H Fiedler scite author profile

Despite its generalized use as drug therapy for multiple sclerosis (MS), the molecular mechanisms of action of interferon beta (IFNB) are still poorly understood. IFNB therapy is long-termed and clinical effects are not immediate, therefore reliable early biomarkers for IFNB activity should maintain a differential expression over time, but longitudinal studies at a transcriptional level have been rare. Microarrays were used to monitor 18 IFNB1b treated MS patients at four time points spanning a period of 1 year. Genes showing in the majority of patients the greatest and most consistent changes in their expression levels were studied. Interferon regulated genes were significantly overrepresented. Fifteen markers were differentially expressed during all three time points and followed a consistent time course pattern: EIF2AK2, IFI6, IFI44, IFI44L, IFIH1, IFIT1, IFIT2, IFIT3, ISG15, MX1, OASL, RSAD2, SN, XAF1 and the marker 238704_at. Except for the last one, these biomarkers were all formerly identified as being indicative for IFNB activity. Expression changes were both early detectable and long lasting and could thus be optimal biomarkers for IFNB activity in long-term studies. Other known biomarkers of IFNB activity were found to be differentially expressed just for certain periods after therapy onset: Interleukin-8 was a short lasting marker and changes in STAT1 were detected with delay.

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Paradoxical glucagon response after stimulation with glucose and arginine in isolated pancreatic sand rat islets

Ziegler

Hahn

Ziegler

et al. 1975

Diabetologia

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Isolated pancreatic islets of normoglycemic sand rats do not respond to 2.5 mM glucose with an enhanced glucagon secretion, which could be observed in normal Wistar rats. Arginine stimulates glucagon release in the presence of 2.5 mM glucose in Wistar rats as well as in sand rats. The secretion pattern is not caused by insulin deficiency since sand rat islets are characterized by an increased insulin secretion rate in vitro. This paradoxical glucagon secretion is not caused by a changed glucagon content but might be related to this species which is able to develop a diabetic syndrome spontaneously.

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Effects of pregnancy on the glucose-induced insulin release from cultivated pancreatic islets of the rat

Ziegler

Fiedler

1978

Experientia

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Studien in der Thiophenreihe. XXXIII. Über die Jodderivate des Thiophens und ihre Umsetzung mit Thiosalicylsäure

Steinkopf

Schmitt.

Fiedler

1937

Justus Liebigs Ann. Chem.

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Investigations on isolated islets in vitro. IX. Influence of food deprivation and glucose refeeding in vitro on insulin secretion

Hahn

Fiedler

1974

Acta diabet. lat

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H Fiedler

Time course transcriptomics of IFNB1b drug therapy in multiple sclerosis

Paradoxical glucagon response after stimulation with glucose and arginine in isolated pancreatic sand rat islets

Effects of pregnancy on the glucose-induced insulin release from cultivated pancreatic islets of the rat

Studien in der Thiophenreihe. XXXIII. Über die Jodderivate des Thiophens und ihre Umsetzung mit Thiosalicylsäure

Investigations on isolated islets in vitro. IX. Influence of food deprivation and glucose refeeding in vitro on insulin secretion

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