LÆKNABLAÐIÐ 1997; 83 217 Nýr doktor í læknisfræði Þann 22. september 1995 varði Sigurður Kristjánsson doktorsritgerð við Háskólann í Gautaborg. Ritgerðin nefnist Inflammatory mediators and treatment effects in childhood asthma and wheezing bronchitis. Ágrip úr rit- gerðinni fer hér á eftir. Eosinophils have the ability to secrete highly toxic proteins such as eosinophil cationic pro- tein (ECP) and eosinophil protein X (EPX), which may play important roles in airway in- flammation. Eosinophil-derived proteins were measured in urine and serum in children with atopic asthma to clarify if these markers can be used to monitor airway inflammation. The re- sults showed that active atopic asthma was as- sociated with increased levels of urinary EPX and serum ECP. Declining levels of the sub- stances after anti-inflammatory treatment seem to reflect suppression of airway inflam- mation. The leukotrienes (LTs) LTC4 LTD4 and LTE4 are strong bronchoconstrictors, while LTB4 is a chemotactic agent for human granu- locytes. In blood, eosinophils are the main source of LTC4 and neutrophils of LTB4. It has been reported that eosinophils from asthmatic patients produce more LTC4 than eosinophils from healthy controls. The ex vivo release of LTs induced by stimulation of leukocytes in children with atopic asthma was determined to clarify whether changed release is due to changed capacity to release LTs or to changed numbers of LT-producing cells. Increased leu- kotriene levels found after the stimulation of peripheral white blood cells obtained from children with atopic asthma seem to be the result of increased numbers of LT-producing cells rather than being due to increased ability of the individual cell to produce LTs. The inhibitory effect of theophylline, terbu- taline and hydrocortisone, separately and in different combinations, on leukotriene pro- duction of human leukocytes in vitro was ex- amined. It was found that all these drugs inhib- ited LT generation from white blood cells and that combinations of the drugs had additive inhibitory effects. p2-agonists have been claimed to lack bene- ficial effects in young children with acute symptoms of wheezing bronchitis. A combined a- and P- agonist, e.g. racemic adrenaline (RA), could offer an interesting treatment al- ternative. The effect of inhaled nebulised RA on acute symptoms of wheezing bronchitis in infants and toddlers was examined. It was shown that nebulised RA improved oxygena- tion and clinical signs in hospitalised children below the age of 18 months with wheezing bronchitis. The treatment is safe and may be used as an alternative for symptom relief in small children with acute wheezing bronchitis. The possible changes in terms of hospital- isation of children with asthma and wheezing bronchitis were determined at a time period when treatment with inhaled steroids as well as the prevalence of asthma has increased. A de- crease in hospitalisation of children with asth- ma, aged 2-18 years was found to have oc- curred despite the fact that the prevalence of the disease has increased. This is most likely due to increasing use of anti-inflammatory treatment, largely in the form of inhaled ste- roids. The results suggest that this is a very cost-effective therapeutic approach.

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