About   Help   FAQ
Phenotypes associated with this allele
Allele Symbol
Allele Name
Allele ID
Acvr1tm1Vk
targeted mutation 1, Vesa Kaartinen
MGI:2651395
Summary 4 genotypes
Jump to Allelic Composition Genetic Background Genotype ID
cn1
Acvr1tm1Glh/Acvr1tm1Vk
Gt(ROSA)26Sortm1.2(CAG-EGFP)Glh/Gt(ROSA)26Sor+
Tg(Tek-cre)1Ywa/0
involves: 129 * C57BL/6 * FVB/N * SJL MGI:7278774
cn2
Acvr1tm1Vk/Acvr1tm1.1Vk
Tg(Tek-cre)12Flv/0
involves: 129S1/Sv * 129X1/SvJ * C3H * C57BL/6 MGI:3697608
cn3
Acvr1tm1Vk/Acvr1tm1.1Vk
H2az2Tg(Wnt1-cre)11Rth/H2az2+
involves: 129S1/Sv * 129X1/SvJ * C57BL/6 * CBA MGI:3697607
cn4
Acvr1tm1Vk/Acvr1tm1.1Vk
Tg(Myh6-cre)2182Mds/0
involves: 129S1/Sv * 129X1/SvJ * FVB/N MGI:3697609


Genotype
MGI:7278774
cn1
Allelic
Composition
Acvr1tm1Glh/Acvr1tm1Vk
Gt(ROSA)26Sortm1.2(CAG-EGFP)Glh/Gt(ROSA)26Sor+
Tg(Tek-cre)1Ywa/0
Genetic
Background
involves: 129 * C57BL/6 * FVB/N * SJL
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Acvr1tm1Glh mutation (0 available); any Acvr1 mutation (44 available)
Acvr1tm1Vk mutation (0 available); any Acvr1 mutation (44 available)
Gt(ROSA)26Sortm1.2(CAG-EGFP)Glh mutation (0 available); any Gt(ROSA)26Sor mutation (993 available)
Tg(Tek-cre)1Ywa mutation (6 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
homeostasis/metabolism
• pinch injury of adult gastrocnemius muscle results in a 50-fold increase in heterotopic ossification volume compared to mice that have one wild-type allele of Acvr1

skeleton
• pinch injury of adult gastrocnemius muscle results in a 50-fold increase in heterotopic ossification volume compared to mice that have one wild-type allele of Acvr1




Genotype
MGI:3697608
cn2
Allelic
Composition
Acvr1tm1Vk/Acvr1tm1.1Vk
Tg(Tek-cre)12Flv/0
Genetic
Background
involves: 129S1/Sv * 129X1/SvJ * C3H * C57BL/6
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Acvr1tm1.1Vk mutation (0 available); any Acvr1 mutation (44 available)
Acvr1tm1Vk mutation (0 available); any Acvr1 mutation (44 available)
Tg(Tek-cre)12Flv mutation (1 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
mortality/aging
• only 10% of the expected 25% of mutants are recovered at E14.5

cardiovascular system
• endothelial cells (atrioventricular canal tissues) fail to transdifferentiate in vitro
• endothelial cells fail to populate the mesenchyme of the atrioventricular cushions
• at E14.5, surviving embryos show a range of cardiac defects
• atrioventricular cushions are of variable shape and degree of fusion with one another, or with other septal structures
• endocardial cushions are smaller at E10; reduction in mesenchymal cell number is particularly evident in the superior cushion
• atrioventricular cushions are of variable size
• 11 of 17 E14.5 embryos have defective atrioventricular valve development
• outgrowth and formation of atrioventricular leaflets is variable
• the primary atrial foramen is still patent at E14.5 in some embryos, allowing blood to shunt between right and the left atria
• 11 of 17 E14.5 embryos have defective atrioventricular septation
• 15 of 17 E14.5 embryos have a ventricular septal defect of varying severity, where the secondary ventricular foramen has not closed
• the primary atrial foramen is still patent at E14.5 in some embryos, allowing blood to shunt between right and the left atria

cellular
• endothelial cells (atrioventricular canal tissues) fail to transdifferentiate in vitro




Genotype
MGI:3697607
cn3
Allelic
Composition
Acvr1tm1Vk/Acvr1tm1.1Vk
H2az2Tg(Wnt1-cre)11Rth/H2az2+
Genetic
Background
involves: 129S1/Sv * 129X1/SvJ * C57BL/6 * CBA
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Acvr1tm1.1Vk mutation (0 available); any Acvr1 mutation (44 available)
Acvr1tm1Vk mutation (0 available); any Acvr1 mutation (44 available)
H2az2Tg(Wnt1-cre)11Rth mutation (2 available); any H2az2 mutation (26 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
mortality/aging
• mutants that are born alive die during the first postnatal day
• about 40% die in utero (J:90453)
• only 60% of expected numbers are recovered at birth, however the expected numbers are recovered at E14, indicating 40% lethality between E14 and birth (J:90988)

cardiovascular system
• display abnormal regression of the pharyngeal arch arteries
• at E11.5, the 6th arteries display bilaterally inappropriate regression
• at E11.5, the 3rd arteries display bilaterally inappropriate regression
• aortic arch defects
• 77% exhibit either a short or missing brachiocephalic artery so that the right common carotid artery directly branches from the truncus arteriosus
• 77% exhibit either a short or missing brachiocephalic artery
• the distal outflow tract has reduced numbers of neural crest cells
• the proximal outflow tract is essentially devoid of neural crest cells
• differentiation of neural crest cells to smooth muscle around aortic arch arteries is deficient
• the proximal outflow tract is essentially devoid of neural crest cells while the distal outflow tract has reduced numbers of neural crest cells
• outflow tract cushions are reduced in size
• 100% penentrance or persistent truncus arteriosus type A2 (complete failure of outflow tract septation)
• persistent truncus arteriosus is associated with a ventricular septation defect
• 100% penetrance
• 85% show hyperplastic right ventricle

nervous system
• the distal outflow tract has reduced numbers of neural crest cells
• the proximal outflow tract is essentially devoid of neural crest cells
• differentiation of neural crest cells to smooth muscle around aortic arch arteries is deficient

craniofacial
• display abnormal regression of the pharyngeal arch arteries
• at E11.5, the 6th arteries display bilaterally inappropriate regression
• at E11.5, the 3rd arteries display bilaterally inappropriate regression
• the anterior cartilage derived from the distal extremity of Meckel's cartilage is absent
• anterior region of Meckel's cartilage displays retarded growth and also fails to fuse at E15
• display approximately a 3-fold reduction in proliferation of chondrocytes in the anterior and interior parts of Meckel's cartilage at E13
• enlarged frontal fontanels in newborns
• squamous parts of the frontal bones lack ossification towards the metopic region, resulting in enlarged frontal fontanels in newborns
• squamal bones lack the retrotympanic process
• the temporal squama is smaller, lacking the lower portion with the mandibular fossa and its joint cartilage
• completely absent zygomatic process of the squamal bone
• zygomatic arches are incomplete in newborns, with developed maxillary zygomatic process but completely absent jugal (zygomatic) bone and zygomatic process of the squamal bone
• the mandibular fossa and its joint cartilage are missing
• coronoid process of the mandible is rudimentary in size
• the mental symphysis is not formed resulting in persistently separate mandibular bones
• the temporomandibular articulation is undetectable
• hypotrophic mandible is apparent as early as E14
• mandible is about 40% shorter
• completely absent jugal (zygomatic) bone
• slightly shorter manubrium mallei
• complete cleft of the secondary palate
• palatal shelves fail to elevate, either bilaterally or unilaterally, at E14
• in newborns, the unfused palatal shelves are bilaterally elevated, indicating that cleft palate develops as a result of delayed, asynchronous elevation of palatal shelves
• newborns have a shorter head

embryo
• display abnormal regression of the pharyngeal arch arteries
• at E11.5, the 6th arteries display bilaterally inappropriate regression
• at E11.5, the 3rd arteries display bilaterally inappropriate regression
• the distal outflow tract has reduced numbers of neural crest cells
• the proximal outflow tract is essentially devoid of neural crest cells
• differentiation of neural crest cells to smooth muscle around aortic arch arteries is deficient
• migration of mutant neural crest cells to the outflow tract is impaired

behavior/neurological
• newborns lack milk in stomachs and fail to suckle

digestive/alimentary system
• complete cleft of the secondary palate
• palatal shelves fail to elevate, either bilaterally or unilaterally, at E14
• in newborns, the unfused palatal shelves are bilaterally elevated, indicating that cleft palate develops as a result of delayed, asynchronous elevation of palatal shelves

hearing/vestibular/ear
• slightly shorter manubrium mallei

skeleton
• enlarged frontal fontanels in newborns
• squamous parts of the frontal bones lack ossification towards the metopic region, resulting in enlarged frontal fontanels in newborns
• squamal bones lack the retrotympanic process
• the temporal squama is smaller, lacking the lower portion with the mandibular fossa and its joint cartilage
• completely absent zygomatic process of the squamal bone
• zygomatic arches are incomplete in newborns, with developed maxillary zygomatic process but completely absent jugal (zygomatic) bone and zygomatic process of the squamal bone
• the mandibular fossa and its joint cartilage are missing
• coronoid process of the mandible is rudimentary in size
• the mental symphysis is not formed resulting in persistently separate mandibular bones
• the temporomandibular articulation is undetectable
• hypotrophic mandible is apparent as early as E14
• mandible is about 40% shorter
• completely absent jugal (zygomatic) bone
• slightly shorter manubrium mallei
• secondary cartilage of the mandibular condyle does not develop, making the temporomandibular articulation undetectable
• the secondary cartilage of the mandibular angular process is completely missing
• the anterior cartilage derived from the distal extremity of Meckel's cartilage is absent
• anterior region of Meckel's cartilage displays retarded growth and also fails to fuse at E15
• display approximately a 3-fold reduction in proliferation of chondrocytes in the anterior and interior parts of Meckel's cartilage at E13

cellular
• differentiation of neural crest cells to smooth muscle around aortic arch arteries is deficient
• migration of mutant neural crest cells to the outflow tract is impaired

growth/size/body
• 100% penetrance
• complete cleft of the secondary palate
• palatal shelves fail to elevate, either bilaterally or unilaterally, at E14
• in newborns, the unfused palatal shelves are bilaterally elevated, indicating that cleft palate develops as a result of delayed, asynchronous elevation of palatal shelves
• newborns have a shorter head




Genotype
MGI:3697609
cn4
Allelic
Composition
Acvr1tm1Vk/Acvr1tm1.1Vk
Tg(Myh6-cre)2182Mds/0
Genetic
Background
involves: 129S1/Sv * 129X1/SvJ * FVB/N
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Acvr1tm1.1Vk mutation (0 available); any Acvr1 mutation (44 available)
Acvr1tm1Vk mutation (0 available); any Acvr1 mutation (44 available)
Tg(Myh6-cre)2182Mds mutation (3 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
cardiovascular system
N
• mutants are viable and fail to display any detectable altered cardiac phenotype





Contributing Projects:
Mouse Genome Database (MGD), Gene Expression Database (GXD), Mouse Models of Human Cancer database (MMHCdb) (formerly Mouse Tumor Biology (MTB)), Gene Ontology (GO)
Citing These Resources
Funding Information
Warranty Disclaimer, Privacy Notice, Licensing, & Copyright
Send questions and comments to User Support.
last database update
11/12/2024
MGI 6.24
The Jackson Laboratory