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ABSTRACT
The authors have recently demonstrated that, in the developing mouse lung, fetal plasma Ca2+ suppresses branching morphogenesis and cell proliferation while promoting fluid secretion via activation of the extracellular Ca2+-sensing receptor (CaSR). The aim of the current study was to further elucidate the role of Ca2+ in lung development by studying the effects of extracellular Ca2+ on fetal lung development in mice lacking the CaSR. These mice were produced by exon 5 deletion in the CaSR gene. Since such a maneuver has been known to induce the expression of an exon 5-less splice variant of the CaSR in some tissues, the molecular and functional expression of this splice variant in the developing mouse lung was also investigated. Whereas there was a mild in vivo phenotype observed in these mice, in vitro sensitivity of Casr−/− lung explants to specific activators of the CaSR was unaffected. These results imply that compensatory expression of an exon 5-less splice variant rescues CaSR function in this mouse model and therefore a lung-specific, complete CaSR knockout model must be developed to fully appreciate the role for this receptor in lung development and the contribution of its ablation to postnatal respiratory disease.