Anti-semaphorin 3A Antibodies Rescue Retinal Ganglion Cells from Cell Death following Optic Nerve Axotomy

Shirvan, Anat; Kimron, Michal; Holdengreber, Vered; Ziv, Ilan; Ben‐Shaul, Yehuda; Melamed, Shlomo; Melamed, Eldad; Barzilai, Ari; Solomon, Arieh S.

doi:10.1074/jbc.m204793200

Cited by 100 publications

(94 citation statements)

References 62 publications

(70 reference statements)

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“…Such molecules have already been successfully used on developing neurons 164,165 but still have to be tested on tumors. Moreover, the 3D-structure of several of these axon guidance proteins, in particular semaphorins and neuropilins, have been recently solved, which should help designing new molecules.…”

Section: Discussionmentioning

confidence: 99%

The brain within the tumor: new roles for axon guidance molecules in cancers

2005

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Slits, semaphorins and netrins are three families of proteins that can attract or repel growing axons and migrating neurons in the developing nervous system of vertebrates and invertebrates. Recent studies have shown that they are widely expressed outside the nervous system and that they may play important roles in cancers. Several of the genes encoding these proteins are localized on chromosomal region associated with frequent loss-of-heterozygosity in tumors and cancer cell lines and there is also significant hypermethylation of their promoter suggesting that they may act as tumor suppressors. In addition, proteins in all these families and their receptors appear to control the vascularization of the tumors. Last, many axon guidance molecules also regulate cell migration and apoptosis in normal and tumorigenic tissues. Overall, this suggests that molecules that could mimick or block the activity of axon guidance molecules may be used as therapeutic agents for the treatment of malignancy.

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Section: Discussionmentioning

confidence: 99%

The brain within the tumor: new roles for axon guidance molecules in cancers

2005

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“…This effect is apparently not mediated by Sema3A (Ohta et al, 1999;Shepherd et al, 1996); therefore, it would be interesting to see whether Sema3D can repel RGCs. In addition to chemorepulsion, Sema3A has been shown to promote apoptosis, including that of RGCs (Bagnard et al, 2001;Shirvan et al, 2002). This is an important process in the developing lens (Jean et al, 1998) to which Sema3A may, …”

Section: Ocular Expressionmentioning

confidence: 99%

Cranial expression of class 3 secreted semaphorins and their neuropilin receptors

Chilton

Guthrie

2003

Developmental Dynamics

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The semaphorin family of chemorepellents and their receptors the neuropilins are implicated in a variety of cellular processes, including axon guidance and cell migration. Semaphorins may bind more than one neuropilin or a heterodimer of both, thus a detailed knowledge of their expression patterns may reveal possible cases of redundancy or mutual antagonism. To assess their involvement in cranial development, we cloned fragments of the chick orthologues of Sema3B and Sema3F. We then carried out mRNA in situ hybridisation of all six class 3 semaphorins and both neuropilins in the embryonic chick head. We present evidence for spatiotemporal regulation of these molecules in the brainstem and developing head, including the eye, ear, and branchial arches. These expression patterns provide a basis for functional analysis of semaphorins and neuropilins in the development of axon projections and the morphogenesis of cranial structures. Developmental Dynamics 228:726 -733, 2003.

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“…We provide evidence in vitro and in vivo for upregulation of both Plexin-A1 and Npn-1 after activation of microglia. Recent reports also implicate semaphorin-mediated neuronal and neuronal progenitor apoptotic cell death (Gagliardini and Fankhauser, 1999;Shirvan et al, 1999Shirvan et al, , 2002Bagnard et al, 2001). We therefore examined whether semaphorin has a similar effect on microglia.…”

Section: Differential Expression Of Plexin-a1 and Npn-1 By Microgliamentioning

confidence: 99%

“…After a 1 h blocking step in 3% normal goat serum (NGS), 30 m sections were incubated overnight with primary antibody in Tris-buffered saline (TBS) containing 0.2% Triton X-100 (Sigma) with 1% NGS. The following antibodies were used: OX42 (1:400; Serotec, Oxford, UK), Plexin-A1 culture supernatant (a gift from H. Fujisawa, National Institute of Genetics, Mishima, Japan) Npn-1 (1:200) (Kolodkin et al, 1997;Pasterkamp et al, 1999), Sema3A (1:250; a gift from A. Barzilai, Tel Aviv University, Tel Aviv, Israel) (Shirvan et al, 2002), and NeuN (1:200; Chemicon, Hampshire, UK). After washing in TBS, sections were incubated in biotinylated secondary antibodies (1:200) for 3 h at room temperature.…”

Section: Methodsmentioning

confidence: 99%

A Novel Role for Sema3A in Neuroprotection from Injury Mediated by Activated Microglia

et al. 2006

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Microglia exist under physiological conditions in a resting state but become activated after neuronal injury. Recent studies have highlighted the reciprocal role of neurons in controlling both the number and activity of microglia. In this study, microglia derived from newborn rat cortices were cultured and activated by interferon-␥ (IFN␥) treatment, then exposed to recombinant Sema3A or conditioned medium derived from stressed embryonic cortical neurons. We found that activation of microglia by IFN␥ induced differential upregulation of the semaphorin receptors Plexin-A1 and Neuropilin-1. This result was confirmed by Northern blotting, reverse transcription-PCR, and Western blotting. Furthermore, recombinant Sema3A induced apoptosis of microglia when added to the in vitro culture, and a similar result was obtained on activated microglia when Sema3A was produced by stressed neurons. Using an in vivo model of microglia activation by striatal injection of lipopolysaccharide demonstrated a corresponding upregulation of Plexin-A1 and Neuropilin-1 in activated microglia and enhanced production of Sema3A by stressed adult neurons. These results suggest a novel semaphorin-mediated mechanism of neuroprotection whereby stressed neurons can protect themselves from further damage by activated microglia.

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Anti-semaphorin 3A Antibodies Rescue Retinal Ganglion Cells from Cell Death following Optic Nerve Axotomy

Cited by 100 publications

References 62 publications

The brain within the tumor: new roles for axon guidance molecules in cancers

The brain within the tumor: new roles for axon guidance molecules in cancers

Cranial expression of class 3 secreted semaphorins and their neuropilin receptors

A Novel Role for Sema3A in Neuroprotection from Injury Mediated by Activated Microglia

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