MBP Interacts with PIP2 at the Oligodendroglial Cell Membrane

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The only protein known to be essential for myelin formation and compaction in the central nervous system is myelin basic protein (MBP). The association of MBP as a positively-charged protein with negatively charged membranes is crucial for myelination, but the mechanisms by which MBP associates with the myelin membrane remains elusive. Here I demonstrate that the signaling lipid PIP2 is important for the stable association of MBP with cellular membranes. This association is lost upon specific decrease of membrane charges through selective hydrolyzation of PIP2 levels or through elevated intracellular Ca2+ levels. Further experiments implicate that one putative PIP2 binding domain of MBP lies within the exon-1 encoded region. The relevance of this protein-lipid interaction was demonstrated for the corpus callosum of mice, after decreasing membrane surface charges in acute brain slices. Here, PIP2 hydrolysis led to the loss of myelin compaction. The results demonstrate that PIP2 plays an important role in MBP association to the plasma membrane. These findings provide a novel link between phosphoinositol metabolism and MBP function in oligodendrocytes in development and disease.

Autorentext

Schanila Nawaz completed her PhD in the field of Neuroscience inJanuary 2009 at the Max Planck Institute for ExperimentalMedicine in Göttingen, which was followed by a short postdocperiod, in the Biophysics department of the University ofGöttingen. She has an undergraduate training in biotechnologyfrom the University of Stuttgart.

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Weitere Informationen

  • Allgemeine Informationen
    • Sprache Englisch
    • Gewicht 173g
    • Untertitel The Role of Phosphoinositides in the Interaction of Myelin Basic Protein with the Oligodendroglial Cell Membrane
    • Autor Schanila Nawaz
    • Titel MBP Interacts with PIP2 at the Oligodendroglial Cell Membrane
    • Veröffentlichung 24.11.2015
    • ISBN 3838120795
    • Format Kartonierter Einband
    • EAN 9783838120799
    • Jahr 2015
    • Größe H220mm x B150mm x T7mm
    • Herausgeber Südwestdeutscher Verlag für Hochschulschriften AG Co. KG
    • Anzahl Seiten 104
    • GTIN 09783838120799

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