X V I I V Í S I N D A R Á Ð S T E F N A H Í F Y L G I R I T 8 2 70 LÆKNAblaðið/Fylgirit 82 2015/101 metótrexat við sóragigt hér á landi. Efniviður og aðferðir: Fengnar voru upplýsingar úr ICEBIO- gagnagrunninum um einstaklinga með sóragigt á sinni fyrstu meðferð með TNFα hemli þar sem til staðar voru upplýsingar um sjúkdóms- virkni við upphaf meðferðar og að minnsta kosti einn af eftirtöldum tímapunktum; 13 vikur, 26 vikur eða 52 vikur (n =83). Notast var við skilmerkin ACR20, ACR50, ACR70 og EULAR response criteria til að meta árangur. Bornir voru saman þeir sem fengu metótrexat samhliða TNFα hemli við þá sem aðeins fengu TNFα hemil. Niðurstöður: Samhliða meðferð með TNFα hemli og metótrexat reynd- ist ekki skila marktækt betri meðferðarárangri fyrr en eftir 52 vikna meðferð. Við þann tímapunkt höfðu 18% sjúklinga á TNFα hemli, en 65% af þeim sem voru jafnframt á metótrexat náð ACR50 (p=0,0165); fyrir ACR20 voru hlutfallið 42% og 65% (p=0,0426). Eftir 52 vikur hafði um helmingur sjúklinga á TNFα hemli, en 92% sjúklinga á samsettri meðferð náð góðri EULAR svörun (p=0,0004) Ályktanir: Niðurstöður rannsóknarinnar benda til þess að sjúklingar á samhliða meðferð með metótrexat og TNFα hemli séu líklegri til að ná betri meðferðarárangri til langs tíma en þeir sem eingöngu fá TNFα hemil. V 41 Sulfobutylether-β-cyclodextrin/chitosan particles and their physicochemical characteristics Phennapha Saokham, Zoltán Fülöp, Þorsteinn Loftsson Faculty of Pharmaceutical Sciences, University of Iceland phs3@hi.is Introduction: Chitosan particles can be prepared by a number of techni- ques but one of the most promising one is ionotropic gelation which is based on ionic interactions between the polycationic chitosan and a polyanionic polymer. These anion sources can be different types of CDs, for example sulfobutylether β-cyclodextrin (SBEβCD). Methods and data: SBEβCD/CS particles were prepared by mixing SBEβCD and CS solutions of equal weight concentrations. The encap- sulation efficiency (EE) of HC in the particles, the mean hydrodynamic diameter and polydispersity index and drug permeation were determ- ined. Results: The particles become larger and contain larger number of SBEβCD molecules with increasing CS:SBEβCD ratio but at the same time their ability to take up HC molecules decreases. The flux of HC from the SBEβCD complexes is higher than the HC flux from the loaded particles at identical SBEβCD concentration. Conclusions: Due to the lipophilic nature of the CD cavities the very hydrophilic NPs could be loaded with poorly water-soluble lipophilic drugs such as HC. The size of the NPs (diameter 200 to 1000 nm) and the drug release rate could be controlled by changing the initial concentration of SBEβCD and CS during the particle preparation. In aqueous solutions the particles were characterized as metastable whe- reas self-assembled cyclodextrin nanoparticles readily dissociate upon media dilution. V 42 Stability of liposomes: effect of size, layer by layer electrostatic deposition and dehydration Ragnhildur Einarsdóttir1, Benjamin Zeeb2, Monika Gibis2, Kristberg Kristbergsson1, Jochen Weiss2 1Faculty of Food Science and Nutrition, University of Iceland, 2Department of Food Physics and Meat Science, Institute of Food Science and Biotechnology, University of Hohenheim rae22@hi.is Introduction: Liposomes are used as delivery systems for bioactives in pharmaceuticals, cosmetics and foods. Liposomes subjected to dehydration are susceptible to fusion and leakage. With the layer by layer electrostatic depositioning, polyelectrolytes adsorb to the liposome surface to form a monolayer. The aim of the study was to increase the stability of liposomes through coating with cold water fish skin gelatin and to study the influence of liposome size on layering properties and physical stability during dehydration. Methods and data: Liposomes were prepared with high pressure homogenization and extrusion through polycarbonate membranes in 10 mM acetate buffer at pH 3.8 to produce three liposomal dispersions of different sizes. Cold water skin fish gelatin was used to coat the liposomes. Liposomal dispersions were placed in dialysis tubes where an outer osmotic pressure created by 0.5 M sucrose, dehydrated the samples with time. Results: The ζ-potential changed from -55 mV for uncoated liposomes to 25 mV for coated liposomes. The relative weight and change in size was measured with a static light scatterer. Original size of liposomes influenced the stability of liposomes during osmotic dehydration, with the 0.09 µm in diameter liposomes being stable for 60 min, compared to 30 minutes for liposomes of 0.40 µm and 2.73 µm. Secondary liposomes were more stable towards aggregation and size change. Conclusions: The results show that cold water fish gelatin can be used to coat liposomes using the layer by layer electrostatic dispositioning method. Moreover it shows that the interfacial membrane protects the liposomes from aggregation and fusion during dehydration. V 43 New nucleosides produced by the marine sponge Geodia macandrewi Margarida Costa1,2, Hongbing Liu1, Eydís Einarsdóttir1,2, Margrét Þorsteinsdóttir1,2, Sesselja Ómarsdóttir1 1Faculty of Pharmaceutical Sciences, University of Iceland, 2ArcticMass sesselo@hi.is Introduction: The ocean exploration for the discovery of new natural compounds has emerged as a promising field in drug-discovery. Among all the biological diversity, marine sponges are recognized as the richest source of marine natural compounds. The first studies looking for mar- ine-derived natural compounds led to the discovery of the nucleosides spongouridine and spongothymidine, that represented the basis for Ara-C and Ara-A. Those compounds were later commercialized as anticancer and antiviral drugs, respectively. To date over 30 nucleosides have been characterized from sponges and they have been shown to possess various bioactivities. Methods and data: In this study, the sponge Geodia macandrewi, collected in deep waters southwest of Iceland was submitted to CH2Cl2:CH3OH (1:1) extraction. The extract was further fractionated by modified Kupchan solvent partition and a polar fraction revealed the presence of several nucleosides. Those compounds were isolated by preparative HPLC. 1D and 2D NMR spectroscopy and QTOF-MS/MS were used to

Page 1
Page 2
Page 3
Page 4
Page 5
Page 6
Page 7
Page 8
Page 9
Page 10
Page 11
Page 12
Page 13
Page 14
Page 15
Page 16
Page 17
Page 18
Page 19
Page 20
Page 21
Page 22
Page 23
Page 24
Page 25
Page 26
Page 27
Page 28
Page 29
Page 30
Page 31
Page 32
Page 33
Page 34
Page 35
Page 36
Page 37
Page 38
Page 39
Page 40
Page 41
Page 42
Page 43
Page 44
Page 45
Page 46
Page 47
Page 48
Page 49
Page 50
Page 51
Page 52
Page 53
Page 54
Page 55
Page 56
Page 57
Page 58
Page 59
Page 60
Page 61
Page 62
Page 63
Page 64
Page 65
Page 66
Page 67
Page 68
Page 69
Page 70
Page 71
Page 72
Page 73
Page 74
Page 75
Page 76
Page 77
Page 78
Page 79
Page 80
Page 81
Page 82
Page 83
Page 84
Page 85
Page 86
Page 87
Page 88
Page 89
Page 90
Page 91
Page 92
Page 93
Page 94
Page 95
Page 96
Page 97
Page 98
Page 99
Page 100
Page 101
Page 102
Page 103
Page 104
Page 105
Page 106
Page 107
Page 108
Page 109
Page 110
Page 111
Page 112
Page 113
Page 114
Page 115
Page 116
Page 117
Page 118
Page 119
Page 120
Page 121
Page 122
Page 123
Page 124
Page 125
Page 126
Page 127
Page 128
Page 129
Page 130
Page 131
Page 132
Page 133
Page 134
Page 135
Page 136
Page 137
Page 138
Page 139
Page 140
Page 141
Page 142
Page 143
Page 144
Page 145
Page 146
Page 147
Page 148
Page 149
Page 150
Page 151
Page 152
Page 153
Page 154
Page 155
Page 156
Page 157
Page 158
Page 159
Page 160
Page 161
Page 162
Page 163
Page 164
Page 165
Page 166
Page 167
Page 168
Page 169
Page 170
Page 171
Page 172
Page 173