Sphingolipids  From Pathology to Therapeutic Perspectives - A Themed Honorary Issue to Prof. Lina Obeid 

 - Basel, Switzerland  MDPI - Multidisciplinary Digital Publishing Institute  2021 
 - 1 online resource (292 p.) 
<br/><br/> Open Access 
<br/><br/> Although sphingolipids are ubiquitous components of cellular membranes, their abundance in cells is generally lower than glycerolipids or cholesterol, representing less than 20% of total lipid mass. Following their discovery in the brain-which contains the largest amounts of sphingolipids in the body-and first description in 1884 by J.L.W. Thudichum, sphingolipids have been overlooked for almost a century, perhaps due to their complexity and enigmatic nature. When sphingolipidoses were discovered, a series of inherited diseases caused by enzyme mutations involved in sphingolipid degradation returned to the limelight. The essential breakthrough came decades later, in the 1990s, with the discovery that sphingolipids were not just structural elements of cellular membranes but intra- and extracellular signaling molecules. It turned out that their lipid backbones, including ceramide and sphingosine-1-phosphate, had selective physiological functions. Thus, sphingolipids emerged as essential players in several pathologies including cancer, diabetes, neurodegenerative disorders, and autoimmune diseases. The present volume reflects upon the unexpectedly eclectic functions of sphingolipids in health, disease, and therapy. This fascinating lipid class will continue to be the subject of up-and-coming future discoveries, especially with regard to new therapeutic strategies. 
<br/><br/><br/>Creative Commons 
<br/><br/><br/>English 
<br/><br/><label>ISBN: </label>9783039439577 9783039439584 books978-3-03943-958-4 
<br/><br/><label>Standard No.: </label>10.3390/books978-3-03943-958-4  doi 
<br/><br/><label>Subjects--Topical Terms: </label><br/>Biology, life sciences<br/>Research & information: general
<br/><br/><label>Subjects--Index Terms: </label>acid sphingomyelinase albumin allyl carbamate derivative animal models anxiety anxiety-like behavior apoptosis Aspergillus fumigatus astrocytes autophagy barrier dysfunction beta-cells calcium cancer cardioprotection ceramidase ceramidases ceramide ceramides CLN3 disease Cln3Δex7/8 mice coronary flow cortex cystic fibrosis cytokines depression depressive-like behavior fingolimod flupirtine forebrain G-protein-coupled receptors gangliosides Gαq/11 hippocampus histone acetylation hypothalamus hypoxia immunotherapy infectious diseases inflammation insulin insulin resistance ischemia/reperfusion islets long non-coding RNA metastasis microRNA multiple sclerosis myocardial function myocardial infarct myriocin n/a neurodegeneration neurodegenerative diseases neurons obesity pancreatic β cell fate phenotype switching S1P S1P receptor S1P transporter S1P-lyase (SGPL1) S1P1-5 SK1 Smpd1 sphingolipids sphingomyelinase sphingosine 1-phoshate sphingosine 1-phosphate Sphingosine 1-phosphate (S1P) sphingosine 1-phosphate antagonistst/inhibitors sphingosine 1-phosphate metabolism sphingosine 1-phosphate receptor sphingosine 1-phosphate signaling sphingosine kinase sphingosine kinase 1 sphingosine-1-phosphate Sphingosine-1-phosphate spinster homolog 2 stroke tau transcription factor type 1 diabetes type 2 diabetes vasoconstriction