Kent Tatiana, Chandramouly Gurushankar, McDevitt Shane Michael, Ozdemir Ahmet Y, Pomerantz Richard T
1] Fels Institute for Cancer Research and Molecular Biology, Temple University School of Medicine, Philadelphia, Pennsylvania, USA. [2] Department of Biochemistry, Temple University School of Medicine, Philadelphia, Pennsylvania, USA.
Nat Struct Mol Biol. 2015 Mar;22(3):230-7. doi: 10.1038/nsmb.2961. Epub 2015 Feb 2.
Microhomology-mediated end-joining (MMEJ) is an error-prone alternative double-strand break-repair pathway that uses sequence microhomology to recombine broken DNA. Although MMEJ has been implicated in cancer development, the mechanism of this pathway is unknown. We demonstrate that purified human DNA polymerase θ (Polθ) performs MMEJ of DNA containing 3' single-strand DNA overhangs with ≥2 bp of homology, including DNA modeled after telomeres, and show that MMEJ is dependent on Polθ in human cells. Our data support a mechanism whereby Polθ facilitates end-joining and microhomology annealing, then uses the opposing overhang as a template in trans to stabilize the DNA synapse. Polθ exhibits a preference for DNA containing a 5'-terminal phosphate, similarly to polymerases involved in nonhomologous end-joining. Finally, we identify a conserved loop domain that is essential for MMEJ and higher-order structures of Polθ that probably promote DNA synapse formation.
微同源性介导的末端连接(MMEJ)是一种易错的双链断裂修复替代途径,它利用序列微同源性来重组断裂的DNA。尽管MMEJ与癌症发展有关,但其途径机制尚不清楚。我们证明,纯化的人类DNA聚合酶θ(Polθ)可对含有3'单链DNA突出端且具有≥2个碱基对同源性的DNA进行MMEJ,包括以端粒为模型的DNA,并表明MMEJ在人类细胞中依赖于Polθ。我们的数据支持一种机制,即Polθ促进末端连接和微同源性退火,然后以反义突出端作为反式模板来稳定DNA突触。与参与非同源末端连接的聚合酶类似,Polθ对含有5'末端磷酸的DNA表现出偏好。最后,我们鉴定出一个保守的环结构域,它对于MMEJ以及可能促进DNA突触形成的Polθ高阶结构至关重要。
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