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Growth hormone responsiveness in children : results from Swedish multicenter clinical trials of growth hormone treatmentLundberg, Elena January 2017 (has links)
The general aims of the thesis were to study GH responsiveness by estimation of pharmacokinetics and bioavailability of injected recombinant human GH (rhGH), of growth response as gain in heightSDS during childhood and puberty, and IGF-I response as change in circulating IGF-ISDS and IGFBP3SDS. Methods Short children were recruited during 1988–1999 into two national randomized multicentre clinical trials on growth until adult height. A group of 117 GHD patients who had been treated from prepuberty with a single GH dose of 33μg/kg/day for at least 1 year were randomized at onset of puberty either to remain on this dose regimen or to an increased dose, GH67μg/kg/day, administered once daily or divided into two doses, GH33x2μg/kg/day. Data on IGF-ISDS and IGF binding protein 3 (IGFBP3)SDS were available from 111 patients and analysed as stated below. The 151 short prepubertal non-GHD patients were randomized into three groups: untreated controls, GH33 or GH67μg/kg/day. A subpopulation from both trials, 128 patients examined annually in Gothenburg, formed the study sample on GH uptake. They received sc GH injections to obtain 16–24 hour GH curves and the GH pharmacokinetics and bioavailability was calculated. Results: A dose-dependent effect on Cmax was found with great intra- and inter-individual variability. Of the Cmax variability, 43% was explained by the rhGH dose and proxies for injection depth. Median bioavailability of the injected dose was 71%, with great variation, mainly dependent on injection depth. In the IGHD group a dose-dependent difference in pubertal gain in heightSDS was found, with mean of 0.8 for the GH67 group and 0.4 for GH33, p<0.01. The mean total gain in heightSDS during treatment was 1.9 for GH67 and 1.4 for GH33, p<0.01. A dose-dependent pubertal ΔIGF-ISDS was 0.5 vs −0.1, p=0.007, correlating to pubertal gain in heightSDS, p=0.003; and was the most important variable to explain the variation in pubertal gain in heightSDS. In the non-GHD group the ΔIGF-ISDS from baseline to mean study level was dose-dependent 2.07 vs 1.20, p=0.001; and correlated negatively with baseline values of IGF-ISDS, rho= -0.56 for GH67, p=0.001, vs rho= -0.82 for GH33, p=0.0001, and correlated positively with gain in heightSDS in both GH-treated groups, rho= 0.42, p<0.001. In multivariable regression analyses, ΔIGF-ISDS was always an important explanatory variable for long-term growth response from the prepubertal period until adult height, while the IGF-ISDS study level per se was not. Conclusion: Growth response to GH treatment was dose dependent with great variability between patients. More pubertal growth was attained by an increased rhGH dose, mimicking the physiology of healthy children, in whom GH secretion rate increases during puberty. This resulted in a gain in IGF-ISDS closely correlating to pubertal gain in heightSDS in both IGHD and non-GHD patients. A broad range in GH responsiveness was found for both growth and IGF response in both diagnostic groups, but lower in the non-GHD group. Higher uptake of a given GH dose was observed after a deep injection and a higher GH concentration. These results are clinically applicable for individuals who remain short close to onset of puberty; by identifying and deeply injecting a rhGH dose that accounts for individual responsiveness, we can stimulate an increment in IGF-ISDS that correlates to gain in heightSDS during puberty.
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Zur Wertigkeit videostroboskopischer und lupenlaryngoskopischer Tonaufnahmen für die objektive Stimmanalyse / The significance of videostroboscopic and magnifying laryngoscopic voice recordings for the objective voice analysisLemm, Leonie 02 July 2013 (has links)
Die objektive Stimmanalyse ist für die tägliche phoniatrische Praxis von grundlegender Bedeutung bezüglich der Diagnostik und Therapie von Stimmstörungen. Als Goldstandard gilt das Göttinger Heiserkeits-Diagramm (GHD), welches die Aufzeichnung von 28 Vokalen durch geschultes Fachpersonal mit einem zeitlichen Aufwand von ca. 15 Minuten pro Patient erfordert. In der vorliegenden Studie wurde untersucht, ob das GHD auch dann valide Ergebnisse für die Stimmqualität liefert, wenn statt des Standardprotokolls gehaltene Phonationen aus indirekter Laryngoskopie oder Videostroboskopie analysiert werden (sog. „reduziertes Protokoll“). Wäre dies der Fall, ließe sich Stimmanalyse und Untersuchung des Larynx in einem Arbeitsschritt durchführen und somit der zeitliche und personelle Aufwand deutlich reduzieren.
Es wurden Stimmaufnahmen aus Stroboskopie und Laryngoskopie von 213 Patienten (97 männlich, 116 weiblich) mit Hilfe des GHD analysiert. Am gleichen Untersuchungstag erfolgte zudem eine typische Mikrophonaufnahme gehaltener Phonationen zur Analyse nach dem vollständigen GHD-Protokoll. Die aus reduziertem und vollständigem Protokoll ermittelten Werte für die Irregularität und die Rauschkomponente des Stimmsignals als objektive Marker der Stimmqualität wurden jeweils korreliert. Sowohl für die Irregularitätskomponente (r=0,65) als auch für die Rauschkomponente (r=0,55) ergaben sich signifikante Korrelationen (p<0,001) zwischen beiden Verfahren. Außerdem zeigte sich, dass bereits eine einzige Stimmgebung aus Laryngoskopie und Stroboskopie ein zuverlässiges Ergebnis liefert. Es konnte eine Mindesttonhaltedauer von 1 Sekunde ermittelt werden. Die Vereinfachung des Vokals während Laryngoskopie beeinflusst das Ergebnis nicht und beide Methoden eignen sich zur klinischen Verlaufskontrolle.
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Funktionelle Ergebnisse nach indirekt laryngoskopischer Abtragung benigner Befunde der Stimmlippen in Oberflächenanästhesie / Results after indirect laryngoscopic surgery of benign tumours in topical anaesthesia.Arand, Katharina 06 April 2011 (has links)
No description available.
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