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Encapsulation of Mithramycin in Liposomes in Response to a Transmembrane Gradient of Calcium Ions
Authors:F FRÉZARD  A GARNIER-SUILLEROT  C DEMICHELI
Institution:(1) Departamento de Bioquímica-Imunologia, Universidade Federal de Minas Gerais, P.O. Box 486, Belo Horizonte, M.G., Brazil, CEP 30161-970;(2) Laboratoire de Physicochimie Biomoléculaire et Cellulaire (CNRS URA 2056) UFR Biomédicale, Université Paris Nord, 74 rue Marcel Cachin, Bobigny Cedex, France, CEP 93017;(3) Departamento de Química, Universidade Federal de Minas Gerais, P.O. Box 702, Belo Horizonte, M.G., Brazil, CEP 30161-970
Abstract:The recent discovery that mithramycin(MTR) in aqueous solution forms a high affinityCa(MTR)4]2- complex led us to the idea thatCa2+-loaded liposomes might be able to accumulateMTR in their aqueous internal compartment. Wetherefore investigated the uptake of MTR into largeunilamellar vesicles (LUV) containing NaCl orCaCl2. Our data show that MTR was efficientlyaccumulated within LUV made fromdipalmitoylphosphatidylcholine and cholesterol, onlywhen the liposomes contained Ca2+ and wereresuspended in a Ca2+-free medium. A drugencapsulation efficiency as high as 60% was achieved,at a drug to lipid molar ratio of 1/18. The circulardichroism and fluorescence excitation spectra ofliposome-encapsulated MTR (LMTR) displayed strongsimilarities with those of the Ca(MTR)4]2-complex. LMTR was found to be stable, when submittedto conditions that destabilized theCa(MTR)4]2- complex. Upon dilution andincubation for 24 h at 37 °C, MTR-containingliposomes did not release a significant amount of MTR.These properties were attributed to the formation ofa high affinity complex between MTR and Ca2+inthe aqueous compartment of liposomes.
Keywords:Mithramycin  calcium ion gradient  liposomes  encapsulation
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