ABSTRACT
Sphingolipidoses are diseases caused by mutations in genes responsible for sphingolipid degradation and thereby lead to sphingolipid accumulation. Most sphingolipidoses have a neurodegenerative manifestation characterized by innate immune activation in the brain. However, the role of the immune response in disease progression is ill-understood. In contrast to infectious diseases, immune activation is unable to eliminate the offending agent in sphingolipidoses resulting in ineffective, chronic inflammation. This paradox begs two fundamental questions: Why has this immune response evolved in sphingolipidoses? What role does it play in disease progression? Here, starting from the observation that sphingolipids (SLs) are elevated also in infectious diseases, I discuss the possibility that the activation of the brain immune response by SLs has evolved as a part of the immune response against pathogens and plays no major role in sphingolipidoses.
Subject(s)
Brain/immunology , Sphingolipidoses/immunology , Sphingolipids/metabolism , Brain/pathology , Disease Progression , Humans , Immunity, Innate , Sphingolipidoses/pathology , Sphingolipids/adverse effectsABSTRACT
Multiple sulfatase deficiency (MSD, MIM #272200) is an ultra-rare disease comprising pathophysiology and clinical features of mucopolysaccharidosis, sphingolipidosis and other sulfatase deficiencies. MSD is caused by impaired posttranslational activation of sulfatases through the formylglycine generating enzyme (FGE) encoded by the sulfatase modifying factor 1 (SUMF1) gene, which is mutated in MSD. FGE is a highly conserved, non-redundant ER protein that activates all cellular sulfatases by oxidizing a conserved cysteine in the active site of sulfatases that is necessary for full catalytic activity. SUMF1 mutations result in unstable, degradation-prone FGE that demonstrates reduced or absent catalytic activity, leading to decreased activity of all sulfatases. As the majority of sulfatases are localized to the lysosome, loss of sulfatase activity induces lysosomal storage of glycosaminoglycans and sulfatides and subsequent cellular pathology. MSD patients combine clinical features of all single sulfatase deficiencies in a systemic disease. Disease severity classifications distinguish cases based on age of onset and disease progression. A genotype- phenotype correlation has been proposed, biomarkers like excreted storage material and residual sulfatase activities do not correlate well with disease severity. The diagnosis of MSD is based on reduced sulfatase activities and detection of mutations in SUMF1. No therapy exists for MSD yet. This review summarizes the unique FGE/ sulfatase physiology, pathophysiology and clinical aspects in patients and their care and outlines future perspectives in MSD.
Subject(s)
Mucopolysaccharidoses/genetics , Multiple Sulfatase Deficiency Disease/genetics , Oxidoreductases Acting on Sulfur Group Donors/genetics , Sphingolipidoses/genetics , Glycine/analogs & derivatives , Glycine/genetics , Glycine/metabolism , Humans , Mucopolysaccharidoses/pathology , Multiple Sulfatase Deficiency Disease/pathology , Mutation/genetics , Protein Processing, Post-Translational/genetics , Sphingolipidoses/pathology , Sulfatases/deficiency , Sulfatases/geneticsABSTRACT
Drug-induced phospholipidosis is a lysosomal storage disorder characterized by excessive accumulation of phospholipids. Its cellular mechanism is still not well understood, but it is known that cationic amphiphilic drugs can induce it. These drugs have a hydrophilic amine head group that can be protonated in the endolysosomal compartment. As cationic amphiphiles, they are trapped in lysosomes, where they interfere with negatively charged intralysosomal vesicles, the major platforms of cellular sphingolipid degradation. Metabolic principles observed in sphingolipid and phospholipid catabolism and inherited sphingolipidoses are of great importance for lysosomal function and physiological lipid turnover at large. Therefore, we also propose intralysosomal vesicles as major platforms for degradation of lipids and phospholipids reaching them by intracellular pathways like autophagy and endocytosis. Phospholipids are catabolized as components of vesicle surfaces by protonated, positively charged phospholipases, electrostatically attracted to the negatively charged vesicles. Model experiments suggest that progressively accumulating cationic amphiphilic drugs inserting into the vesicle membrane with their hydrophobic molecular moieties disturb and attenuate the main mechanism of lipid degradation as discussed here. By compensating the negative surface charge, cationic enzymes are released from the surface of vesicles and proteolytically degraded, triggering a progressive lipid storage and the formation of inactive lamellar bodies.
Subject(s)
Lipid Metabolism/genetics , Lysosomal Storage Diseases/genetics , Phospholipids/metabolism , Sphingolipidoses/genetics , Humans , Hydrophobic and Hydrophilic Interactions , Lipids/chemistry , Lipids/genetics , Lysosomal Storage Diseases/chemically induced , Lysosomal Storage Diseases/metabolism , Lysosomal Storage Diseases/pathology , Lysosomes/genetics , Lysosomes/metabolism , Organelles/metabolism , Phospholipids/genetics , Sphingolipidoses/chemically induced , Sphingolipidoses/metabolism , Sphingolipidoses/pathologyABSTRACT
Ceramide, sphingomyelin, and glycosphingolipids (both neutral and acidic) are characterized by the presence in the lipid moiety of an aliphatic base known as sphingosine. Altogether, they are called sphingolipids and are particularly abundant in neuronal plasma membranes, where, via interactions with the other membrane lipids and membrane proteins, they play a specific role in modulating the cell signaling processes. The metabolic pathways determining the plasma membrane sphingolipid composition are thus the key point for functional changes of the cell properties. Unnatural changes of the neuronal properties are observed in sphingolipidoses, lysosomal storage diseases occurring when a lysosomal sphingolipid hydrolase is not working, leading to the accumulation of the substrate and to its distribution to all the cell membranes interacting with lysosomes. Moreover, secondary accumulation of sphingolipids is a common trait of other lysosomal storage diseases. This article is part of the Special Issue "Lysosomal Storage Disorders".
Subject(s)
Lysosomal Storage Diseases/metabolism , Nerve Degeneration/metabolism , Sphingolipidoses/metabolism , Sphingolipids/metabolism , Animals , Humans , Lysosomal Storage Diseases/pathology , Lysosomes/metabolism , Lysosomes/pathology , Nerve Degeneration/pathology , Sphingolipidoses/pathologyABSTRACT
Sphingolipidoses are genetically inherited diseases in which genetic mutations lead to functional deficiencies in the enzymes needed for lysosomal degradation of sphingolipid substrates. As a consequence, nondegradable lipids enrich in the lysosomes and lead to fatal pathological phenotypes in affected individuals. In this review, different drug-based treatment strategies including enzyme replacement therapy and substrate reduction therapy are discussed. A special focus is on the concept of pharmacological chaperones, one of which recently acquired clinical approval within the EU. On the basis of the different limitations for each approach, possible future directions of research are discussed.
Subject(s)
Enzyme Therapy , Sphingolipidoses/drug therapy , Enzyme Replacement Therapy , Enzymes/genetics , Enzymes/metabolism , Fabry Disease/drug therapy , Gaucher Disease/drug therapy , Glucosylceramidase/genetics , Glucosylceramidase/metabolism , Glucosylceramidase/therapeutic use , Humans , Lysosomes/metabolism , Recombinant Proteins/biosynthesis , Recombinant Proteins/isolation & purification , Recombinant Proteins/therapeutic use , Sphingolipidoses/genetics , Sphingolipidoses/pathology , Sphingolipids/metabolism , alpha-Galactosidase/genetics , alpha-Galactosidase/metabolism , alpha-Galactosidase/therapeutic useABSTRACT
PURPOSE OF REVIEW: The aim of this study is to review the published human-induced pluripotent stem cell-derived cardiomyocyte (hiPSC-CM) models of cardiac storage disorders and to evaluate the limitations and future applications of this technology. RECENT FINDINGS: Several cardiac storage disorders (CSDs) have been modeled using patient-specific hiPSC-CMs, including Anderson-Fabry disease, Danon disease, and Pompe disease. These models have shown that patient-specific hiPSC-CMs faithfully recapitulate key phenotypic features of CSDs and respond predictably to pharmacologic manipulation. hiPSC-CMs generated from patients with CSDs are representative models of the patient disease state and can be used as an in vitro system for the study of human cardiomyocytes. While these models suffer from several limitations, they are likely to play an important role in future mechanistic studies of cardiac storage disorders and the development of targeted therapeutics for these diseases.
Subject(s)
Heart Diseases/pathology , Induced Pluripotent Stem Cells/pathology , Metabolism, Inborn Errors/pathology , Myocytes, Cardiac/pathology , Fabry Disease , Glycogen Storage Disease Type II/pathology , Glycogen Storage Disease Type IIb/pathology , Humans , Mucopolysaccharidoses/pathology , Sphingolipidoses/pathologyABSTRACT
Sphingolipidoses arise from inherited loss of function of key enzymes regulating the sphingolipid (SL) metabolism and the accumulation of large quantities of these lipids in affected cells. Most frequently, toxicity is manifested in the nervous system, where survival and function of neurons and glial cells are most affected. Although detailed information is available on neuroglial alterations during terminal stages of the disease, the initial pathogenic mechanisms triggering neuropathology are largely unclear. Because they are key components of biological membranes, changes in the local concentration of SLs are likely to impact the organization of membrane domains and functions. This Commentary proposes that SL toxicity involves initial defects in the integrity of lipid domains, membrane fluidity, and membrane bending, leading to membrane deformation and deregulation of cell signaling and function. Understanding how SLs alter membrane architecture may provide breakthroughs for more efficient treatment of sphingolipidoses. © 2016 Wiley Periodicals, Inc.
Subject(s)
Membrane Fluidity/physiology , Membrane Lipids/genetics , Sphingolipidoses/genetics , Sphingolipidoses/pathology , Animals , Humans , Membrane Lipids/deficiencyABSTRACT
The presence of life-threatening neurological symptoms in more than two-thirds of lysosomal storage diseases (LSDs) underscores how vulnerable the nervous system is to lysosomal failure. Neurological dysfunction in LSDs has historically been attributed to the disruption of neuronal and glial homeostasis resulting from the progressive jamming of the endosomal/lysosomal pathway. In neurons, a dysfunctional endosomal-lysosomal system can elicit dire consequences. Given that neurons are largely postmitotic after birth, one can clearly understand that the inability of these cells to proliferate obliterates any possibility of diluting stored lysosomal material by means of cellular division. At its most advanced stage, this situation constitutes a terminal factor in neuronal life, resulting in cell death. However, synaptic deficits in the absence of classical neuronal cell death appear to be common features during the early stages in many LSDs, particularly sphingolipidoses. In essence, failure of synapses to convey their messages, even without major structural damage to the neuronal bodies, is a form of physiological death. This concept of dying-back neuropathology is highly relevant not only for understanding the dynamics of the neurological decline in these diseases, but, more importantly; it might also constitute an important target for molecular therapies to protect perhaps the "Achilles" point in the entire physiological architecture of the brain, thus avoiding an irreversible journey to neuronal demise. © 2016 Wiley Periodicals, Inc.
Subject(s)
Nervous System/pathology , Neurons/pathology , Sphingolipidoses/pathology , Synapses/physiology , Animals , Humans , Models, NeurologicalABSTRACT
Sphingolipidoses are a class of inherited diseases that result from the toxic accumulation of undigested sphingolipids in lysosomes and other cellular membranes. Sphingolipids are particularly enriched in cells of the nervous system, and their excessive accumulation during disease has a significant impact on the nervous system. Neuronal dysfunction followed by neurological compromise is a common feature in many of these diseases; however, the underlying mechanisms that cause vulnerability of neurons are not fully understood. The plasma membrane plays a critical role in regulating cellular survival pathways, and its dysfunction has been implicated in neuronal failure in various adult-onset neuropathies. In the context of sphingolipidoses, we hypothesize that gradual accumulation of undigested lipids in plasma membranes causes local disruptions in lipid raft domains, leading to deregulation of multiple signaling pathways important for neuronal survival and function. We propose that defects in downstream signaling as a result of membrane dysfunction are common mechanisms underlying neuronal vulnerability in sphingolipid storage disorders with neurological compromise. © 2016 Wiley Periodicals, Inc.
Subject(s)
Cell Membrane/metabolism , Nervous System/pathology , Neurons/pathology , Sphingolipidoses/pathology , Sphingolipids/metabolism , Animals , Cell Membrane/pathology , Humans , Sphingolipids/toxicityABSTRACT
The discovery that most cells produce extracellular vesicles (EVs) and release them in the extracellular milieu has spurred the idea that these membranous cargoes spread pathogenic mechanisms. In the brain, EVs may have multifold and important physiological functions, from deregulating synaptic activity to promoting demyelination to changes in microglial activity. The finding that small EVs (exosomes) contain α-synuclein and ß-amyloid, among other pathogenic proteins, is an example of this notion, underscoring their potential role in the brains of patients with Parkinson's and Alzheimer's diseases. Given that they are membranous vesicles, we speculate that EVs also have an intrinsic capacity to incorporate sphingolipids. In conditions under which these lipids are elevated to toxic levels, such as in Krabbe's disease and metachromatic leukodystrophy, EVs may contribute to spread disease from sick to healthy cells. In this essay, we discuss a working hypothesis that brain cells in sphingolipidoses clear some of the accumulated lipid material to attempt restoring cell homeostasis via EV secretion. We hypothesize that secreted sphingolipid-loaded EVs shuttle pathogenic lipids to cells that are not intrinsically affected, contributing to establishing non-cell-autonomous defects. © 2016 Wiley Periodicals, Inc.
Subject(s)
Biological Transport/physiology , Brain/cytology , Cell Communication/physiology , Extracellular Vesicles/metabolism , Sphingolipids/metabolism , Animals , Humans , Models, Biological , Sphingolipidoses/pathology , Sphingolipids/toxicityABSTRACT
Lysosomal storage diseases (LSDs) often manifest with severe systemic and central nervous system (CNS) symptoms. The existing treatment options are limited and have no or only modest efficacy against neurological manifestations of disease. We demonstrate that recombinant human heat shock protein 70 (HSP70) improves the binding of several sphingolipid-degrading enzymes to their essential cofactor bis(monoacyl)glycerophosphate in vitro. HSP70 treatment reversed lysosomal pathology in primary fibroblasts from 14 patients with eight different LSDs. HSP70 penetrated effectively into murine tissues including the CNS and inhibited glycosphingolipid accumulation in murine models of Fabry disease (Gla(-/-)), Sandhoff disease (Hexb(-/-)), and Niemann-Pick disease type C (Npc1(-/-)) and attenuated a wide spectrum of disease-associated neurological symptoms in Hexb(-/-) and Npc1(-/-) mice. Oral administration of arimoclomol, a small-molecule coinducer of HSPs that is currently in clinical trials for Niemann-Pick disease type C (NPC), recapitulated the effects of recombinant human HSP70, suggesting that heat shock protein-based therapies merit clinical evaluation for treating LSDs.
Subject(s)
Heat-Shock Proteins/therapeutic use , Sphingolipidoses/drug therapy , Administration, Intravenous , Animals , Blood-Brain Barrier/drug effects , Blood-Brain Barrier/pathology , Bone Morphogenetic Proteins/metabolism , Disease Models, Animal , Disease Progression , Fabry Disease/drug therapy , Fabry Disease/pathology , Fibroblasts/drug effects , Fibroblasts/metabolism , Fibroblasts/pathology , Glycosphingolipids/metabolism , Heat-Shock Proteins/pharmacology , Humans , Hydroxylamines/pharmacology , Hydroxylamines/therapeutic use , Injections, Intraperitoneal , Intracellular Signaling Peptides and Proteins , Lysosomes/drug effects , Lysosomes/pathology , Niemann-Pick C1 Protein , Niemann-Pick Disease, Type C/drug therapy , Proteins/metabolism , Recombinant Proteins/pharmacokinetics , Recombinant Proteins/pharmacology , Recombinant Proteins/therapeutic use , Sphingolipidoses/pathology , Tissue DistributionABSTRACT
Lysosomal storage disorders (LSDs) are a group of >50 different types of inherited metabolic disorders that result from defects in the lysosome. The aim of this study was to investigate the distribution and demographic characteristics of the different subtypes of LSDs in Eastern China. From 2006 to 2012, 376 out of 1331 clinically suspected patients were diagnosed with 17 different subtypes of LSDs at our hospital. Mucopolysaccharidoses (MPS) were the most common group of LSDs (50.5%), followed by sphingolipidoses (25.4%) and Pompe disease (19.8%). Mucolipidosis type II/III accounted for the remaining 4% of diagnosed LSDs. MPS II was the most common form of MPS, comprising 47.4% of all MPS cases diagnosed, followed by MPS IVA (26.8%) and MPS I (16.3%). Gaucher disease and Niemann-Pick disease type A/B were the two most common forms of sphingolipidoses. There was a large variation in the time between disease onset and eventual diagnosis, from 0.3 years in infantile-onset Pompe disease to 30 years in Fabry disease, highlighting timely and accurate diagnosis of LSDs as the main challenge in China.
Subject(s)
Lysosomal Storage Diseases/genetics , Lysosomes/genetics , Adolescent , Adult , Age of Onset , Child , Child, Preschool , China , Fabry Disease/genetics , Fabry Disease/pathology , Female , Gaucher Disease/genetics , Gaucher Disease/pathology , Glycogen Storage Disease Type II/genetics , Glycogen Storage Disease Type II/pathology , Humans , Infant , Lysosomal Storage Diseases/classification , Lysosomal Storage Diseases/pathology , Lysosomes/pathology , Male , Mucolipidoses/genetics , Mucolipidoses/pathology , Niemann-Pick Diseases/genetics , Niemann-Pick Diseases/pathology , Sphingolipidoses/genetics , Sphingolipidoses/pathologyABSTRACT
DNA molecules can be assembled into custom predesigned shapes via hybridization of sequence-complementary domains. The folded structures have high spatial addressability and a tremendous potential to serve as platforms and active components in a plethora of bionanotechnological applications. DNA is a truly programmable material, and its nanoscale engineering thus opens up numerous attractive possibilities to develop novel methods for therapeutics. The tailored molecular devices could be used in targeting cells and triggering the cellular actions in the biological environment. In this review we focus on the DNA-based assemblies - primarily DNA origami nanostructures - that could perform complex tasks in cells and serve as smart drug-delivery vehicles in, for example, cancer therapy, prodrug medication, and enzyme replacement therapy.
Subject(s)
DNA/chemistry , Drug Delivery Systems/methods , Nanostructures/chemistry , Nanotechnology/methods , Base Pairing , DNA/metabolism , Drug Delivery Systems/instrumentation , Enzyme Replacement Therapy/methods , Humans , Nanotechnology/instrumentation , Neoplasms/pathology , Neoplasms/therapy , Nucleic Acid Conformation , Signal Transduction , Sphingolipidoses/pathology , Sphingolipidoses/therapyABSTRACT
The endolysosomal system is critical for the maintenance of cellular homeostasis. However, how endolysosomal compartment is regulated by mitochondrial function is largely unknown. We have generated a mouse model with defective mitochondrial function in CD4(+) T lymphocytes by genetic deletion of the mitochondrial transcription factor A (Tfam). Mitochondrial respiration deficiency impairs lysosome function, promotes p62 and sphingomyelin accumulation, and disrupts endolysosomal trafficking pathways and autophagy, thus linking a primary mitochondrial dysfunction to a lysosomal storage disorder. The impaired lysosome function in Tfam-deficient cells subverts T cell differentiation toward proinflammatory subsets and exacerbates the in vivo inflammatory response. Restoration of NAD(+) levels improves lysosome function and corrects the inflammatory defects in Tfam-deficient T cells. Our results uncover a mechanism by which mitochondria regulate lysosome function to preserve T cell differentiation and effector functions, and identify strategies for intervention in mitochondrial-related diseases.
Subject(s)
DNA-Binding Proteins/immunology , Lysosomal Storage Diseases/immunology , Lysosomes/immunology , Mitochondria/immunology , Mitochondrial Proteins/immunology , Sphingolipidoses/immunology , T-Lymphocytes/immunology , Transcription Factors/immunology , Animals , CD4-Positive T-Lymphocytes/immunology , CD4-Positive T-Lymphocytes/metabolism , CD4-Positive T-Lymphocytes/pathology , Cell Respiration , DNA-Binding Proteins/genetics , Gene Deletion , Immunity, Cellular , Lysosomal Storage Diseases/genetics , Lysosomal Storage Diseases/pathology , Lysosomes/genetics , Lysosomes/pathology , Mice , Mitochondria/genetics , Mitochondria/pathology , Mitochondrial Proteins/genetics , Sphingolipidoses/genetics , Sphingolipidoses/pathology , T-Lymphocytes/metabolism , T-Lymphocytes/pathology , Transcription Factors/geneticsABSTRACT
The mechanism of action of 2-hydroxyoleic acid (2OHOA), a potent antitumor drug, involves the rapid and specific activation of sphingomyelin synthase (SMS), leading to a 4-fold increase in SM mass in tumor cells. In the present study, we investigated the source of the ceramides required to sustain this dramatic increase in SM. Through radioactive and fluorescent labeling, we demonstrated that sphingolipid metabolism was altered by a 24 h exposure to 2OHOA, and we observed a consistent increase in the number of lysosomes and the presence of unidentified storage materials in treated cells. Mass spectroscopy revealed that different sphingolipid classes accumulated in human glioma U118 cells after exposure to 2OHOA, demonstrating a specific effect on C16-, C20-, and C22-containing sphingolipids. Based on these findings, we propose that the demand for ceramides required to sustain the SMS activation (ca. 200-fold higher than the basal level) profoundly modifies both sphingolipid and phospholipid metabolism. As the treatment is prolonged, tumor cells fail to adequately metabolize sphingolipids, leading to a situation resembling sphingolipidosis, whereby cell viability is compromised.
Subject(s)
Glioma/metabolism , Oleic Acids/pharmacology , Sphingolipidoses/metabolism , Transferases (Other Substituted Phosphate Groups)/metabolism , Cell Line, Tumor , Cell Survival/drug effects , Ceramides/metabolism , Ceramides/pharmacology , Glioma/pathology , Humans , Sphingolipidoses/chemically induced , Sphingolipidoses/pathology , Sphingolipids/metabolismABSTRACT
Analysis of lipid storage in postmortem brains of patients with amaurotic idiocy led to the recognition of five lysosomal ganglioside storage diseases and identification of their inherited metabolic blocks. Purification of lysosomal acid sphingomyelinase and ceramidase and analysis of their gene structures were the prerequisites for the clarification of Niemann-Pick and Farber disease. For lipid catabolism, intraendosomal vesicles are formed during the endocytotic pathway. They are subjected to lipid sorting processes and were identified as luminal platforms for cellular lipid and membrane degradation. Lipid binding glycoproteins solubilize lipids from these cholesterol poor membranes and present them to water-soluble hydrolases for digestion. Biosynthesis and intracellular trafficking of lysosomal hydrolases (hexosaminidases, acid sphingomyelinase and ceramidase) and lipid binding and transfer proteins (GM2 activator, saposins) were analyzed to identify the molecular and metabolic basis of several sphingolipidoses. Studies on the biosynthesis of glycosphingolipids yielded the scheme of Combinatorial Ganglioside Biosynthesis involving promiscuous glycosyltransferases. Their defects in mutagenized mice impair brain development and function.
Subject(s)
Sphingolipidoses/metabolism , Sphingolipids/metabolism , Animals , Brain/metabolism , Brain/pathology , Endocytosis , Humans , Lysosomes/enzymology , Lysosomes/metabolism , Sphingolipid Activator Proteins/chemistry , Sphingolipid Activator Proteins/metabolism , Sphingolipidoses/enzymology , Sphingolipidoses/genetics , Sphingolipidoses/pathology , Sphingolipids/biosynthesisABSTRACT
Kunihiko Suzuki is a neurologist by training whose research accomplishments range widely from basic research in brain lipids, their metabolism to genetic disorders involving the nervous system. Among them are identification of the enzymatic defect, the pathogenetic mechanism, and animal models of Krabbe's globoid cell leukodystrophy, the chemical and molecular pathologies of many glycosphingolipidoses, discovery of the abnormal accumulation of very long chain fatty acids in adrenoleukodystrophy, and elucidation of the complex metabolic interrelationship among sphingolipids with extensive use of the gene targeting technology. This reflections and perspectives highlight his accomplishments briefly.
Subject(s)
Leukodystrophy, Globoid Cell/enzymology , Sphingolipidoses/history , Adrenoleukodystrophy/genetics , Adrenoleukodystrophy/pathology , Animals , Disease Models, Animal , History, 20th Century , History, 21st Century , Japan , Leukodystrophy, Globoid Cell/history , Leukodystrophy, Globoid Cell/pathology , Mice , Sphingolipidoses/pathology , United StatesABSTRACT
Sphingolipid and glycosphingolipid levels and expression of sphingolipid metabolizing enzymes are altered in a variety of diseases or in response to drug treatment. Inherited defects of enzymes and other proteins required for the lysosomal degradation of these lipids lead to human sphingolipidoses. Also genetic defects that affect sphingolipid biosynthesis are known. Although the molecular details are often far from clear, (glyco)sphingolipids have been implicated to play a role in atherosclerosis, insulin resistance, cancer, and infections by pathogens. More general aspects of selected diseases are discussed.
Subject(s)
Disease , Sphingolipids , Animals , Carbohydrate Sequence , Disease/genetics , Glycosphingolipids/biosynthesis , Glycosphingolipids/chemistry , Glycosphingolipids/metabolism , Humans , Lysosomes/metabolism , Molecular Sequence Data , Sphingolipidoses/chemically induced , Sphingolipidoses/enzymology , Sphingolipidoses/metabolism , Sphingolipidoses/pathology , Sphingolipids/biosynthesis , Sphingolipids/chemistry , Sphingolipids/metabolismABSTRACT
Sphingolipidoses constitute a large subgroup of lysosomal storage disorders (LSDs). Many of them are associated with a progressive neurodegeneration. As is the case for LSDs in general, most sphingolipidoses are caused by deficiencies in lysosomal hydrolases. However, accumulation of sphingolipids can also result from deficiencies in proteins involved in the transport or posttranslational modification of lysosomal enzymes, transport of lipids, or lysosomal membrane proteins required for transport of lysosomal degradation end products. The accumulation of sphingolipids in the lysosome together with secondary changes in the concentration and localization of other lipids may cause trafficking defects of membrane lipids and proteins, affect calcium homeostasis, induce the unfolded protein response, activate apoptotic cascades, and affect various signal transduction pathways. To what extent, however, these changes contribute to the pathogenesis of the diseases is not fully understood. Currently, there is no cure for sphingolipidoses. Therapies like enzyme replacement, pharmacological chaperone, and substrate reduction therapy, which have been shown to be efficient in non-neuronopathic LSDs, are currently evaluated in clinical trials of neuronopathic sphingolipidoses. In the future, neural stem cell therapy and gene therapy may become an option for these disorders.
Subject(s)
Neurodegenerative Diseases/metabolism , Neurodegenerative Diseases/therapy , Sphingolipidoses/metabolism , Sphingolipidoses/therapy , Sphingolipids/metabolism , Animals , Calcium/metabolism , Endocytosis/drug effects , Enzyme Replacement Therapy , Genetic Therapy , Humans , Lysosomes/drug effects , Lysosomes/metabolism , Mice , Molecular Chaperones/therapeutic use , Neurodegenerative Diseases/drug therapy , Neurodegenerative Diseases/pathology , Protein Unfolding/drug effects , Rats , Signal Transduction/drug effects , Sphingolipidoses/drug therapy , Sphingolipidoses/pathology , Sphingolipids/genetics , Stem Cell TransplantationABSTRACT
Sphingolipids are polar membrane lipids present as minor components in eukaryotic cell membranes. Sphingolipids are highly enriched in nervous cells, where they exert important biological functions. They deeply affect the structural and geometrical properties and the lateral order of cellular membranes, modulate the function of several membrane-associated proteins, and give rise to important intra- and extracellular lipid mediators. Sphingolipid metabolism is regulated along the differentiation and development of the nervous system, and the expression of a peculiar spatially and temporarily regulated sphingolipid pattern is essential for the maintenance of the functional integrity of the nervous system: sphingolipids in the nervous system participate to several signaling pathways controlling neuronal survival, migration, and differentiation, responsiveness to trophic factors, synaptic stability and synaptic transmission, and neuron-glia interactions, including the formation and stability of central and peripheral myelin. In several neurodegenerative diseases, sphingolipid metabolism is deeply deregulated, leading to the expression of abnormal sphingolipid patterns and altered membrane organization that participate to several events related to the pathogenesis of these diseases. The most impressive consequence of this deregulation is represented by anomalous sphingolipid-protein interactions that are at least, in part, responsible for the misfolding events that cause the fibrillogenic and amyloidogenic processing of disease-specific protein isoforms, such as amyloid beta peptide in Alzheimer's disease, huntingtin in Huntington's disease, alpha-synuclein in Parkinson's disease, and prions in transmissible encephalopathies. Targeting sphingolipid metabolism represents today an underexploited but realistic opportunity to design novel therapeutic strategies for the intervention in these diseases.
