Natural genetic variation of integrin alpha L (Itgal) modulates ischemic brain injury in stroke.
Date
2013-01
Editor
Hunter, Kent W
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Abstract
During ischemic stroke, occlusion of the cerebrovasculature causes neuronal cell death
(infarction), but naturally occurring genetic factors modulating infarction have been
difficult to identify in human populations. In a surgically induced mouse model of
ischemic stroke, we have previously mapped Civq1 to distal chromosome 7 as a quantitative
trait locus determining infarct volume. In this study, genome-wide association mapping
using 32 inbred mouse strains and an additional linkage scan for infarct volume confirmed
that the size of the infarct is determined by ancestral alleles of the causative gene(s).
The genetically isolated Civq1 locus in reciprocal recombinant congenic mice refined
the critical interval and demonstrated that infarct size is determined by both vascular
(collateral vessel anatomy) and non-vascular (neuroprotection) effects. Through the
use of interval-specific SNP haplotype analysis, we further refined the Civq1 locus
and identified integrin alpha L (Itgal) as one of the causative genes for Civq1. Itgal
is the only gene that exhibits both strain-specific amino acid substitutions and expression
differences. Coding SNPs, a 5-bp insertion in exon 30b, and increased mRNA and protein
expression of a splice variant of the gene (Itgal-003, ENSMUST00000120857), all segregate
with infarct volume. Mice lacking Itgal show increased neuronal cell death in both
ex vivo brain slice and in vivo focal cerebral ischemia. Our data demonstrate that
sequence variation in Itgal modulates ischemic brain injury, and that infarct volume
is determined by both vascular and non-vascular mechanisms.
Type
Journal articleSubject
AnimalsHumans
Mice
Brain Injuries
Brain Ischemia
Disease Models, Animal
Integrin alpha Chains
Haplotypes
Polymorphism, Single Nucleotide
Alleles
Quantitative Trait Loci
Stroke
Genome-Wide Association Study
Genetic Linkage
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https://hdl.handle.net/10161/26127Published Version (Please cite this version)
10.1371/journal.pgen.1003807Publication Info
Keum, Sehoon; Lee, Han Kyu; Chu, Pei-Lun; Kan, Matthew J; Huang, Min-Nung; Gallione,
Carol J; ... Marchuk, Douglas A (2013). Natural genetic variation of integrin alpha L (Itgal) modulates ischemic brain injury
in stroke. PLoS genetics, 9(10). pp. e1003807. 10.1371/journal.pgen.1003807. Retrieved from https://hdl.handle.net/10161/26127.This is constructed from limited available data and may be imprecise. To cite this
article, please review & use the official citation provided by the journal.
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Show full item recordScholars@Duke
Michael Dee Gunn
Professor of Medicine
The focus of my work is on understanding how dendritic cells, monocytes, and macrophages
regulate immune responses, contribute to specific disease pathologies, and can be
manipulated to stimulate or inhibit specific immune responses. We are also using our
knowledge of immunology to develop diagnostics and therapeutics for a variety of human
diseases.
Lab History The lab started with our discovery of the lymphoid chemokines, which regulate
the mi
Han Kyu Lee
Assistant Research Professor in Molecular Genetics and Microbiology
Donald Ching-Tze Lo
Associate Professor in Neurobiology
Dr. Lo's laboratory focuses on the translation of basic neuroscience research into
the identification new drug candidates and targets for neuropsychiatric diseases including
Alzheimer's disease, Huntington's disease, stroke, and glaucoma. In this context,
the laboratory has developed a series of discovery technologies, based on high-content
screening and chemical genetics, to drive towards the efficient identification of
new neurological drug candidates with strong likelihood of clinical s
This author no longer has a Scholars@Duke profile, so the information shown here reflects
their Duke status at the time this item was deposited.
Douglas Alan Marchuk
James B. Duke Distinguished Professor of Molecular Genetics and Microbiology
Vascular Morphogenesis: A Human Genetics Approach Advances in our understanding of
fundamental biological events can often be made by the analysis of defects manifested
in inherited diseases. The genes responsible for these genetic syndromes often encode
proteins that act at critical points of the pathways that control fundamental biological
processes such as cell division, differentiation, and cell death. This approach has
lead to the discovery of novel gene products and/or biochem
Alphabetical list of authors with Scholars@Duke profiles.

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