Ma Jianbing, Xu Chunhua, Li Jinghua, Hou Xi-Miao, Da Lin-Tai, Jia Qi, Huang Xingyuan, Yu Jin, Xi Xuguang, Lu Ying, Li Ming
Songshan Lake Materials Laboratory, Dongguan, Guangdong 523808, China.
Beijing National Laboratory for Condensed Matter Physics, Institute of Physics, Chinese Academy of Sciences, Beijing 100190, China.
iScience. 2021 Dec 10;25(1):103606. doi: 10.1016/j.isci.2021.103606. eCollection 2022 Jan 21.
The RecQ family of helicases are important for maintenance of genomic integrity. Although functions of constructive subdomains of this family of helicases have been extensively studied, the helical hairpin (HH) in the RecQ-C-terminal domain (RQC) has been underappreciated and remains poorly understood. Here by using single-molecule fluorescence resonance energy transfer, we found that HH in the human BLM transiently intercepts different numbers of nucleotides when it is unwinding a double-stranded DNA. Single-site mutations in HH that disrupt hydrogen bonds and/or salt bridges between DNA and HH change the DNA binding conformations and the unwinding features significantly. Our results, together with recent clinical tests that correlate single-site mutations in HH of human BLM with the phenotype of cancer-predisposing syndrome or Bloom's syndrome, implicate pivotal roles of HH in BLM's DNA unwinding activity. Similar mechanisms might also apply to other RecQ family helicases, calling for more attention to the RQC helical hairpin.
解旋酶RecQ家族对于维持基因组完整性至关重要。尽管对该家族解旋酶的结构亚域功能已进行了广泛研究,但RecQ C末端结构域(RQC)中的螺旋发夹(HH)一直未得到充分重视,人们对其了解仍然很少。在此,我们通过单分子荧光共振能量转移发现,人类BLM中的HH在解旋双链DNA时会短暂拦截不同数量的核苷酸。HH中破坏DNA与HH之间氢键和/或盐桥的单点突变会显著改变DNA结合构象和解旋特征。我们的结果,连同最近将人类BLM的HH中的单点突变与癌症易感综合征或布卢姆综合征的表型相关联的临床试验,表明HH在BLM的DNA解旋活性中起关键作用。类似的机制可能也适用于其他RecQ家族解旋酶,这需要更多地关注RQC螺旋发夹。
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