A Resource of Induced Pluripotent Stem Cell (iPSC) Lines Including Clinical, Genomic, and Cellular Data from Genetically Isolated Families with Mood and Psychotic Disorders

Overview

Journal Transl Psychiatry

Specialties Psychiatry
Public Health

Date 2023 Dec 16

PMID 38104115

Authors

Sevilla D Detera-Wadleigh

Layla Kassem

Emily Besancon

Fabiana Lopes

Nirmala Akula

Heejong Sung

Meghan Blattner

Laura Sheridan

Ley Nadine Lacbawan

Joshua Garcia

Francis Gordovez

Katherine Hosey

Cassandra Donner

Claudio Salvini

Thomas Schulze

David T W Chen

Bryce England

Joanna Cross

Xueying Jiang

Winston Corona

Jill Russ

Barbara Mallon

Amalia Dutra

Evgenia Pak

Joe Steiner

Nasir Malik

Theresa de Guzman

Natia Horato

Mariana B Mallmann

Victoria Mendes

Amanda L Duck

Antonio E Nardi

Francis J McMahon

Affiliations

Soon will be listed here.

Abstract

Genome-wide (GWAS) and copy number variant (CNV) association studies have reproducibly identified numerous risk alleles associated with bipolar disorder (BD), major depressive disorder (MDD), and schizophrenia (SCZ), but biological characterization of these alleles lags gene discovery, owing to the inaccessibility of live human brain cells and inadequate animal models for human psychiatric conditions. Human-derived induced pluripotent stem cells (iPSCs) provide a renewable cellular reagent that can be differentiated into living, disease-relevant cells and 3D brain organoids carrying the full complement of genetic variants present in the donor germline. Experimental studies of iPSC-derived cells allow functional characterization of risk alleles, establishment of causal relationships between genes and neurobiology, and screening for novel therapeutics. Here we report the creation and availability of an iPSC resource comprising clinical, genomic, and cellular data obtained from genetically isolated families with BD and related conditions. Results from the first 324 study participants, 61 of whom have validated pluripotent clones, show enrichment of rare single nucleotide variants and CNVs overlapping many known risk genes and pathogenic CNVs. This growing iPSC resource is available to scientists pursuing functional genomic studies of BD and related conditions.

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