Mutations in the BMP pathway in mice support the existence of two molecular classes of holoprosencephaly | Zendy

Marie Fernandes | Zendy; Grigoriy Gutin | Zendy; Heather Alcorn | Zendy; Susan K. McConnell | Zendy; Jean M. Hébert | Zendy

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Mutations in the BMP pathway in mice support the existence of two molecular classes of holoprosencephaly

Author(s) -

Marie Fernandes,

Grigoriy Gutin,

Heather Alcorn,

Susan K. McConnell,

Jean M. Hébert

Publication year - 2007

Publication title -

development

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 3.754

H-Index - 325

eISSN - 1477-9129

pISSN - 0950-1991

DOI - 10.1242/dev.004325

Subject(s) - holoprosencephaly , biology , cerebrum , forebrain , anatomy , morphogenesis , sonic hedgehog , embryonic stem cell , ganglionic eminence , microbiology and biotechnology , neuroscience , genetics , central nervous system , gene , signal transduction , fetus , pregnancy

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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