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From sheep to mice to cells: Tools for the study of the sphingolipidoses
Authors:Hila Zigdon  Anna MeshcheriakovaAnthony H. Futerman
Affiliation:Department of Biological Chemistry, Weizmann Institute of Science, Rehovot 76100, Israel
Abstract:The sphingolipidoses are a group of inherited lysosomal storage diseases in which sphingolipids accumulate due to the defective activity of one or other enzymes involved in their degradation. For most of the sphingolipidoses, little is known about the molecular mechanisms that lead to disease, which has negatively impacted attempts to develop therapies for these devastating human diseases. Use of both genetically-modified animals, ranging from mice to larger mammals, and of novel cell culture systems, is of utmost importance in delineating the molecular mechanisms that cause pathophysiology, and in providing tools that enable testing the efficacy of new therapies. In this review, we discuss eight sphingolipidoses, namely Gaucher disease, Fabry disease, metachromatic leukodystrophy, Krabbe disease, Niemann–Pick diseases A and B, Farber disease, GM1 gangliosidoses, and GM2 gangliosidoses, and describe the tools that are currently available for their study. This article is part of a Special Issue entitled Tools to study lipid functions.
Keywords:α-Gal A, α-galactosidase A   ASA, arylsulfatase A   ASM, acid sphingomyelinase   β-Hex, β-hexosaminidase   CBE, conduritol-B-epoxide   CNS, central nervous system   DOX, doxycycline   GALC, galactosylceramidase   GD, Gaucher disease   GCase, glucosylceramidase   GlcCer, glucosylceramide   HEXA, hexosaminidase A   HEXB, hexosaminidase B   GM2, monosialoganglioside 2   LSD, lysosomal storage disorder   MLD, metachromatic leukodystrophy   NPA, Niemann&ndash  Pick disease type A   NPB, Niemann&ndash  Pick disease type B   PNS, peripheral nervous system   RNAi, RNA interference   Sap-B, saposin B   Sap-C, saposin C   shRNA, short hairpin RNA   SLs, sphingolipids
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