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Development ePress online publication date 3 Oct 2007
doi: 10.1242/dev.004325
Research report
Mutations in the BMP pathway in mice support the existence of two molecular classes of holoprosencephaly
Marie Fernandes,
Grigoriy Gutin,
Heather Alcorn,
Susan K. McConnell,
and
Jean M. Hébert*
* Author for correspondence (e-mail: jhebert{at}aecom.yu.edu)
Holoprosencephaly (HPE) is a devastating forebrain abnormality with a range of morphological defects characterized by loss of midline tissue. In the telencephalon, the embryonic precursor of the cerebral hemispheres, specialized cell types form a midline that separates the hemispheres. In the present study, deletion of the BMP receptor genes, Bmpr1b and Bmpr1a, in the mouse telencephalon results in a loss of all dorsal midline cell types without affecting the specification of cortical and ventral precursors. In the holoprosencephalic Shh-/- mutant, by contrast, ventral patterning is disrupted, whereas the dorsal midline initially forms. This suggests that two separate developmental mechanisms can underlie the ontogeny of HPE. The Bmpr1a;Bmpr1b mutant provides a model for a subclass of HPE in humans: midline inter-hemispheric HPE.

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© The Company of Biologists Ltd 2007