GeneSet Information

Tier II GS135646 • cardiac modifier of nmd 3 (Cmn3, Published QTL Chr 16)

DESCRIPTION:

QTL associated with cardiac modifier of nmd 3. This interval was obtained by using a fixed interval width of 25 Mbp around the peak marker (57459606)

LABEL:

QTL-Cmn3-Mouse-Chr 16

SCORE TYPE:

Binary

DATE ADDED:

2012-04-02

DATE UPDATED:

2020-05-06

SPECIES:

URI:

http://www.informatics.jax.org/searches/accession_report.cgi?id=MGI:3612502

AUTHORS:

Maddatu TP, Garvey SM, Schroeder DG, Zhang W, Kim SY, Nicholson AI, Davis CJ, Cox GA

TITLE:

Dilated cardiomyopathy in the nmd mouse: transgenic rescue and QTLs that improve cardiac function and survival.

JOURNAL:

Human molecular genetics Nov 2005, Vol 14, pp. 3179-89

ABSTRACT:

Mutations in the immunoglobulin mu binding protein-2 (Ighmbp2) gene cause motor neuron disease and dilated cardiomyopathy (DCM) in the neuromuscular degeneration (nmd) mouse and spinal muscular atrophy with respiratory distress (SMARD1) in humans. To investigate the role of IGHMBP2 in the pathogenesis of DCM, we generated transgenic mice expressing the full-length Ighmbp2 cDNA specifically in myocytes under the control of the mouse titin promoter. This tissue-specific transgene increased the lifespan of nmd mice up to 8-fold by preventing primary DCM and showed complete functional correction as measured by ECG, echocardiography and plasma creatine kinase-MB. Double-transgenic nmd mice expressing Ighmbp2 both in myocytes and in neurons display correction of both DCM and motor neuron disease, resulting in an essentially wild-type appearance. Additionally, quantitative trait locus (QTL) analysis was undertaken to identify genetic modifier loci responsible for the preservation of cardiac function and a marked delay in the onset of cardiomyopathy in a CAST/EiJ backcross population. Three major CAST-derived cardiac modifiers of nmd were identified on chromosomes 9, 10 and 16, which account for over 26% of the genetic variance and that continue to suppress the exacerbation of cardiomyopathy, otherwise resulting in early death, as incipient B6.CAST congenics. Overall, our results verify the tissue-specific requirement for IGHMBP2 in cardiomyocyte maintenance and survival and describe genetic modifiers that can alter the course of DCM through cardiac functional adaptation and physical remodeling in response to changes in load and respiratory demand. PUBMED: 16174646
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Annotation Information

No sequence read archive data associated with this GeneSet.


Motor Neurons (D009046)
Immunoglobulins (D007136)
Humans (D006801)
Mice (D051379)
Myocytes, Cardiac (D032383)
Chromosomes (D002875)
Death (D003643)
Muscular Atrophy, Spinal (D009134)
Echocardiography (D004452)
Creatine (D003401)
Transgenes (D019076)
Quantitative Trait Loci (D040641)
Mice, Transgenic (D008822)
Motor Neuron Disease (D016472)
Maintenance (D008283)
Atrophy (D001284)
Role (D012380)
Neurons (D009474)
Overall (D016424)
Cardiomyopathies (D009202)
Muscular Atrophy (D009133)
Plasma (D010949)
Muscle Cells (D032342)
Cardiomyopathy, Dilated (D002311)
DNA, Complementary (D018076)
Survival (D013534)
Electrocardiography (D004562)
Mutation (D009154)
plasma (MA:0002501)
muscular atrophy (MP:0002269)
no abnormal phenotype detected (MP:0002169)
cardiomyopathy (MP:0005330)
respiratory distress (MP:0001954)
dilated cardiomyopathy (MP:0002795)
pathogenesis (GO:0009405)
binding (GO:0005488)
death (GO:0016265)
QTL map (EDAM_data:1860)

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Supported by NIH R01 AA18776 jointly funded by NIAAA and NIDA, and JAX Center for Precision Genetics NIH U54 OD 020351