A DNA
Origami Platform for Single-Pair Förster
Resonance Energy Transfer Investigation of DNA–DNA Interactions
and Ligation
Posted on 2020-01-02 - 19:33
DNA double-strand breaks (DSBs) pose
an everyday threat to the
conservation of genetic information and therefore life itself. Several
pathways have evolved to repair these cytotoxic lesions by rejoining
broken ends, among them the nonhomologous end-joining mechanism that
utilizes a DNA ligase. Here, we use a custom-designed DNA origami
nanostructure as a model system to specifically mimic a DNA DSB, enabling
us to study the end-joining of two fluorescently labeled DNA with
the T4 DNA ligase on the single-molecule level. The ligation reaction
is monitored by Förster resonance energy transfer (FRET) experiments
both in solution and on surface-anchored origamis. Due to the modularity
of DNA nanotechnology, DNA double strands with different complementary
overhang lengths can be studied using the same DNA origami design.
We show that the T4 DNA ligase repairs sticky ends more efficiently
than blunt ends and that the ligation efficiency is influenced by
both DNA sequence and the incubation conditions. Before ligation,
dynamic fluctuations of the FRET signal are observed due to transient
binding of the sticky overhangs. After ligation, the FRET signal becomes
static. Thus, we can directly monitor the ligation reaction through
the transition from dynamic to static FRET signals. Finally, we revert
the ligation process using a restriction enzyme digestion and religate
the resulting blunt ends. The here-presented DNA origami platform
is thus suited to study complex multistep reactions occurring over
several cycles of enzymatic treatment.
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Bartnik, Kira; Barth, Anders; Pilo-Pais, Mauricio; Crevenna, Alvaro H.; Liedl, Tim; Lamb, Don C. (2019). A DNA
Origami Platform for Single-Pair Förster
Resonance Energy Transfer Investigation of DNA–DNA Interactions
and Ligation. ACS Publications. Collection. https://doi.org/10.1021/jacs.9b09093