Mice homozygous for a targeted disruption of the proto-oncogene int-2 have developmental defects in the tail and inner ear

S.L. Mansour; J.M. Goddard; M.R. Capecchi

doi:10.1242/dev.117.1.13

Mice homozygous for a targeted disruption of the proto-oncogene int-2 have developmental defects in the tail and inner ear

Development ◽

10.1242/dev.117.1.13 ◽

1993 ◽

Vol 117 (1) ◽

pp. 13-28 ◽

Cited By ~ 65

Author(s):

S.L. Mansour ◽

J.M. Goddard ◽

M.R. Capecchi

Keyword(s):

Inner Ear ◽

Genetic Background ◽

Mutant Allele ◽

Primitive Streak ◽

Otic Vesicle ◽

Stochastic Variation ◽

Targeted Disruption ◽

Developmental Defects ◽

Variable Expressivity ◽

Reduced Penetrance

We derived mice that carry a targeted insertion of a neor gene in the int-2 (Fgf-3) proto-oncogene coding sequences. The mutation was found to be recessive and mice that were homozygous for the insertion did not often survive to adulthood. The mutant mice had defects in the development of the tail and inner ear that could be correlated with disruption of int-2 expression in the posterior primitive streak and hindbrain or otic vesicle. While the tail phenotype was 100% penetrant, we found that the inner ear phenotype had reduced penetrance and variable expressivity. The variable expressivity could not be attributed to variability in the genetic background of the mutant allele or to leaky expression from the mutant allele. Thus, we conclude that even in a uniform genetic background, stochastic variation in the expression of a developmental circuit can result in dramatic differences in phenotypic consequences.

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Targeted disruption ofint-2 (fgf-3) causes developmental defects in the tail and inner ear

Molecular Reproduction and Development ◽

10.1002/mrd.1080390111 ◽

1994 ◽

Vol 39 (1) ◽

pp. 62-68 ◽

Cited By ~ 40

Author(s):

Suzanne L. Mansour

Keyword(s):

Inner Ear ◽

Targeted Disruption ◽

Developmental Defects

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Inner Ear and Muscle Developmental Defects in Smpx-Deficient Zebrafish Embryos

International Journal of Molecular Sciences ◽

10.3390/ijms22126497 ◽

2021 ◽

Vol 22 (12) ◽

pp. 6497

Author(s):

Anna Ghilardi ◽

Alberto Diana ◽

Renato Bacchetta ◽

Nadia Santo ◽

Miriam Ascagni ◽

...

Keyword(s):

Hearing Loss ◽

Inner Ear ◽

Hair Cells ◽

Muscle Fibers ◽

Underlying Mechanism ◽

Loss Of Function ◽

Zebrafish Model ◽

Developmental Defects ◽

Inner Ear Development ◽

Syndromic Hearing Loss

The last decade has witnessed the identification of several families affected by hereditary non-syndromic hearing loss (NSHL) caused by mutations in the SMPX gene and the loss of function has been suggested as the underlying mechanism. In the attempt to confirm this hypothesis we generated an Smpx-deficient zebrafish model, pointing out its crucial role in proper inner ear development. Indeed, a marked decrease in the number of kinocilia together with structural alterations of the stereocilia and the kinocilium itself in the hair cells of the inner ear were observed. We also report the impairment of the mechanotransduction by the hair cells, making SMPX a potential key player in the construction of the machinery necessary for sound detection. This wealth of evidence provides the first possible explanation for hearing loss in SMPX-mutated patients. Additionally, we observed a clear muscular phenotype consisting of the defective organization and functioning of muscle fibers, strongly suggesting a potential role for the protein in the development of muscle fibers. This piece of evidence highlights the need for more in-depth analyses in search for possible correlations between SMPX mutations and muscular disorders in humans, thus potentially turning this non-syndromic hearing loss-associated gene into the genetic cause of dysfunctions characterized by more than one symptom, making SMPX a novel syndromic gene.

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The abnormalities of the inner ear in kreisler mice

Development ◽

10.1242/dev.12.3.475 ◽

1964 ◽

Vol 12 (3) ◽

pp. 475-490

Author(s):

M. S. Deol

Keyword(s):

Inner Ear ◽

Recessive Gene ◽

Cresyl Violet ◽

Otic Vesicle ◽

Litter Mate ◽

Abnormal Position ◽

Sectioned Material

The recessive gene kreisler (symbol kr) was discovered by Hertwig (1942a), who later described its effects on behaviour (1942b) and the inner ear (1944, 1956). She found that it was possible to trace the anomalies of the ear back to 9-day embryos, when the otic vesicle can be seen to be situated in an abnormal position. The present study was aimed at discovering the cause of this abnormality, and at giving a fuller account of the later development of the ear. Material and Methods The particulars of the sectioned material are given in Table 1. Only litter-mate controls were used throughout. The embryos were fixed in Bouin's fluid, sectioned at 7½ or 10 μ, depending on their age, and stained with Ehrlich's haematoxylin and eosin. The older material was fixed in Witmaack's fluid or formalin, sectioned at 10 μ, and stained either the same way or with cresyl violet or Weil's iron haematoxylin.

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Inherited variants in CHD3 demonstrate variable expressivity in Snijders Blok-Campeau syndrome

10.1101/2021.10.04.21264162 ◽

2021 ◽

Author(s):

Jet van der Spek ◽

Joery den Hoed ◽

Lot Snijders Blok ◽

Alexander J. M. Dingemans ◽

Dick Schijven ◽

...

Keyword(s):

De Novo ◽

Neurodevelopmental Disorder ◽

Underlying Mechanism ◽

Next Generation Sequencing Data ◽

Sequencing Data ◽

Human Phenotype ◽

Variable Expressivity ◽

Pathogenic Variants ◽

Reduced Penetrance ◽

Coding Variants

Interpretation of next-generation sequencing data of individuals with an apparent sporadic neurodevelopmental disorder (NDD) often focusses on pathogenic variants in genes associated with NDD, assuming full clinical penetrance with limited variable expressivity. Consequently, inherited variants in genes associated with dominant disorders may be overlooked when the transmitting parent is clinically unaffected. While de novo variants explain a substantial proportion of cases with NDDs, a significant number remains undiagnosed possibly explained by coding variants associated with reduced penetrance and variable expressivity. We characterized twenty families with inherited heterozygous missense or protein-truncating variants (PTVs) in CHD3, a gene in which de novo variants cause Snijders Blok-Campeau syndrome, characterized by intellectual disability, speech delay and recognizable facial features (SNIBCPS). Notably, the majority of the inherited CHD3 variants were maternally transmitted. Computational facial and human phenotype ontology-based comparisons demonstrated that the phenotypic features of probands with inherited CHD3 variants overlap with the phenotype previously associated with de novo variants in the gene, while carrier parents are mildly or not affected, suggesting variable expressivity. Additionally, similarly reduced expression levels of CHD3 protein in cells of an affected proband and of related healthy carriers with a CHD3 PTV, suggested that compensation of expression from the wildtype allele is unlikely to be an underlying mechanism. Our results point to a significant role of inherited variation in SNIBCPS, a finding that is critical for correct variant interpretation and genetic counseling and warrants further investigation towards understanding the broader contributions of such variation to the landscape of human disease.

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Retinoic acid modulation of the early development of the inner ear is associated with the control of c-fos expression

Development ◽

10.1242/dev.110.4.1081 ◽

1990 ◽

Vol 110 (4) ◽

pp. 1081-1090 ◽

Cited By ~ 2

Author(s):

J. Represa ◽

A. Sanchez ◽

C. Miner ◽

J. Lewis ◽

F. Giraldez

Keyword(s):

Cell Proliferation ◽

Retinoic Acid ◽

Inner Ear ◽

Early Development ◽

Otic Vesicle ◽

Low Concentrations ◽

Full Effect ◽

20 Nm ◽

Otic Vesicles

The effects of retinoic acid (RA) on the early development of the inner ear were studied in vitro using isolated chick embryo vesicles. Low concentrations of RA (1–50 nM) inhibited vesicular growth in stage 18 otic vesicles that were made quiescent and then reactivated by either serum or bombesin. Growth inhibition was concentration-dependent and was paralleled by a reduction in the rate of DNA synthesis as measured by [3H]thymidine incorporation. Half-inhibition occurred between 1 and 10 nM RA, and the full effect at 20 nM. Retinoic acid, in the presence of serum, induced the precocious differentiation of (1) secretory epithelium, the tegmentum vasculosum and endolymphatic sac and (2) early sensory and supporting epithelia. These structures were positioned in their corresponding normal presumptive areas. The overall direction of growth was reversed by RA and the ratio of the internal to the external vesicular surface area increased with RA concentration. The expression of the nuclear proto-oncogene c-fos in the developing otic vesicle was transient and stage-dependent. High levels of c-fos mRNA were positively correlated with cell proliferation. Incubation of growth-arrested otic vesicles with bombesin plus insulin at concentrations that induced cell proliferation produced a strong induction of c-fos. This mitogen-induced expression was suppressed by 25 nM RA. The results suggest (1) a role for retinoic acid in controlling the early development of the inner ear and (2) that this control is effected through the regulation of the proto-oncogene c-fos.

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Pattern of expression of the jun family of transcription factors during the early development of the inner ear: implications in apoptosis

Journal of Cell Science ◽

10.1242/jcs.112.22.3967 ◽

1999 ◽

Vol 112 (22) ◽

pp. 3967-3974

Author(s):

C. Sanz ◽

Y. Leon ◽

S. Canon ◽

L. Alvarez ◽

F. Giraldez ◽

...

Keyword(s):

Cell Death ◽

Transcription Factors ◽

Nerve Growth Factor ◽

Growth Factor ◽

Inner Ear ◽

Otic Vesicle ◽

Mobility Shift ◽

Nerve Growth ◽

Vestibular Ganglion ◽

Amino Terminal

Jun transcription factors have been implicated in the regulation of cell proliferation, differentiation and apoptosis. We have investigated the relationship between Jun expression and cell death in the developing chicken inner ear. c-jun and junD transcripts were expressed in the epithelium of the otic placode and otic vesicle. c-jun expression was restricted to the dorsal area of the otic pit (stages 14–17), dorsal otic vesicle and cochleo-vestibular ganglion (stages 18–20). junD expression was transient and occurred in the dorsal and upper medial aspects of the otic pit and otic cup, but it was down-regulated in the otic vesicle. A parallel TUNEL analysis revealed that expression of c-jun co-located within areas of intense apoptosis. Furthermore, phosphorylation of c-Jun at serine-63 by Jun amino-terminal-kinases was detected in the dorsal otic pit, otic vesicle and cochleo-vestibular ganglion. c-Jun protein exhibited DNA binding activity, as assessed by gel mobility shift assays. The association between c-Jun and apoptosis was further demonstrated by studying nerve growth factor-induced apoptosis in cultured otic vesicles. Nerve growth factor-induced cell death and c-Jun phosphorylation that were suppressed by insulin-like growth factor-I and by viral-mediated overexpression of Raf, which had survival effects. In conclusion, the precise regulation of the expression and activity of Jun proteins in the otic primordium suggests that it may operate as a fundamental mechanism during organogenesis.

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Nkx5-1 controls semicircular canal formation in the mouse inner ear

Development ◽

10.1242/dev.125.1.33 ◽

1998 ◽

Vol 125 (1) ◽

pp. 33-39 ◽

Cited By ~ 5

Author(s):

T. Hadrys ◽

T. Braun ◽

S. Rinkwitz-Brandt ◽

H.H. Arnold ◽

E. Bober

Keyword(s):

Homologous Recombination ◽

Inner Ear ◽

Homeobox Gene ◽

Semicircular Canals ◽

Otic Vesicle ◽

Null Mutation ◽

Complex Structures ◽

Vestibular Organ ◽

Inner Ear Development ◽

Vestibular Organs

The inner ear develops from the otic vesicle, a one-cell-thick epithelium, which eventually transforms into highly complex structures including the sensory organs for balance (vestibulum) and hearing (cochlea). Several mouse inner ear mutations with hearing and balance defects have been described but for most the underlying genes have not been identified, for example, the genes controlling the development of the vestibular organs. Here, we report the inactivation of the homeobox gene, Nkx5-1, by homologous recombination in mice. This gene is expressed in vestibular structures throughout inner ear development. Mice carrying the Nkx5-1 null mutation exhibit behavioural abnormalities that resemble the typical hyperactivity and circling movements of the shaker/waltzer type mutants. The balance defect correlates with severe malformations of the vestibular organ in Nkx5-1(−/−) mutants, which fail to develop the semicircular canals. Nkx5-1 is the first ear-specific molecule identified to play a crucial role in the formation of the mammalian vestibular system.

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Mutations affecting development of the zebrafish inner ear and lateral line

Development ◽

10.1242/dev.123.1.241 ◽

1996 ◽

Vol 123 (1) ◽

pp. 241-254 ◽

Cited By ~ 33

Author(s):

T.T. Whitfield ◽

M. Granato ◽

F.J. van Eeden ◽

U. Schach ◽

M. Brand ◽

...

Keyword(s):

Inner Ear ◽

Lateral Line ◽

Large Scale ◽

Sensory System ◽

Semicircular Canals ◽

Abnormal Development ◽

Pigment Cells ◽

Otic Vesicle ◽

In The Wild ◽

Complementation Groups

Mutations giving rise to anatomical defects in the inner ear have been isolated in a large scale screen for mutations causing visible abnormalities in the zebrafish embryo (Haffter, P., Granato, M., Brand, M. et al. (1996) Development 123, 1–36). 58 mutants have been classified as having a primary ear phenotype; these fall into several phenotypic classes, affecting presence or size of the otoliths, size and shape of the otic vesicle and formation of the semicircular canals, and define at least 20 complementation groups. Mutations in seven genes cause loss of one or both otoliths, but do not appear to affect development of other structures within the ear. Mutations in seven genes affect morphology and patterning of the inner ear epithelium, including formation of the semicircular canals and, in some, development of sensory patches (maculae and cristae). Within this class, dog-eared mutants show abnormal development of semicircular canals and lack cristae within the ear, while in van gogh, semicircular canals fail to form altogether, resulting in a tiny otic vesicle containing a single sensory patch. Both these mutants show defects in the expression of homeobox genes within the otic vesicle. In a further class of mutants, ear size is affected while patterning appears to be relatively normal; mutations in three genes cause expansion of the otic vesicle, while in little ears and microtic, the ear is abnormally small, but still contains all five sensory patches, as in the wild type. Many of the ear and otolith mutants show an expected behavioural phenotype: embryos fail to balance correctly, and may swim on their sides, upside down, or in circles. Several mutants with similar balance defects have also been isolated that have no obvious structural ear defect, but that may include mutants with vestibular dysfunction of the inner ear (Granato, M., van Eeden, F. J. M., Schach, U. et al. (1996) Development, 123, 399–413,). Mutations in 19 genes causing primary defects in other structures also show an ear defect. In particular, ear phenotypes are often found in conjunction with defects of neural crest derivatives (pigment cells and/or cartilaginous elements of the jaw). At least one mutant, dog-eared, shows defects in both the ear and another placodally derived sensory system, the lateral line, while hypersensitive mutants have additional trunk lateral line organs.

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Spemann organizer gene Goosecoid promotes delamination of neuroblasts from the otic vesicle

Proceedings of the National Academy of Sciences ◽

10.1073/pnas.1609146113 ◽

2016 ◽

Vol 113 (44) ◽

pp. E6840-E6848 ◽

Cited By ~ 7

Author(s):

Husniye Kantarci ◽

Andrea Gerberding ◽

Bruce B. Riley

Keyword(s):

Inner Ear ◽

Epithelial To Mesenchymal Transition ◽

Otic Vesicle ◽

General Function ◽

Cellular Dynamics ◽

Mesenchymal Transition ◽

Spemann Organizer ◽

Developmental Role ◽

Overlapping Domains ◽

Low Incidence

Neurons of the Statoacoustic Ganglion (SAG), which innervate the inner ear, originate as neuroblasts in the floor of the otic vesicle and subsequently delaminate and migrate toward the hindbrain before completing differentiation. In all vertebrates, locally expressed Fgf initiates SAG development by inducing expression of Neurogenin1 (Ngn1) in the floor of the otic vesicle. However, not all Ngn1-positive cells undergo delamination, nor has the mechanism controlling SAG delamination been elucidated. Here we report that Goosecoid (Gsc), best known for regulating cellular dynamics in the Spemann organizer, regulates delamination of neuroblasts in the otic vesicle. In zebrafish, Fgf coregulates expression of Gsc and Ngn1 in partially overlapping domains, with delamination occurring primarily in the zone of overlap. Loss of Gsc severely inhibits delamination, whereas overexpression of Gsc greatly increases delamination. Comisexpression of Ngn1 and Gsc induces ectopic delamination of some cells from the medial wall of the otic vesicle but with a low incidence, suggesting the action of a local inhibitor. The medial marker Pax2a is required to restrict the domain of gsc expression, and misexpression of Pax2a is sufficient to block delamination and fully suppress the effects of Gsc. The opposing activities of Gsc and Pax2a correlate with repression or up-regulation, respectively, of E-cadherin (cdh1). These data resolve a genetic mechanism controlling delamination of otic neuroblasts. The data also elucidate a developmental role for Gsc consistent with a general function in promoting epithelial-to-mesenchymal transition (EMT).

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The Sound of Silence: Mouse Models for Hearing Loss

Genetics Research International ◽

10.4061/2011/416450 ◽

2011 ◽

Vol 2011 ◽

pp. 1-9 ◽

Cited By ~ 2

Author(s):

Sumantra Chatterjee ◽

Thomas Lufkin

Keyword(s):

Hearing Loss ◽

Inner Ear ◽

Hearing Impairment ◽

Economic Loss ◽

Signaling Cascades ◽

Otic Vesicle ◽

New Genes ◽

Personal Loss ◽

The Individual

Sensorineural hearing loss is one of the most common disabilities in humans. It is estimated that about 278 million people worldwide have slight to extreme hearing loss in both ears, which results in an economic loss for the country and personal loss for the individual. It is thus critical to have a deeper understanding of the causes for hearing loss to better manage and treat the affected individuals. The mouse serves as an excellent model to study and recapitulate some of these phenotypes, identify new genes which cause deafness, and to study their roles in vivo and in detail. Mutant mice have been instrumental in elucidating the function and mechanisms of the inner ear. The development and morphogenesis of the inner ear from an ectodermal layer into distinct auditory and vestibular components depends on well-coordinated gene expression and well-orchestrated signaling cascades within the otic vesicle and interactions with surrounding layers of tissues. Any disruption in these pathways can lead to hearing impairment. This review takes a look at some of the genes and their corresponding mice mutants that have shed light on the mechanism governing hearing impairment (HI) in humans.

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