Restoration Of Retinal Regenerative Potentialof Müller Glia By Disrupting Intercellularprox1 Transfer Eun Jung Lee Museong Kim Sooyeon Park Ji Hyeon Shim Hyunju Cho Jung Ah Park Kihyun Park Dongeun Lee Jeong Hwan Kim Haeun Jeong Fumio Matsuzaki Seonyoung Kim Jaehoon Kim Hanseul Yang Jeongsoo Lee Jin Woo Kim by Eun Jung Lee & Museong Kim & Sooyeon Park & Ji Hyeon Shim & Hyun-ju Cho & Jung Ah Park & Kihyun Park & Dongeun Lee & Jeong Hwan Kim & Haeun Jeong & Fumio Matsuzaki & Seon-young Kim & Jaehoon Kim & Hanseul Yang & Jeong-soo Lee & Jin Woo Kim 101038/S41467025582908 instant download after payment.

Individuals with retinal degenerative diseases struggle to restore vision due tothe inability to regenerate retinal cells. Unlike cold-blooded vertebrates,mammals lack Müller glia (MG)-mediated retinal regeneration, indicating thelimited regenerative capacity of mammalian MG. Here, we identify prosperorelated homeobox 1 (Prox1) as a key factor restricting this process. Prox1accumulates in MG of degenerating human and mouse retinas but not inregenerating zebrafish. In mice, Prox1 in MG originates from neighboringretinal neurons via intercellular transfer. Blocking this transfer enables MGreprogramming into retinal progenitor cells in injured mouse retinas. Moreover, adeno-associated viral delivery of an anti-Prox1 antibody, whichsequesters extracellular Prox1, promotes retinal neuron regeneration anddelays vision loss in a retinitis pigmentosa model. These findings establishProx1 as a barrier to MG-mediated regeneration and highlight anti-Prox1therapy as a promising strategy for restoring retinal regeneration in mammals