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2 research outputs found

iPSCORE: A Resource of 222 iPSC Lines Enabling Functional Characterization of Genetic Variation across a Variety of Cell Types.

Author: Adler Eric
Aguirre Aitor
Arias Angelo D
Benaglio Paola
Berggren W Travis
Borja Victor
Chi Neil C
Cook Megan
D'Antonio Matteo
D'Antonio-Chronowska Agnieszka
Dargitz Carl T
DeBoever Christopher
Diffenderfer Kenneth E
Donovan Margaret KR
Drees Frauke
Evans Sylvia M
Farnam KathyJean
Feiring Rachel
Frazer Kelly A
Garcia Melvin
Goldstein Lawrence SB
Greenwald William W
Grinstein Jonathan D
Harismendy Olivier
Hashem Sherin I
Hishida Yuriko
Izpisua Belmonte Juan Carlos
Jakubosky David A
Jepsen Kristen
Li He
Loring Jeanne F
Matsui Hiroko
McGarry Thomas J
Miller Carl A
Modesto Veronica
Müller Franz-Josef
Nariai Naoki
Nelson Bradley C
O'Connor Daniel T
Okubo Jonathan
Panopoulos Athanasia D
Rao Fangwen
Reyna Joaquin
Schuldt Bernhard M
Smith Erin N
Williams Roy
Yeo Gene W
Zhao Chang
Publication venue: eScholarship, University of California
Publication date: 01/04/2017
Field of study

Large-scale collections of induced pluripotent stem cells (iPSCs) could serve as powerful model systems for examining how genetic variation affects biology and disease. Here we describe the iPSCORE resource: a collection of systematically derived and characterized iPSC lines from 222 ethnically diverse individuals that allows for both familial and association-based genetic studies. iPSCORE lines are pluripotent with high genomic integrity (no or low numbers of somatic copy-number variants) as determined using high-throughput RNA-sequencing and genotyping arrays, respectively. Using iPSCs from a family of individuals, we show that iPSC-derived cardiomyocytes demonstrate gene expression patterns that cluster by genetic background, and can be used to examine variants associated with physiological and disease phenotypes. The iPSCORE collection contains representative individuals for risk and non-risk alleles for 95% of SNPs associated with human phenotypes through genome-wide association studies. Our study demonstrates the utility of iPSCORE for examining how genetic variants influence molecular and physiological traits in iPSCs and derived cell lines

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eScholarship - University of California

Functional Gene Correction for Cystic Fibrosis in Lung Epithelial Cells Generated from Patient iPSCs

Author: Ajai Khanna
Amy L. Firth
Benjamin M. Lewis
Carl T. Dargitz
Eugene Ke
Fred H. Gage
Gregory S. Parker
Inder M. Verma
Rebecca Wright
Susan J. Qualls
Tushar Menon
Publication venue: 'Elsevier BV'
Publication date: 01/09/2015
Field of study

Lung disease is a major cause of death in the United States, with current therapeutic approaches serving only to manage symptoms. The most common chronic and life-threatening genetic disease of the lung is cystic fibrosis (CF) caused by mutations in the cystic fibrosis transmembrane regulator (CFTR). We have generated induced pluripotent stem cells (iPSCs) from CF patients carrying a homozygous deletion of F508 in the CFTR gene, which results in defective processing of CFTR to the cell membrane. This mutation was precisely corrected using CRISPR to target corrective sequences to the endogenous CFTR genomic locus, in combination with a completely excisable selection system, which significantly improved the efficiency of this correction. The corrected iPSCs were subsequently differentiated to mature airway epithelial cells where recovery of normal CFTR expression and function was demonstrated. This isogenic iPSC-based model system for CF could be adapted for the development of new therapeutic approaches

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