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Dive into the research topics where Jesper Söndergaard Hansen is active.

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Featured researches published by Jesper Söndergaard Hansen.


Scientific Reports | 2016

Onset of main Phanerozoic marine radiation sparked by emerging Mid Ordovician icehouse

Christian M. Ø. Rasmussen; Clemens V. Ullmann; Kristian G. Jakobsen; Anders Lindskog; Jesper Söndergaard Hansen; Thomas Willum Hansen; Mats E. Eriksson; Andrei Dronov; Robert Frei; Christoph Korte; Arne T. Nielsen; David A. T. Harper

The Great Ordovician Biodiversification Event (GOBE) was the most rapid and sustained increase in marine Phanerozoic biodiversity. What generated this biotic response across Palaeozoic seascapes is a matter of debate; several intrinsic and extrinsic drivers have been suggested. One is Ordovician climate, which in recent years has undergone a paradigm shift from a text-book example of an extended greenhouse to an interval with transient cooling intervals – at least during the Late Ordovician. Here, we show the first unambiguous evidence for a sudden Mid Ordovician icehouse, comparable in magnitude to the Quaternary glaciations. We further demonstrate the initiation of this icehouse to coincide with the onset of the GOBE. This finding is based on both abiotic and biotic proxies obtained from the most comprehensive geochemical and palaeobiological dataset yet collected through this interval. We argue that the icehouse conditions increased latitudinal and bathymetrical temperature and oxygen gradients initiating an Early Palaeozoic Great Ocean Conveyor Belt. This fuelled the GOBE, as upwelling zones created new ecospace for the primary producers. A subsequent rise in δ13C ratios known as the Middle Darriwilian Isotopic Carbon Excursion (MDICE) may reflect a global response to increased bioproductivity encouraged by the onset of the GOBE.


Chemical Communications | 2015

Glucose transport machinery reconstituted in cell models

Jesper Söndergaard Hansen; Karin Elbing; James R. Thompson; Noah Malmstadt; Karin Lindkvist-Petersson

Here we demonstrate the production of a functioning cell model by formation of giant vesicles reconstituted with the GLUT1 glucose transporter and a glucose oxidase and hydrogen peroxidase linked fluorescent reporter internally. Hence, a simplified artificial cell is formed that is able to take up glucose and process it.


Metabolism-clinical and Experimental | 2016

Perilipin 1 binds to aquaporin 7 in human adipocytes and controls its mobility via protein kinase A mediated phosphorylation

Jesper Söndergaard Hansen; Christian Krintel; Malin Hernebring; Tatu J K Haataja; Sofia de Marè; Sebastian Wasserstrom; Urszula Kosinska-Eriksson; Madelene Palmgren; Cecilia Holm; Karin G. Stenkula; Helena A. Jones; Karin Lindkvist-Petersson

Accumulating evidence suggests that dysregulated glycerol metabolism contributes to the pathophysiology of obesity and type 2 diabetes. Glycerol efflux from adipocytes is regulated by the aquaglyceroporin AQP7, which is translocated upon hormone stimulation. Here, we propose a molecular mechanism where the AQP7 mobility in adipocytes is dependent on perilipin 1 and protein kinase A. Biochemical analyses combined with ex vivo studies in human primary adipocytes, demonstrate that perilipin 1 binds to AQP7, and that catecholamine activated protein kinase A phosphorylates the N-terminus of AQP7, thereby reducing complex formation. Together, these findings are indicative of how glycerol release is controlled in adipocytes, and may pave the way for the future design of drugs against human metabolic pathologies.


Journal of Paleontology | 2010

First Fossils of the Isopod Genus Aega Leach, 1815

Thomas Willum Hansen; Jesper Söndergaard Hansen

Abstract Two abdominal molts representing a small cymothoid isopod are described from the marine late Miocene Gram Formation of southern Denmark. Abdominal molts are generally regarded as being difficult or even impossible to assign to genus or family due to overlap of morphological characters. A preliminary study supported by statistical and multivariate analysis of the genera most closely resembling the specimens reveals that although some overlap in characters do occur, the genera can to a large extent be defined by a diagnostic set of features. The Danish Miocene taxon described herein is assigned to AegaLeach, 1815 as the only known fossil of this important cosmopolitan genus.


Scientific Reports | 2017

Visualization of lipid directed dynamics of perilipin 1 in human primary adipocytes

Jesper Söndergaard Hansen; Sofia de Marè; Helena A. Jones; Olga Göransson; Karin Lindkvist-Petersson

Perilipin 1 is a lipid droplet coating protein known to regulate lipid metabolism in adipocytes by serving as a physical barrier as well as a recruitment site for lipases to the lipid droplet. Phosphorylation of perilipin 1 by protein kinase A rapidly initiates lipolysis, but the detailed mechanism on how perilipin 1 controls lipolysis is unknown. Here, we identify specific lipid binding properties of perilipin 1 that regulate the dynamics of lipolysis in human primary adipocytes. Cellular imaging combined with biochemical and biophysical analyses demonstrate that perilipin 1 specifically binds to cholesteryl esters, and that their dynamic properties direct segregation of perilipin 1 into topologically distinct micro domains on the lipid droplet. Together, our data points to a simple unifying mechanism that lipid assembly and segregation control lipolysis in human primary adipocytes.


PLOS ONE | 2017

Thermal stability and structural changes in bacterial toxins responsible for food poisoning

Paulina Regenthal; Jesper Söndergaard Hansen; Ingemar André; Karin Lindkvist-Petersson

The staphylococcal enterotoxins (SEs) are secreted by the bacteria Staphylococcus aureus and are the most common causative agent in staphylococcal food poisoning. The staphylococcal enterotoxin A (SEA) has been associated with large staphylococcal food poisoning outbreaks, but newer identified SEs, like staphylococcal enterotoxin H (SEH) has recently been shown to be present at similar levels as SEA in food poisoning outbreaks. Thus, we set out to investigate the thermo-stability of the three-dimensional structures of SEA, SEH and staphylococcal enterotoxin E (SEE), since heat inactivation is a common method to inactivate toxins during food processing. Interestingly, the investigated toxins behaved distinctly different upon heating. SEA and SEE were more stable at slightly acidic pH values, while SEH adopted an extremely stable structure at neutral pH, with almost no effects on secondary structural elements upon heating to 95°C, and with reversible formation of tertiary structure upon subsequent cooling to room temperature. Taken together, the data suggests that the family of staphylococcal enterotoxins have different ability to withstand heat, and thus the exact profile of heat inactivation for all SEs causing food poisoning needs to be considered to improve food safety.


Bioinspiration & Biomimetics | 2017

Tuning biomimetic membrane barrier properties by hydrocarbon, cholesterol and polymeric additives

Marta Espina Palanco; Nils Skovgaard; Jesper Söndergaard Hansen; Kirstine Berg-Sørensen; Claus Hélix-Nielsen

The barrier properties of cellular membranes are increasingly attracting attention as a source of inspiration for designing biomimetic membranes. The broad range of potential technological applications makes the use of lipid and lately also polymeric materials a popular choice for constructing biomimetic membranes, where the barrier properties can be controlled by the composition of the membrane constituent elements. Here we investigate the membrane properties reported by the light-induced proton pumping activity of bacteriorhodopsin (bR) reconstituted in three vesicle systems of different membrane composition. Specifically we quantify how the resulting proton influx and efflux rates are influenced by the membrane composition using a variety of membrane modulators. We demonstrate that by adding hydrocarbons to vesicles with reconstituted bR formed from asolectin lipids the resulting transmembrane proton fluxes changes proportional to the carbon chain length when compared against control. We observe a similar proportionality in single-component 1,2-Dioleoyl-sn-glycero-3-phosphocholine model membranes when using cholesterol. Lastly we investigate the effects of adding the amphiphilic di-block co-polymer polybutadiene-polyethyleneoxide (PB12-PEO10) to phospholipid membranes formed from 1,2-Dioleoyl-sn-glycero-3-phosphocholine, 1,2-Dioleoyl-sn-glycero-3-phosphatidylethanolamine, and 1,2-Dioleoyl-sn-glycero-3-phosphatidylserine. The proton pumping activity of bR (measured as a change in extra-vesicular pH) in mixed lipid/PB12-PEO10 lipid systems is up to six-fold higher compared to that observed for bR containing vesicles made from PB12-PEO10 alone. Interestingly, bR inserts with apparent opposite orientation in pure PB12-PEO10 vesicles as compared to pure lipid vesicles. Addition of equimolar amounts of lipids to PB12-PEO10 results in bR orientation similar to that observed for pure lipids. In conclusion our results show how the barrier properties of the membranes can be controlled by the composition of the membrane. In particular the use of mixed lipid-polymer systems may pave the way for constructing biomimetic membranes tailored for optimal properties in various applications including drug delivery systems, biosensors and energy conservation technology.


Methods of Molecular Biology | 2018

Glucose transport activity measured in giant vesicles

Jesper Söndergaard Hansen; Karin Lindkvist-Petersson

Incorporation of membrane proteins and internal reporter systems directly into giant vesicles, during their formation from a hydrogel surface, has emerged as a promising new concept in membrane protein characterization. Here, we provide the detailed protocol for a glucose transporter activity assay based on giant vesicles containing a fluorescent enzyme-linked reporter system internally. This assay is applicable for the functional analysis of a variety of hexose-transporting proteins. We furthermore believe that it can aid in the development of drugs targeting hexose transporters.


The Journal of Membrane Biology | 2017

Quantification of the Intracellular Life Time of Water Molecules to Measure Transport Rates of Human Aquaglyceroporins.

Madelene Palmgren; Malin Hernebring; Stefanie Eriksson; Karin Elbing; Cecilia Geijer; Samo Lasič; Peter Dahl; Jesper Söndergaard Hansen; Daniel Topgaard; Karin Lindkvist-Petersson

Orthodox aquaporins are transmembrane channel proteins that facilitate rapid diffusion of water, while aquaglyceroporins facilitate the diffusion of small uncharged molecules such as glycerol and arsenic trioxide. Aquaglyceroporins play important roles in human physiology, in particular for glycerol metabolism and arsenic detoxification. We have developed a unique system applying the strain of the yeast Pichia pastoris, where the endogenous aquaporins/aquaglyceroporins have been removed and human aquaglyceroporins AQP3, AQP7, and AQP9 are recombinantly expressed enabling comparative permeability measurements between the expressed proteins. Using a newly established Nuclear Magnetic Resonance approach based on measurement of the intracellular life time of water, we propose that human aquaglyceroporins are poor facilitators of water and that the water transport efficiency is similar to that of passive diffusion across native cell membranes. This is distinctly different from glycerol and arsenic trioxide, where high glycerol transport efficiency was recorded.


Lethaia | 2008

The late Sandbian – earliest Katian (Ordovician) brachiopod immigration and its influence on the brachiopod fauna in the Oslo Region, Norway

Jesper Söndergaard Hansen; David A. T. Harper

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Claus Hélix-Nielsen

Technical University of Denmark

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Thomas Willum Hansen

Technical University of Denmark

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