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 LÆKNAblaðið/Fylgirit 91 2017/103 29 P < 0.05). TNFi adherence was shorter in obese patients, the median TNFi duration was 2.5 years (95% CI 1.7, 3.2) in obese vs 5.9 (4.1, 7.7) in non-o- bese patients (P < 0.01). A EULAR good or moderate (EGOM) response was achieved by 55% of obese vs 65% of non-obese patients (P = 0.02). Inmultivariable analyses, obesity increased the risk of TNFi withdrawal [HR 1.6 (95% CI 1.3, 2.0)] and reduced odds for EGOM response [OR 0.47 (95% CI 0.29, 0.72)]. The impact of obesitywas significant across genders and TNFi types. Conclusion: Obesity wasassociated with higher disease activity and seemed to diminish response and adherence to TNFIs in PsA. E 72 Reduced carriage of vaccine type pneumococci in children following vaccination with the 10-valent pneumococcal vaccine Samúel Sigurðsson1, Helga Erlendsdóttir2, Birgir Hrafnkelsson3, Karl G. Kristinsson2, Ásgeir Haraldsson4 1Faculty of Medicine, University of Iceland, 2Department of Clinical Microbiology, Landspitali, University Hospital, 3Department of Mathematics, University of Iceland, 4Children’s Hospital Iceland, Landspitali, University Hospital samuelsigurds@gmail.com Introduction: Vaccination with the 10-valent pneumococcal conjugate vaccine (PCV-10) was initiated in Iceland in 2011 for children born in 2011 and later without catch-up. Aim: To determine the impact of PCV-10 on nasopharyngeal carriage of pneumococci. Methods: An ongoing, repeated cross-sectional study where nasoph- aryngeal swabs were collected in March every year from 2009-2015, from children attending 15 Day Care Centres in the Reykjavik capital area. Isolates were cultured selectively for pneumococci and serotyped with PCR and/or latex agglutination. To attain compatible age distribution, only children < 4 years of age were included and the Non-Vaccine Eligible cohorts (NVEC, born ≤2010) compared with the Vaccine Eligible Cohorts (VEC, born ≥2011). To exclude possible herd effect bias NVECs sampled in 2013 and later were excluded. Results: There were 917 isolates in the VEC and 387 in the NVEC included in this study. The average age was higher in the NVEC than the VEC (2.89 vs 2.80, p=0.02). Nosignificant differences was in carriage (69.5% in both groups) or sex (51.5% vs 53.8% males). Vaccine types represented 51.1% and 4.5% of the pneumococcal isolates for NVEC and VEC respectively. Pooled vaccine efficacy for acquisition of vaccine types for the VEC compared to the NVEC was 94% (95%CI:90-96%). For the vaccine-associ- ated serotypes (6A and 19A) a 33% (95%CI:1%-55%) reduction was found. There was a significant increased prevalence of the non-vaccine serotypes in the VEC. Conclusion: Vaccine serotypes were almost eliminated from carriage following the vaccination. In addition, a reduction of vaccine-associated serotypes (6A,19A) was seen, indicating possible cross-reactivity. E 73 Decreased anti-microbial resistance in healthy children attending Day Care Centres after pneumococcal vaccination in Iceland Samúel Sigurðsson1, Helga Erlendsdóttir2, Birgir Hrafnkelsson3, Karl G. Kristinsson2, Ásgeir Haraldsson4 1Faculty of Medicine, University of Iceland, 2Department of Clinical Microbiology, Landspitali, University Hospital, 3Department of Mathematics, University of Iceland, 4Children’s Hospital Iceland, Landspitali, University Hospital samuelsigurds@gmail.com Introduction: 10-valent pneumococcal conjugate vaccination (PHiD- CV) was initiated in Iceland for children born in 2011 and later, without catchup. Aim: To determine the impact of PHiD-CV on anti-microbial resistance of pneumococcal isolates in children attending Day Care Centres (DCCs). Methods: Cross-sectional carriage studies were conducted every March 2009-2015 and NP swabs collected from children attending DCCs in Reykjavik, for pneumococcal culture, susceptibility testing and serotyp- ing. Resistant and intermediately resistant isolates were defined as non- -susceptible, and multi-resistance as non-susceptibility to >3 antimicrobial classes. To attain comparable age distribution, only children <4 years of age were included; the Non-Vaccine Eligible cohorts (NVEC, born 2010 and earlier) were compared to the Vaccine Eligible Cohorts (VEC, born 2011 and later). To exclude possible herd effect bias NVECs sampled in 2013 and later were excluded. Non-typeable pneumococci were excluded. Results: 870 pneumococcal isolates were included in the NVEC and 365 in the VEC. There were no significant differences in carriage (69.5% vs 70.1%, p=0.8) between the groups. The NVEC group had higher parent reported recent antibiotic usage (p<0.05) and average age (2.89 vs 2.80, p<0.05) than the VEC. The NVEC group excibited higher MIC against Penicillin than the VEC. Non-susceptibility to erythromycin, co-trimoxazole and multi- -resistance declined significantly (NVEC vs. VEC: 13.1% vs. 9.0%, p<0.05, 22.2% vs 12.1%, p<0.001 and 9.3% vs 4.4%, p=0.004, respectively). In NVEC serotype 19F caused 89.0% of multi-resistance, in VEC serotype 15 was the most prevalent. Conclusion: Emerging non-vaccine serotypes exhibit lower anti-microbial resistance, mainly driven by the reduction of serotype 19F. E 74 Cell membrane permeable but not impermeable carbonic anhydrase inhibitors dilate pre-contracted pig retinal arteries Þór Eysteinsson1, Hrönn Guðmundsdóttir1, Arnar Ö. Harðarson1, Fabrizio Carta2, Claudiu Supruran2 1Physiology, University of Iceland, 2 Neurofarba University of Florence thoreys@hi.is Introduction: Carbonic anhydrase inhibitors (CAI’s) are used to lower intraocular pressure in glaucoma. Some have also been found to elevate retinal PO2 and dilate retinal arteries. But the mechanism is unknown. The aim is to identify which carbonic anhydrase isoenzymes are involved in control of vascular wall tension, and whether located intracellularly or on the surface of cell membranes. Selective membrane permeable and impermeable CAI’s were used for this purpose. Materials and methods: Dissected segments of porcine retinal arteries were mounted in a wire myograph for measurement of contractile activity and precontracted with 10-6M U-46619, a prostaglandin analog, added to the organ bath. With the vascular tone stabilized the CAI’s tested were applied separately to the bath, and the effects of each on the tone recorded. Results are presented as mean ± SEM percentage of the max- imum vasodilation, as compared to the prior vasoconstriction induced by 10-6M U-46619. Results: The membrane permeable CAI dorzolamide (10-3M) induced a mean relaxation of 76 ± 8% (p < 0.02) when precontracted with U-46619. Benzolamide, considered a membrane impermeable CAI, induced a dose-dependent, significant mean relaxation of 85 ± 8% (p < 0.01). The pyr- idinium derivative FC5-207A (10-3M), a membrane impermeable CAI, had no effects on vascular wall tension. Three other membrane impermeable CAIs, sulfonamides MB9-512B, MB9-523R9A, and MB9-527R2A, had no significant effects on wall tension.

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