The aim of this study was to see if IL-6 could pass the placenta in a rat pregnancy. Material and Methods: Timed pregnant Wistar dams were injected intravenously (i.v.) with 1.4ml/kg 125I-IL-6. The amount of IL-6 used is considered to be physiological equivalent to maternal infection. Blood samples were collected before and during 30 minutes. Then section was performed and amniotic fluid, placentas, fetuses, right atrium and kidney collected from each dam. The radioactivity was measured with a gamma-counter. Results: Radioactivity was detected in all samples except amniotic fluid. Results are given on a per gram basis as sample/blood ratio R ((L/g) ( S.E.M. Right atrium = 3,92 ( 1,04; Placenta = 8,59 ( 1,13; Fetus = 0,18 ( 0,08; Kidney = 67,59 ( 14,9. Discussion: IL-6 passes the placenta with non-mediated transport. Highest values were in blood rich organs like the kidney and placenta. Radioactivity in the fetuses is low but could be enough to change the fetal IL-6 concentration so it can affect the fetal homeostasis. Key words: Fetal programming, lnterleukin-6, placental passage Immunization Coverage in the Monkey Bay Head Zone Malawi Þórður Þórarinn Þórðarsonl Halldór Jónsson2 Ásgeir Haraldsson3 Geir Gunnlaugsson4 1 University of lceland, Faculty of Medicine. 2lcelandic International Development Agency. 3Children’s Hospital lceland, Landspitali University Hospital, lceland. 4Centre for Child Health Services, Reykjavik, lceland. Introduction In context of ICEIDA's efforts to improve health care services in the Monkey Bay area in Malawi, a survey was conducted to estimate immunization coverage of children aged 12- 23 months in the Monkey Bay head zone. The head zone consists of 97 villages with a population of around 105000. Five health centres provide immunization services in the area. Methods The method used was a 30 by 7 cluster sample survey, as defined by WHO’s Expanded Programme on Immunization (EPI). Two hundred and seventeen children in 30 clusters were randomly selected and their immunization status as registered by immunization card or history was evaluated. Results Immunization coverage by card or history was 97,2% for BCG, and 99,1%, 94,9% and 84,7% for DTP1, DTP2 and DTP3 respectively. Coverage of OPV1, OPV2 and OPV3 by card or history was 99,1%, 93,1% and 85,2% respectively. Coverage for measles by card or history was 78,2%. Fully immunized children by card or history were 152 or 70,4%. Drop-out rate from DTP1 to DTP3 vaccination by card or history was 14,5%, and drop-out from DTP1 to Measles by card or history was 21,0%. Only two children had not received any immunizations. Discussion - According to this survey, immunzation coverage in the Monkey Bay head zone is higherthan previous estimates indicate, and in general above national levels of 2002. The results indicate that access to the immunzation system ín the Monkey Bay Head Zone is good, but drop-out is high which indicates that coverage could be raised through improved utilization of the immunization system available. Keywords Immunization Coverage, Monkey Bay, Malawi Hvað stjórnar tjáningu á mRKS fyrir IL-13 og IL-13R(1 í hnatt- kjarna frumum úr blóði astmasjúklinga? Hallgerður Lind Kristjánsdóttirl, Ásta Sóllilja Guðmundsdóttir2, Hákon Hákonarson2 og Unnur Steina Björnsdóttir3. 1) Háskóli íslands, 2) Islensk erfðagreining, 3)Landspítali Háskólasjúkrahús Inngangur: Astmi erflókinn bólgusjúkdómur ílungum og tilurð hans er ekki að fullu skilin. Ljóst er að IL-13 á þátt í miðlun sjúkdómsins þar sem sýnt hefur verið fram á að tilvist þess er bæði nauðsynleg og nægjanleg til að valda helstu einkennum astma, svo sem berkjuauðreitni, slímofframleiðslu, auknum fjölda rauðkyrninga (eosínófíla) og aukinni bandvefsmyndun undir þekju öndunarvega. Markmið rannsóknarinnar var að komast nær því hvað stjórnar tjáningu á mRKS fyrir IL-13 og IL-13R( 1 í hnattkjarna frumum úr blóði (peripheral blood mononuclear cells) astmasjúklinga. Efni og aðferðir: Fengið var blóð úr 8 astmasjúklingum, 4 með og 4 án ofnæmi. Hnattkjarna frumur voru einangraðar úr blóðinu og ræktaðar við 30 mismunandi meðferðarskilyrði í 0, 6,12 eða 24 tíma. Flotið var hirt eftir ræktun og magn IL-13 próteinsins mælt með ensímtengdri mótefnamælingu. RKS var einangrað úr frumunum og tjáning á mRKS fyrir IL-13 og IL-13R(1 var mæld með rauntíma-öfugumritunar- keðjumögnun (RT-PCR). Niðurstöður: Örvun með ofnæmisvökum, Lípópólysakkaríði (LPS) og Phytohemagglutíníni (PHA) olli marktækt aukinni örvun á tjáningu á mRKS fyrir IL-13 eftir 6- eða 12 tíma ræktun hjá astmasjúklingum með og án ofnæmis. IL-4 og 9 ollu ekki marktækt aukinni tjáningu á IL-13 mRKS en IL-5 smávægilegri en tölfræðilega marktækri. PHA var eina áreitið sem leiddi til markvissar aukinnar seytunar á IL-13 próteininu. Ekkert af áreitunum eykur marktækt

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