Sorbitol Is a Severity Biomarker for PMM2-CDG with Therapeutic Implications.
Anna N LigezkaSilvia RadenkovicMayank SaraswatKishore GarapatiWasantha RanatungaWirginia KrzysciakHitoshi YanaiharaGraeme PrestonWilliam BruckerRenee M McGovernJoel M ReidDavid CassimanKarthik MuthusamyChristin JohnsenSaadet Mercimek-AndrewsAustin LarsonChristina LamAndrew C EdmondsonBart GhesquièrePeter WittersKimiyo RaymondDevin OglesbeeAkhilesh PandeyEthan O PerlsteinTamas KoziczEva MoravaPublished in: Annals of neurology (2021)
Epalrestat improved PMM enzyme activity, N-glycosylation, and glycosylation biomarkers in vitro. Leveraging cellular glycoproteome assessment, we provided a systems-level view of treatment efficacy and discovered potential novel biosignatures of therapy response. Epalrestat was well-tolerated and led to significant clinical improvements in the first pediatric patient with PMM2-CDG treated with epalrestat. We also propose urinary sorbitol as a novel biomarker for disease severity and treatment response in future clinical trials in PMM2-CDG. ANN NEUROL 20219999:n/a-n/a.