Secondary palate development

The development of the secondary palate commences in the sixth week of human embryological development. It is characterised by the formation of two palatal shelves on the maxillary prominences, the elevation of these shelves to a horizontal position, and then a process of palatal fusion between the horizontal shelves. The shelves will also fuse anteriorly upon the primary palate, with the incisive foramen being the landmark between the primary palate and secondary palate. This forms what is known as the roof of the mouth, or the hard palate.

The formation and development of the secondary palate occurs through signalling molecules SHH, BMP-2, FGF-8 among others.

Failure of the secondary palate to develop correctly may result in a Cleft palate disorder.

Formation of palatal shelves
The formation of the vertical palatal shelves occurs during week 7 of embryological development, on the maxillary processes of the head of embryo, lateral to the developing tongue.

Palatal shelf elevation
The elevation of the palatal shelves from a vertical position to a horizontal one occurs during week 8 of embryological development. It is unknown as to what exactly is the direct cause of this movement is, but a number of possibilities have been identified as follows:


 * Muscular contraction;
 * Hydrostatic forces exerted by Glycosaminoglycans and Hyaluronan;
 * Mesenchymal reorganisation;
 * Mesenchyme cell contraction;
 * Epithelial reogranisation
 * Movement of the developing tongue

Suggested mechanisms for palatal fusion
Fusion between the two palatal shelves occurs during week 9 of embryonic development. In this time, the elevated palatal shelves join together to form one continuous structure, with the medial edge epithelium (the shelf surfaces which are closest to each other) disappearing.

The specific mechanism by which the medial edge epithelium disappears has been differed over by academics. The three most distinguished theories related to the explanation of palatal fusion are as follows:


 * Epithelial apoptosis;
 * Epithelial-to-mesenchymal transformation;
 * Epithelial cell migration.