Ciliary Hedgehog signaling regulates cell survival to build the facial midline

Abstract

AbstractCraniofacial defects are among the most common phenotypes caused by ciliopathies, yet the developmental and molecular etiology of these defects is poorly understood. We investigated multiple mouse models of human ciliopathies (includingTctn2, Cc2d2aandTmem231mutants)and discovered that each displays hypotelorism, a narrowing of the midface. As early in development as the end of gastrulation,Tctn2mutants displayed reduced activation of the Hedgehog (HH) pathway in the prechordal plate, the head organizer. This prechordal plate defect preceded a reduction of HH pathway activation andShhexpression in the adjacent neurectoderm. Concomitant with the reduction of HH pathway activity,Tctn2mutants exhibited increased cell death in the neurectoderm and facial ectoderm, culminating in a collapse of the facial midline. Enhancing HH signaling by decreasing the gene dosage of a negative regulator of the pathway,Ptch1,decreased cell death and rescued the midface defect in bothTctn2andCc2d2amutants. These results reveal that ciliary HH signaling mediates communication between the prechordal plate and the neurectoderm to provide cellular survival cues essential for development of the facial midline.