Generation of gene edited hiPSC from familial Alzheimer's disease patient carrying N141I missense mutation in presenilin 2

Hany E. Marei; Asmaa Althani; Nahla Afifi; Anwarul Hasan; Thomas Caceci; Giacomo Pozzoli; Carlo Cenciarelli

doi:10.1016/j.scr.2021.102552

Generation of gene edited hiPSC from familial Alzheimer's disease patient carrying N141I missense mutation in presenilin 2

Hany E. Marei^*
, Asmaa Althani
, Nahla Afifi
, Anwarul Hasan
, Thomas Caceci
, Giacomo Pozzoli
, Carlo Cenciarelli

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

3 Scopus citations

Abstract

Alzheimer's disease (AD) is the major cause of dementia worldwide. Early-onset familial AD accounts for about 0.5% of all AD and is caused by single major gene mutations and autosomal dominant inheritance. An N141I missense mutation is associated with a significant increase in basal cell death and apoptosis. In this work we generated hiPSC from skin fibroblasts obtained from an AD patient carrying a N141I missense mutation in PSEN2. The generated iPSC colonies grew and were characterized by pluripotency marker staining; the N141I missense mutation was corrected using genome editing technology.

Original language	English
Article number	102552
Journal	Stem Cell Research
Volume	56
DOIs	https://doi.org/10.1016/j.scr.2021.102552
State	Published - Oct 2021
Externally published	Yes

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Publisher Copyright:
© 2021 The Author(s)

ASJC Scopus subject areas

Developmental Biology
Cell Biology

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title = "Generation of gene edited hiPSC from familial Alzheimer's disease patient carrying N141I missense mutation in presenilin 2",

abstract = "Alzheimer's disease (AD) is the major cause of dementia worldwide. Early-onset familial AD accounts for about 0.5\% of all AD and is caused by single major gene mutations and autosomal dominant inheritance. An N141I missense mutation is associated with a significant increase in basal cell death and apoptosis. In this work we generated hiPSC from skin fibroblasts obtained from an AD patient carrying a N141I missense mutation in PSEN2. The generated iPSC colonies grew and were characterized by pluripotency marker staining; the N141I missense mutation was corrected using genome editing technology.",

author = "Marei, \{Hany E.\} and Asmaa Althani and Nahla Afifi and Anwarul Hasan and Thomas Caceci and Giacomo Pozzoli and Carlo Cenciarelli",

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AU - Marei, Hany E.

AU - Althani, Asmaa

AU - Afifi, Nahla

AU - Hasan, Anwarul

AU - Caceci, Thomas

AU - Pozzoli, Giacomo

AU - Cenciarelli, Carlo

PY - 2021/10

Y1 - 2021/10

N2 - Alzheimer's disease (AD) is the major cause of dementia worldwide. Early-onset familial AD accounts for about 0.5% of all AD and is caused by single major gene mutations and autosomal dominant inheritance. An N141I missense mutation is associated with a significant increase in basal cell death and apoptosis. In this work we generated hiPSC from skin fibroblasts obtained from an AD patient carrying a N141I missense mutation in PSEN2. The generated iPSC colonies grew and were characterized by pluripotency marker staining; the N141I missense mutation was corrected using genome editing technology.

AB - Alzheimer's disease (AD) is the major cause of dementia worldwide. Early-onset familial AD accounts for about 0.5% of all AD and is caused by single major gene mutations and autosomal dominant inheritance. An N141I missense mutation is associated with a significant increase in basal cell death and apoptosis. In this work we generated hiPSC from skin fibroblasts obtained from an AD patient carrying a N141I missense mutation in PSEN2. The generated iPSC colonies grew and were characterized by pluripotency marker staining; the N141I missense mutation was corrected using genome editing technology.

UR - https://www.scopus.com/pages/publications/85116566714

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DO - 10.1016/j.scr.2021.102552

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AN - SCOPUS:85116566714

SN - 1873-5061

VL - 56

JO - Stem Cell Research

JF - Stem Cell Research

M1 - 102552

ER -

Generation of gene edited hiPSC from familial Alzheimer's disease patient carrying N141I missense mutation in presenilin 2

Abstract

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