Disruption of Semaphorin III/D Gene Causes Severe Abnormality in Peripheral Nerve Projection

Taniguchi, Masahiko; Yuasa, Shigeki; Fujisawa, Hajime; Naruse, Ichiro; Saga, Shinsuke; Mishina, Masayoshi; Yagi, Takeshi

doi:10.1016/s0896-6273(00)80368-2

Cited by 496 publications

(353 citation statements)

References 43 publications

(21 reference statements)

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“…The expression of sema3s in the zebrafish retina appears to differ from that reported in other species. For instance, while sema3Aa is expressed in a select population of cells in the INL of the zebrafish retina well after the optic projection has formed, in both the chick and mouse retinas Sema3A is found throughout the embryonic eye (Taniguchi et al, 1997;Chilton and Guthrie, 2003). Moreover, we found no sema3E label in the zebrafish retina, but sema3E is expressed in the outer layers of the embryonic mouse retina (Steinbach et al, 2002).…”

Section: Retinal Expression Of Sema3smentioning

confidence: 51%

“…For example, in Sema3A null mice sensory axons grow aberrantly into regions of the spinal cord that normally express Sema3A and neuronal processes of pyramidal neurons are oriented randomly rather than towards the brain surface (Behar et al, 1996). There are also severe defects in cranial nerve axon fasciculation in these mice (Taniguchi et al, 1997;Catalano et al, 1998). Furthermore, perturbation of Sema3Aa signalling in zebrafish causes the axons of ventral spinal motoneurons, which normally grow along the medial portion of the somite, to extend aberrantly into anterior or posterior regions (Shoji et al, 1998;Sato-Maeda et al, 2006).…”

Section: Introductionmentioning

confidence: 99%

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Expression of multiple class three semaphorins in the retina and along the path of zebrafish retinal axons

Callander

Lamont

Childs

et al. 2007

Developmental Dynamics

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Retinal ganglion cells (RGCs) extend axons that exit the eye, cross the midline at the optic chiasm, and synapse on target cells in the optic tectum. Class three semaphorins (Sema3s) are a family of molecules known to direct axon growth. We undertook an expression screen to identify sema3s expressed in the retina and/or brain close to in-growing RGC axons, which might therefore influence retinal-tectal pathfinding. We find that sema3Aa, 3Fa, 3Ga, and 3Gb are expressed in the retina, although only sema3Fa is present during the time window when the axons extend. Also, we show that sema3Aa and sema3E are present near or at the optic chiasm. Furthermore, sema3C, 3Fa, 3Ga, and 3Gb are expressed in regions of the diencephalon near the path taken by RGC axons. Finally, the optic tectum expresses sema3Aa, 3Fa, 3Fb, and 3Gb. Thus, sema3s are spatiotemporally placed to influence RGC axon growth. Developmental Dynamics 236:2918 -2924, 2007.

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Section: Retinal Expression Of Sema3smentioning

confidence: 51%

Section: Introductionmentioning

confidence: 99%

Expression of multiple class three semaphorins in the retina and along the path of zebrafish retinal axons

Callander

Lamont

Childs

et al. 2007

Developmental Dynamics

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“…Finally, we examined whether axons that exhibit pathfinding errors in embryos with defective Sema3A signalling (namely the ARTICLE Sema3A, Nrp1 and Plexin-A mutants 25,29,55,56 ) also misproject in ADAM10/17 double-knockout embryos. Contrary to the former mutants, whose axons extend beyond their normal targets due to lack of Sema3A inhibitory signalling, axonal projections of the ADAM knockouts are expected to be more restricted than wild type due to increased sensitivity to the repellant.…”

Section: Resultsmentioning

confidence: 99%

ADAM metalloproteases promote a developmental switch in responsiveness to the axonal repellant Sema3A

et al. 2014

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During embryonic development, axons can gain and lose sensitivity to guidance cues, and this flexibility is essential for the correct wiring of the nervous system. Yet, the underlying molecular mechanisms are largely unknown. Here we show that receptor cleavage by ADAM (A Disintegrin And Metalloprotease) metalloproteases promotes murine sensory axons loss of responsiveness to the chemorepellant Sema3A. Genetic ablation of ADAM10 and ADAM17 disrupts the developmental downregulation of Neuropilin-1 (Nrp1), the receptor for Sema3A, in sensory axons. Moreover, this is correlated with gain of repulsive response to Sema3A. Overexpression of Nrp1 in neurons reverses axonal desensitization to Sema3A, but this is hampered in a mutant Nrp1 with high susceptibility to cleavage. Lastly, we detect guidance errors of proprioceptive axons in ADAM knockouts that are consistent with enhanced response to Sema3A. Our results provide the first evidence for involvement of ADAMs in regulating developmental switch in responsiveness to axonal guidance cues.

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“…In mouse, a Sema3A receptor gene, Neuropilin2, is expressed in BMNs (Chen et al, 2000), whereas Sema3A is expressed in the first and second branchial arches . The nV and nVII cranial nerves (containing nV and nVII BMN axons, respectively) are slightly defasciculated in Neuropilin2 knockout mice (Chen et al, 2000;Giger et al, 2000) and more severely defasciculated in Neuropilin1 and Sema3A knockout mice (Kitsukawa et al, 1997;Taniguchi et al, 1997). These data suggest strongly that Semaphorin-mediated repulsive interactions channel the extension of BMN axons into the branchial arch mesenchyme but are likely not involved in guiding axons of different BMN subtypes to specific arch targets.…”

Section: Chemorepellent Mechanismsmentioning

confidence: 88%

Turning heads: Development of vertebrate branchiomotor neurons

Chandrasekhar

2003

Developmental Dynamics

164

204

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The cranial motor neurons innervate muscles that control eye, jaw, and facial movements of the vertebrate head and parasympathetic neurons that innervate certain glands and organs. These efferent neurons develop at characteristic locations in the brainstem, and their axons exit the neural tube in well-defined trajectories to innervate target tissues. This review is focused on a subset of cranial motor neurons called the branchiomotor neurons, which innervate muscles derived from the branchial (pharyngeal) arches. First, the organization of the branchiomotor pathways in zebrafish, chick, and mouse embryos will be compared, and the underlying axon guidance mechanisms will be addressed. Next, the molecular mechanisms that generate branchiomotor neurons and specify their identities will be discussed. Finally, the caudally directed or tangential migration of facial branchiomotor neurons will be examined. Given the advances in the characterization and analysis of vertebrate genomes, we can expect rapid progress in elucidating the cellular and molecular mechanisms underlying the development of these vital neuronal networks.

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Disruption of Semaphorin III/D Gene Causes Severe Abnormality in Peripheral Nerve Projection

Cited by 496 publications

References 43 publications

Expression of multiple class three semaphorins in the retina and along the path of zebrafish retinal axons

Expression of multiple class three semaphorins in the retina and along the path of zebrafish retinal axons

ADAM metalloproteases promote a developmental switch in responsiveness to the axonal repellant Sema3A

Turning heads: Development of vertebrate branchiomotor neurons

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