Fyziologické a patofyziologické aspekty některých vybraných endokrinopatií. Vztah k metabolizmu tukové tkáně a inzulínové rezistenci / Physiologic and pathophysiologic aspects of selected endocrinopathies. Their relationship to adipose tissue matebolism and insulin resistance

Ďurovcová, Viktória

January 2012

The pathogenesis of insulin resistance is a complex and still intensively studied issue. Endocrine and paracrine activity of the adipose tissue together with mi- tochondrial dysfunction are the most discussed potential factors included in the development of insulin resistance. In the first part of our study we examined the involvement of the adipose tissue and its secretory products in the etiopathogenesis of insulin resistance in patients with Cushing's syndrome, acromegaly and simple obesity. We focused on three important regulators of metabolic homeostasis - fibroblast growth factors 21 and 19 (FGF-21 and FGF-19) and adipocyte fatty acid binding protein (FABP-4). We found significantly elevated circulating levels of FGF-21 and FABP-4 ac- companying insulin resistance in both patients with simple obesity and patients with obesity connected to Cushing's syndrome, as compared to healthy controls. The concentrations of both substances were comparable between hypercortisolic and obese patients. This finding together with the absence of correlation be- tween the levels of FGF-21 resp. FABP-4 and cortisol suggest that the reason for elevation of their concentrations is obesity and its metabolic consequences themselves rather then the effect of hypercortisolism on FGF-21 and FABP-4 production. We found no...

Perorální podání acipimoxu během fyzické zátěže způsobuje negativní zpětnovazebný mechanismus růstového hormonu na sekreci ghrelinu u pacientek s mentální bulimií a zdravých žen:Úloha lipolýzy / Acipimox during Short-Term Exercise Exerts A Negative Feedback of Growth Hormone on Ghrelin Secretion in Patients with Bulimia Nervosa and in Healthy Women: The Role of Lipolysis

Smitka, Kvido

January 2011

Title: Acipimox during Short-Term Exercise Exerts A Negative Feedback of Growth Hormone on Ghrelin Secretion in Patients with Bulimia Nervosa and in Healthy Women: The Role of Lipolysis Objective: Eating disorders, such as bulimia nervosa (BN) and anorexia nervosa (AN), are characterized by abnormal eating behavior. The main features of BN are binge-eating and inappropriate compensatory methods to prevent weight gain. The appetite-modulating peptide ghrelin is secreted by the stomach and shows a strong release of growth hormone (GH). A potential GH-ghrelin feedback loop between stomach and the pituitary has been recently reported. Acipimox (Aci), an analogue of nicotinic acid, inhibits lipolysis in adipose tissue (AT) and reduces plasma glycerol and free fatty acids (FFA) levels. Exercise and Aci are stimulators of GH secretion. We suppose that a negative feedback from increased GH levels during exercise may play a role in reducing plasma ghrelin levels. We surmised that altered baseline activity and exercise-induced activation of the sympathetic nervous system (SNS) results in excessive stimulation of lipolysis associated with negative energy balance and may lead to abnormal AT metabolism in patients with BN. Disruption of the gut-brain-AT axis might be involved in the pathogenesis of BN. The...

Hemolysgränser på Immulite 2000 Xpi vid analys avtillväxthormon (GH) och insulinliknande tillväxtfaktor (IGF-1). / Hemolysis limits on Immulite 2000 Xpi when analyzing growth hormone (GH) and insulin like growth factor(IGF-1).

Matroud, Eslam

January 2023

Tillväxthormon och insulinliknande tillväxtfaktor-1 är blodprover som tas vid misstanke om akromegali. Immulite 2000 XPi är ett instrument som använder chemiluminescent microparticle immunoassay metodik för att kvantitativt mäta koncentrationen av GH och IGF-1. Analys av biokemiska markörer påverkas av flera olika faktorer. En viktig sådan faktor är hemolys. Hemolys innebär att de röda blodkropparna går sönder, vilket leder till frisättning av dess innehåll såsom hemoglobin i serum/plasma. Syftet med detta projekt var att undersöka hur hemolys påverkar resultatet av GH- och IGF-1-prover på immulite 2000 XPi. Utifrån erhållna resultat kommer klinisk kemi vid Universitetssjukhuset Örebros laboratorie rutiner vid hemolytiska prover på GH eller IGF-1 att uppdateras . Hemolys tillverkades och tillsattes till olika serumprover med låg och hög nivå av GH respektive IGF-1 för att erhålla prover med varierande grad av hemolys. Resultatet visade att ökande hemolysindex korrelerar med GH- respektive IGF-1-koncentrationer, med undantag för den låga GH koncentrationen som inte uppvisade någon korrelation till hemolysindex. En 10%:ig skillnad av GH och IGF-1- koncentrationer uppnåddes vid en ökning av hemolysindex med 555,40 mg/dL för GH respektive 333,3 mg/dL för IGF-1.Utifrån resultaten var hemolysgränsen likvärdig med tillverkarens gränser. Därför kan klinisk kemi på Universitetssjukhuset Örebro fortsätta med nuvarande hemolysgränser. / Growth hormone and insulin-like growth factor-1 are blood samples taken upon suspicion of acromegaly and for follow-up of acromegaly treatment. Immulite 2000 XPi is an instrument that uses chemiluminescent microparticle immunoassay method to quantitatively measure the concentration of GH and IGF-1. Analysis of biochemical markers is affected by several different factors. An important such factor is hemolysis. Hemolysis means that the red blood cells break, whose contents leak into the serum/plasma. The study aimed to investigate how hemolysis affects the results of GH and IGF-1 samples on the Immulite 2000 XPi. The results will determine the routines for hemolytic samples for GH or IGF-1 at Örebro University Hospital. Hemolysis was produced and added to various serum samples with low and high levels of GH and IGF-1 to obtain samples with varying degrees of hemolysis. The results showed that increasing hemolysis index correlates with GH and IGF-1 concentrations, with the exception of low GH concentration, which did not show any correlation to hemolysis index. A 10% difference in GH and IGF-1 concentrations was achieved with an increase in hemolysis index of 555.40 mg/dL for GH and 333.3 mg/dL for IGF-1. Based on the results, the hemolysis limit was equivalent to the manufacturer's limits. Therefore, clinical chemistry at Örebro University Hospital can continue with current hemolysis limits.

Growth hormone (GH)

Insulin-like growth factor (IGF-1)

hemolysis

Immulite 2000 XPi

Tillväxthormon (GH)

insulin liknande tillväxtfaktor

hemolys

Immulite 2000 XPi

Biomedical Laboratory Science/Technology

Fibroblast Growth Factor 21 Expression in Mice with Altered Growth Hormone Action: Links to Obesity, Type 2 Diabetes Mellitus, and Increased Longevity

Brooks, Nicole E.

10 May 2016

No description available.

Biology

Biomedical Research

Molecular Biology

FGF21

fibroblast growth factor 21

Fgfr1

fibroblast growth factor receptor 1

Klb

beta klotho

GH

growth hormone

FGF21 resistance

AT

adipose tissue

liver

brown adipose tissue

white adipose tissue

Die Anwendung von rekombinantem homologen Wachstumshormon bei der Distraktionsosteogenese / Radiologische, histomorphometrische, biomechanische und serologische Untersuchungen am Minischwein

Bail, Hermann Josef

01 November 2004

An Yucatan Micropig(R) wurde überprüft, ob die systemische Applikation von Wachstumshormon (GH) in der Lage ist, die Regeneratkonsolidierung bei der Distraktionsosteogenese signifikant zu beschleunigen. Es erfolgte die Entwicklung eines speziellen externen Fixateurs (Halbringf.) mit welchem biomechanische in-vivo Messungen durchgeführte werden konnten. Ebenso wurden serologische, sonographische, röntgenologische, computertomographische, histomorphometrische und post mortem biomechanische Untersuchungen entwickelt und durchgeführt. Die Applikation von rekombinantem spezies-spezifischen Wachstumshormon bei der Distraktionsosteogenese zeigte bei dem von uns gewählten Tiermodell eine signifikante Beschleunigung der Regeneratkonsolidierung. Die biomechanischen Messungen ergaben eine mehr als verdoppelte Steifigkeit und Festigkeit der distrahierten Tibiae nach nur 10 Tagen Konsolidierungszeit im Vergleich zur Kontrollgruppe. Die CT erbrachte für die mit GH behandelten Tiere einen signifikant erhöhten Mineralisierungsgrad im Regenerat, zum gleichen Ergebnis kam die digitale Lumineszenzradiographie und die sonographische Vermessung des Regeneratdurchbaus. Somit zeigten alle Meßmethoden eine deutliche Beschleunigung der Regeneratkonsolidierung durch systemisch appliziertes GH. In den serologischen Untersuchungen fand sich eine signifikante Korrelation zwischen dem Serumspiegel der b-ALP und dem des IGF-I. Dies ist ein Hinweis darauf, dass die Wirkung des Wachstumshormons auf das Regenerat durch seinen Mediator IGF-I bedingt ist. / To investigate the effect of systemic growth hormone (GH) application experiments were performed in a micropig animal model. Systemic daily s.c. injection of species-specific recombinant GH was investigated in Yucatan micropigs to evaluate the effect on intramembranous bone formation in distraction osteogenesis. Quantitative computed tomography (qCT), quantitative ultrasound, digital luminescence radiography, biomechanical in-vivo and post mortem testing, serological investigations as well as histomorphometric analyses were performed to investigate differences in regenerate formation. Systemic GH administration significantly increased in the present animal model the torsional stability of the regenerate in-vivo as well as post mortem in comparison to the contralateral side. Also all additional methods showed an accelerated regenerate consolidation in case of GH application. Systemic Insulin-like growth factor -I levels correlated well with the bone specific alkaline phosphatase levels. This may indicate, that the effect of GH on the distraction osteogenesis is IGF-I mediated.

Wachstumshormon

Distraktionsosteogenese

Histomorphometrie

quantitative Computertomographie

Digitale Lumineszenzradiographie

quantitative Sonographie

Biomechanik

distraction osteogenesis

histomorphometry

Growth Hormone

quantitative computertomography

digital luminescence radiography

quantitative ultrasound

biomechanics

610 Medizin und Gesundheit

33 Medizin

ddc:610

Praćenje vrednosti insulinu sličnog faktora rasta tip 1 u serumu i brzine rasta tokom terapije hormonom rasta kod dece / Monitoring the levels of insulin-like growth factor type 1 in serum and the rate of growth velocity during growth hormone therapy in children

Vorgučin Ivana

18 December 2015

<p>Hormon rasta ima ključnu ulogu u mnogim fiziolo&scaron;kim procesima, anabolički efekti, stimulisanje rasta dugih kostiju, regulacija transkripcije gena u ciljnim ćelijama su uglavnom posredovani preko mitogenog polipeptida, insulinu sličan faktor rasta tip 1 (insulin like growth factor 1-IGF-1). Hormon rasta indukuje proizvodnju IGF-1 u jetri, koji reaguje sa receptorima ciljnih organa indukujući rast, odnosno IGF-1 posreduje svim stimulativnim dejstvima hormona rasta na kost, hrskavicu, rast mi&scaron;ić a i na metabolizam masti i ugljenih hidrata. U proceni redovnosti, bezbednosti i efikasnosti terapije hormonom rasta koristi se merenje koncentracije IGF-1 u serumu. Istraživanje je urađeno kao retrospektivno-prospektivna studija, a obuhvatilo je 80 pacijenata na terapiji hormonom rasta koja se kontroli&scaron;u i leče na Odeljenju za endokrinologiju, dijabetes i bolesti metabolizma Instituta za zdravstvenu za&scaron;titu dece i omladine Vojvodine u Novom Sadu. Istraživani uzorak je obuhvatio 80 pacijenata, od kojih 35 dece sa nedostatkom hormona rasta, 24 dece rođene male za gestacionu dob i 21 devojčicu sa Tarnerovim sindromom. Svi ispitanici su praćeni od početka primene hormona rasta i tokom prve dve godine terapije hormonom rasta. U ovom istraživanju su praćeni auksolo&scaron;ki i laboratorijski parametri u cilju ispitivanja odgovora na terapiju hormonom rasta. Praćene su bazalne vrednosti IGF-1 i promene nivoa IGF-1 u serumu tokom terapije hormonom rasta i kori&scaron;ćene da bi se ispitao odgovor na terapiju hormonom rasta, praćenjem brzine rasta, promena skora standardnih devijacija - SSD za telesnu visinu i ko&scaron;tanog sazrevanja. Ciljevi istraživanja su bili da se utvrdi povezanost vrednosti insulinu sličnog faktora rasta tip 1, brzine rasta i ko&scaron;tanog sazrevanja tokom terapije hormonom rasta. Takođe je poređena brzina rasta dece sa deficitom hormona rasta, devojčica sa T arnerovim sindromom i dece rođene male za gestaciono doba na terapiji hormonom rasta. U istraživanom uzorku, dvogodi&scaron;njim praćenjem terapije hormonom rasta je postignut dobar odgovor na terapiju, među decom sa nedostatkom hormona rasta je 71,5% postiglo normalnu telesnu visinu (&plusmn;2 SSDTV) posle dve godine terapije hormonom rasta, 79,2% dece rođene male za gestacionu dob i 42,9% devojčica sa Tarnerovim sindromom. Značajna zastupljenost dece prepubertetskog uzrasta na početku terapije hormonom rasta, među decom sa nedostatkom hormona rasta 77,2%, među decom rođenom malom za gestacionu dob 79,1% i među devojčicama sa Tarnerovim sindromom 90,5% &scaron;to je značajno uticalo na uspe&scaron;nost terapije. Tokom terapije hormonom rasta je utvrđeno povećanje brzine rasta i SSD TV kod sve tri grupe ispitanika. U sve tri grupe ispitanika je tokom terapije hormonom rasta utvrđen porast nivoa IGF-1 seruma i SSDIGF-1 i ubrzanje ko&scaron;tanog sazrevanja tokom terapije hormonom rasta. Za prvih &scaron;est meseci terapije nema statistički značajnih razlika među grupama u brzini rasta (p&gt;0,05), dok je za period prve i druge godine terapije hormonom rasta utvrđeno da postoji statistički značajna razlika među grupama (p&lt;0,05), da je brzina rasta kod devojčica za Tarnerovim sindromom statistički značajno manja i od brzine rasta kod dece sa nedostatkom hormona rasta (p &lt;0,05), i od brzine rasta kod dece rođene male za gestacionu dob (p&lt;0,05). Među decom sa nedostatkom hormona rasta i dece rođene male za gestacionu dob nema statistički značajne razlike u brzini rasta (p&gt;0,5). U ovom istraživanju je praćenjem auskolo&scaron;kih i laboratrijskih parametara tokom dvogodi&scaron;nje primene hormona rasta, konstruisano vi&scaron;e matematičkih modela za predviđanje odgovora na terapiju hormona rasta koji su statistički veoma značajani sa visokim koeficijentom vi&scaron;estruke linearne korelacije. U ovom istraživanju nije dobijena statistički značajna korelacija izmedju nivoa promene IGF-1 i brzine rasta za ceo uzorak, kao ni za decu sa nedostatkom hormona rasta, decu rođenu malu za gestacionu dob i devojčice za Tarnerovim sindromom. Nije dobijena statistički značajna korelacija izmedju nivoa promene IGF-1 i ubrzanja ko&scaron;tanog sazrevanja za ceo uzorak i za tri grupe pacijenata.</p> / <p>Growth hormone plays a key role in many physiological processes. The anabolic effects, the stimulation of growth of the long bones and the regulation of gene transcription in the target cells are mediated mainly via mitogenic polypeptide and insulin-like growth factor type 1 (insulin like growth factor 1-IGF-1). Growth hormone induces the production of IGF-1 in the liver, which interacts with receptors of the target organs inducing growth, that is, IGF-1 mediates all the stimulating effects of growth hormone on bone, cartilage, muscle growth and the metabolism of fats and carbohydrates. In assessing the regularity, safety and efficacy of growth hormone therapy, measuring the concentration of IGF-1 in serum is used. The survey was conducted as a retrospective-prospective study and involved 80 patients treated with growth hormone, monitored and treated at the Department of Endocrinology, Diabetes and Metabolic Diseases, at the Institute for Health Protection of Children and Youth of Vojvodina in Novi Sad. Investigated sample included 80 patients, of whom 35 children have growth hormone deficiency, 24 children were born small for gestational age and 21 girls with Turner syndrome. All the patients were monitored from the beginning of the administration of growth hormone and during the first two years of growth hormone therapy. In this study, auxological and laboratory parameters were monitored for the purpose of examining the response to treatment of growth hormone. The basal values of IGF-1 and changes in IGF-1 levels in serum, along with monitoring the rate of growth velocity and recent changes in standard deviation - SSD for body height and bone maturation, were monitored during growth hormone therapy and used for the evaluation of the response to growth hormone therapy. The objectives of the study were to determine the correlation of insulin-like growth factor type 1 values, the growth velocity and maturation of bone during growth hormone therapy. Also, the growth velocity in children with growth hormone deficiency was compared with the growth velocity in girls with Turner syndrome and in children born small for gestational age while treated with growth hormone. Two-year monitoring of growth hormone therapy in the study sample has show n good response to therapy. 71.5% of children with growth hormone deficiency, 79.2% of children born small for gestational age, and 42.9% of girls with Turner syndrome achieved normal body height (&plusmn; 2 SSDTV) after two years of growth hormone therapy. There was a significant share of children at prepubertal age at the beginning of growth hormone therapy: 77.2% of children with growth hormone deficiency, 79.1% of children born small for gestational age and 90.5% of girls with Turner syndrome, which significantly influenced the success of the therapy. During the growth hormone therapy there was an increase of growth velocity and SSD TV in all three groups of children. An increase in levels of IGF-1 serum and SSDIGF-1 and acceleration of bone maturation were determined in all three groups of patients during growth hormone therapy. For the first six months of therapy there was no statistically significant difference between groups in growth velocity (p&gt; 0.05), while the period of the first and second year of growth hormone therapy showed a statistically significant difference between groups (p &lt;0.05). The growth velocity in girls with Turner syndrome was significantly lower than the growth velocity in children with growth hormone deficiency (p &lt;0.05) and in children born small for gestational age (p &lt;0.05). Between children with growth hormone deficiency and children born small for gestational age there was no statistically significant difference in growth velocity (p&gt; 0.5). By monitoring auxological and laboratory parameters during the two years of application of growth hormone, several highly statistically significant mathematical models for predicting the response to treatment of growth hormone were constructed in this study with a high coefficient of multiple linear correlation. In this study, there was no statistically significant correlation between the level of change in IGF-1 and growth velocity for the entire sample, as well as for children with growth hormone deficiency, children born small for gestational age and girls for Turner syndrome. There was no statistically significant correlation between the level of change in IGF-1 and acceleration of bone maturation for the entire sample and for the three groups of patients.</p>

Le récepteur CD36 : implication dans le développement de l'athérosclérose et dans le recrutement des leucocytes aux sites inflammatoires

Harb, Diala

01 1900

Le CD36 est un récepteur éboueur de classe B exprimé par plusieurs types cellulaires dont les macrophages et les cellules endothéliales de la microvasculature. Le CD36 présente une haute affinité de liaison pour les ligands lipidiques tels que les lipoprotéines oxydées de basse densité (LDLox). De part sa capacité à internaliser les LDLox au niveau des macrophages et de son implication dans la formation des cellules spumeuses, le CD36 joue un rôle critique dans le développement des lésions athérosclérotiques. Nous avons testé l'hypothèse selon laquelle le EP 80317, un ligand synthétique sélectif du CD36, exerce des effets anti-athérosclérotiques chez les souris déficientes en apolipoprotéine E. Un traitement prolongé (12 semaines) avec le EP 80317 réduit fortement (de 51%) la surface des lésions athérosclérotiques par comparaison aux souris témoins. L'effet anti-athérosclérotique est associé à une diminution des taux de cholestérol plasmatique, à une réduction de l’internalisation des LDLox au niveau des macrophages et à une augmentation de l’expression des protéines impliquées dans le transport inverse du cholestérol. De plus, un traitement par le EP 80317 est également associé une diminution de l’expression aortique et plasmatique de protéines pro-inflammatoires. Nos études ont aussi montré un rôle pour le CD36 dans le recrutement des phagocytes mononucléés au niveau des lésions athérosclérotiques, tel que démontré par une réduction de l’accumulation des phagocytes mononucléés radiomarqués CD36–/– par rapport aux cellules CD36+/+. À l’échelle moléculaire, nous avons montré que les phospholipides oxydés induisent la phosphorylation de la kinase Pyk2 des podosomes des monocytes/macrophages de manière dépendante de l’expression du CD36 et de Src. Cette phosphorylation est atténuée par un traitement par le EP80317. Nos résultats appuient le rôle important du CD36 dans l’athérosclérose et suggèrent que les ligands synthétiques qui modulent la fonction du CD36 représentent potentiellement une nouvelle classe d'agents anti-athérosclérotiques. Le CD36 exprimé par les cellules endothéliales de la microvasculature est un récepteur de l’hétérodimère protéique S100A8/A9. Ces protéines s’associent à l’acide arachidonique intracellulaire (AA) des neutrophiles polymorphonucléaires (PMN) et le complexe S100A8/A9/AA peut être sécrété par les PMN activés au contact de l’endothélium. Nous avons vérifié l’hypothèse selon laquelle le CD36 exprimé par la microvasculature est impliqué dans le métabolisme transcellulaire de l’AA par la liaison du complexe S100A8/A9/AA et la réponse inflammatoire. Chez deux modèles murins d'inflammation aiguë (ischémie/reperfusion des membres inférieurs et poche d’air dorsale), nous avons observé que la réponse inflammatoire, notamment l’accumulation des PMN au niveau des sites inflammatoires, est diminuée en moyenne de 63% chez les souris CD36-/-. De même, un traitement par le EP 80317 ou par les anticorps anti-S100A8/A9 diminue chacun de 60% en moyenne l’extravasation des PMN vers les tissus inflammatoires. L’administration simultanée des deux traitements n’a aucun effet supplémentaire, et ces traitements n’exercent aucun effet chez les souris CD36-/-. Nos résultats appuient le rôle du récepteur CD36 de la microvasculature dans la régulation de la réponse inflammatoire. L’utilisation des ligands synthétiques du CD36 pourrait représenter une nouvelle avenue thérapeutique dans le traitement des réponses inflammatoires aiguës. / CD36 is a class B scavenger receptor expressed by multiple cell types such as macrophages and microvascular endothelial cells. CD36 shows a high affinity binding towards lipid-based ligands such as oxidized low-density lipoproteins (oxLDL). Macrophage CD36 has been shown to play a critical role in the development of atherosclerotic lesions by its ability to internalize oxLDL and to lead to foam cell formation. We tested the hypothesis that EP 80317, a selective CD36 ligand, exerts anti-atherosclerotic effects in apolipoprotein E-deficient (apoE–/–) mice fed on atherogenic diet. Long term treatment (12 weeks) with EP 80317 results in a striking reduction (51%) of lesion areas in EP 80317-treated apoE–/– mice. This effect was associated with a decrease in plasma cholesterol, a reduced oxLDL internalization within macrophages and an up-regulation of proteins involved in cholesterol efflux. Additionally, treatment with EP 80317 was associated with a reduced expression of vascular and plasma pro-inflammatory proteins. Our studies also showed a role of CD36 in modulating the recruitment of mononuclear phagocytes to the arterial wall, as shown by a reduced migration of radiolabeled CD36-/- macrophages into atherosclerotic lesions compared to CD36+/+ cells. At the molecular level, our studies showed that oxidized phospholipids induced the phosphorylation of the adhesion kinase Pyk2 in monocytes/macrophages, in a CD36- and Src-dependent manner. The Pyk2 phosphorylation is attenuated by treatment with EP80317. Our results strongly support the role of CD36 in atherosclerosis development and suggest that synthetic ligands featuring modulatory effect on CD36 function may represent a novel class of anti-atherosclerotic agents. CD36 expressed by microvascular endothelial cells is a receptor for the heterodimer S100A8/A9. These proteins bind intracellular arachidonic acid (AA) within polymorphonuclear neutrophils (PMN) and the complex S100A8/A9-AA may be secreted at sites of inflammation where it exerts chemotactic activities. We aimed to delineate the role of microvascular CD36, as a receptor for the S100A8/A9, in the AA transcellular metabolism and the regulation of the associated PMN trafficking to inflammatory sites. In two mouse models of acute inflammation (hind limb ischemia/reperfusion and dorsal air pouch), CD36 regulated trafficking of PMN to inflammatory sites, as shown by a mean of 63% reduction of PMN accumulation in CD36-/- mice. Treatment with EP 80317 or with S100A8/A9 antibodies reduced, each by ~ 60%, the recruitment of PMN to inflammatory sites. The combined administration of anti-S100A8/A9 and EP 80317 did not exert any additional inhibitory effect and neither treatment featured a modulatory effect in CD36-/- mice. Our results strongly support a role for microvascular CD36 in regulating PMN trafficking to inflammatory sites. Targeting CD36 might represent a novel therapeutic avenue for the treatment of acute inflammatory responses.

CD36

athérosclérose

lipoprotéine oxydée de basse densité

macrophage

migration des phagocytes mononucléés

inflammation vasculaire

S100A8/A9

neutrophiles polymorphonucléés

ischémie/reperfusion

CD36

atherosclerosis

growth hormone-releasing peptides

oxidized low density lipoproteins

macrophage

mononuclear phagocyte trafficking

vascular inflammation

S100A8/A9

ploymorphonuclear neutrophils

ischemia/reperfusion

Gesundheitsbezogene Lebensqualität von kleinwüchsigen Kindern und Jugendlichen aus elterlicher Perspektive-Ergebnisse einer quantitativen und qualitativen Analyse / Health-Related Quality of Life of Children and Adolescents with Short Stature from a Parental Perspective-Findings from a Qualitative and Quantitative Analysis

Stohrer, Jasmin

10 August 2016

Die Erfassung der gesundheitsbezogenen Lebensqualität speziell von kleinwüchsigen Kindern und Jugendlichen gewinnt im medizinischen und psychologischen Bereich an Bedeutung. Neben dem Selbstbericht der betroffenen Kinder stellt die elterliche Perspektive zur gesundheitsbezogenen Lebensqualität eine zusätzliche Informationsquelle dar. In der vorliegenden Arbeit wurde quantitativ und qualitativ die gesundheitsbezogene Lebensqualität von kleinwüchsigen Kindern und Jugendlichen mit Wachstumshormonmangel (GHD) und idiopathischem Kleinwuchs (ISS) aus elterlicher Perspektive (n = 33) untersucht. Grundlage der quantitativen Untersuchung war die Erhebung der gesundheitsbezogenen Lebensqualität mithilfe des KIDSCREEN-52-Fragebogens aus Elternperspektive. Dieser Datensatz wurde mit den Normdaten des KIDSCREEN-52-Fragebogens deutscher Eltern normalwüchsiger Kinder (N ~ 1683) verglichen. Zusätzlich wurden Gruppenunterschiede (Geschlechter-, Alters- und Diagnosegruppen sowie der Behandlungsstatus) innerhalb der Stichprobe überprüft. Es wurden inferenzstatistische Auswertungsverfahren verwendet. Zudem wurden Eltern über die gesundheitsbezogene Lebensqualität ihrer kleinwüchsigen Kinder im Rahmen von strukturierten Fokusgruppeninterviews in Deutschland befragt. Diese Daten wurden qualitativ mithilfe der Software MaxQDA (MaxQDA 10/11, VERBI Software) ausgewertet. Die Ergebnisse der quantitativen Analyse zeigen signifikante Unterschiede zu normalgroßen Kindern in den Bereichen „Selbstwahrnehmung“, „Selbstständigkeit“ und „Soziale Akzeptanz“. Im Bereich „Schule“ schätzten Eltern mit kleinwüchsigen Söhnen die gesundheitsbezogene Lebensqualität schlechter ein als befragte Eltern mit kleinwüchsigen Töchtern. Die qualitative Auswertung zeigt, dass in bestimmten Lebensbereichen kleinwüchsiger Kinder Einschränkungen vorliegen. Neben physischen Defiziten wurden von emotionalen Problemen und sozialen Schwierigkeiten berichtet. Bewältigungsstrategien wurden positiv beschrieben. Insgesamt wurden nur geringfügige Gruppenunterschiede gefunden. In der Kategorie „Auswirkungen auf die Eltern und Zukunftsgedanken der Eltern“ zeigten sich Einschränkungen in der gesundheitsbezogenen Lebensqualität der Eltern. Zudem wurde die Unterstützung durch die Eltern als bedeutsam für die gesundheitsbezogene Lebensqualität ihrer kleinwüchsigen Kinder identifiziert.

610

Gesundheitsbezogene Lebensqualität

Kinder und Jugendliche

kleinwüchsige Kinder und Jugendliche

Wachstumshormonmangel

idiopathischer Kleinwuchs

Elternperspektive

Health-Related Quality of Life

Children and Adolescents

Growth hormone deficiency

Idiopathic short stature

parental perspective

Avaliação do padrão de crescimento na síndrome de Noonan em pacientes com mutações identificadas nos genes PTPN11, SOS1, RAF1 e KRAS / Growth pattern of patients with Noonan syndrome with identified mutations in PTPN11, SOS1, RAF1 e KRAS genes

Ribeiro, Alexsandra Christianne Malaquias de Moura

30 May 2011

A Síndrome de Noonan (SN) é caracterizada por baixa estatura proporcionada de início pós-natal, dismorfismos faciais, cardiopatia congênita e deformidade torácica. A frequência da SN é estimada entre 1:1000 e 1:2500 nascidos vivos, com distribuição semelhante em ambos os sexos. A herança é autossômica dominante com penetrância completa, porém a maioria dos casos é esporádica. Até o momento, mutações em genes da via RAS-MAPK (PTPN11, KRAS, SOS1, RAF1, MEK1, NRAS e SHOC2) foram identificadas em aproximadamente 70% dos pacientes. Uma das principais características fenotípicas da SN é a baixa estatura pós-natal, embora o mecanismo fisiopatológico do déficit de crescimento nesta síndrome ainda não esteja totalmente esclarecido. Estudos que avaliaram o padrão de crescimento linear em crianças com SN foram realizados anteriormente ao conhecimento do diagnóstico molecular dessa síndrome. No presente estudo, avaliamos a frequência de mutação nos genes PTPN11, SOS1, RAF1 e KRAS em 152 pacientes com SN e o padrão de crescimento linear (altura) e ponderal [índice de massa corpórea (IMC)] dos pacientes com mutação identificada. No total, mutações nos genes relacionados foram encontradas em 99 pacientes (65%) do nosso estudo, com predominância do gene PTPN11 (47%), seguido do SOS1 (9%), RAF1 (7%) e KRAS (3%). Foram construídas curvas específicas para SN de Altura e IMC para idade e sexo utilizando o método LMS. Os pacientes com SN apresentaram crescimento pré-natal preservado, porém o comprometimento do crescimento pós-natal foi observado desde o primeiro ano de vida, atingindo uma altura final de -2,5 e -2,2 desvios-padrão da média para população brasileira em homens e mulheres, respectivamente. O prejuízo da altura foi maior nos pacientes com mutação no gene RAF1 em comparação com os genes PTPN11 e SOS1. O IMC dos pacientes com SN apresentou queda de 1 desvio-padrão em relação à média da população brasileira normal. O comprometimento do IMC foi menor nos pacientes carreadores de mutação no RAF1. Pacientes com mutação nos genes PTPN11 e SOS1 apresentaram maior frequência de estenose de valva pulmonar, enquanto a miocardiopatia hipertrófica foi mais frequente nos pacientes com mutação no gene RAF1. A variabilidade fenotípica observada nos pacientes com mutação no PTPN11 não pode ser explicada pelo grau que estas mutações influenciam a atividade tirosina fosfatase da SHP-2 nem pela presença de polimorfismos no gene KRAS. Com a análise dos éxons 3, 8 e 13 do PTPN11, seguido dos éxons 6 e 10 do SOS1 e éxon 7 do RAF1 identificamos 86% dos pacientes carreadores de mutações nos genes relacionados, propondo uma forma mais eficiente de avaliação molecular na SN. Acreditamos que a variabilidade fenotípica presente nessa síndrome esteja diretamente ligada aos diferentes papéis exercidos pelas proteínas que participam da via RAS/MAPK. Entretanto, mais estudos em relação à via RAS/MAPK serão necessários para esclarecer as questões relacionadas ao crescimento e outras características fenotípicas da SN / Noonan Syndrome (NS) is characterized by distinctive facial features, short stature and congenital heart defects. The estimated prevalence is 1:1000 to 1:2500 live births, affecting equally both sexes. It is an autosomal dominant disorder with complete penetrance, but most cases are sporadic. To date, mutations in the RAS/MAPK pathway genes (PTPN11, KRAS, SOS1, RAF1, MEK1, NRAS and SHOC2) were identified in approximately 70% of patients. One of the cardinal signs of NS is proportional postnatal short stature although the physiopathological mechanism of growth impairment remains unclear. The current knowledge about the natural history of growth associated with NS was described before molecular diagnosis era. In this study, we performed PTPN11, SOS1, RAF1, and KRAS mutation analysis in a cohort of 152 NS patients and studied the natural linear (height) and ponderal growth [body mass index (BMI)] of NS patients with related mutations. Mutations in NS-causative genes were found in 99 patients (65%) of our cohort. The most common mutated gene was PTPN11 (47%), followed by SOS1 (9%), RAF1 (7%) and KRAS (3%). Sex-specific percentile curves for height and BMI were constructed using the LMS method. NS patients had birth weight and length within normal ranges but the postnatal growth impairment was observed during the first year of life, reaching a final height of -2.3 and -2.2 standard deviations from the mean for Brazilian healthy men and women, respectively. Postnatal growth impairment was higher in RAF1 mutation patients than in patients with SOS1 and PTPN11 mutations. BMI values in NS patients were lower in comparison with normal Brazilian population. BMI values were higher in patients with RAF1 mutations than in patients with other genotypes. Patients with mutations in PTPN11 and SOS1 genes were more likely to have pulmonary valve stenosis, whereas hypertrophic cardiomyopathy was more common in patients with mutations in the gene RAF1. The intensity of constitutive tyrosine phosphatase activity of SHP-2 due to PTPN11 mutations, as well as the presence of polymorphisms in KRAS gene did not influence the phenotype of NS patients with mutation in PTPN11 gene. Analysis of exons 3, 8 and 13 of PTPN11 gene, followed by exons 6 and 10 of SOS1 gene and exon 7of RAF1 gene identified 86% of patients harboring mutations in related genes, suggesting a more efficient evaluation of NS molecular diagnosis. We believe that the phenotypic variability in this syndrome is directly linked to the different roles played by proteins that participate in RAS/MAPK pathway. However, further studies in RAS/MAPK pathway are needed to clarify issues related to growth and other phenotypic characteristics of SN

Body mass index

Crescimento/genética

Gráficos de crescimento

Growth

Growth charts

Growth disorders

Growth hormone

Hormônio do crescimento/análise

Insulin-like growth factor I

MAP quinase quinase quinases/genética

Mitogen-activated protein kinase 1

Noonan syndrome

Proteínas son of sevenless/genética

Síndrome de Noonan/diagnóstico

Síndrome de Noonan/etiologia

Síndrome de Noonan/genética

Somatomedinas/análise

Son of sevenless homolog 1

Transtornos do crescimento/genética

Polimorfismos dos genes dos receptores de dopamina D2 e de somatostatina subtipos 2 e 5 e resposta ao tratamento medicamentoso de pacientes portadores de adenomas hipofisários / The influence of dopamine receptor type 2 and somatostatin receptors type 2 and 5 polymorphisms in medical treatment of pituitary adenomas

Bueno, Cristina Bellotti Formiga

04 November 2016

Os adenomas hipofisários podem ser tratados clinicamente com agonistas dopaminérgicos (AD) e/ou ligantes dos receptores de somatostatina (LRS). Alguns estudos apontam para o papel de polimorfismos dos genes DRD2, SSTR2 e SSTR5 na eficácia desses tratamentos clínicos. O objetivo do estudo foi avaliar o papel dos polimorfismos no gene DRD2 em pacientes com prolactinomas (n=118), corticotrofinomas (n=15), adenomas clinicamente não funcionantes (ACNF) (n=35) e somatotrofinomas (n=40), bem como de polimorfismos nos genes SSTR2 e SSTR5 em pacientes com somatotrofinomas (n=88), na resposta ao tratamento clínico com AD e LRS. Adicionalmente, comparar a frequência desses polimorfismos em pacientes portadores de adenomas hipofisários, de diferentes naturezas, a indivíduos saudáveis. Os polimorfismos foram genotipados por PCR em tempo real (sistema TaqMan) e seqüenciamento automático (método Sanger). Todos os genótipos estavam em equilíbrio de Hardy-Weinberg. Em nosso estudo, não houve correlação entre os polimorfismos de DRD2, SSTR2 e SSTR5 e a resposta ao tratamento clínico, com cabergolina (CAB) e/ou octreotida-LAR (OCT-LAR) respectivamente, em pacientes com prolactinomas, somatotrofinomas e corticotrofinomas. Nossos dados estão de acordo com estudos prévios em acromegálicos, no entanto não confirmaram associação de polimorfismo de DRD2 (rs6275) com resistência à CAB, anteriormente descrita em prolactinomas. Adicionalmente, os polimorfismos rs1800497 (alelo T) e rs1076560 (alelo A) de DRD2 foram correlacionados a macroadenomas, este último fator preditivo de resistência à CAB em prolactinomas. Quanto aos ACNF, nossos dados são inéditos e o polimorfismo rs6275 (alelo T) de DRD2 se correlacionou à progressão tumoral nos casos tratados com CAB. Comparando os adenomas hipofisários com indivíduos saudáveis, a presença do alelo raro A de rs1079597 de DRD2 foi inversamente associada à frequência de ACNF, enquanto que nos outros tipos tumorais não houve diferença. Em conclusão, os polimorfismos rs1079597 e rs6275 de DRD2 podem estar associados à tumorigênese e à resposta a CAB, no grupo ACNF respectivamente. Outros estudos ainda são necessários para definir o papel das variantes genéticas desses genes como um mecanismo envolvido na resistência aos AD e LRS e na tumorigênese hipofisária / Medical treatment of pituitary adenomas is mainly performed with dopamine agonist (DA) and/or somatostatin ligant receptor (SLR) drugs. In addition to dopamine receptor 2 (DRD2) and somatostatin receptors 2 and 5 (SSTR2 and SSTR5) tumor density, results of some studies pointed to the role of polymorphisms in the efficacy of clinical treatment. One of the goals of this study was to evaluate the association between DRD2 polymorphisms in patients with prolactinomas (n=118), corticotrophinomas (n=15), clinically nonfunctioning pituitary adenomas (CNFPA) (n=35) and somatotrophinoma (n=101) and polymorphisms in STTR2 and SSTR5, only in the last group; and response to treatment with DA and/or SLR. Another objective was to evaluate the frequency of polymorphisms in patients with different types of pituitary adenomas and compare them to healthy subjects. Polymorphisms were genotyped by real-time PCR (TaqMan system) and Sanger sequencing. All genotypes were in Hardy-Weinberg equilibrium. In patients with prolactinomas, somatotrophinomas and corticotrophinomas there was no association between genetic variants in DRD2 and response to treatment, like data in literature. However, an association between rs6275 (allele T) in DRD2 and CAB resistance in prolactinomas has been proposed. In addition, there was an association betweenrs1800497 (allele T) and rs1076560 (alelle A) in DRD2 and macroprolactinomas, this one predictive factor related to CAB resistance. The presence of rs6275 (allele T) in DRD2 was correlated with tumoral progression in CNFPA treated with CAB, never published previously. Comparing pituitary adenomas and health subjects, the presence of rs1079597 (allele A) was inversely associated with the frequency of CNFPA, otherwise there was no association for others pituitary adenomas. In conclusion, rs1079597 and rs6275 DRD2 polymorphisms might have an influence in tumorigenesis and CAB efficacy in patients with CNFPA, respectively. However, the results in the literature are conflicting and more studies are necessary to determine the role of these genetic variants like a mechanism involving in dopamine and somatostatin resistance and pituitary tumorigenesis

Acromegalia

Acromegaly

ACTH-secreting pituitary adenoma

Adenoma hipofisário secretor de ACTH

Agonistas de dopamina

Dopamine agonists

Neoplasias hipofisárias

Pituitary neoplasms

Polimorfismo genético

Polymorphism genetic

Prolactinoma

Prolactinoma

Receptores de dopamina D2

Receptores de somatostatina

Receptors dopamine D2

Somatostatin receptor