Generation of a set of isogenic, gene-edited iPSC lines homozygous for all main APOE variants and an APOE knock-out line

Benjamin Schmid,Kennie R. Prehn,Natakarn Nimsanor,Blanca Irene Aldana Garcia,Ulla B. Poulsen,Ida Jørring,Mikkel A. Rasmussen,Christian Clausen,Ulrike A. Mau-Holzmann,Sarayu Ramakrishna,Ravi Sondekoppa Muddashetty,Rachel Steeg,Kevin Bruce,Peter Mackintosh,Andreas Ebneth,Bjørn Holst,Alfredo Cabrera-Socorro

Generation of a set of isogenic, gene-edited iPSC lines homozygous for all main APOE variants and an APOE knock-out line

2019

Benjamin Schmid
Kennie R. Prehn
Natakarn Nimsanor
Blanca Irene Aldana Garcia
Ulla B. Poulsen
Ida Jørring
Mikkel A. Rasmussen
Christian Clausen
Ulrike A. Mau-Holzmann
Sarayu Ramakrishna
Ravi Sondekoppa Muddashetty
Rachel Steeg
Kevin Bruce
Peter Mackintosh
Andreas Ebneth
Bjørn Holst
Alfredo Cabrera-Socorro

Abstract Alzheimer's disease (AD) is the most frequent neurodegenerative disease amongst the elderly. The SNPs rs429358 and rs7412 in the APOE gene are the most common risk factor for sporadic AD, and there are three different alleles commonly referred to as APOE-e2, APOE-e3 and APOE-e4. Induced pluripotent stem cells (iPSCs) hold great promise to model AD as such cells can be differentiated in vitro to the required cell type. Here we report the use of CRISPR/Cas9 technology employed on iPSCs from a healthy individual with an APOE-e3/e4 genotype to obtain isogenic APOE-e2/e2, APOE-e3/e3, APOE-e4/e4 lines as well as an APOE-knock-out line.

Keywords:

CRISPR
Genetics
Induced pluripotent stem cell
Cas9
Apolipoprotein E
Genotype
Gene
Allele
Single-nucleotide polymorphism
Biology
Cell type

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