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Self-Association of Amphotericin B: Spontaneous Formation of Molecular Structures Responsible for the Toxic Side Effects of the Antibiotic
62
Citations
36
References
2014
Year
Amb DimersMolecular Self-assemblyAntimicrobial ChemotherapyChemical BiologyAntibiotic ResistanceDrug ResistanceMedicinal ChemistryAmphotericin BAmb MoleculesMolecular RecognitionAntimicrobial ResistanceBiophysicsBiochemistryMedicineSpontaneous FormationAntimicrobial CompoundPharmacologyAntimicrobial SusceptibilityAntibioticsNatural SciencesRational Drug DesignMicrobiologyMolecular DockingToxic Side EffectsDrug Discovery
Amphotericin B (AmB) is a lifesaving antibiotic used to treat deep-seated mycotic infections. Both the pharmaceutical activity and highly toxic side effects of the drug rely on its interaction with biomembranes, which is governed by the molecular organization of AmB. In the present work, we present a detailed analysis of self-assembly of AmB molecules in different environments, interesting from the physiological standpoint, based on molecular spectroscopy techniques: electronic absorption, circular dichroism, steady state and time-resolved fluorescence and molecular dynamic calculations. The results show that, in the water medium, AmB self-associates to dimeric structures, referred to as "parallel" and "antiparallel". AmB dimers can further assemble into tetramers which can play a role of transmembrane ion channels, affecting electrophysiological homeostasis of a living cell. Understanding structural determinants of self-assembly of AmB opens a way to engineering preparations of the drug which retain pharmaceutical effectiveness under reduced toxicity.
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