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首页> 外文期刊>Genes and Development: a Journal Devoted to the Molecular Analysis of Gene Expression in Eukaryotes, Prokaryotes, and Viruses >Long-range spreading of dosage compensation in Drosophila captures transcribed autosomal genes inserted on X.
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Long-range spreading of dosage compensation in Drosophila captures transcribed autosomal genes inserted on X.

机译:在果蝇中剂量补偿的远程传播捕获了插入X上的转录的常染色体基因。

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摘要

Dosage compensation in Drosophila melanogaster males is achieved via targeting of male-specific lethal (MSL) complex to X-linked genes. This is proposed to involve sequence-specific recognition of the X at approximately 150-300 chromatin entry sites, and subsequent spreading to active genes. Here we ask whether the spreading step requires transcription and is sequence-independent. We find that MSL complex binds, acetylates, and up-regulates autosomal genes inserted on X, but only if transcriptionally active. We conclude that a long-sought specific DNA sequence within X-linked genes is not obligatory for MSL binding. Instead, linkage and transcription play the pivotal roles in MSL targeting irrespective of gene origin and DNA sequence.
机译:果蝇果蝇雄性的剂量补偿是通过将雄性特异性致死(MSL)复合物靶向X连锁基因来实现的。提出这涉及在约150-300个染色质进入位点处对X进行序列特异性识别,并随后传播至活性基因。在这里,我们询问扩展步骤是否需要转录并且是否与序列无关。我们发现,MSL复合物结合,乙酰化并上调插入X的常染色体基因,但仅在转录活跃的情况下。我们得出的结论是,X连锁基因内长期寻求的特定DNA序列对于MSL结合不是必须的。取而代之的是,链接和转录在MSL靶向中起着关键作用,而与基因来源和DNA序列无关。

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