Mouse (47 sources):
abnormal apoptosis,
abnormal cardiac muscle relaxation,
abnormal diaphragm morphology,
abnormal fetal atrioventricular canal morphology,
abnormal gastrulation,
abnormal heart shape,
abnormal intercalated disk morphology,
abnormal interventricular groove morphology,
abnormal mature B cell morphology,
abnormal myocardial fiber morphology,
abnormal myocardium layer morphology,
abnormal pericardium morphology,
abnormal Z line morphology,
absent marginal zone B cells,
absent mesoderm,
cardiac fibrosis,
cardiac hypertrophy,
cardiovascular system phenotype,
craniofacial phenotype,
decreased B-1 B cell number,
decreased birth weight,
decreased CD4-positive, alpha beta T cell number,
decreased embryo size,
decreased skeletal muscle mass,
decreased thymocyte number,
decreased ventricle muscle contractility,
dilated heart ventricle,
disorganized myocardium,
distended pericardium,
embryonic growth arrest,
embryonic growth retardation,
embryonic lethality, complete penetrance,
embryonic lethality during organogenesis, complete penetrance,
failure of primitive streak formation,
hearing/vestibular/ear phenotype,
increased cardiomyocyte apoptosis,
increased heart left ventricle size,
mandible hypoplasia,
neonatal lethality, complete penetrance,
no abnormal phenotype detected,
no spontaneous movement,
postnatal lethality, complete penetrance,
premature death,
thin interventricular septum,
thin myocardium,
trabecula carnea hypoplasia,
vascular smooth muscle hypotrophy
[+]
|
Gene expression phenotype annotations where the gene of interest has been
disrupted (manipulated) or is the gene assayed (assayed). Computed annotations are derived from
differential expression analysis from Xenbase processed GEO data with the criteria of a TPM >= 1,
FDR <= 0.05 and an absolute LogFC >= 2.