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1,6- epi-Cyclophellitol Cyclosulfamidate Is a Bona Fide Lysosomal α-Glucosidase Stabilizer for the Treatment of Pompe Disease
來源: | 作者:Ken Kok 1, Chi-Lin Kuo 1, Rebecca E Katzy 1, Lindsey T Lelieveld 1, Liang Wu 2, Véronique Roig-Zamboni 3, Gijsbert A van der Marel 4, Jeroen D C Codée 4, Gerlind Sulzenbacher 3, Gideon J Davies 2, Herman S Overkleeft 4, Johannes M F G Aerts 1, Marta Artol | 發(fā)布時間: 2022-08-13 | 457 次瀏覽 | 分享到:

α-Glucosidase inhibitors are potential therapeutics for the treatment of diabetes, viral infections, and Pompe disease. Herein, we report a 1,6-epi-cyclophellitol cyclosulfamidate as a new class of reversible α-glucosidase inhibitors that displays enzyme inhibitory activity by virtue of its conformational mimicry of the substrate when bound in the Michaelis complex. The α-d-glc-configured cyclophellitol cyclosulfamidate 4 binds in a competitive manner the human lysosomal acid α-glucosidase (GAA), ER α-glucosidases, and, at higher concentrations, intestinal α-glucosidases, displaying an excellent selectivity over the human β-glucosidases GBA and GBA2 and glucosylceramide synthase (GCS). Cyclosulfamidate 4 stabilizes recombinant human GAA (rhGAA, alglucosidase alfa, Myozyme) in cell medium and plasma and facilitates enzyme trafficking to lysosomes. It stabilizes rhGAA more effectively than existing small-molecule chaperones and does so in vitroin cellulo, and in vivo in zebrafish, thus representing a promising therapeutic alternative to Miglustat for Pompe disease.

原文地址:http://www.ncbi.nlm.nih.gov/pubmed/35917590

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