Cookies help us deliver our services. By using our services, you agree to our use of cookies. More information

Difference between revisions of "Jelenik 2014 Diabetes"

From Bioblast
 
Line 11: Line 11:
{{Labeling
{{Labeling
|area=Respiration
|area=Respiration
|diseases=Diabetes
|organism=Mouse
|organism=Mouse
|tissues=Skeletal muscle, Liver
|tissues=Skeletal muscle, Liver
|preparations=Permeabilized tissue, Isolated mitochondria
|preparations=Permeabilized tissue, Isolated mitochondria
|diseases=Diabetes
|couplingstates=OXPHOS, ET
|couplingstates=OXPHOS, ETS
|pathways=N, NS, ROX
|pathways=N, NS, ROX
|instruments=Oxygraph-2k
|instruments=Oxygraph-2k
}}
}}

Latest revision as of 13:46, 13 November 2017

Publications in the MiPMap
Jelenik T, Séquaris G, Kaul K, Ouwens DM, Phielix E, Kotzka J, Knebel B, Weiß J, Reinbeck AL, Janke L, Nowotny P, Partke HJ, Zhang D, Shulman GI, Szendroedi J, Roden M (2014) Tissue-specific differences in the development of insulin resistance in a mouse model for type 1 diabetes. Diabetes 63:3856-67.

» PMID: 24917575

Jelenik T, Sequaris G, Kaul K, Ouwens DM, Phielix E, Kotzka J, Knebel B, Weiß J, Reinbeck AL, Janke L, Nowotny P, Partke HJ, Zhang D, Shulman GI, Szendroedi J, Roden M (2014) Diabetes

Abstract: While insulin resistance is known to underlie type 2 diabetes, its role in the development of type 1 diabetes is gaining increasing interest more recently. In a model of type 1 diabetes, the non-obese diabetic (NOD) mouse, we found that insulin resistance driven by lipid- and glucose-independent mechanisms is already present in liver of pre-diabetic mice. Hepatic insulin resistance is associated with a transient rise in mitochondrial respiration, followed by increased production of lipid peroxides and c-jun N-terminal kinase (JNK) activity. At the onset of diabetes, increased adipose tissue lipolysis promotes myocellular diacylglycerol accumulation. This is paralleled by increased myocellular protein kinase C theta (PKCθ) activity and serum fetuin A levels. Muscle mitochondrial oxidative capacity is unchanged at the onset, but decreases at later stages of diabetes. In conclusion, hepatic and muscle insulin resistance manifest at different stages and involve distinct cellular mechanisms during the development of diabetes in the NOD mouse. Keywords: DE Duesseldorf Roden M

O2k-Network Lab: DE Duesseldorf Roden M


Labels: MiParea: Respiration  Pathology: Diabetes 

Organism: Mouse  Tissue;cell: Skeletal muscle, Liver  Preparation: Permeabilized tissue, Isolated mitochondria 


Coupling state: OXPHOS, ET  Pathway: N, NS, ROX  HRR: Oxygraph-2k