Placental overgrowth in mice lacking the imprinted gene Ipl
AUTOR(ES)
Frank, Dale
FONTE
The National Academy of Sciences
RESUMO
The Ipl (Tssc3) gene lies in an extended imprinted region of distal mouse chromosome 7, which also contains the Igf2 gene. Expression of Ipl is highest in placenta and yolk sac, where its mRNA is derived almost entirely from the maternal allele. Ipl encodes a small cytoplasmic protein with a pleckstrin-homology (PH) domain. We constructed two lines of mice with germ-line deletions of this gene (Iplneo and IplloxP) and another line deleted for the similar but nonimprinted gene Tih1. All three lines were viable. There was consistent overgrowth of the Ipl-null placentas, with expansion of the spongiotrophoblast. These larger placentas did not confer a fetal growth advantage; fetal size was normal in Ipl nulls with the Iplneo allele and was decreased slightly in nulls with the IplloxP allele. When bred into an Igf2 mutant background, the Ipl deletion partially rescued the placental but not fetal growth deficiency. Neither fetal nor placental growth was affected by deletion of Tih1. These results show a nonredundant function for Ipl in restraining placental growth. The data further indicate that Ipl can act, at least in part, independently of insulin-like growth factor-2 signaling. Thus, genomic imprinting regulates multiple pathways to control placental size.
ACESSO AO ARTIGO
http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=124258Documentos Relacionados
- Placental failure in mice lacking the homeobox gene Dlx3
- Placental Failure in Mice Lacking the Mammalian Homolog of Glial Cells Missing, GCMa
- Disruption of the imprinted Grb10 gene leads to disproportionate overgrowth by an Igf2-independent mechanism
- Placental defects and embryonic lethality in mice lacking suppressor of cytokine signaling 3
- Immune function in mice lacking the perforin gene.
