Conditional DNA repair mutants enable highly precise genome engineering | Zendy

Ákos Nyerges | Zendy; Bálint Csörgő | Zendy; István Nagy | Zendy; Dóra Latinovics | Zendy; Béla Szamecz | Zendy; György Pósfai | Zendy; Csaba Pál | Zendy

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Conditional DNA repair mutants enable highly precise genome engineering

Author(s) -

Ákos Nyerges,

Bálint Csörgő,

István Nagy,

Dóra Latinovics,

Béla Szamecz,

György Pósfai,

Csaba Pál

Publication year - 2014

Publication title -

nucleic acids research

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 9.008

H-Index - 537

eISSN - 1362-4954

pISSN - 0305-1048

DOI - 10.1093/nar/gku105

Subject(s) - biology , oligonucleotide , multiplex , dna repair , dna mismatch repair , genetics , mutant , genome , dna , genome engineering , computational biology , genome editing , gene

Oligonucleotide-mediated multiplex genome engineering is an important tool for bacterial genome editing. The efficient application of this technique requires the inactivation of the endogenous methyl-directed mismatch repair system that in turn leads to a drastically elevated genomic mutation rate and the consequent accumulation of undesired off-target mutations. Here, we present a novel strategy for mismatch repair evasion using temperature-sensitive DNA repair mutants and temporal inactivation of the mismatch repair protein complex in Escherichia coli . Our method relies on the transient suppression of DNA repair during mismatch carrying oligonucleotide integration. Using temperature-sensitive control of methyl-directed mismatch repair protein activity during multiplex genome engineering, we reduced the number of off-target mutations by 85%, concurrently maintaining highly efficient and unbiased allelic replacement.

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