Glycosphingolipid storage leads to the enhanced degradation of the B cell receptor in Sandhoff disease mice.

[gm1 gangliosidosis]

Glycosphingolipid storage diseases are a group of inherited metabolic diseases in which glycosphingolipids accumulate due to their impaired lysosomal breakdown . Splenic B cells isolated from NPC 1 , Sandhoff , GM 1 -gangliosidosis and Fabry disease mouse models showed large (20 - to 30 -fold ) increases in disease specific glycosphingolipids and up to a 4 -fold increase in cholesterol . The magnitude of glycosphingolipid storage was in the order NPC 1 > Sandhoff approximately GM 1 gangliosidosis > Fabry . Except for Fabry disease , glycosphingolipid storage led to an increase in the lysosomal compartment and altered glycosphingolipid trafficking . In order to investigate the consequences of storage on B cell function , the levels of surface expression of B cell IgM receptor and its associated components were quantitated in Sandhoff B cells , since they are all raft-associated on activation . Both the B cell receptor , CD 2 1 and CD 19 had decreased cell surface expression . In contrast , CD 40 and MHC II , surface receptors that do not associate with lipid rafts , were unchanged . Using a pulse chase biotinylation procedure , surface B cell receptors on a Sandhoff lymphoblast cell line were found to have a significantly decreased half -life . Increased co -localization of fluorescently conjugated cholera toxin and lysosomes was also observed in Sandhoff B cells . Glycosphingolipid storage leads to the enhanced formation of lysosomal lipid rafts , altered endocytic trafficking and increased degradation of the B cell receptor .

Diseases
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Diseases presenting "significantly decreased half-life" symptom

gm1 gangliosidosis

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