Phenotypes associated with this allele

• Allele Symbol: Atp2a2⁺
• Allele Name: wild type
• Allele ID: MGI:2430041
• Summary: 7 genotypes

Jump to	Allelic Composition	Genetic Background	Genotype ID
ht1	Atp2a2^tm1.1Raco/Atp2a2^+	C57BL/6J-Atp2a2^tm1.1Raco/Raco	MGI:5780878
ht2	Atp2a2^tm1b(EUCOMM)Hmgu/Atp2a2^+	C57BL/6N-Atp2a2^tm1b(EUCOMM)Hmgu/H	MGI:5756748
ht3	Atp2a2^tm1Ges/Atp2a2^+	involves: 129X1/SvJ	MGI:5502163
ht4	Atp2a2^tm1Ges/Atp2a2^+	involves: 129X1/SvJ * Black Swiss	MGI:2655642
cn5	Atp2a2^tm1.1Iemr/Atp2a2^+ Myl2^tm1(cre)Krc/Myl2^+	involves: 129P2/OlaHsd * 129S4/SvJae * C57BL/6Crl * C57BL/6J	MGI:4415177
cx6	Atp2a2^tm1Ges/Atp2a2^+ Tg(Myh6/tetO-Tnnc1*I61Q)1Jmol/0 Tg(Myh6-tTA)55Rbns/0	involves: 129X1/SvJ * FVB	MGI:5897399
cx7	Atp2a2^tm1Ges/Atp2a2^+ Tg(Myh6/tetO-Tnnc1*L48Q)2Jmol/0 Tg(Myh6-tTA)55Rbns/0	involves: 129X1/SvJ * FVB	MGI:5897401

Genotype
MGI:5780878

ht1

• Allelic Composition: Atp2a2^tm1.1Raco/Atp2a2⁺
• Genetic Background: C57BL/6J-Atp2a2^tm1.1Raco/Raco

• ♀: phenotype observed in females
• ♂: phenotype observed in males
• N: normal phenotype

Impaired blood flow recovery at 21 and 28 days post hind limb ischemia in Atp2a2^tm1.1Raco/Atp2a2⁺ mice

cardiovascular system

abnormal physiological neovascularization ( J:216004 )

• impaired ischemic angiogenesis at 21 and 28 days after femoral artery ligation relative to wild-type controls

• significantly lower increase in SERCA S-glutathione adducts in the ischemic hind limb muscle at 3 days post femoral artery ligation relative to wild-type controls

decreased angiogenesis ( J:216004 )

• in a Matrigel assay, both basal and VEGF-induced capillary-like network formation are significantly impaired in cultured endothelial cells relative to wild-type cells

abnormal vascular endothelial cell migration ( J:216004 )

• impaired VEGF-mediated migration of microvascular endothelial cells in an in vitro monolayer scratch wound assay

• adenoviral overexpression of calreticulin, an ER Ca²⁺ binding protein, restores endothelial cell migration

abnormal blood circulation ( J:216004 )

• impaired blood flow recovery at 21 and 28 days post hind limb ischemia in adult (8- to 12-week-old) mice relative to wild-type controls

abnormal vascular endothelial cell physiology ( J:216004 )

• no significant increase in SERCA S-glutathione adducts in primary cardiac microvascular endothelial cells at 24 h after induction of hypoxia, unlike in wild-type endothelial cells

• decreased nitric oxide-induced (thapsigargin-sensitive) ⁴⁵Ca²⁺ uptake into the endoplasmic reticulum (ER) in cultured endothelial cells relative to wild-type cells

• in a Matrigel assay, both basal and vascular endothelial growth factor (VEGF)-induced capillary-like network formation are significantly impaired in cultured endothelial cells relative to wild-type cells

homeostasis/metabolism

abnormal calcium ion homeostasis ( J:216004 )

• decreased nitric oxide-induced ⁴⁵Ca²⁺ uptake into the ER in cultured cardiac microvascular endothelial cells relative to wild-type cells

• Fura-2 studies revealed decreased Ca²⁺ stores and decreased VEGF- and nitric oxide-induced Ca²⁺ influx

• adenoviral overexpression of calreticulin, an ER Ca²⁺ binding protein, increases ionomycin-releasable stores and VEGF-induced Ca²⁺ influx

cellular

abnormal vascular endothelial cell migration ( J:216004 )

• impaired VEGF-mediated migration of microvascular endothelial cells in an in vitro monolayer scratch wound assay

• adenoviral overexpression of calreticulin, an ER Ca²⁺ binding protein, restores endothelial cell migration

Genotype
MGI:5756748

ht2

• Allelic Composition: Atp2a2^{tm1b(EUCOMM)Hmgu}/Atp2a2⁺
• Genetic Background: C57BL/6N-Atp2a2^{tm1b(EUCOMM)Hmgu}/H
• Cell Lines: HEPD0714_3_B04

Data Sources

IMPC Data for Atp2a2

hematopoietic system

decreased mean platelet volume ( J:211773 )

♀

IMPC - HAR

homeostasis/metabolism

increased fasting circulating glucose level ( J:211773 )

♂

IMPC - HAR

decreased circulating alkaline phosphatase level ( J:211773 )

♀

IMPC - HAR

Genotype
MGI:5502163

ht3

• Allelic Composition: Atp2a2^tm1Ges/Atp2a2⁺
• Genetic Background: involves: 129X1/SvJ

skeleton

abnormal osteoclast differentiation ( J:198051 )

• impaired

• however, osteoclast differentiation is rescued by retroviral expression of CREB1

cellular

abnormal osteoclast differentiation ( J:198051 )

• impaired

• however, osteoclast differentiation is rescued by retroviral expression of CREB1

hematopoietic system

abnormal osteoclast differentiation ( J:198051 )

• impaired

• however, osteoclast differentiation is rescued by retroviral expression of CREB1

immune system

abnormal osteoclast differentiation ( J:198051 )

• impaired

• however, osteoclast differentiation is rescued by retroviral expression of CREB1

Genotype
MGI:2655642

ht4

• Allelic Composition: Atp2a2^tm1Ges/Atp2a2⁺
• Genetic Background: involves: 129X1/SvJ * Black Swiss

mortality/aging

increased susceptibility to induced morbidity/mortality ( J:95608 )

• when subjected to aortic coarctation at 10-12 wks of age, 4 of 11 heterozygotes die of heart failure between 4 and 8 wks of pressure overload whereas no mortality is observed in wild-type mice

premature death ( J:69754 )

• 2 of 16 aging heterozygotes died of unknown causes; one exhibited a prolapsed penis

• 14 of 16 aging heterozygotes with overt disease symptoms showed a sharp decline in survival between 53-81 wks of age

cardiovascular system

cardiac hypertrophy ( J:95608 )

• after 10 wks of pressure overload, coarcted wild-type hearts exhibit mild cardiomyocyte hypertrophy whereas coarcted heterozygous mutant hearts show diffuse, moderate myocyte hypertrophy

• coarcted failing heterozygotes exhibit an eccentric, dilated form of cardiac hypertrophy whereas coarcted wild-type mice and nonfailing heterozygotes show a concentric form of hypertrophy

heart left ventricle hypertrophy ( J:95608 )

• after pressure overload, failing heterozygotes show a significantly greater increase in LV mass and LV hypertrophy relative to coarcted wild-type mice at 5 and 10 wks of aortic coarctation

increased heart left ventricle posterior wall thickness ( J:95608 )

• after pressure overload, failing heterozygotes show a a significant increase in LV posterior wall thickness relative to coarcted wild-type mice

dilated heart left ventricle ( J:95608 )

• after pressure overload, failing heterozygotes show a significant increase in LV chamber dilation relative to coarcted wild-type mice

cardiac fibrosis ( J:69754 , J:95608 )

• at age 53-81 weeks, some diseased heterozygotes displayed mild cardiac fibrosis, with no major cardiac lesions or hypertrophy (J:69754)

• after 10 wks of pressure overload, coarcted wild-type hearts show mild perivascular fibrosis whereas coarcted heterozygous mutant hearts exhibit moderate multifocal fibrosis (J:95608)

decreased heart ventricle muscle contractility ( J:52186 , J:95608 )

• after 10 wks of pressure overload, a portion of coarcted heterozygotes show significant systolic cardiac dysfunction i.e. reduced rate of contraction (+dP/dt) relative to coarcted wild-type mice (J:95608)

♂ • male heterozygotes exhibit a significant reduction in the absolute value of positive dP/dt (dP/dtmax) relative to wild-type males under non-stimulated conditions and at all levels of beta-adrenergic stimulation (J:52186)

decreased heart left ventricle muscle contractility ( J:66006 )

• left ventricular cardiomyocytes isolated from adult heterozygotes and paced at 0.25 Hz display a ~30% decrease in the percentage of cell shortening as well as a ~40% reduction in the rate of cell shortening and cell relengthening

abnormal cardiac muscle relaxation ( J:52186 , J:95608 )

• after 10 wks of pressure overload, a portion of coarcted heterozygotes show significant diastolic cardiac dysfunction i.e. reduced rate of relaxation (-dP/dt) relative to coarcted wild-type mice (J:95608)

♂ • male heterozygotes exhibit a significant reduction in the absolute value of negative dP/dt (dP/dtmin) relative to wild-type males under non-stimulated conditions and at all levels of beta-adrenergic stimulation (J:52186)

decreased left ventricle systolic pressure ( J:52186 )

♂ • male heterozygotes exhibit a significantly lower LV systolic pressure than wild-type males under non-stimulated conditions and at low doses of dobutamine (1-2 ng/min/g of body weight), but not at higher levels of beta-adrenergic stimulation (4-32 ng/min/g)

increased left ventricle diastolic pressure ( J:95608 )

• after 10 wks of pressure overload, LV end-diastolic pressure is significantly elevated in coarcted failing heterozygotes relative to coarcted wild-type mice

increased response of heart to induced stress ( J:95608 )

• after pressure overload, exhibit an eccentric dilated form of cardiac hypertrophy instead of the concentric form of hypertrophy seen in wild-type controls, and show a greater increase in cardiac fibrosis, left ventricle hypertrophy, dilation, posterior wall thickness, and end-diastolic pressure, and reduced contraction and relaxation rates, resulting in heart failure that is not observed in wild-type

decreased systemic arterial blood pressure ( J:52186 )

• heterozygotes are viable and healthy, with no cardiac hypertrophy or overt signs of a disease phenotype

• however, 12-14-week-old male heterozygotes exhibit a significantly lower mean arterial blood pressure than wild-type males under non-stimulated conditions and at low doses of dobutamine (1-2 ng/min/g of body weight), but not at higher levels of beta-adrenergic stimulation (4-32 ng/min/g)

• no significant differences are noted in mean heart rate under non-stimulated conditions or at low doses of dobutamine

congestive heart failure ( J:95608 )

• after 10 wk of pressure overload, ~64% of coarcted heterozygotes are in heart failure compared with 0% of coarcted wild-type mice

homeostasis/metabolism

increased response of heart to induced stress ( J:95608 )

• after pressure overload, exhibit an eccentric dilated form of cardiac hypertrophy instead of the concentric form of hypertrophy seen in wild-type controls, and show a greater increase in cardiac fibrosis, left ventricle hypertrophy, dilation, posterior wall thickness, and end-diastolic pressure, and reduced contraction and relaxation rates, resulting in heart failure that is not observed in wild-type

pulmonary edema ( J:95608 )

• after 10 wk of pressure overload, 64% of coarcted heterozygotes exhibit pulmonary edema (i.e. a significantly increased wet lung weight-to-body weight ratio) relative to 0% of coarcted wild-type mice

abnormal calcium ion homeostasis ( J:52186 , J:66006 )

• cardiac homogenates from 15-16-week-old heterozygotes show a ~33% reduction in the maximum velocity of Ca²⁺ uptake by sarcoplasmic reticulum relative to wild-type homogenates (J:52186)

• however, no signifiant differences in the Ca²⁺ dependence of Ca²⁺ uptake activity are observed (J:52186)

• left ventricular cardiomyocytes isolated from adult heterozygotes and paced at 0.25 Hz show a ~40-60% and a ~30-40% reduction in SR Ca²⁺ stores and Ca²⁺ release, respectively (J:66006)

• however, the rate of Ca²⁺ transient decline (tau) is not altered significantly, suggesting no change in the rate of Ca²⁺ removal from the cytosol (J:66006)

muscle

heart left ventricle hypertrophy ( J:95608 )

• after pressure overload, failing heterozygotes show a significantly greater increase in LV mass and LV hypertrophy relative to coarcted wild-type mice at 5 and 10 wks of aortic coarctation

decreased heart ventricle muscle contractility ( J:52186 , J:95608 )

• after 10 wks of pressure overload, a portion of coarcted heterozygotes show significant systolic cardiac dysfunction i.e. reduced rate of contraction (+dP/dt) relative to coarcted wild-type mice (J:95608)

♂ • male heterozygotes exhibit a significant reduction in the absolute value of positive dP/dt (dP/dtmax) relative to wild-type males under non-stimulated conditions and at all levels of beta-adrenergic stimulation (J:52186)

decreased heart left ventricle muscle contractility ( J:66006 )

• left ventricular cardiomyocytes isolated from adult heterozygotes and paced at 0.25 Hz display a ~30% decrease in the percentage of cell shortening as well as a ~40% reduction in the rate of cell shortening and cell relengthening

abnormal cardiac muscle relaxation ( J:52186 , J:95608 )

• after 10 wks of pressure overload, a portion of coarcted heterozygotes show significant diastolic cardiac dysfunction i.e. reduced rate of relaxation (-dP/dt) relative to coarcted wild-type mice (J:95608)

♂ • male heterozygotes exhibit a significant reduction in the absolute value of negative dP/dt (dP/dtmin) relative to wild-type males under non-stimulated conditions and at all levels of beta-adrenergic stimulation (J:52186)

respiratory system

pulmonary edema ( J:95608 )

• after 10 wk of pressure overload, 64% of coarcted heterozygotes exhibit pulmonary edema (i.e. a significantly increased wet lung weight-to-body weight ratio) relative to 0% of coarcted wild-type mice

behavior/neurological

lethargy ( J:69754 )

• aging heterozygotes with squamous cell tumors were lethargic

digestive/alimentary system

increased tongue papilloma incidence ( J:69754 )

• 3 of 10 aging heterozygotes showed squamous cell papillomas of the tongue

esophageal epithelium hyperplasia ( J:69754 )

• aging heterozygotes frequently displayed hyperplastic changes in the epithelial lining of the esophagus, even in the absence of overt esophageal tumors

increased esophageal papilloma incidence ( J:69754 )

• 7 of 14 aging heterozygotes displayed squamous cell papillomas of the esophagus

• squamous cell papillomas were also observed in forestomachs, although less commonly than carcinomas

stomach epithelial hyperplasia ( J:69754 )

• aging heterozygotes frequently displayed hyperplastic changes in the epithelial lining of the forestomach, even in the absence of overt stomach tumors

growth/size/body

cardiac hypertrophy ( J:95608 )

• after 10 wks of pressure overload, coarcted wild-type hearts exhibit mild cardiomyocyte hypertrophy whereas coarcted heterozygous mutant hearts show diffuse, moderate myocyte hypertrophy

• coarcted failing heterozygotes exhibit an eccentric, dilated form of cardiac hypertrophy whereas coarcted wild-type mice and nonfailing heterozygotes show a concentric form of hypertrophy

heart left ventricle hypertrophy ( J:95608 )

• after pressure overload, failing heterozygotes show a significantly greater increase in LV mass and LV hypertrophy relative to coarcted wild-type mice at 5 and 10 wks of aortic coarctation

increased tongue papilloma incidence ( J:69754 )

• 3 of 10 aging heterozygotes showed squamous cell papillomas of the tongue

cachexia ( J:69754 )

• aging heterozygotes with squamous cell tumors exhibited wasting

integument

toenail hyperkeratosis ( J:69754 )

• 2 of 14 diseased heterozygotes showed extreme hyperkeratosis of a toenail, and another heterozygote had a large keratinized cyst bordered by squamous epithelium

hyperkeratosis ( J:69754 )

• 6 of 14 heterozygotes displayed hyperkeratinized squamous cell carcinomas of the forestomach

increased skin papilloma incidence ( J:69754 )

• 1 of 14 aging heterozygotes displayed a squamous cell papilloma of the penis

renal/urinary system

penis prolapse ( J:69754 )

♂ • aging heterozygotes with squamous cell tumors displayed penile prolapse

reproductive system

penis prolapse ( J:69754 )

♂ • aging heterozygotes with squamous cell tumors displayed penile prolapse

neoplasm

increased tumor incidence ( J:69754 )

• aging heterozygotes (53-81 weeks of age) exhibited a high predisposition to squamous cell tumor formation, with 30 squamous cell tumors noted among 14 heterozygotes vs none in wild-type controls

increased tongue papilloma incidence ( J:69754 )

• 3 of 10 aging heterozygotes showed squamous cell papillomas of the tongue

increased esophageal papilloma incidence ( J:69754 )

• 7 of 14 aging heterozygotes displayed squamous cell papillomas of the esophagus

• squamous cell papillomas were also observed in forestomachs, although less commonly than carcinomas

increased skin papilloma incidence ( J:69754 )

• 1 of 14 aging heterozygotes displayed a squamous cell papilloma of the penis

increased squamous cell carcinoma incidence ( J:69754 )

• at age 53-81 weeks, 13 of 14 (93%) of heterozygotes had hyperkeratinized squamous cell tumors of the stomach, esophagus, tongue, oral mucosa, and skin, with an average of more than two tumors per mouse

• 10/14 (71%) of heterozygotes had squamous cell tumors of the forestomach (non-glandular mucosa) and esophagus

• 9 of 10 of heterozygotes had squamous cell tumors in the tongue or oral mucosa (4 tongue carcinomas, 3 tongue papillomas and 2 oral mucosa (cheek) carcinomas)

• 5/14 of heterozygotes had squamous cell tumors of the skin (2 face carcinomas, 2 penis carcinomas and 1 penis papilloma)

• additional squamous cell tumors were observed in retired heterozygous breeders, including carcinomas of the esophagus, lip, palette, and the skin adjacent to the vagina, penis, and anus

craniofacial

increased tongue papilloma incidence ( J:69754 )

• 3 of 10 aging heterozygotes showed squamous cell papillomas of the tongue

Mouse Models of Human Disease		DO ID	OMIM ID(s)	Ref(s)
keratosis follicularis		DOID:2734	OMIM:124200	J:69754

Genotype
MGI:4415177

cn5

• Allelic Composition: Atp2a2^tm1.1Iemr/Atp2a2⁺; Myl2^tm1(cre)Krc/Myl2⁺
• Genetic Background: involves: 129P2/OlaHsd * 129S4/SvJae * C57BL/6Crl * C57BL/6J

cardiovascular system

cardiovascular system phenotype ( J:155628 )

N • mice exhibit normal heart weight and cardiac function

Genotype
MGI:5897399

cx6

• Allelic Composition: Atp2a2^tm1Ges/Atp2a2⁺; Tg(Myh6/tetO-Tnnc1*I61Q)1Jmol/0; Tg(Myh6-tTA)55Rbns/0
• Genetic Background: involves: 129X1/SvJ * FVB

cardiovascular system

increased heart weight ( J:234490 )

• more so than in Tg(Myh6/tetO-Tnnc1*I61Q)1Jmol mice

increased heart left ventricle size ( J:234490 )

• improved compared to in Tg(Myh6/tetO-Tnnc1*I61Q)1Jmol mice

abnormal myocardial fiber physiology ( J:234490 )

• increased unloaded twitch force

growth/size/body

increased heart weight ( J:234490 )

• more so than in Tg(Myh6/tetO-Tnnc1*I61Q)1Jmol mice

muscle

abnormal myocardial fiber physiology ( J:234490 )

• increased unloaded twitch force

Genotype
MGI:5897401

cx7

• Allelic Composition: Atp2a2^tm1Ges/Atp2a2⁺; Tg(Myh6/tetO-Tnnc1*L48Q)2Jmol/0; Tg(Myh6-tTA)55Rbns/0
• Genetic Background: involves: 129X1/SvJ * FVB

cardiovascular system

thick interventricular septum ( J:234490 )

• compared to in Tg(Myh6/tetO-Tnnc1*L48Q)2Jmol mice

increased heart weight ( J:234490 )

• more so than in Tg(Myh6/tetO-Tnnc1*L48Q)2Jmol mice

abnormal heart left ventricle morphology ( J:234490 )

• increased left ventricle wall thickness compared to in Tg(Myh6/tetO-Tnnc1*L48Q)2Jmol mice

abnormal myocardial fiber physiology ( J:234490 )

• increased unloaded twitch force

growth/size/body

increased heart weight ( J:234490 )

• more so than in Tg(Myh6/tetO-Tnnc1*L48Q)2Jmol mice

muscle

abnormal myocardial fiber physiology ( J:234490 )

• increased unloaded twitch force