TY - JOUR A1 - Busch, Martin A1 - Nadal, Jennifer A1 - Schmid, Matthias A1 - Paul, Katharina A1 - Titze, Stephanie A1 - Hübner, Silvia A1 - Köttgen, Anna A1 - Schultheiss, Ulla T. A1 - Baid-Agrawal, Seema A1 - Lorenzen, Johan A1 - Schlieper, Georg A1 - Sommerer, Claudia A1 - Krane, Vera A1 - Hilge, Robert A1 - Kielstein, Jan T. A1 - Kronenberg, Florian A1 - Wanner, Christoph A1 - Eckardt, Kai-Uwe A1 - Wolf, Gunter T1 - Glycaemic control and antidiabetic therapy in patients with diabetes mellitus and chronic kidney disease - cross-sectional data from the German Chronic Kidney Disease (GCKD) cohort JF - BMC Nephrology N2 - Background Diabetes mellitus (DM) is the leading cause of end-stage renal disease. Little is known about practice patterns of anti-diabetic therapy in the presence of chronic kidney disease (CKD) and correlates with glycaemic control. We therefore aimed to analyze current antidiabetic treatment and correlates of metabolic control in a large contemporary prospective cohort of patients with diabetes and CKD. Methods The German Chronic Kidney Disease (GCKD) study enrolled 5217 patients aged 18–74 years with an estimated glomerular filtration rate (eGFR) between 30–60 mL/min/1.73 m2 or proteinuria >0.5 g/d. The use of diet prescription, oral anti-diabetic medication, and insulin was assessed at baseline. HbA1c, measured centrally, was the main outcome measure. Results At baseline, DM was present in 1842 patients (35 %) and the median HbA1C was 7.0 % (25th–75th percentile: 6.8–7.9 %), equalling 53 mmol/mol (51, 63); 24.2 % of patients received dietary treatment only, 25.5 % oral antidiabetic drugs but not insulin, 8.4 % oral antidiabetic drugs with insulin, and 41.8 % insulin alone. Metformin was used by 18.8 %. Factors associated with an HbA1C level >7.0 % (53 mmol/mol) were higher BMI (OR = 1.04 per increase of 1 kg/m2, 95 % CI 1.02–1.06), hemoglobin (OR = 1.11 per increase of 1 g/dL, 95 % CI 1.04–1.18), treatment with insulin alone (OR = 5.63, 95 % CI 4.26–7.45) or in combination with oral antidiabetic agents (OR = 4.23, 95 % CI 2.77–6.46) but not monotherapy with metformin, DPP-4 inhibitors, or glinides. Conclusions Within the GCKD cohort of patients with CKD stage 3 or overt proteinuria, antidiabetic treatment patterns were highly variable with a remarkably high proportion of more than 50 % receiving insulin-based therapies. Metabolic control was overall satisfactory, but insulin use was associated with higher HbA1C levels. KW - Chronic kidney disease KW - Glycaemic control KW - Hemoglobin A1C KW - Insulin therapy KW - Oral antidiabetic drugs KW - Diabetes mellitus Y1 - 2016 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-164687 VL - 17 IS - 59 ER - TY - THES A1 - Schober, Kilian T1 - Der Einfluss von CLEC16A auf Autophagie - ein neuer Mechanismus in der Pathogenese von Typ-1-Diabetes T1 - The influence of CLEC16A on autophagy - a new mechanism in the pathogenesis of type 1 diabetes N2 - Das Gen CLEC16A ist mit der Autoimmunerkrankung Typ-1-Diabetes assoziiert. NOD-Mäuse mit einem Clec16a-KD sind vor der Entwicklung von Diabetes geschützt, der entscheidende Wirkungsort für Clec16a sind dabei TECs. Im Rahmen zentraler Toleranz präsentieren TECs CD4+ Thymozyten Selbstantigene auf MHC II-Komplexen. Autophagie ist ein Zellprozess, der in TECs MHC II-Komplexen Selbstantigene zuführt und so für die Entwicklung zentraler Toleranz essentiell ist. Das Ortholog von CLEC16A, ema, fördert die Bildung von Autophagosomen. So wurde vermutet, dass CLEC16A ein Suszeptibilitätsgen für Typ-1-Diabetes ist, weil es Autophagie in TECs und somit deren MHC II-Beladung verändert. Die vorliegende Arbeit schaltete CLEC16A in einer humanen Zelllinie durch RNAi aus und untersuchte die autophagische Aktivität dieser Zellen. Außerdem untersuchte sie die Autophagie von TECs aus NOD-Clec16a-KD-Mäusen. Die Beurteilung erfolgte morphologisch durch Immunzytochemie bzw. -histochemie und funktionell durch Immunoblots. Es wurde gezeigt, dass der KD von CLEC16A in vitro und in vivo Autophagie funktionell beeinträchtigt. Damit liefert die vorliegende Arbeit zusammen mit den Ergebnissen der Arbeitsgruppe Kissler einen möglichen Erklärungsansatz, warum CLEC16A ein mit Typ-1-Diabetes assoziiertes Gen ist. CLEC16A fördert Autophagie in TECs, was die Selbstantigen-Beladung von MHC II-Komplexen verändert. Selbstreaktive CD4+ Thymozyten führen so zum Verlust zentraler Toleranz und der Entwicklung von Typ-1-Diabetes. Weitere Untersuchungen sind jedoch notwendig, um diese Hypothese zu bekräftigen. N2 - The gene CLEC16A is associated with type 1 diabetes. NOD mice with a Clec16a-KD are protected from diabetes. Specifically, the protection is dependent on a Clec16a-KD in TECs. TECs present self-antigens to CD4+ thymocytes for positive selection and central tolerance. Some TECs show constitutive levels of autophagy and in these cells, autophagy changes the TCR ligandome of self antigens, thereby modulating central tolerance. The orthologous gene of CLEC16A in Drosophila, ema, promotes the formation of autophagosomes. It was therefore hypothesized that CLEC16A is associated with type 1 diabetes, as it changes autophagy in TECs. This doctoral thesis knocked down CLEC16A in a human cell line, using RNA interference, and investigated TECs from NOD-Clec16a-KD mice. Autophagic flux was determined using immunocytochemistry/immunohistochemistry and immunoblot of the autophagic markers p62 and LC3. It was shown that a KD of CLEC16A compromises autophagic activity in vitro and in vivo. Together with further results from the lab of Stephan Kissler, a change in autophagy in TECs through CLEC16A provides a possible reason for the association with type 1 diabetes, but also other autoimmune diseases: CLEC16A enhances autophagy in TECs, which modulates MHC II self-peptide loading. Self reactive CD4+ T cells are thus not eliminated by central tolerance and contribute to the pathogenesis of type 1 diabetes. KW - Thymus KW - Autophagie KW - Diabetes mellitus KW - Typ-1-Diabetes KW - Autophagie KW - Zentrale Toleranz Y1 - 2016 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-138715 ER -