FGF/FGFR-2(IIIb) Signaling Is Essential for Inner Ear Morphogenesis

Pirvola, Ulla; Spencer‐Dene, Bradley; Liang, Xiaofang; Kettunen, Päivi; Thesleff, Irma; Fritzsch, Bernd; Dickson, Clive; Ylikoski, Jukka

doi:10.1523/jneurosci.20-16-06125.2000

Cited by 202 publications

(287 citation statements)

References 48 publications

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“…Fgfr2-DN (Celli et al, 1998), Fgfr2b Ϫ/Ϫ (De Moerlooze et al, 2000) and Fgfr2b Ϫ/ ϪLacZ (Revest et al, 2001) embryos exhibited dysgenesis in kidney formation; however, all Fgfr2 ⌬III/⌬III embryos do not have this organ (Li and Deng, unpublished observation). Inner ear defects of the Fgfr2 ⌬III/⌬III embryos also seem more severe than that of Fgfr2b Ϫ/Ϫ embryos (Pirvola et al, 2000;Li and Deng, unpublished observation). Apparently, the Fgfr2 ⌬III/⌬III embryo represents a more severe allele as it lacks both Fgfr2b and Fgfr2c isoforms.…”

Section: Discussionmentioning

confidence: 84%

“…In contrast, mouse embryos with a homozygous deletion of Fgfr2 Ig domain III (Fgfr2 ⌬lgIII/⌬lgIII ), which is shared by both FGFR2b and FGFR2c isoforms, died at E10.5 due to placental defects . Analysis of these mutant embryos revealed that FGFR2 is essential for induction and patterning of multiple organs, including limb, lung, inner ear, placenta, and skin (Arman et al, 1998(Arman et al, , 1999De Moerlooze et al, 2000;Pirvola et al, 2000;Revest et al, 2001;Xu et al, 1998). A similar observation was also made in embryos that overexpress a dominant-negative secreted Fgfr2 (Celli et al, 1998).…”

Section: Introductionmentioning

confidence: 99%

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Fibroblast growth factor receptor 2 (Fgfr2) plays an important role in eyelid and skin formation and patterning

Guo

et al. 2001

Developmental Dynamics

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Initiating as protruding ridges above and below the optic vesicle, the eyelids of mice grow across the eye and temporarily fuse in fetal life. Mutations of a number of genes disrupt this developmental process and result in a birth defect, "open-eyelids at birth." Here we show that a critical event for eyelid induction occurs at embryonic day 11.5 (E11.5) when the single cell-layered ectoderm in the presumptive eyelid territory increases proliferation and undergoes morphologic transition to form cube-shaped epithelial cells. Using embryos lacking the Fgfr2 Ig domain III (Fgfr2 ⌬III/⌬III ) generated by tetraploid rescue and chimeric embryo formation approaches, we demonstrate that this event is controlled by Fgfr2 signals as the Fgfr2 ⌬III/⌬III mutation blocks these changes and results in embryos without eyelids. Fgfr2 and its ligands are differentially expressed in the ectoderm and underlying mesenchyme and function in a reciprocal interacting loop that specifies eyelid development. We also demonstrate that similar defects account for failure of skin formation at early stages. Interestingly, Fgfr2-independent skin formation occurs at E14.5 mutant embryos, resulting in much thinner, yet well-differentiated epidermis. Notably, mutant skin remains thin with decreased hair density after transplantation to wild-type recipients. These data demonstrate an essential role of Fgfr2 in eyelid and skin formation and patterning. Published 2001 Wiley-Liss, Inc. †

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Section: Discussionmentioning

confidence: 84%

Section: Introductionmentioning

confidence: 99%

Fibroblast growth factor receptor 2 (Fgfr2) plays an important role in eyelid and skin formation and patterning

Guo

et al. 2001

Developmental Dynamics

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“…At early stages of embryogenesis, Fgfr1, Fgfr2, and several FGFs, including FGF3, FGF8, FGF10, and FGF19, are critical for either the induction of the otic vesicle or the initial development of the sensory epithelium (Mansour et al, 1993;Ladher et al, 2000Ladher et al, , 2005Pirvola et al, 2000Pirvola et al, , 2002Phillips et al, 2001Phillips et al, , 2004Pauley et al, 2003;. At intermediate stages of development, FGF signaling is also important; tissuespecific deletion of Fgfr1 results in severe defects in the development of the auditory sensory epithelium apparently due to a severe reduction in the precursor cells that give rise to the organ of Corti.…”

Section: Introductionmentioning

confidence: 99%

Loss of Fgfr3 leads to excess hair cell development in the mouse organ of Corti

Hayashi

Cunningham

Bermingham‐McDonogh

2006

Developmental Dynamics

111

108

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“…Fibroblast growth factor (FGF) molecules have been identified as inductive signals for otic placode development in several vertebrate species (Represa et al, 1991;Mansour et al, 1993;De Moerlooze et al, 2000;Ohuchi et al, 2000;Pirvola et al, 2000Pirvola et al, , 2002Vendrell et al, 2000;Phillips et al, 2001;Leger and Brand, 2002;Maroon et al, 2002). Depletion of FGF3 prevents otic vesicle formation in tissue explants from chick (Represa et al, 1991).…”

Section: Introductionmentioning

confidence: 99%

“…Furthermore, ectopic otic vesicles can be induced by misexpression of FGF3 in chick (Vendrell et al, 2000) or implants of beads soaked with Fgf2 and Fgf3 in Xenopus posterior trunk ectoderm . Mice with null mutations for Fgf3, Fgf10, or FGF receptors Fgfr2IIIb or Fgfr1 exhibit defects in patterning and differentiation of the inner ear (Mansour et al, 1993;De Moerlooze et al, 2000;Ohuchi et al, 2000;Pirvola et al, 2000Pirvola et al, , 2002. In zebrafish, combined loss of function for fgf3 and fgf8 (fgf3/8) leads to the complete absence of the otic placodes in most embryos (Phillips et al, 2001;Leger and Brand, 2002;Maroon et al, 2002).…”

Section: Introductionmentioning

confidence: 99%

Genetic interactions underlying otic placode induction and formation

Solomon

Kwak

Fritz

2004

Developmental Dynamics

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The formation of the otic placode is a complex process requiring multiple inductive signals. In zebrafish, fgf3 and fgf8, dlx3b and dlx4b, and foxi1 have been identified as the earliest-acting genes in this process. fgf3 and fgf8 are required as inductive signals, whereas dlx3b, dlx4b, and foxi1 appear to act directly within otic primordia. We have investigated potential interactions among these genes. Depletion of either dlx3b and dlx4b or foxi1 leads to a delay of pax2a expression in the otic primordia and reduction of the otic vesicle. Depletion of both foxi1 and dlx3b results in a complete ablation of otic placode formation. A strong synergistic interaction is also observed among foxi1, fgf3, and fgf8, and a weaker interaction among dlx3b, fgf3, and fgf8. Misexpression of foxi1 can induce expression of pax8, an early marker for the otic primordia, in embryos treated with an inhibitor of fibroblast growth factor (FGF) signaling. Conversely, morpholino knockdown of foxi1 blocks ectopic pax8 expression and otic vesicle formation induced by misexpression of fgf3 and/or fgf8. The observed genetic interactions suggest a model in which foxi1 and dlx3b/dlx4b act in independent pathways together with distinct phases of FGF signaling to promote otic placode induction and development. Developmental Dynamics 230:419 -433, 2004.

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FGF/FGFR-2(IIIb) Signaling Is Essential for Inner Ear Morphogenesis

Cited by 202 publications

References 48 publications

Fibroblast growth factor receptor 2 (Fgfr2) plays an important role in eyelid and skin formation and patterning

Fibroblast growth factor receptor 2 (Fgfr2) plays an important role in eyelid and skin formation and patterning

Loss of Fgfr3 leads to excess hair cell development in the mouse organ of Corti

Genetic interactions underlying otic placode induction and formation

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