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Inhibition of DNA synthesis facilitates expansion of low-complexity repeats Is strand slippage stimulated by transient local depletion of specific dNTPs?

机译:DNA合成的抑制促进低复杂度重复序列的扩展特定dNTP的瞬时局部消耗是否刺激了链的滑动?

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Simple DNA repeats (trinucleotide repeats, micro- and minisatellites) are prone to expansion/contraction via formation of secondary structures during DNA synthesis. Such structures both inhibit replication forks and create opportunities for template-primer slippage, making these repeats unstable. Certain aspects of simple repeat instability, however, suggest additional mechanisms of replication inhibition dependent on the primary DNA sequence, rather than on secondary structure formation. I argue that expanded simple repeats, due to their lower DNA complexity, should transiently inhibit DNA synthesis by locally depleting specific DNA precursors. Such transient inhibition would promote formation of secondary structures and would stabilize these structures, facilitating strand slippage. Thus, replication problems at simple repeats could be explained by potentiated toxicity, where the secondary structure-driven repeat instability is enhanced by DNA polymerase stalling at the low complexity template DNA. This minireview is dedicated to the FASEB-2012 meeting Dynamic DNA Structures in Biology, organized by Nancy Maizels and Sergei Mirkin.
机译:简单的DNA重复序列(三核苷酸重复序列,微卫星和微型卫星)在DNA合成过程中会通过形成二级结构而易于扩展/收缩。这样的结构既抑制了复制叉,又为模板引物滑动创造了机会,使这些重复变得不稳定。但是,简单重复不稳定性的某些方面表明复制抑制的其他机制取决于一级DNA序列,而不是二级结构的形成。我认为扩展的简单重复序列由于其较低的DNA复杂性,应该通过局部消耗特定的DNA前体来暂时抑制DNA合成。这种瞬时抑制将促进二级结构的形成并且将稳定这些结构,从而促进链滑动。因此,简单重复的复制问题可以用增强的毒性来解释,其中二级结构驱动的重复不稳定性通过低复杂度模板DNA上的DNA聚合酶停滞而增强。这份小型回顾会议专门讨论了由Nancy Maizels和Sergei Mirkin组织的FASEB-2012会议生物学动态DNA结构。

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