Literature DB >> 11514093

MFAME, N-methyl-N-D-fructosyl amphotericin B methyl ester, a new amphotericin B derivative of low toxicity: relationship between self-association and effects on red blood cells.

J Szlinder-Richert1, J Mazerski, B Cybulska, J Grzybowska, E Borowski.   

Abstract

In aqueous solutions N-methyl-N-D-fructosyl amphotericin B methyl ester (MFAME), a novel amphotericin B derivative with low animal toxicity, similar to its parent antibiotic, exists in three forms: monomeric, soluble and insoluble aggregates in equilibrium [1]. The aim of our work was to examine the influence of medium composition on the MFAME self-association and the relationship between MFAME self-association and its toxicity towards red blood cells. The toxicity of MFAME in aggregated state towards red blood cells was tested by measuring the induction of potassium leakage and extent of haemolysis. The proportions of antibiotic species present in various aqueous media were determined by analysis of the UV-Vis spectra as a function of the antibiotic concentration. Numeric decomposition of the spectra allowed identification of four spectral species present in MFAME solutions: monomeric and three aggregated forms. Our results indicate that these aggregates, named type I, type II and type III, are different in terms of spectral properties, as well as effectiveness towards red blood cells. Soluble aggregate types I and III are the active forms of MFAME towards erythrocytes. The medium composition seems to be the main factor determining which type of antibiotic aggregate prevails in solution.

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Year:  2001        PMID: 11514093     DOI: 10.1016/s0304-4165(01)00166-0

Source DB:  PubMed          Journal:  Biochim Biophys Acta        ISSN: 0006-3002


  11 in total

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3.  Molecular aspects of the interaction between amphotericin B and a phospholipid bilayer: molecular dynamics studies.

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4.  The effect of sterols on amphotericin B self-aggregation in a lipid bilayer as revealed by free energy simulations.

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6.  Engineered biosynthesis of disaccharide-modified polyene macrolides.

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Journal:  Appl Environ Microbiol       Date:  2013-08-02       Impact factor: 4.792

7.  Enhancing the production of amphotericin B by Strepyomyces nodosus in a 50-ton bioreactor based on comparative genomic analysis.

Authors:  Kai Huang; Bo Zhang; Yu Chen; Zhe-Ming Wu; Zhi-Qiang Liu; Yu-Guo Zheng
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8.  New Rimocidin/CE-108 Derivatives Obtained by a Crotonyl-CoA Carboxylase/Reductase Gene Disruption in Streptomyces diastaticus var. 108: Substrates for the Polyene Carboxamide Synthase PcsA.

Authors:  Leticia Escudero; Mahmoud Al-Refai; Cristina Nieto; Hartmut Laatsch; Francisco Malpartida; Elena M Seco
Journal:  PLoS One       Date:  2015-08-18       Impact factor: 3.240

9.  An Amphotericin B Derivative Equally Potent to Amphotericin B and with Increased Safety.

Authors:  Armando Antillón; Alexander H de Vries; Marcel Espinosa-Caballero; José Marcos Falcón-González; David Flores Romero; Javier González-Damián; Fabiola Eloísa Jiménez-Montejo; Angel León-Buitimea; Manuel López-Ortiz; Ricardo Magaña; Siewert J Marrink; Rosmarbel Morales-Nava; Xavier Periole; Jorge Reyes-Esparza; Josué Rodríguez Lozada; Tania Minerva Santiago-Angelino; María Cristina Vargas González; Ignacio Regla; Mauricio Carrillo-Tripp; Mario Fernández-Zertuche; Lourdes Rodríguez-Fragoso; Iván Ortega-Blake
Journal:  PLoS One       Date:  2016-09-28       Impact factor: 3.240

10.  Thermodynamics and kinetics of amphotericin B self-association in aqueous solution characterized in molecular detail.

Authors:  Joanna Zielińska; Miłosz Wieczór; Tomasz Bączek; Marcin Gruszecki; Jacek Czub
Journal:  Sci Rep       Date:  2016-01-08       Impact factor: 4.379

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