heavy-strand promoters (LSP, HSP1). TFAM also binds mitochondrial DNA in a non-sequence specific (NSS) fashion and facilitates its packaging into nucleoid structures. However, the requirement and contribution of DNA-bending for these two different binding modes has not been addressed in detail, which prompted this comparison of binding and bending properties of TFAM on promoter and non-promoter DNA. Promoter DNA increased the stability of TFAM to a greater degree than non-promoter DNA. However, the thermodynamic properties of DNA binding for TFAM with promoter and non-specific (NS) DNA were similar to each other and to other NSS HMG-box proteins. Fluorescence resonance energy transfer assays showed that TFAM bends promoter DNA to a greater degree than NS DNA. In contrast, TFAM lacking the C-terminal tail distorted both promoter and non-promoter DNA to a significantly reduced degree, corresponding with markedly decreased transcriptional activation capacity at LSP and HSP1 in vitro. Thus, the enhanced bending of promoter DNA imparted by the C-terminal tail is a critical component of the ability of TFAM to activate promoter-specific initiation by the core mitochondrial transcription machinery.
机译:线粒体转录因子A(mtTFA / TFAM)是一种核编码的高迁移率族盒(HMG-box)蛋白,可通过特异性识别轻链和重链启动子(LSP,HSP1)来调节线粒体基因组的转录)。 TFAM还以非序列特异性(NSS)方式结合线粒体DNA,并有助于将其包装成类核苷酸结构。但是,对于这两种不同的结合模式,DNA弯曲的要求和贡献尚未得到详细解决,这促使TFAM在启动子和非启动子DNA上的结合和弯曲特性进行了比较。启动子DNA比非启动子DNA更大程度地提高了TFAM的稳定性。但是,与启动子和非特异性(NS)DNA结合TFAM的DNA的热力学性质彼此相似,并且与其他NSS HMG-box蛋白相似。荧光共振能量转移试验表明,TFAM比NS DNA弯曲启动子DNA的程度更大。相比之下,缺乏C末端尾巴的TFAM使启动子和非启动子DNA畸变的程度都大大降低,这与LSP和HSP1在体外的转录激活能力明显降低有关。因此,由C末端尾部赋予的启动子DNA弯曲的增强是TFAM通过核心线粒体转录机制激活启动子特异性起始的能力的关键组成部分。

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