Elucidating mechanisms of premature ovarian failure using a transgenic mouse model

Kaune Galaz, Heidy

January 2015

No description available.

618.1

The role of the transcription factor GATA3 in calcium homeostasis and tumourigenesis

Gaynor, Katherine Ursula

January 2011

No description available.

572

Studies of epigenetic deregulation in parathyroid tumors and small intestinal neuroendocrine tumors

Barazeghi, Elham

January 2017

Deregulation of the epigenome is associated with the initiation and progression of various types of human cancers. Here we investigated the level of 5-hydroxymethylcytosine (5hmC), expression and function of TET1 and TET2, and DNA methylation in parathyroid tumors and small intestinal neuroendocrine tumors (SI-NETs). In Paper I, an undetectable/very low level of 5hmC in parathyroid carcinomas (PCs) compared to parathyroid adenomas with positive staining, suggested that 5hmC may represent a novel biomarker for parathyroid malignancy. Immunohistochemistry revealed that increased tumor weight in adenomas was associated with a more aberrant staining pattern of 5hmC and TET1. A growth regulatory role of TET1 was demonstrated in parathyroid tumor cells. Paper II revealed that the expression of TET2 was also deregulated in PCs, and promoter hypermethylation was detected in PCs when compared to normal parathyroid tissues. 5-aza-2′-deoxycytidine treatment of a primary PC cell culture induced TET2 expression and further supported involvement of promoter hypermethylation in TET2 gene repression. TET2 knockout demonstrated a role for TET2 in cell growth and migration, and as a candidate tumor suppressor gene. In Paper III, variable levels of 5hmC, and aberrant expression of TET1 and TET2 were observed in SI-NETs. We demonstrated a growth regulatory role for TET1, and cytoplasmic expression with absent nuclear localization for TET2 in SI-NETs. In vitro experiments supported the involvement of exportin-1 in TET2 mislocalization, and suggested that KPT-330/selinexor, an orally bioavailable selective inhibitor of exportin-1 and nuclear export, with anti-cancer effects, could be further investigated as a therapeutic option in patients with SI-NETs. In Paper IV, DNA methylation was compared between SI-NET primary tumors and metastases by reduced representation bisulfite sequencing. Three differentially methylated regions (DMR) on chromosome 18 were detected and chosen for further analyses. The PTPRM gene, at 18p11, displayed low expression in SI-NETs with high levels of methylation in the presumed CpG island shores, and in the DMR rather than the promoter region or exon 1/intron 1 boundary. PTPRM overexpression resulted in inhibition of cell growth, proliferation, and induction of apoptosis in SI-NET cells, suggesting a role for PTPRM as an epigenetically deregulated candidate tumor suppressor gene in SI-NETs.

Epigenetics

5hmC

TET1

TET2

parathyroid tumors

SI-NET

RRBS

PTPRM

Cancer and Oncology

Cancer och onkologi

Endocrinology and Diabetes

Endokrinologi och diabetes

Nouvelles molécules thérapeutiques en développement pour les tumeurs neuroendocrines d'origine gastroentéropencréatiques et hypophysaires : preuves de concept in vitro / New therapy in gastroenteropancreatic neuroendocrine cells and pituitary adenomas : Proof of concept in vitro

Mohamed, Amerh Amira

05 November 2013

Les GEPNETs (tumeurs neuroendocrines gastroentéropancréatiques), représentent le deuxième cancer digestif. L’octréotide (agoniste Sst2) contrôle efficacement leurs sécrétions et plus modérément la croissance cellulaire. Au cours de ma première partie de thèse, j’ai développé la culture primaire de GEPNETs humaines. Ceci m’a permis d’étudier l’effet antiprolifératif et antisécretoire du pasireotide (pan agoniste Sst) et de l’évérolimus (inhibiteur de la voie pi3 kinase Akt) en comparaison avec l’octréotide. J’ai mis en évidence un effet inhibiteur significatif et similaire de l’octréotide et du pasiréotide sur la viabilité cellulaire et la sécrétion de chromogranine A. Cependant, le trafic intracellulaire du Sst2 est diffèrent en présence de pasireotide. L’évérolimus inhibe la viabilité et la secretion cellulaire des GEPNETs de manière similaire aux SSA. Nous n’avons pas retrouvé d’additivité entre l’évérolimus et les SSA. Dans la deuxième partie de mon travail j'ai étudié l’effet de la surexpression du Sst2 dans les cellules de prolactinomes et NFPA humains. Apres surexpression de Sst2, l’octréotide est capable d’inhiber la sécrétion de PRL et la prolifération cellulaire des NFPAs. Cette surexpression n’améliore pas la sensibilité aux dopastatines (agonistes chimériques Sst2-D2DR) des prolactinomes alors qu’une amélioration est bien observée dans les NFPAs. En conclusion, la culture primaire des GEPNETs représente un bon modèle d’étude pharmacologique. La coopération Sst2–D2DR dans les NFPA est effective dans ce modèle et permettra l’étude des mécanismes mises en jeu par les dopastatines. / GEPNETs represent, in terms of prevalence, the second digestive cancer. Octreotide (Sst2 agonists) effectively control their secretion and partially cell growth. we developed a primary cell culture of human GEPNETs. Cell culture allowed the study of antisecretory and antiproliferative effect of pasireotide and everolimus, alone or in combination, as compared to octreotide, in 20 tumors. We highlighted a significant and similar maximal inhibitory effect of octreotide and Pasireotide either on cell viability or on chromogranin A secretion in all analyzed tumors. However, the intracellular trafficking of Sst2 was strikely different in the presence of pasireotide and octreotide. In all analyzed tumors, everolimus inhibits cell viability and secretion of GEPNETs similarly to SSA. We couldn’t reveal any additivity between everolimus and SSA in cell viability suppression.My second goal was to study the effect of overexpression of Sst2 by adenoviral transfer in cells of human prolactinomas and NFPA. In both cell types. Nevertheless, octreotide efficiently suppressed PRL secretion and cell proliferation (NFPA). Overexpression of Sst2 did not improve the efficcacy of dopastatines (chimeric Sst2 - D2DR agonists) on prolactin secretion in prolactinomas, but clealy improved suppression of cell proliferation in NFPA. These results suggest that dopostatin promotes a Sst2 D2DR cooperation in NFPA, but not in prolactinomas, where DRDR activation remains dominant. In conclusion, GEPNETs primary cell culture represents a good model for pharmacological In pituitary adenomas, Sst2 overexpression opens an interesting perspective for gene therapy in recurrent NFPA after surgery.

Endocrinologie

Tumeurs neuroendocrine

Adenomes hypophysaires

Recepteur à la somatostatine

Pasireotide

Everolimus,

Endocrinology

Pituitary adenomas

Neuroendocrine tumors

Somatostatin receptor

Pasireotide

Everolimus

IFNγ Mediated Monocyte Metabolic Reprogramming

McCann, Katelyn J.

21 July 2021

IFNγ is an essential and pleiotropic activator of monocytes, but little is known about the effects IFNγ on cellular metabolism. Therefore, we sought to characterize and elucidate the mechanisms by which IFNγ reprograms monocyte metabolism to support its immunologic activities. First, we identified a critical role for IFNγ in the induction of immunoresponsive gene 1 (IRG1) and its product, itaconate. The immunometabolite, itaconate, has been reported to have antibacterial, anti-inflammatory and antioxidant activity. Irg1-/- mice, lacking itaconate, are highly susceptible and phenotypically similar to IFNγ knock out (GKO) mice upon infection with Mycobacterium tuberculosis. Therefore, we assessed the role of IRG1/itaconate in the context of non-tuberculous mycobacterial (NTM) infection, the most common type of infection in patients with immunodeficiencies caused by defects in IFNγ signaling. Our data suggest that impaired induction of itaconate in the context of mycobacterial infection may contribute to mycobacterial susceptibility and immune dysregulation in patients with defects in IFNγ signaling. Next, we evaluated the metabolic phenotype of IFNγ-stimulated human monocytes and found that IFNγ increased oxygen consumption rates (OCR), indicative of reactive oxygen species generation by both mitochondria and NADPH oxidase. Transcriptional profiling of human macrophages revealed that this oxidative phenotype was dependent on IFNγ-induced, nicotinamide phosphoribosyltransferase (NAMPT)-mediated NAD+ salvage to generate NADH and NADPH for oxidation by mitochondrial complex I and NADPH oxidase, respectively. These data identify an IFNγ-induced, NAMPT-dependent, NAD+ salvage pathway that is critical for complete induction of the respiratory burst in IFNγ stimulated human monocytes.

innate immunity

macrophage metabolism

immunometabolism

interferon gamma

mycobacteria

primary immunodeficiency

Allergy and Immunology

Endocrinology, Diabetes, and Metabolism

Immunology and Infectious Disease

Infectious Disease

Use of Hair Cortisol Analysis to Evaluate the Influence of Housing Systems on Long-Term Stress in Horses

Werner, Jade Elizabeth

January 2020

No description available.

Animal Sciences

Animals

Agriculture

Endocrinology

Welfare

Horses

Cortisol

Hair Cortisol

Stress

Horse Management Systems

Novel Object Test

Krüppel-Like Factor 15 Orchestrates Systemic Metabolic Homeostasis

Fan, Liyan

01 September 2021

No description available.

Pathology

Cellular Biology

Endocrinology

Molecular Biology

metabolism

skeletal muscle

lipid

nutrition

metabolic homeostasis

transcription

obesity

metabolic disease

Radiojodbehandling vid Graves sjukdom: långvarig effekt och påverkan på livskvalitet / Radioiodine therapy for Graves´ disease: long-term effects and impact on quality of life

Vareman, Klara

January 2021

Bakgrund: Graves sjukdom är den vanligaste formen av hypertyreos med en incidens på 20 fall per 100 000 individer och år. Graves sjukdom är ett autoimmunt tillstånd där autoantikroppar riktade mot tyreoideastimulerande hormonreceptorer (TSH-R) orsakar okontrollerad syntes och sekretion av tyreoideahormonerna trijodtyronin (T3) och tyroxin (T4). Hur tillståndet uppkommer är inte fullständigt förstått, riskfaktorer inkluderar dock rökning, kvinnligt kön och emotionell stress. Det finns i dagsläget tre etablerade behandlingsmetoder vid Graves sjukdom, dessa är tyreostatikabehandling, radiojodbehandling och tyreoidektomi. Behandling med tyreostatika pågår i regel i 12-18 månader, efter avslutad behandling är risken för recidiv mellan 50-60%. Både tyreoidektomi och radiojodbehandling är definitiva behandlingsmetoder som för majoriteten innebär övergång i hypotyreos med livslångt behov av levotyroxin-(LT4)behandling. Syfte: Syftet med examensarbetet var att undersöka långvarig effekt av radiojodbehandling vid Graves sjukdom och hur radiojodbehandling påverkar livskvalitet. Metod: Arbetet utfördes som en litteraturstudie, en sökning efter kliniska studier gjordes i PubMed med sökorden ”Graves disease” AND ”iodine radioisotopes”. Totalt åtta artiklar som i praktiken baserades på fem studier inkluderades i litteraturstudien. Resultat: Studie 1A, 1B och 1C var uppföljningsstudier av en tidigare utförd randomiserad klinisk studie. I studie 1A sågs det att samtliga individer som behandlats för Graves sjukdom hade sämre livskvalitet än den generella befolkningen 14-21 år efter behandling, ingen skillnad kunde ses beroende på behandlingsmetod. Studie 1B visade att skillnaderna i livskvalitet som funnits i studie 1A inte berodde på tyreoideahormonstatus. Resultaten i studie 1C visade att autoimmun aktivitet i form av tyreoideastimulerande hormonreceptorantikropp(TRAk)-nivåer var förhöjda bland individer som behandlats med radiojod i samtliga fem år som uppföljningen skedde, bland tyreostatika- och kirurgibehandlade individer var TRAk-nivåer normaliserade ett år efter behandling.  Studie 2 visade att tidig insättning av LT4 efter radiojodbehandling kunde förebygga försämring i livskvalitet de sex första månaderna efter radiojodbehandling. I studie 3 sågs det att större andel individer utvecklade oftalmopati efter radiojodbehandling jämfört med tyreostatika, vidare sågs sämre livskvalitet bland individer som utvecklat oftalmopati jämfört med individer utan oftalmopati. Studie 4 eftersökte optimumdosering av radiojod för att uppnå eutyreos bland individer med Graves sjukdom, det fanns att 1,85 MBq/g resulterade i eutyreos hos 72% 12 år efter behandling. I studie 5A sågs det att majoriteten av radiojodbehandlade individer övergick i hypotyreos samt att andelen som upplevde återställning 6-10 år efter diagnostisering var mindre bland de som efter behandling av Graves sjukdom var i behov av LT4-behandling. Studie 5B visade att radiojodbehandlade individer hade sämre livskvalitet jämfört med individer som behandlats med tyreostatika eller kirurgi 6-10 år efter behandling av Graves sjukdom. Vidare hade hela studiepopulationen, oavsett behandlingsmetod, sämre livskvalitet jämfört med den generella populationen. Slutsats: På grund av skillnader i upplägg och utfallsvariabler i de inkluderade studierna kan inga generella slutsatser dras utifrån samtliga studieresultat. Sammantaget sågs dock att individer som behandlats för Graves sjukdom har sämre livskvalitet jämfört med den generella befolkningen många år efter behandling. Det förefaller finnas ökad risk för sämre livskvalitet efter radiojodbehandling av Graves sjukdom jämfört med tyreostatika och tyreoidektomi, det krävs dock fler studier för att säkerställa dessa resultat samt undersöka hur och varför radiojodbehandling påverkar livskvalitet. / Graves´ disease is an autoimmune disease resulting in uncontrolled auto antibody-mediated secretion of the thyroid hormones triiodothyronine (T3) and thyroxine (T4). Graves´ disease is the most common cause of hyperthyroidism and has an annual incidence of 20 cases per 100 000 inhabitants. The pathogenesis of the disease is not yet fully understood, but risk factors include smoking, female gender and emotional stress. Since thyroid hormones act in almost every cell in the body, an imbalance in thyroid hormone levels can lead to severe consequences and affected quality of life. Symptoms of Graves´ disease include weight loss, tremor, tachycardia, heat intolerance, increased sweating, anxiety, fatigue and loss of libido.  There are three established treatment approaches for Graves´ disease including antithyroid drugs, radioiodine treatment and surgical thyroidectomy. The treatment goal for Graves´ disease is to stop the hyperthyroid state and reduce the risk of complications from the condition. Antithyroid drugs is the treatment modality most frequently used in newly diagnosed Graves´ disease and the duration of treatment is normally 12-18 months. The risk of recurrence after antithyroid drugs is 50-60%. Both radioiodine treatment and surgery are considered definitive treatments for Graves´ disease, the majority of treated individuals become hypothyroid with a life-long need for levothyroxine (LT4) treatment. The three available treatment options have both advantages and disadvantages that should be discussed with the patient in each individual case.  The aim of this study was to evaluate the long-term effects of radioiodine treatment for Graves´ disease and how radioiodine treatment affects the quality of life.  This is a literature study based on eight articles that, in practice, were based on five different clinical trials. The included studies were collected from the database PubMed. Since the included studies were different in both study design and outcome, no general conclusion can be drawn from all of the included studies. Two of the studies examined long-term effects on the quality of life of radioiodine treatment for Graves´ disease. Both studies found that persons diagnosed with Graves´ disease have a lower quality of life many years after treatment compared to the general population. The quality of life in individuals treated for Graves´ disease seems to be lower than the general population regardless of thyroid hormone state and mode of treatment. There seems to be an increased risk for lower quality of life among individuals treated with radioiodine compared to antithyroid drugs and surgery. Early administration of LT4 after radioiodine treatment could prevent worsening of quality of life according to the short form health survey (SF-36), whilst the long-term need for LT4 treatment after treatment of Graves´ disease is associated with a lower chance of feeling fully recovered 6-10 years after diagnosis.  There is a need for future studies to determine the effects of radioiodine treatment, especially regarding the long-term quality of life. There is also a need to determine the pathogenesis of Graves´ disease and to find new treatment options for the disease since the established treatment methods result in chronic illness or risk of recurrence.

Graves´ disease

iodine radioisotopes

quality of life

treatment outcome

Graves sjukdom

radiojodbehandling

livskvalitet

behandlingsresultat

Endocrinology and Diabetes

Endokrinologi och diabetes

National Trend in Multivessel Percutaneous Coronary Intervention in Patients with Diabetes Mellitus in the United States

AbuSara, Ashraf, Zheng, Shimin, Cao, Yan, Panchal, Hemang B., Bhatheja, Samit, Mogusu, Eunice, Albalbissi, Kais, Paul, Timir K.

13 October 2015

Abstract available through the Journal of the American College of Cardiology.

diabetes

percutaneous coronary intervention trend

Biostatistics and Epidemiology

Biostatistics

Cardiology

Endocrinology, Diabetes, and Metabolism

Epidemiology

Public Health

Management of Type 1 Diabetes: A Family Affair

Grubbs, Emily

03 April 2020

People who live with Type 1 diabetes (T1D) have to carefully self-administer insulin to keep blood glucose levels in a safe healthy range – a complex and demanding task (WHO, 2016). Social support has been found to alleviate diabetes-stress and increase management behaviors (Mackey et al., 2016). Social support from family members is especially advantageous, however currently no single family-based intervention has been established to show reliable improvements in T1D outcomes (Rosland et al., 2010). A review of the literature reveals that social support promoting autonomy is associated with the best T1D outcomes; social support that undermines autonomy is associated with worse T1D outcomes (Kelly & Berg, 2018). These findings are consistent with the self-determination theory (SDT), which identifies autonomy as a psychological need (Ng et al., 2012). The findings of this literature review support the need for a disease-specific family-based intervention that is built on the foundations of SDT.

Type 1 Diabetes

family-based intervention

social support

autonomy

self-determination theory

Endocrinology, Diabetes, and Metabolism

Mental and Social Health