S1PR1 signaling attenuates apoptosis of retinal ganglioncells via modulation of cJun/Bim cascade and Badphosphorylation in a mouse model of glaucoma

Basavarajappa, Devaraj; Gupta, Vivek; Vander Wall, Roshana; Gupta, Veer; Chitranshi, Nitin; Mirshahvaladi, Seyed Shahab Oddin; Palanivel, Viswanthram; You, Yuyi; Mirzaei, Mehdi; Klistorner, Alexander; Graham, Stuart L

doi:10.1096/fj.202201346r

Title

S1PR1 signaling attenuates apoptosis of retinal ganglioncells via modulation of cJun/Bim cascade and Badphosphorylation in a mouse model of glaucoma

Publication Date

2023-01

Author(s)

Basavarajappa, Devaraj

Gupta, Vivek

Vander Wall, Roshana

Gupta, Veer

Chitranshi, Nitin

( author )
OrcID: https://orcid.org/0000-0002-6508-9865
Email: nchitran@une.edu.au
UNE Id une-id:nchitran

Mirshahvaladi, Seyed Shahab Oddin

Palanivel, Viswanthram

You, Yuyi

Mirzaei, Mehdi

Klistorner, Alexander

Graham, Stuart L

Type of document

Journal Article

Language

en

Entity Type

Publication

Publisher

John Wiley & Sons, Inc

Place of publication

United States of America

DOI

10.1096/fj.202201346r

UNE publication id

une:1959.11/71669

Abstract

Glaucoma is a complex neurodegenerative disease characterized by optic nerve damage and apoptotic retinal ganglion cell (RGC) death, and is the leading cause of irreversible blindness worldwide. Among the sphingosine 1-phosphate receptors (S1PRs) family, S1PR1 is a highly expressed subtype in the central nervous system and has gained rapid attention as an important mediator of pathophysiological processes in the brain and the retina. Our recent study showed that mice treated orally with siponimod drug exerted neuroprotection via modulation of neuronal S1PR1 in experimental glaucoma. This study identified the molecular signaling pathway modulated by S1PR1 activation with siponimod treatment in RGCs in glaucomatous injury. We investigated the critical neuroprotective signaling pathway in vivo using mice deleted for S1PR1 in RGCs. Our results showed marked upregulation of the apoptotic pathway was associated with decreased Akt and Erk1/2 activation levels in the retina in glaucoma conditions. Activation of S1PR1 with siponimod treatment significantly increased neuroprotective Akt and Erk1/2 activation and attenuated the apoptotic signaling via suppression of c-Jun/Bim cascade and by increasing Bad phosphorylation. Conversely, deletion of S1PR1 in RGCs significantly increased the apoptotic cells in the ganglion cell layer in glaucoma and diminished the neuroprotective effects of siponimod treatment on Akt/Erk1/2 activation, c-Jun/Bim cascade, and Bad phosphorylation. Our data demonstrated that activation of S1PR1 in RGCs induces crucial neuroprotective signaling that suppresses the proapoptotic c-Jun/Bim cascade and increases antiapoptotic Bad phosphorylation. Our findings suggest that S1PR1 is a potential therapeutic target for neuroprotection of RGCs in glaucoma.

Link

link

Citation

The FASEB Journal, 37(1), p. 1-16

ISSN

1530-6860

0892-6638

Start page

1

End page

16

Rights

Attribution 4.0 International

S1PR1 signaling attenuates apoptosis of retinal ganglioncells via modulation of cJun/Bim cascade and Badphosphorylation in a mouse model of glaucoma

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