| Monarch Ortholog Phenotypes
|
Mouse (40 sources):
abnormal double-negative T cell morphology,
abnormal pancreatic beta cell physiology,
abnormal placenta labyrinth morphology,
abnormal placental labyrinth vasculature morphology,
abnormal placenta morphology,
decreased cell proliferation,
decreased DN1 thymic pro-T cell number,
decreased DN2 thymocyte number,
decreased DN3 thymocyte number,
decreased DN4 thymocyte number,
decreased double-positive T cell number,
decreased embryo size,
decreased insulin secretion,
decreased pancreatic beta cell mass,
decreased pancreatic beta cell proliferation,
decreased single-positive T cell number,
decreased T cell proliferation,
decreased thymus weight,
embryonic growth retardation,
embryonic lethality during organogenesis, complete penetrance,
hematopoietic system phenotype,
immune system phenotype,
improved glucose tolerance,
increased body length,
increased bone mineral content,
increased circulating insulin-like growth factor I level,
increased double-negative T cell number,
increased epididymal fat pad weight,
increased heart weight,
increased kidney weight,
increased lean body mass,
increased liver weight,
increased pancreas weight,
increased spleen weight,
increased susceptibility to weight gain,
lethality throughout fetal growth and development, complete penetrance,
lethality throughout fetal growth and development, incomplete penetrance,
macrovesicular hepatic steatosis,
muscle phenotype,
thick placenta labyrinth
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|
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.