Introduction: The neonatal immune system is immature. Antibody (Ab) responses are slow and transient due to reduced survival of antibody- -secreting cells (AbSCs) in the bone marrow (BM). The aim was to study the effect of neonatal immunization w/wo adjuvant LT-K63 on BM cell subsets and their production of the AbSC survival signals APRIL and IL-6. Materials and methods: We assessed the frequency of neutrophils, eosinophils (EOs), monocytes, macrophages and megakaryocytes (MKCs), as well as APRIL- and IL-6-secreting cells in BM by FACS at different time points after neonatal immunization with pneumococcal conjugate (Pnc1-TT) w/wo the adjuvant LT-K63. Vaccine-specific AbSCs in BM and serum Abs were measured by ELISPOT and ELISA. Results: Frequency of MKCs and EOs, and APRIL- and IL-6-secreting MKCs and EOs was significantly increased in mice immunized with Pnc1- TT+LT-K63 compared to Pnc1-TT. Furthermore, the fraction of EOs that were APRIL+ and IL-6+ and MKCs that were APRIL+ was larger in mice immunized with Pnc1-TT+LT-K63. This correlates with higher vaccine- -specific Ab levels and number of AbSCs that persist in the BM of mice that receive LT-K63 together with the vaccine. Conclucion: The results suggest that the adjuvant LT-K63 not only incre- ases the frequency of EOs and MKCs in BM of neonatal mice but also act- ivates a higher percentage of EOs to secrete APRIL and IL-6 and a higher percentage of MKCs to secrete APRIL. This might contribute to increased survival of AbSCs in BM at early age when LT-K63 is administered to- gether with Pnc1-TT. E 89 Endotheliomics: The metabolic response of the endothelium to LPS and hypoxia Sarah McGarrity1, Ósk Anuforo2, Haraldur Halldórsson3, Óttar Rolfsson3 1School of Engineering and Natural Sciences, Center for Systems Biology, 2Center for Systems Biology, 3Faculty of Medicine, School of Health Sciences sarahm@hi.is Introduction: Endothelial cells line blood vessels and their dysfunction plays a key role in many diseases, especially inflammatory conditions including sepsis. Context specific genome scale metabolic models (GEMs) have been built to explore metabolic changes in different endot- helial cell types when grown with lipopolysaccharide (LPS) and under hypoxia. These models combine existing transcriptomic data with novel metabolomic data. Methods: Using the COBRAtoolbox and the Fastcore algorithm the RECON1 model was constrained to produce three cell type specific GEMs related to human umbilical vein, pulmonary artery and microvascular endothelial cells (HUVEC, HPAEC and HMVEC) using publically available transcriptomic data. The HUVEC model was further constrained to reflect HUVECs grown with LPS and the HPAEC model to reflect cells grown under hypoxia. Metabolomic data from HUVECs with and without LPS was collected using mass spectrometry and app- lied to further constrain the model. Comparisons between models were made; analysing the differences in lethal reactions between models and MOMA to analyse changes in growth rates. Results: Preliminary analysis of cell type specific GEMs show small differences between endothelial cell types in glycolysis and amino acid metabolism between different endothelial cell types. Differences in nucleotide metabolism and pyruvate metabolism appear between HUVECs with and without LPS and HPAECs grown under normoxic and hypoxic conditions show differences in pyruvate metabolism and amino acid metabolism. Conclusions: Combining metabolomics analysis with models based on transcriptomics data highlights context specific differences endothelial cell metabolism that may have functional implications. E 90 Clarifying the role of signal transduction of keratinocytes in the pathogenesis of psoriasis Hildur Sigurgrímsdóttir1,2, Fannar P. Theódórs1,2, Jóna Freysdóttir1,2,3, Björn R. Lúðvíksson1,2 1Faculty of Medicine, Biomedical Center, University of Iceland, 2Dept of Immunology, Landspitali – The National University Hospital of Iceland, 3Centre for Rheumatology Research, Landspitali – The National University Hospital of Iceland hildursigur@hotmail.com Introduction: Psoriasis is a chronic inflammatory skin disease, character- ized by infiltration of T cells and epidermal thickening. Several cytokines and anti-microbial peptides are upregulated in psoriasis patients, inclu- ding IFNγ, IL-17, IL-22 and TNFα and together with immune cells in- filtrating the skin they drive the pathogenesis of psoriasis. Phsophoflow is a new way of measuring intra-cellular signaling pathways by flow cytometry. It provides advantages over the older method, western blotting, as it can measure both the percentage of activated cells within a homo- or heterogeneous population and the mean expression level. The main aim of this research is to characterize the intracellular response of keratinocytes to different stimuli using phosphoflow. Material and methods: HaCaT cells (immortalized keratinocytes) stimulated with selected cytokines were stained for phosphorylated intracellular proteins and analyzed using flow cytometry. Results: Using phosphoflow, phosphorylation of cytokine-dependent signaling molecules in HaCaT cells could be detected. The response to IFNγ, the main Th1 cytokine, was characterized by phosphorylation of STAT1 while the main cytokines in a Th17 response, IL-17 and IL-22, induced an increase in ERK1/2 phosphorylation. IL-4, which directs Th2 differentiaion, induced phosphorylation of STAT6. Conclusion: This study shows that phosphoflow can be used to inve- stigate keratinocyte signaling pathways which may shed further light on how pro-inflammatory cytokines and/or anti-microbial peptides influence keratinocytes and subsequently the pathogenesis of psoriasis. E 91 Innleiðing og notagildi Klínískra leiðbeininga um hjúkrun heilablóðfallsjúklinga í endurhæfingu Ingibjörg Bjartmarz1, Helga Jónsdóttir2, Þóra B. Hafsteinsdóttir3 1Endurhæfingardeild á Grensás, 2Hjúkrunarfræðideild, Heilbrigðisvísindasvið, 3Department of Rehabilitation, Nursing Science and Sport, Brain Centre Rudolf Magnus, University Medical Center Utrecht ingibjart@simnet.is Inngangur: Tilgangur rannsóknarinnar var að meta innleiðingu og hag- nýta notkun “Klínískra leiðbeininga um hjúkrun heilablóðfallssjúklinga í endurhæfingu” sem fela í sér ráðleggingar um hreyfi- og sjálfsbjargargetu, þunglyndi og fræðslu. Einnig var metin reynsla hjúkrunarfræðinga og sjúkraliða af innleiðingu og notkun leiðbeininganna. Efniviður og aðferðir: Klínísku leiðbeiningarnar á formi skriflegra, myndrænna, netupplýsinga og veggspjalda voru innleiddar á taugalækn- ingadeild og endurhæfingardeild Grensás á Landspítala. Eftirfarandi ferli var notað við innleiðinguna: a) valdir voru lykilhjúkrunarfræðingar og sjúkraliðar til að styðja við innleiðinguna; b) fræðslufundir voru haldnir með öllu starfsfólki; c) hjúkrunarfræðingar og sjúkraliðar fengu kennslu og starfsþjálfun. Til þess að meta áhrif innleiðingarinnar á skráningu og 34 LÆKNAblaðið/Fylgirit 91 2017/103 X V I 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 9 1

Síða 1
Síða 2
Síða 3
Síða 4
Síða 5
Síða 6
Síða 7
Síða 8
Síða 9
Síða 10
Síða 11
Síða 12
Síða 13
Síða 14
Síða 15
Síða 16
Síða 17
Síða 18
Síða 19
Síða 20
Síða 21
Síða 22
Síða 23
Síða 24
Síða 25
Síða 26
Síða 27
Síða 28
Síða 29
Síða 30
Síða 31
Síða 32
Síða 33
Síða 34
Síða 35
Síða 36
Síða 37
Síða 38
Síða 39
Síða 40
Síða 41
Síða 42
Síða 43
Síða 44
Síða 45
Síða 46
Síða 47
Síða 48
Síða 49
Síða 50
Síða 51
Síða 52
Síða 53
Síða 54
Síða 55
Síða 56
Síða 57
Síða 58
Síða 59
Síða 60
Síða 61
Síða 62
Síða 63
Síða 64
Síða 65
Síða 66
Síða 67
Síða 68
Síða 69
Síða 70
Síða 71
Síða 72
Síða 73
Síða 74
Síða 75
Síða 76
Síða 77
Síða 78
Síða 79
Síða 80
Síða 81
Síða 82
Síða 83
Síða 84
Síða 85
Síða 86
Síða 87
Síða 88
Síða 89
Síða 90
Síða 91
Síða 92
Síða 93
Síða 94
Síða 95
Síða 96
Síða 97
Síða 98
Síða 99
Síða 100