Raising CGMP Restores Proteasome Function and Myelination in Mice with a Proteotoxic Neuropathy

Overview

Journal Brain

Publisher Oxford University Press

Specialty Neurology

Date 2021 Aug 12

PMID 34382059

Citations 6

Authors

Jordan J S VerPlank

Joseph Gawron

Nicholas J Silvestri

M Laura Feltri

Lawrence Wrabetz

Alfred L Goldberg

Affiliations

Soon will be listed here.

Abstract

Agents that raise cyclic guanosine monophosphate (cGMP) by activating protein kinase G increase 26S proteasome activities, protein ubiquitination and degradation of misfolded proteins. Therefore, they may be useful in treating neurodegenerative and other diseases caused by an accumulation of misfolded proteins. Mutations in myelin protein zero (MPZ) cause the peripheral neuropathy Charcot-Marie-Tooth type 1B (CMT1B). In peripheral nerves of a mouse model of CMT1B, where the mutant MPZS63del is expressed, proteasome activities are reduced, mutant MPZS63del and polyubiquitinated proteins accumulate and the unfolded protein response (p-eif2α) is induced. In HEK293 cells, raising cGMP stimulated ubiquitination and degradation of MPZS63del, but not of wild-type MPZ. Treating S63del mice with the phosphodiesterase 5 inhibitor, sildenafil-to raise cGMP-increased proteasome activity in sciatic nerves and reduced the levels of polyubiquitinated proteins, the proteasome reporter ubG76V-GFP and p-elF2α. Furthermore, sildenafil treatment reduced the number of amyelinated axons, and increased myelin thickness and nerve conduction velocity in sciatic nerves. Thus, agents that raise cGMP, including those widely used in medicine, may be useful therapies for CMT1B and other proteotoxic diseases.

Citing Articles

Activation of the 26S Proteasome to Reduce Proteotoxic Stress and Improve the Efficacy of PROTACs.

Sedlacek J ACS Pharmacol Transl Sci. 2025; 8(1):21-35.

PMID: 39816802 PMC: 11729432. DOI: 10.1021/acsptsci.4c00408.

Pharmacologically increasing cGMP improves proteostasis and reduces neuropathy in mouse models of CMT1.

Moore S, Gawron J, Stevens M, Marziali L, Buys E, Milne G Cell Mol Life Sci. 2024; 81(1):434.

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Navigating the Landscape of CMT1B: Understanding Genetic Pathways, Disease Models, and Potential Therapeutic Approaches.

McCulloch M, Mehryab F, Rashnonejad A Int J Mol Sci. 2024; 25(17).

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Genetic blockade of the activation of 26S proteasomes by PKA is well tolerated by mice at baseline.

Yang L, Ahammed M, Wu P, Sternburg J, Liu J, Wang X Am J Cardiovasc Dis. 2024; 14(2):90-105.

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Activation of XBP1s attenuates disease severity in models of proteotoxic Charcot-Marie-Tooth type 1B.

Touvier T, Veneri F, Claessens A, Ferri C, Mastrangelo R, Sorgiati N bioRxiv. 2024; .

PMID: 38352425 PMC: 10862880. DOI: 10.1101/2024.01.31.577760.

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