EphrinA5 protein distribution in the developing mouse brain

Deschamps, Claire; Morel, Milena; Janet, Thierry; Page, G.K.; Jaber, Mohamed; Gaillard, Afsaneh; Prestoz, Laetitia

doi:10.1186/1471-2202-11-105

Cited by 18 publications

(9 citation statements)

References 66 publications

(119 reference statements)

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“…Next, we investigated the effects of ephrinA ligands for in vivo 5-HT axon targeting using an overexpression strategy. We focused on the amygdala and piriform cortex, which are preferential targets of the DR 5-HT neurons ( Muzerelle et al 2016 ) and express only very low levels of the main EphA5 ligands, ephrinA2, ephrinA3, and ephrinA5, based on our own observations, confirming previously published reports ( Deschamps et al, 2010 ; Gerstmann et al 2015 ) and available public resources (Allen Brain Atlas, http://developingmouse.brain-map.org/gene/show/ 1341 5 , 13416, 13418). This suggested that the amygdala and piriform cortex could be permissive for the ingrowth of DR axons that express high levels of EphA5 receptors.…”

Section: Resultssupporting

confidence: 86%

“…EphA5 expression in 5-HT raphe neurons was dynamically expressed, being maximal during axon growth in embryonic life, reaching target during the early postnatal period, and showing decreased expression, similarly to what has reported for ephrinA5 expression ( Deschamps et al, 2010 ). Given the potential of 5-HT neurons to regenerate and grow, it will be interesting to know whether the present developmental mechanisms are reactivated after a lesion, and whether the propensity of serotonin axons to regrow ( Müllner et al, 2008 ) is linked to their EphA content.…”

Section: Discussionsupporting

confidence: 83%

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EphrinA5 Signaling Is Required for the Distinctive Targeting of Raphe Serotonin Neurons in the Forebrain

Teng¹,

Gaillard²,

Muzerelle³

et al. 2017

eNeuro

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Section: Resultssupporting

confidence: 86%

Section: Discussionsupporting

confidence: 83%

EphrinA5 Signaling Is Required for the Distinctive Targeting of Raphe Serotonin Neurons in the Forebrain

Teng¹,

Gaillard²,

Muzerelle³

et al. 2017

eNeuro

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“…82 Supplementation of PRDX6 has been shown to attenuate reactive oxygen species and TGFβ-induced insult to glaucomatous trabecular meshwork cells in vitro, as well as to decrease the senescence process in these cells. 83 Moreover, the glaucomatous neuroprotective effects of this antioxidant factor have been demonstrated on RGC, as demonstrated by observations that reactive oxygen species-mediated suppression of PRDX6 in these cells can be prevented by over-expression of PRDX.6 84 Observations that high levels of PRDX6 are expressed by Müller glia further support the antioxidant role of these cells within the retina. Production of this molecule by Müller glia upon retinal injury may limit the damage caused by reactive oxygen species on retinal neurons and may play a major neuroprotective role in many retinal degenerative diseases such as glaucoma and macular degeneration.…”

Section: Müller Glia As a Source Of Antioxidants In The Neural Retinamentioning

confidence: 94%

Potential of Müller Glia for Retina Neuroprotection

Eastlake

Luis

Limb

2019

Current Eye Research

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Müller glia constitute the main glial cells of the retina. They are spatially distributed along this tissue, facilitating their close membrane interactions with all retinal neurons. Müller glia are characterized by their active metabolic functions, which are neuroprotective in nature. Although they can become reactive under pathological conditions, leading to their production of inflammatory and neurotoxic factors, their main metabolic functions confer neuroprotection to the retina, resulting in the promotion of neural cell repair and survival. In addition to their protective metabolic features, Müller glia release several neurotrophic factors and antioxidants into the retinal microenvironment, which are taken up by retinal neurons for their survival. This review summarizes the Müller glial neuroprotective mechanisms and describes advances made on the clinical application of these factors for the treatment of retinal degenerative diseases. It also discusses prospects for the use of these cells as a vehicle to deliver neuroprotective factors into the retina. ARTICLE HISTORY

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“…The expression of EphA7 by a subpopulation of striatal neurons during development makes this tyrosine kinase receptor a prime candidate for regulating intracompartmental sorting of matrix neurons. For example, several studies indicate that ephrins known to bind to EphA7 are expressed in the developing striatum (Passante et al, 2008;Cooper et al, 2009;Deschamps et al, 2009Deschamps et al, , 2010. Thus, EphA7 may interact with specific ephrins during development to facilitate the organization of striatal neurons into unique ''matrisome'' subcompartments within the matrix in a fashion similar to how other Eph receptors facilitate the formation of rhombomeres (Becker et al, 1994;Cooke et al, 2001Cooke et al, , 2005, mediate neural crest cell migration (Wang and Anderson, 1997;Krull et al, 1997;Koblar et al, 2000;McLennan and Krull, 2002;Kasemeier-Kulesa et al, 2006;Davy and Soriano, 2007;Kuriyama and Mayor, 2008), and establish cellular boundaries in the cortex (Vanderhaeghen et al, 2000;Miller et al, 2006).…”

Section: Epha7 Identifies a Unique Striatal Subcompartmentmentioning

confidence: 99%

EphA7 expression identifies a unique neuronal compartment in the rat striatum

Tai

Cassidy

Kromer

2013

J of Comparative Neurology

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Prior studies have identified two anatomically and neurochemically distinct cellular compartments within the mammalian striatum, termed striosomes and matrix, which express μ-opioid receptors (μOR) and EphA4, respectively. Here we identify and characterize an additional compartment in the rat striatum composed of neurons that express EphA7. In situ hybridization and immunohistochemical data indicate that neurons expressing EphA7 mRNA and protein are arranged in a banded "matrisome-like" pattern confined to the matrix in the dorsal striatum. Within the ventral striatum, EphA7-positive (+) neurons have a less organized mosaic pattern that partially overlaps areas expressing μOR. Immunolabeling data demonstrate that EphA7+ striatofugal axons form distinct fascicles leaving the striatum. Within the globus pallidus, EphA7+ axons terminate primarily within ventromedial areas of the nucleus and along its striatal border. EphA7+ axons avoid regions containing dopamine neurons within the substantia nigra and preferentially innervate areas near the rostral and caudal margins of the nucleus. Within both nuclei, EphA7+ axons have similar but more restricted terminal fields than the entire population of EphA4+ matrix axons, indicating that EphA7+ axons comprise a subpopulation of matrix axons. Ligand binding data demonstrate that ephrin-A5 selectively binds areas of the striatum, globus pallidus, and substantia nigra containing EphA7+ neurons and axons, but not areas expressing only EphA4. Our findings demonstrate that EphA7 expression identifies a novel "matrisome" compartment within the matrix that binds ephrin-A5 and possesses unique axonal projections. Our findings also suggest that EphA7 and ephrin-A5 may participate in the formation of this matrisome subcompartment and its striatofugal projections.

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EphrinA5 protein distribution in the developing mouse brain

Cited by 18 publications

References 66 publications

EphrinA5 Signaling Is Required for the Distinctive Targeting of Raphe Serotonin Neurons in the Forebrain

EphrinA5 Signaling Is Required for the Distinctive Targeting of Raphe Serotonin Neurons in the Forebrain

Potential of Müller Glia for Retina Neuroprotection

EphA7 expression identifies a unique neuronal compartment in the rat striatum

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