Literature DB >> 15229178

Fgf3 signaling from the ventral diencephalon is required for early specification and subsequent survival of the zebrafish adenohypophysis.

Wiebke Herzog1, Carmen Sonntag, Sophia von der Hardt, Henry H Roehl, Zoltan M Varga, Matthias Hammerschmidt.   

Abstract

The pituitary gland consists of two major parts: the neurohypophysis, which is of neural origin; and the adenohypophysis, which is of non-neural ectodermal origin. Development of the adenohypophysis is governed by signaling proteins from the infundibulum, a ventral structure of the diencephalon that gives rise to the neurohypophysis. In mouse, the fibroblast growth factors Fgf8, Fgf10 and Fgf18 are thought to affect multiple processes of pituitary development: morphogenesis and patterning of the adenohypophyseal anlage; and survival, proliferation and differential specification of adenohypophyseal progenitor cells. Here, we investigate the role of Fgf3 during pituitary development in the zebrafish, analyzing lia/fgf3 null mutants. We show that Fgf3 signaling from the ventral diencephalon is required in a non-cell autonomous fashion to induce the expression of lim3, pit1 and other pituitary-specific genes in the underlying adenohypophyseal progenitor cells. Despite the absence of such early specification steps, fgf3 mutants continue to form a distinct pituitary anlage of normal size and shape, until adenohypophyseal cells die by apoptosis. We further show that Sonic Hedgehog (Shh) cannot rescue pituitary development, although it is able to induce adenohypophyseal cells in ectopic placodal regions of fgf3 mutants, indicating that Fgf3 does not act via Shh, and that Shh can act independently of Fgf3. In sum, our data suggest that Fgf3 signaling primarily promotes the transcriptional activation of genes regulating early specification steps of adenohypophyseal progenitor cells. This early specification seems to be essential for the subsequent survival of pituitary cells, but not for pituitary morphogenesis or pituitary cell proliferation.

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Year:  2004        PMID: 15229178     DOI: 10.1242/dev.01235

Source DB:  PubMed          Journal:  Development        ISSN: 0950-1991            Impact factor:   6.868


  38 in total

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3.  Graded hedgehog and fibroblast growth factor signaling independently regulate pituitary cell fates and help establish the pars distalis and pars intermedia of the zebrafish adenohypophysis.

Authors:  Burcu Guner; A Tuba Ozacar; Jeanne E Thomas; Rolf O Karlstrom
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4.  Fgf and Hh signalling act on a symmetrical pre-pattern to specify anterior and posterior identity in the zebrafish otic placode and vesicle.

Authors:  Katherine L Hammond; Tanya T Whitfield
Journal:  Development       Date:  2011-08-10       Impact factor: 6.868

5.  Overlapping functions of Pea3 ETS transcription factors in FGF signaling during zebrafish development.

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6.  FGF-dependent midline-derived progenitor cells in hypothalamic infundibular development.

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Journal:  Development       Date:  2011-06       Impact factor: 6.868

7.  Otx2b mutant zebrafish have pituitary, eye and mandible defects that model mammalian disease.

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Review 8.  Establishing the pre-placodal region and breaking it into placodes with distinct identities.

Authors:  Jean-Pierre Saint-Jeannet; Sally A Moody
Journal:  Dev Biol       Date:  2014-02-24       Impact factor: 3.582

9.  Influence of growth and transcriptional factors, and signaling molecules on early human pituitary development.

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10.  Dynamic coupling of pattern formation and morphogenesis in the developing vertebrate retina.

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