Generation of a set of isogenic iPSC lines carrying all APOE genetic variants (Ɛ2/Ɛ3/Ɛ4) and knock-out for the study of APOE biology in health and disease

Benjamin Schmid,Bjørn Holst,Christian Clausen,Lamiaa Bahnassawy,Peter Reinhardt,Margot H. M. Bakker,Eva Díaz-Guerra,Carlos Vicario,Pamela V. Martino Adami,Michaela Thoenes,Alfredo Ramirez,Klaus Flissbach,Clara Grezella,Oliver Brüstle,Michael Peitz,Andreas Ebneth,Alfredo Cabrera-Socorro

Generation of a set of isogenic iPSC lines carrying all APOE genetic variants (Ɛ2/Ɛ3/Ɛ4) and knock-out for the study of APOE biology in health and disease

2021

Benjamin Schmid
Bjørn Holst
Christian Clausen
Lamiaa Bahnassawy
Peter Reinhardt
Margot H. M. Bakker
Eva Díaz-Guerra
Carlos Vicario
Pamela V. Martino Adami
Michaela Thoenes
Alfredo Ramirez
Klaus Flissbach
Clara Grezella
Oliver Brüstle
Michael Peitz
Andreas Ebneth
Alfredo Cabrera-Socorro

APOE genotype is the strongest genetic risk factor for Alzheimer's Disease (AD). The low degree of homology between mouse and human APOE is a concerning issue in preclinical models currently used to study the role of this gene in AD pathophysiology. A key objective of ADAPTED (Alzheimer's Disease Apolipoprotein Pathology for Treatment Elucidation and Development) project was to generate in vitro models that better recapitulate human APOE biology. We describe a new set of induced pluripotent stem cells (iPSC) lines carrying common APOE variants (Ɛ2, Ɛ3, and Ɛ3/Ɛ4) and a knock-out isogenic to the parental APOE Ɛ4/Ɛ4 line (UKBi011-A).

Keywords:

Induced pluripotent stem cell
Genetics
Disease
Genotype
Apolipoprotein B
Apolipoprotein E
Homology (biology)
Gene
In vitro
Biology

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