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Phenotypes associated with this allele
Allele Symbol
Allele Name
Allele ID 		Lamp2tm1.2Ces
targeted mutation 1.2, Christine E Seidman
MGI:7339104
Summary 2 genotypes
Jump to Allelic Composition Genetic Background Genotype ID
cx1
 		Kcne1tm1Rdn/Kcne1+
Lamp2tm1.2Ces/Y 		involves: 129 * 129S4/SvJae * 129S6/SvEvTac * C57BL/6 * SJL MGI:7339179
ot2
 		Lamp2tm1.2Ces/Y involves: 129 * 129S4/SvJae * 129S6/SvEvTac * C57BL/6 * SJL MGI:7339154


Genotype
MGI:7339179
cx1
Allelic
Composition		 Kcne1tm1Rdn/Kcne1+
Lamp2tm1.2Ces/Y
Genetic
Background		 involves: 129 * 129S4/SvJae * 129S6/SvEvTac * C57BL/6 * SJL
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Kcne1tm1Rdn mutation (2 available); any Kcne1 mutation (13 available)
Lamp2tm1.2Ces mutation (0 available); any Lamp2 mutation (15 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
cardiovascular system
abnormal atrioventricular bundle morphology ( J:328713 )
• mice show disorganization of the proximal bundle of His
abnormal atrioventricular node morphology ( J:328713 )
• the atrioventricular node is more disorganized and fibrosis and large vacuoles are seen in the atrioventricular region
• hearts exhibit fewer conduction cells

muscle
abnormal atrioventricular bundle morphology ( J:328713 )
• mice show disorganization of the proximal bundle of His
abnormal atrioventricular node morphology ( J:328713 )
• the atrioventricular node is more disorganized and fibrosis and large vacuoles are seen in the atrioventricular region
• hearts exhibit fewer conduction cells




Genotype
MGI:7339154
ot2
Allelic
Composition		 Lamp2tm1.2Ces/Y
Genetic
Background		 involves: 129 * 129S4/SvJae * 129S6/SvEvTac * C57BL/6 * SJL
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Lamp2tm1.2Ces mutation (0 available); any Lamp2 mutation (15 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
mortality/aging
neonatal lethality, incomplete penetrance ( J:328713 )
• neonatal death in about 25% of hemizygous males
• surviving males exhibit normal survival

growth/size/body
increased heart weight ( J:328713 )
• heart to body weight is increased at 40 weeks of age
cardiac hypertrophy ( J:328713 )
• males develop significant cardiac hypertrophy after 20 weeks of age
• mice treated for 2 weeks with cyclosporine A that blocks mitochondrial autophagy show a attenuation of cardiac hypertrophy, however fractional shortening and fibrosis are unaffected
heart left ventricle hypertrophy ( J:328713 )
• left ventricular hypertrophy by 20 weeks of age; echocardiograms show hypertrophy of the intra-ventricular septum and posterior wall
decreased birth body size ( J:328713 )
• surviving males are initially smaller but achieve comparable size and weight by 12 weeks of age

cardiovascular system
increased cardiac muscle glycogen level ( J:328713 )
• hearts contain approximately 2 times the glycogen content as wild-type hearts
• however, no PAS+ inclusions are seen
abnormal myocardial fiber morphology ( J:328713 )
• left ventricle myocytes have abundant bilayer membrane vesicles containing inclusions composed of cytoplasmic remnants, partially degraded organelles, and amorphous materials characteristic of autophagosomes that disrupt the normal sarcomere organization
• lysosomes are dispersed throughout the cytosol instead of being clustered in the perinuclear regions
increased heart weight ( J:328713 )
• heart to body weight is increased at 40 weeks of age
cardiac hypertrophy ( J:328713 )
• males develop significant cardiac hypertrophy after 20 weeks of age
• mice treated for 2 weeks with cyclosporine A that blocks mitochondrial autophagy show a attenuation of cardiac hypertrophy, however fractional shortening and fibrosis are unaffected
heart left ventricle hypertrophy ( J:328713 )
• left ventricular hypertrophy by 20 weeks of age; echocardiograms show hypertrophy of the intra-ventricular septum and posterior wall
cardiac fibrosis ( J:328713 )
• mice show progressive myocardial fibrosis, with interstitial fibrosis at 20 weeks and both interstitial fibrosis and areas of scarring by 40 weeks of age
decreased cardiac muscle contractility ( J:328713 )
• aged (about 40 weeks) mice show decreased fractional shortening
irregular heartbeat ( J:328713 )
• pacing induces ventricular arrhythmias in 75% of mice
• however, no difference in average sinus heart rate is seen and mice do not exhibit ventricular pre-excitation or spontaneous arrhythmias
atrioventricular block ( J:328713 )
• intermittent atrio-ventricular block in 60% of mice
abnormal sinoatrial node conduction ( J:328713 )
• 15-week-old mice show transient sinus node arrest
abnormal myocardial fiber physiology ( J:328713 )
• durations of contraction and relaxation are prolonged in myocytes
• however, the extent of shortening or relaxation is not different in cardiomyocytes
• the mean amplitude of calcium transients is higher in myocytes
• catecholamines further increase mean calcium transient amplitudes to higher levels than in controls indicating increased sensitivity to catecholamines
• marker analysis indicates incomplete lysosome biogenesis
• catecholamines produce spontaneous and frequent sarcoplasmic reticulum calcium release events in about 75% of myocytes compared to 8% of wild-type myocytes
cardiomyopathy ( J:328713 )
• mice develop progressive cardiomyopathy

muscle
increased cardiac muscle glycogen level ( J:328713 )
• hearts contain approximately 2 times the glycogen content as wild-type hearts
• however, no PAS+ inclusions are seen
abnormal myocardial fiber morphology ( J:328713 )
• left ventricle myocytes have abundant bilayer membrane vesicles containing inclusions composed of cytoplasmic remnants, partially degraded organelles, and amorphous materials characteristic of autophagosomes that disrupt the normal sarcomere organization
• lysosomes are dispersed throughout the cytosol instead of being clustered in the perinuclear regions
heart left ventricle hypertrophy ( J:328713 )
• left ventricular hypertrophy by 20 weeks of age; echocardiograms show hypertrophy of the intra-ventricular septum and posterior wall
decreased cardiac muscle contractility ( J:328713 )
• aged (about 40 weeks) mice show decreased fractional shortening
cardiomyopathy ( J:328713 )
• mice develop progressive cardiomyopathy

homeostasis/metabolism
increased cardiac muscle glycogen level ( J:328713 )
• hearts contain approximately 2 times the glycogen content as wild-type hearts
• however, no PAS+ inclusions are seen
abnormal autophagy ( J:328713 )
• autophagy is stimulated in myocytes but the later stages in the processing of autophagosomes are blocked, resulting in accumulated autophagosomes, absent phagolysosomes, and myocytes that are unable to clear cellular debris indicating a block in autophagy at the step of formation of autolysosomes
increased circulating troponin T level ( J:328713 )
• elevation of serum cardiac troponin T, indicating an ongoing myocardial injury

cellular
abnormal autophagy ( J:328713 )
• autophagy is stimulated in myocytes but the later stages in the processing of autophagosomes are blocked, resulting in accumulated autophagosomes, absent phagolysosomes, and myocytes that are unable to clear cellular debris indicating a block in autophagy at the step of formation of autolysosomes

behavior/neurological
behavior/neurological phenotype ( J:328713 )
N
• surviving males exhibit normal voluntary activity

Mouse Models of Human Disease
 DO ID OMIM ID(s) Ref(s)
Danon disease DOID:0050437 OMIM:300257
 J:328713




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Mouse Genome Database (MGD), Gene Expression Database (GXD), Mouse Models of Human Cancer database (MMHCdb) (formerly Mouse Tumor Biology (MTB)), Gene Ontology (GO)
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Send questions and comments to User Support. 		last database update
11/19/2024
MGI 6.24 		The Jackson Laboratory