Wells Robert D
Center for Genome Research, Institute of Biosciences and Technology, Texas A&M University System Health Science Center, Texas Medical Center, 2121 West Holcombe Boulevard, Houston, TX 77030-3303, USA.
Trends Biochem Sci. 2007 Jun;32(6):271-8. doi: 10.1016/j.tibs.2007.04.003. Epub 2007 May 9.
Recent discoveries have revealed that simple repeating DNA sequences, which are known to adopt non-B DNA conformations (such as triplexes, cruciforms, slipped structures, left-handed Z-DNA and tetraplexes), are mutagenic. The mutagenesis is due to the non-B DNA conformation rather than to the DNA sequence per se in the orthodox right-handed Watson-Crick B-form. The human genetic consequences of these non-B structures are approximately 20 neurological diseases, approximately 50 genomic disorders (caused by gross deletions, inversions, duplications and translocations), and several psychiatric diseases involving polymorphisms in simple repeating sequences. Thus, the convergence of biochemical, genetic and genomic studies has demonstrated a new paradigm implicating the non-B DNA conformations as the mutagenesis specificity determinants, not the sequences as such.
最近的发现表明,已知能形成非B型DNA构象(如三链体、十字形、滑移结构、左手Z-DNA和四链体)的简单重复DNA序列具有致突变性。这种诱变作用是由于非B型DNA构象,而非正统右手沃森-克里克B型中的DNA序列本身。这些非B型结构对人类遗传的影响包括约20种神经疾病、约50种基因组疾病(由大片段缺失、倒位、重复和易位引起)以及几种涉及简单重复序列多态性的精神疾病。因此,生物化学、遗传学和基因组学研究的融合证明了一种新的范式,即非B型DNA构象是诱变特异性的决定因素,而非序列本身。
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