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Dive into the research topics where Soren Tullin is active.

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Featured researches published by Soren Tullin.


Journal of Biological Chemistry | 2010

Adiponectin Promotes Macrophage Polarization toward an Anti-inflammatory Phenotype

Koji Ohashi; Jennifer L. Parker; Noriyuki Ouchi; Akiko Higuchi; Joseph A. Vita; Noyan Gokce; Anette A. Pedersen; Christoph Kalthoff; Soren Tullin; Anette Sams; Ross Summer; Kenneth Walsh

It is established that the adipocyte-derived cytokine adiponectin protects against cardiovascular and metabolic diseases, but the effect of this adipokine on macrophage polarization, an important mediator of disease progression, has never been assessed. We hypothesized that adiponectin modulates macrophage polarization from that resembling a classically activated M1 phenotype to that resembling alternatively-activated M2 cells. Peritoneal macrophages and the stromal vascular fraction (SVF) cells of adipose tissue isolated from adiponectin knock-out mice displayed increased M1 markers, including tumor necrosis factor-α, interleukin-6, and monocyte chemoattractant protein-1 and decreased M2 markers, including arginase-1, macrophage galactose N-acetyl-galactosamine specific lectin-1, and interleukin-10. The systemic delivery of adenovirus expressing adiponectin significantly augmented arginase-1 expression in peritoneal macrophages and SVF cells in both wild-type and adiponectin knock-out mice. In culture, the treatment of macrophages with recombinant adiponectin protein led to an increase in the levels of M2 markers and a reduction of reactive oxygen species and reactive oxygen species-related gene expression. Adiponectin also stimulated the expression of M2 markers and attenuated the expression of M1 markers in human monocyte-derived macrophages and SVF cells isolated from human adipose tissue. These data show that adiponectin functions as a regulator of macrophage polarization, and they indicate that conditions of high adiponectin expression may deter metabolic and cardiovascular disease progression by favoring an anti-inflammatory phenotype in macrophages.


Biochemical Journal | 2007

Mitochondrial uncouplers with an extraordinary dynamic range

Phing-How Lou; Birgit Sehested Hansen; Preben H. Olsen; Soren Tullin; Michael P. Murphy; Martin D. Brand

We have discovered that some weak uncouplers (typified by butylated hydroxytoluene) have a dynamic range of more than 10(6) in vitro: the concentration giving measurable uncoupling is less than one millionth of the concentration causing full uncoupling. They achieve this through a high-affinity interaction with the mitochondrial adenine nucleotide translocase that causes significant but limited uncoupling at extremely low uncoupler concentrations, together with more conventional uncoupling at much higher concentrations. Uncoupling at the translocase is not by a conventional weak acid/anion cycling mechanism since it is also caused by substituted triphenylphosphonium molecules, which are not anionic and cannot protonate. Covalent attachment of the uncoupler to a mitochondrially targeted hydrophobic cation sensitizes it to membrane potential, giving a small additional effect. The wide dynamic range of these uncouplers in isolated mitochondria and intact cells reveals a novel allosteric activation of proton transport through the adenine nucleotide translocase and provides a promising starting point for designing safer uncouplers for obesity therapy.


PLOS ONE | 2012

Recombinant Adiponectin Does Not Lower Plasma Glucose in Animal Models of Type 2 Diabetes

Soren Tullin; Anette Sams; Jakob Brandt; Kirsten Dahl; Wei Gong; Claus Bekker Jeppesen; Thomas Nylandsted Krogh; Grith Skytte Olsen; Yun Liu; Anette A. Pedersen; Jørn Meidahl Petersen; Bidda Rolin; Per-Olof Wahlund; Christoph Kalthoff

Aims/Hypothesis Several studies have shown that adiponectin can lower blood glucose in diabetic mice. The aim of this study was to establish an effective adiponectin production process and to evaluate the anti-diabetic potential of the different adiponectin forms in diabetic mice and sand rats. Methods Human high molecular weight, mouse low molecular weight and mouse plus human globular adiponectin forms were expressed and purified from mammalian cells or yeast. The purified protein was administered at 10–30 mg/kg i.p. b.i.d. to diabetic db/db mice for 2 weeks. Furthermore, high molecular weight human and globular mouse adiponectin batches were administered at 5–15 mg/kg i.p. b.i.d. to diabetic sand rats for 12 days. Results Surprisingly, none of our batches had any effect on blood glucose, HbA1c, plasma lipids or body weight in diabetic db/db mice or sand rats. In vitro biological, biochemical and biophysical data suggest that the protein was correctly folded and biologically active. Conclusions/Interpretation Recombinant adiponectin is ineffective at lowering blood glucose in diabetic db/db mice or sand rats.


Molecular Pharmacology | 2001

Iodo-Resiniferatoxin, a New Potent Vanilloid Receptor Antagonist

Philip Wahl; Christian Foged; Soren Tullin; Christian Thomsen


Archive | 1998

Method for extracting quantitative information relating to an influence on a cellular response

Ole Thastrup; Sara Petersen Bjørn; Soren Tullin; Kasper Almholt; Kurt Scudder


Archive | 1996

A method of detecting biologically active substances

Ole Thastrup; Soren Tullin; Lars Kongsbak Poulsen; Sara Petersen Bjørn


Endocrinology | 2000

Adenosine Is an Agonist of the Growth Hormone Secretagogue Receptor

Soren Tullin; Birgit Sehested Hansen; Michael Ankersen; Jette Møller; Karen Arevad von Cappelen; Lars Thim


Archive | 2001

Use of compounds for the regulation of food intake

Maibritt Bansholm Andersen; Birgit Sehested Hansen; Kirsten Raun; Soren Tullin; Lars Thim


Archive | 1996

Novel variants of green fluorescent protein, gfp

Ole Thastrup; Soren Tullin; Lars Kongsbak Poulsen; Sara Petersen Bjørn


Biochemical Journal | 1999

SIMULTANEOUS VISUALIZATION OF THE TRANSLOCATION OF PROTEIN KINASE CALPHA -GREEN FLUORESCENT PROTEIN HYBRIDS AND INTRACELLULAR CALCIUM CONCENTRATIONS

Kasper Almholt; Per Arkhammar; Ole Thastrup; Soren Tullin

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Lars Kongsbak Poulsen

Technical University of Denmark

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Kurt Scudder

University of Washington

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