Litcius/Paper detail

Pharmacological Inhibition of the VCP/Proteasome Axis Rescues Photoreceptor Degeneration in RHOP23H Rat Retinal Explants

Merve Sen, Oksana Kutsyr, Bowen Cao, Sylvia Bolz, Blanca Arango‐González, Marius Ueffing

2021Biomolecules18 citationsDOIOpen Access PDF

Abstract

Rhodopsin (RHO) misfolding mutations are a common cause of the blinding disease autosomal dominant retinitis pigmentosa (adRP). The most prevalent mutation, RHOP23H, results in its misfolding and retention in the endoplasmic reticulum (ER). Under homeostatic conditions, misfolded proteins are selectively identified, retained at the ER, and cleared via ER-associated degradation (ERAD). Overload of these degradation processes for a prolonged period leads to imbalanced proteostasis and may eventually result in cell death. ERAD of misfolded proteins, such as RHOP23H, includes the subsequent steps of protein recognition, targeting for ERAD, retrotranslocation, and proteasomal degradation. In the present study, we investigated and compared pharmacological modulation of ERAD at these four different major steps. We show that inhibition of the VCP/proteasome activity favors cell survival and suppresses P23H-mediated retinal degeneration in RHOP23H rat retinal explants. We suggest targeting this activity as a therapeutic approach for patients with currently untreatable adRP.

Topics & Concepts

Endoplasmic-reticulum-associated protein degradationProteostasisEndoplasmic reticulumProteasomeCell biologyRetinal degenerationRetinitis pigmentosaUnfolded protein responseBiologyProtein degradationRetinalBiochemistryRetinal Development and DisordersCellular transport and secretionRetinal and Macular Surgery