Effects of Cx43 gene deletion on mouse fetal development in different genetics backgrounds: Emphasis in osteogenesis

Connexins are proteins that compose the gap junctions, and the reduction in its expression has been related with diverse physiological alterations, like some syndromes, malformations, the increase of the cellular proliferation and carcinogenesis. Among isoforms of the connexins in animal cells, the Cx43 is the most abundant and studied, having its importance been shown up in alive mice that had one allele of Cx43 (Cx43+/-) deleted. REAUME et al. related that Cx43-/- mice presented cardiac malformation and died immediately after birth. Considering the fact that this gene is expressed in many cell types, we evaluate the possibility of other tissues also to present alterations during the fetal development. Due to this, we studied the mouse development initiating in 12.5 to 19.5 DE (embryologic day) and evaluated the histology of C57BL/6 and CD1 mice searching for anomalies of Cx43+/- and Cx43-/- mice in relation to the Cx43+/+ animals. We did not find alterations in the main organs that express Cx43, nor alterations due to blood out flow related to cardiac malformations. We only found significant difference was the bones; through the evaluation of the ribs and tibia. It has been observed a delay in the development, that was more important in Cx43 knockout mice. We observed clearly that the process of cellular differentiation occurs in less efficient way, delaying processes as deposition of collagen and bone matrix. In conclusion, this study showed that Cx43 is important for bone development in mice. (AU)