Large dataset enables prediction of repair after CRISPR–Cas9 editing in primary T cells

Ryan T. Leenay,Amirali Aghazadeh,Joseph B. Hiatt,David Tse,Theodore L. Roth,Ryan Apathy,Eric Shifrut,Judd F. Hultquist,Nevan J. Krogan,Zhenqin Wu,Giana Cirolia,Hera Canaj,Manuel D. Leonetti,Alexander Marson,Andrew P. May,James Zou

Large dataset enables prediction of repair after CRISPR–Cas9 editing in primary T cells

2019

Ryan T. Leenay
Amirali Aghazadeh
Joseph B. Hiatt
David Tse
Theodore L. Roth
Ryan Apathy
Eric Shifrut
Judd F. Hultquist
Nevan J. Krogan
Zhenqin Wu
Giana Cirolia
Hera Canaj
Manuel D. Leonetti
Alexander Marson
Andrew P. May
James Zou

Understanding of repair outcomes after Cas9-induced DNA cleavage is still limited, especially in primary human cells. We sequence repair outcomes at 1,656 on-target genomic sites in primary human T cells and use these data to train a machine learning model, which we have called CRISPR Repair Outcome (SPROUT). SPROUT accurately predicts the length, probability and sequence of nucleotide insertions and deletions, and will facilitate design of SpCas9 guide RNAs in therapeutically important primary human cells.

Keywords:

Molecular biology
Computational biology
DNA
CRISPR
Guide RNA
Cleavage (embryo)
Biology
dna cleavage

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