Literature DB >> 23800850

A novel genetic locus modulates infarct volume independently of the extent of collateral circulation.

Pei-Lun Chu1, Sehoon Keum, Douglas A Marchuk.   

Abstract

In the mouse model of permanent, middle cerebral artery occlusion, infarct volume varies widely across inbred strains but generally is inversely correlated with collateral vessel number. However, we also observed certain mouse strains that share similar collateral vessel anatomy but exhibit significantly different infarct volume. To identify genetic factors determining infarct volume in a collateral vessel-independent manner, we performed quantitative trait locus analysis on a F2 cross between C57BL/6J and C3H/HeJ strains. We mapped four novel loci (Civq4 through Civq7) that modulate infarct volume. Civq4, on chromosome 8, is the strongest locus (logarithm of the odds 9.8) that contributes 21% of the phenotypic variance of infarct volume in the cross. The Civq4 and Civq6 loci represent transgressive B6 alleles that render animals susceptible to larger infarcts. Based on genomic sequence and microarray analyses, we propose candidate genes for the Civq4 locus. By selecting inbred strains with similar collateral vessel anatomy but that vary significantly in infarct volume, we have mapped four loci determining infarct volume in a mouse model of ischemic stroke. Two of the loci appear to modulate infarct volume through a collateral vessel-independent mechanism. Based on strain-specific sequence variants and differences in transcript levels, Msr1 and Mtmr7 appear to be strong candidate genes for Civq4. Identifying the underlying genetic factors of these loci will elucidate the genetic architecture response to cerebral ischemia, shed new light on disease mechanisms of ischemic stroke, and identify potential therapeutic targets for clinical applications.

Entities:  

Keywords:  collateral circulation; ischemic stroke; quantitative trait locus; stroke genetics; transgressive segregation

Mesh:

Substances:

Year:  2013        PMID: 23800850      PMCID: PMC3763066          DOI: 10.1152/physiolgenomics.00063.2013

Source DB:  PubMed          Journal:  Physiol Genomics        ISSN: 1094-8341            Impact factor:   3.107


  43 in total

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Authors:  Sehoon Keum; Douglas A Marchuk
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  13 in total

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3.  The impact of native leptomeningeal collateralization on rapid blood flow recruitment following ischemic stroke.

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4.  Embracing Biological and Methodological Variance in a New Approach to Pre-Clinical Stroke Testing.

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5.  Novel Neuroprotective Loci Modulating Ischemic Stroke Volume in Wild-Derived Inbred Mouse Strains.

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6.  Neuronal IL-4Rα modulates neuronal apoptosis and cell viability during the acute phases of cerebral ischemia.

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7.  Robust effects of genetic background on responses to subarachnoid hemorrhage in mice.

Authors:  Josephine A D'Abbondanza; Jinglu Ai; Elliot Lass; Hoyee Wan; Shakira Brathwaite; Michael K Tso; Charles Lee; Philip A Marsden; R Loch Macdonald
Journal:  J Cereb Blood Flow Metab       Date:  2015-10-26       Impact factor: 6.200

8.  Congenic fine-mapping identifies a major causal locus for variation in the native collateral circulation and ischemic injury in brain and lower extremity.

Authors:  Robert Sealock; Hua Zhang; Jennifer L Lucitti; Scott M Moore; James E Faber
Journal:  Circ Res       Date:  2013-12-03       Impact factor: 17.367

Review 9.  Animal models of ischemic stroke and their application in clinical research.

Authors:  Felix Fluri; Michael K Schuhmann; Christoph Kleinschnitz
Journal:  Drug Des Devel Ther       Date:  2015-07-02       Impact factor: 4.162

10.  Natural genetic variation of integrin alpha L (Itgal) modulates ischemic brain injury in stroke.

Authors:  Sehoon Keum; Han Kyu Lee; Pei-Lun Chu; Matthew J Kan; Min-Nung Huang; Carol J Gallione; Michael D Gunn; Donald C Lo; Douglas A Marchuk
Journal:  PLoS Genet       Date:  2013-10-10       Impact factor: 5.917

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