Your search keyword '"Helene Andersson"' showing total 26 results

1. Levels of human proteins in plasma associated with acute paediatric malaria

Author

Reuterswärd, Philippa, Bergström, Sofia, Orikiiriza, Judy, Lindquist, Elisabeth, Bergström, Sven, Svahn, Helene Andersson, Ayoglu, Burcu, Uhlén, Mathias, Wahlgren, Mats, Normark, Johan, Ribacke, Ulf, Nilsson, Peter, Reuterswärd, Philippa, Bergström, Sofia, Orikiiriza, Judy, Lindquist, Elisabeth, Bergström, Sven, Svahn, Helene Andersson, Ayoglu, Burcu, Uhlén, Mathias, Wahlgren, Mats, Normark, Johan, Ribacke, Ulf, and Nilsson, Peter

Abstract

Background: The intimate interaction between the pathophysiology of the human host and the biology of the Plasmodium falciparum parasite results in a wide spectrum of disease outcomes in malaria. Development of severe disease is associated with a progressively augmented imbalance in pro- and anti-inflammatory responses to high parasite loads and sequestration of parasitized erythrocytes. Although these phenomena collectively constitute common denominators for the wide variety of discrete severe malaria manifestations, the mechanistic rationales behind discrepancies in outcome are poorly understood. Exploration of the human pathophysiological response by variations in protein profiles in plasma presents an excellent opportunity to increase the understanding. This is ultimately required for better prediction, prevention and treatment of malaria, which is essential for ongoing elimination and eradication efforts. Results: An affinity proteomics approach was used to analyse 541 paediatric plasma samples collected from community controls and patients with mild or severe malaria in Rwanda. Protein profiles were generated with an antibody-based suspension bead array containing 255 antibodies targetting 115 human proteins. Here, 57 proteins were identified with significantly altered levels (adjusted p-values < 0.001) in patients with malaria compared to controls. From these, the 27 most significant proteins (adjusted p-values < 10−14) were selected for a stringent analysis approach. Here, 24 proteins showed elevated levels in malaria patients and included proteins involved in acute inflammatory response as well as cell adhesion. The remaining three proteins, also implicated in immune regulation and cellular adhesivity, displayed lower abundance in malaria patients. In addition, 37 proteins (adjusted p-values < 0.05) were identified with increased levels in patients with severe compared to mild malaria. This set includes, proteins involved in tissue remodelling and

Published

2018

2. Levels of human proteins in plasma associated with acute paediatric malaria

Author

Reuterswärd, Philippa, Bergström, Sofia, Orikiiriza, Judy, Lindquist, Elisabeth, Bergström, Sven, Svahn, Helene Andersson, Ayoglu, Burcu, Uhlén, Mathias, Wahlgren, Mats, Normark, Johan, Ribacke, Ulf, Nilsson, Peter, Reuterswärd, Philippa, Bergström, Sofia, Orikiiriza, Judy, Lindquist, Elisabeth, Bergström, Sven, Svahn, Helene Andersson, Ayoglu, Burcu, Uhlén, Mathias, Wahlgren, Mats, Normark, Johan, Ribacke, Ulf, and Nilsson, Peter

Abstract

Background: The intimate interaction between the pathophysiology of the human host and the biology of the Plasmodium falciparum parasite results in a wide spectrum of disease outcomes in malaria. Development of severe disease is associated with a progressively augmented imbalance in pro- and anti-inflammatory responses to high parasite loads and sequestration of parasitized erythrocytes. Although these phenomena collectively constitute common denominators for the wide variety of discrete severe malaria manifestations, the mechanistic rationales behind discrepancies in outcome are poorly understood. Exploration of the human pathophysiological response by variations in protein profiles in plasma presents an excellent opportunity to increase the understanding. This is ultimately required for better prediction, prevention and treatment of malaria, which is essential for ongoing elimination and eradication efforts. Results: An affinity proteomics approach was used to analyse 541 paediatric plasma samples collected from community controls and patients with mild or severe malaria in Rwanda. Protein profiles were generated with an antibody-based suspension bead array containing 255 antibodies targetting 115 human proteins. Here, 57 proteins were identified with significantly altered levels (adjusted p-values < 0.001) in patients with malaria compared to controls. From these, the 27 most significant proteins (adjusted p-values < 10−14) were selected for a stringent analysis approach. Here, 24 proteins showed elevated levels in malaria patients and included proteins involved in acute inflammatory response as well as cell adhesion. The remaining three proteins, also implicated in immune regulation and cellular adhesivity, displayed lower abundance in malaria patients. In addition, 37 proteins (adjusted p-values < 0.05) were identified with increased levels in patients with severe compared to mild malaria. This set includes, proteins involved in tissue remodelling and

Published

2018

3. Levels of human proteins in plasma associated with acute paediatric malaria

Author

Reuterswärd, Philippa, Bergström, Sofia, Orikiiriza, Judy, Lindquist, Elisabeth, Bergström, Sven, Svahn, Helene Andersson, Ayoglu, Burcu, Uhlén, Mathias, Wahlgren, Mats, Normark, Johan, Ribacke, Ulf, Nilsson, Peter, Reuterswärd, Philippa, Bergström, Sofia, Orikiiriza, Judy, Lindquist, Elisabeth, Bergström, Sven, Svahn, Helene Andersson, Ayoglu, Burcu, Uhlén, Mathias, Wahlgren, Mats, Normark, Johan, Ribacke, Ulf, and Nilsson, Peter

Abstract

Background: The intimate interaction between the pathophysiology of the human host and the biology of the Plasmodium falciparum parasite results in a wide spectrum of disease outcomes in malaria. Development of severe disease is associated with a progressively augmented imbalance in pro- and anti-inflammatory responses to high parasite loads and sequestration of parasitized erythrocytes. Although these phenomena collectively constitute common denominators for the wide variety of discrete severe malaria manifestations, the mechanistic rationales behind discrepancies in outcome are poorly understood. Exploration of the human pathophysiological response by variations in protein profiles in plasma presents an excellent opportunity to increase the understanding. This is ultimately required for better prediction, prevention and treatment of malaria, which is essential for ongoing elimination and eradication efforts. Results: An affinity proteomics approach was used to analyse 541 paediatric plasma samples collected from community controls and patients with mild or severe malaria in Rwanda. Protein profiles were generated with an antibody-based suspension bead array containing 255 antibodies targetting 115 human proteins. Here, 57 proteins were identified with significantly altered levels (adjusted p-values < 0.001) in patients with malaria compared to controls. From these, the 27 most significant proteins (adjusted p-values < 10−14) were selected for a stringent analysis approach. Here, 24 proteins showed elevated levels in malaria patients and included proteins involved in acute inflammatory response as well as cell adhesion. The remaining three proteins, also implicated in immune regulation and cellular adhesivity, displayed lower abundance in malaria patients. In addition, 37 proteins (adjusted p-values < 0.05) were identified with increased levels in patients with severe compared to mild malaria. This set includes, proteins involved in tissue remodelling and

Published

2018

4. Levels of human proteins in plasma associated with acute paediatric malaria

Author

Reuterswärd, Philippa, Bergström, Sofia, Orikiiriza, Judy, Lindquist, Elisabeth, Bergström, Sven, Svahn, Helene Andersson, Ayoglu, Burcu, Uhlén, Mathias, Wahlgren, Mats, Normark, Johan, Ribacke, Ulf, Nilsson, Peter, Reuterswärd, Philippa, Bergström, Sofia, Orikiiriza, Judy, Lindquist, Elisabeth, Bergström, Sven, Svahn, Helene Andersson, Ayoglu, Burcu, Uhlén, Mathias, Wahlgren, Mats, Normark, Johan, Ribacke, Ulf, and Nilsson, Peter

Abstract

Background: The intimate interaction between the pathophysiology of the human host and the biology of the Plasmodium falciparum parasite results in a wide spectrum of disease outcomes in malaria. Development of severe disease is associated with a progressively augmented imbalance in pro- and anti-inflammatory responses to high parasite loads and sequestration of parasitized erythrocytes. Although these phenomena collectively constitute common denominators for the wide variety of discrete severe malaria manifestations, the mechanistic rationales behind discrepancies in outcome are poorly understood. Exploration of the human pathophysiological response by variations in protein profiles in plasma presents an excellent opportunity to increase the understanding. This is ultimately required for better prediction, prevention and treatment of malaria, which is essential for ongoing elimination and eradication efforts. Results: An affinity proteomics approach was used to analyse 541 paediatric plasma samples collected from community controls and patients with mild or severe malaria in Rwanda. Protein profiles were generated with an antibody-based suspension bead array containing 255 antibodies targetting 115 human proteins. Here, 57 proteins were identified with significantly altered levels (adjusted p-values < 0.001) in patients with malaria compared to controls. From these, the 27 most significant proteins (adjusted p-values < 10−14) were selected for a stringent analysis approach. Here, 24 proteins showed elevated levels in malaria patients and included proteins involved in acute inflammatory response as well as cell adhesion. The remaining three proteins, also implicated in immune regulation and cellular adhesivity, displayed lower abundance in malaria patients. In addition, 37 proteins (adjusted p-values < 0.05) were identified with increased levels in patients with severe compared to mild malaria. This set includes, proteins involved in tissue remodelling and

Published

2018

5. Levels of human proteins in plasma associated with acute paediatric malaria

Author

Reuterswärd, Philippa, Bergström, Sofia, Orikiiriza, Judy, Lindquist, Elisabeth, Bergström, Sven, Svahn, Helene Andersson, Ayoglu, Burcu, Uhlén, Mathias, Wahlgren, Mats, Normark, Johan, Ribacke, Ulf, Nilsson, Peter, Reuterswärd, Philippa, Bergström, Sofia, Orikiiriza, Judy, Lindquist, Elisabeth, Bergström, Sven, Svahn, Helene Andersson, Ayoglu, Burcu, Uhlén, Mathias, Wahlgren, Mats, Normark, Johan, Ribacke, Ulf, and Nilsson, Peter

Abstract

Background: The intimate interaction between the pathophysiology of the human host and the biology of the Plasmodium falciparum parasite results in a wide spectrum of disease outcomes in malaria. Development of severe disease is associated with a progressively augmented imbalance in pro- and anti-inflammatory responses to high parasite loads and sequestration of parasitized erythrocytes. Although these phenomena collectively constitute common denominators for the wide variety of discrete severe malaria manifestations, the mechanistic rationales behind discrepancies in outcome are poorly understood. Exploration of the human pathophysiological response by variations in protein profiles in plasma presents an excellent opportunity to increase the understanding. This is ultimately required for better prediction, prevention and treatment of malaria, which is essential for ongoing elimination and eradication efforts. Results: An affinity proteomics approach was used to analyse 541 paediatric plasma samples collected from community controls and patients with mild or severe malaria in Rwanda. Protein profiles were generated with an antibody-based suspension bead array containing 255 antibodies targetting 115 human proteins. Here, 57 proteins were identified with significantly altered levels (adjusted p-values < 0.001) in patients with malaria compared to controls. From these, the 27 most significant proteins (adjusted p-values < 10−14) were selected for a stringent analysis approach. Here, 24 proteins showed elevated levels in malaria patients and included proteins involved in acute inflammatory response as well as cell adhesion. The remaining three proteins, also implicated in immune regulation and cellular adhesivity, displayed lower abundance in malaria patients. In addition, 37 proteins (adjusted p-values < 0.05) were identified with increased levels in patients with severe compared to mild malaria. This set includes, proteins involved in tissue remodelling and

Published

2018

6. Health care workers' perceptions of point-of-care testing in a low-income country-A qualitative study in Southwestern Uganda

Author

Rasti, Reza, Nanjebe, Deborah, Karlstrom, Jonas, Muchunguzi, Charles, Mwanga-Amumpaire, Juliet, Gantelius, Jesper, Mårtensson, Andreas, Rivas, Lourdes, Galban, Francesc, Reutersward, Philippa, Svahn, Helene Andersson, Alvesson, Helle M., Boum, Yap, II, Alfven, Tobias, Rasti, Reza, Nanjebe, Deborah, Karlstrom, Jonas, Muchunguzi, Charles, Mwanga-Amumpaire, Juliet, Gantelius, Jesper, Mårtensson, Andreas, Rivas, Lourdes, Galban, Francesc, Reutersward, Philippa, Svahn, Helene Andersson, Alvesson, Helle M., Boum, Yap, II, and Alfven, Tobias

Abstract

Background Point-of-care (POC) tests have become increasingly available and more widely used in recent years. They have been of particular importance to low-income settings, enabling them with clinical capacities that had previously been limited. POC testing programs hold a great potential for significant improvement in low-income health systems. However, as most POC tests are developed in high-income countries, disengagement between developers and end-users inhibit their full potential. This study explores perceptions of POC test end-users in a low-income setting, aiming to support the development of novel POC tests for low-income countries. Methods A qualitative study was conducted in Mbarara District, Southwestern Uganda, in October 2014. Fifty health care workers were included in seven focus groups, comprising midwives, laboratory technicians, clinical and medical officers, junior and senior nurses, and medical doctors. Discussions were audio-recorded and transcribed verbatim. Transcripts were coded through a data-driven approach for qualitative content analysis. Results Nineteen different POC tests were identified as currently being in use. While participants displayed being widely accustomed to and appreciative of the use of POC tests, they also assessed the use and characteristics of current tests as imperfect. An ideal POC test was characterized as being adapted to local conditions, thoughtfully implemented in the specific health system, and capable of improving the care of patients. Tests for specific medical conditions were requested. Opinions differed with regard to the ideal distribution of POC tests in the local health system. Conclusion POC tests are commonly used and greatly appreciated in this study setting. However, there are dissatisfactions with current POC tests and their use. To maximize benefit, stakeholders need to include end-user perspectives in the development and implementation of POC tests. Insights from this study will influence our ongo

Published

2017

7. Health care workers' perceptions of point-of-care testing in a low-income country-A qualitative study in Southwestern Uganda

Author

Rasti, Reza, Nanjebe, Deborah, Karlstrom, Jonas, Muchunguzi, Charles, Mwanga-Amumpaire, Juliet, Gantelius, Jesper, Mårtensson, Andreas, Rivas, Lourdes, Galban, Francesc, Reutersward, Philippa, Svahn, Helene Andersson, Alvesson, Helle M., Boum, Yap, II, Alfven, Tobias, Rasti, Reza, Nanjebe, Deborah, Karlstrom, Jonas, Muchunguzi, Charles, Mwanga-Amumpaire, Juliet, Gantelius, Jesper, Mårtensson, Andreas, Rivas, Lourdes, Galban, Francesc, Reutersward, Philippa, Svahn, Helene Andersson, Alvesson, Helle M., Boum, Yap, II, and Alfven, Tobias

Abstract

Background Point-of-care (POC) tests have become increasingly available and more widely used in recent years. They have been of particular importance to low-income settings, enabling them with clinical capacities that had previously been limited. POC testing programs hold a great potential for significant improvement in low-income health systems. However, as most POC tests are developed in high-income countries, disengagement between developers and end-users inhibit their full potential. This study explores perceptions of POC test end-users in a low-income setting, aiming to support the development of novel POC tests for low-income countries. Methods A qualitative study was conducted in Mbarara District, Southwestern Uganda, in October 2014. Fifty health care workers were included in seven focus groups, comprising midwives, laboratory technicians, clinical and medical officers, junior and senior nurses, and medical doctors. Discussions were audio-recorded and transcribed verbatim. Transcripts were coded through a data-driven approach for qualitative content analysis. Results Nineteen different POC tests were identified as currently being in use. While participants displayed being widely accustomed to and appreciative of the use of POC tests, they also assessed the use and characteristics of current tests as imperfect. An ideal POC test was characterized as being adapted to local conditions, thoughtfully implemented in the specific health system, and capable of improving the care of patients. Tests for specific medical conditions were requested. Opinions differed with regard to the ideal distribution of POC tests in the local health system. Conclusion POC tests are commonly used and greatly appreciated in this study setting. However, there are dissatisfactions with current POC tests and their use. To maximize benefit, stakeholders need to include end-user perspectives in the development and implementation of POC tests. Insights from this study will influence our ongo

Published

2017

8. Health care workers' perceptions of point-of-care testing in a low-income country-A qualitative study in Southwestern Uganda

Author

Rasti, Reza, Nanjebe, Deborah, Karlstrom, Jonas, Muchunguzi, Charles, Mwanga-Amumpaire, Juliet, Gantelius, Jesper, Mårtensson, Andreas, Rivas, Lourdes, Galban, Francesc, Reutersward, Philippa, Svahn, Helene Andersson, Alvesson, Helle M., Boum, Yap, II, Alfven, Tobias, Rasti, Reza, Nanjebe, Deborah, Karlstrom, Jonas, Muchunguzi, Charles, Mwanga-Amumpaire, Juliet, Gantelius, Jesper, Mårtensson, Andreas, Rivas, Lourdes, Galban, Francesc, Reutersward, Philippa, Svahn, Helene Andersson, Alvesson, Helle M., Boum, Yap, II, and Alfven, Tobias

Abstract

Background Point-of-care (POC) tests have become increasingly available and more widely used in recent years. They have been of particular importance to low-income settings, enabling them with clinical capacities that had previously been limited. POC testing programs hold a great potential for significant improvement in low-income health systems. However, as most POC tests are developed in high-income countries, disengagement between developers and end-users inhibit their full potential. This study explores perceptions of POC test end-users in a low-income setting, aiming to support the development of novel POC tests for low-income countries. Methods A qualitative study was conducted in Mbarara District, Southwestern Uganda, in October 2014. Fifty health care workers were included in seven focus groups, comprising midwives, laboratory technicians, clinical and medical officers, junior and senior nurses, and medical doctors. Discussions were audio-recorded and transcribed verbatim. Transcripts were coded through a data-driven approach for qualitative content analysis. Results Nineteen different POC tests were identified as currently being in use. While participants displayed being widely accustomed to and appreciative of the use of POC tests, they also assessed the use and characteristics of current tests as imperfect. An ideal POC test was characterized as being adapted to local conditions, thoughtfully implemented in the specific health system, and capable of improving the care of patients. Tests for specific medical conditions were requested. Opinions differed with regard to the ideal distribution of POC tests in the local health system. Conclusion POC tests are commonly used and greatly appreciated in this study setting. However, there are dissatisfactions with current POC tests and their use. To maximize benefit, stakeholders need to include end-user perspectives in the development and implementation of POC tests. Insights from this study will influence our ongo

Published

2017

9. Health care workers' perceptions of point-of-care testing in a low-income country-A qualitative study in Southwestern Uganda

Author

Rasti, Reza, Nanjebe, Deborah, Karlstrom, Jonas, Muchunguzi, Charles, Mwanga-Amumpaire, Juliet, Gantelius, Jesper, Mårtensson, Andreas, Rivas, Lourdes, Galban, Francesc, Reutersward, Philippa, Svahn, Helene Andersson, Alvesson, Helle M., Boum, Yap, II, Alfven, Tobias, Rasti, Reza, Nanjebe, Deborah, Karlstrom, Jonas, Muchunguzi, Charles, Mwanga-Amumpaire, Juliet, Gantelius, Jesper, Mårtensson, Andreas, Rivas, Lourdes, Galban, Francesc, Reutersward, Philippa, Svahn, Helene Andersson, Alvesson, Helle M., Boum, Yap, II, and Alfven, Tobias

Abstract

Background Point-of-care (POC) tests have become increasingly available and more widely used in recent years. They have been of particular importance to low-income settings, enabling them with clinical capacities that had previously been limited. POC testing programs hold a great potential for significant improvement in low-income health systems. However, as most POC tests are developed in high-income countries, disengagement between developers and end-users inhibit their full potential. This study explores perceptions of POC test end-users in a low-income setting, aiming to support the development of novel POC tests for low-income countries. Methods A qualitative study was conducted in Mbarara District, Southwestern Uganda, in October 2014. Fifty health care workers were included in seven focus groups, comprising midwives, laboratory technicians, clinical and medical officers, junior and senior nurses, and medical doctors. Discussions were audio-recorded and transcribed verbatim. Transcripts were coded through a data-driven approach for qualitative content analysis. Results Nineteen different POC tests were identified as currently being in use. While participants displayed being widely accustomed to and appreciative of the use of POC tests, they also assessed the use and characteristics of current tests as imperfect. An ideal POC test was characterized as being adapted to local conditions, thoughtfully implemented in the specific health system, and capable of improving the care of patients. Tests for specific medical conditions were requested. Opinions differed with regard to the ideal distribution of POC tests in the local health system. Conclusion POC tests are commonly used and greatly appreciated in this study setting. However, there are dissatisfactions with current POC tests and their use. To maximize benefit, stakeholders need to include end-user perspectives in the development and implementation of POC tests. Insights from this study will influence our ongo

Published

2017

10. Health care workers' perceptions of point-of-care testing in a low-income country-A qualitative study in Southwestern Uganda

Author

Rasti, Reza, Nanjebe, Deborah, Karlstrom, Jonas, Muchunguzi, Charles, Mwanga-Amumpaire, Juliet, Gantelius, Jesper, Mårtensson, Andreas, Rivas, Lourdes, Galban, Francesc, Reutersward, Philippa, Svahn, Helene Andersson, Alvesson, Helle M., Boum, Yap, II, Alfven, Tobias, Rasti, Reza, Nanjebe, Deborah, Karlstrom, Jonas, Muchunguzi, Charles, Mwanga-Amumpaire, Juliet, Gantelius, Jesper, Mårtensson, Andreas, Rivas, Lourdes, Galban, Francesc, Reutersward, Philippa, Svahn, Helene Andersson, Alvesson, Helle M., Boum, Yap, II, and Alfven, Tobias

Abstract

Background Point-of-care (POC) tests have become increasingly available and more widely used in recent years. They have been of particular importance to low-income settings, enabling them with clinical capacities that had previously been limited. POC testing programs hold a great potential for significant improvement in low-income health systems. However, as most POC tests are developed in high-income countries, disengagement between developers and end-users inhibit their full potential. This study explores perceptions of POC test end-users in a low-income setting, aiming to support the development of novel POC tests for low-income countries. Methods A qualitative study was conducted in Mbarara District, Southwestern Uganda, in October 2014. Fifty health care workers were included in seven focus groups, comprising midwives, laboratory technicians, clinical and medical officers, junior and senior nurses, and medical doctors. Discussions were audio-recorded and transcribed verbatim. Transcripts were coded through a data-driven approach for qualitative content analysis. Results Nineteen different POC tests were identified as currently being in use. While participants displayed being widely accustomed to and appreciative of the use of POC tests, they also assessed the use and characteristics of current tests as imperfect. An ideal POC test was characterized as being adapted to local conditions, thoughtfully implemented in the specific health system, and capable of improving the care of patients. Tests for specific medical conditions were requested. Opinions differed with regard to the ideal distribution of POC tests in the local health system. Conclusion POC tests are commonly used and greatly appreciated in this study setting. However, there are dissatisfactions with current POC tests and their use. To maximize benefit, stakeholders need to include end-user perspectives in the development and implementation of POC tests. Insights from this study will influence our ongo

Published

2017

11. 3D Bioprinting of Tissue/Organ Models

Author

Pati, Falguni, Gantelius, Jesper, Svahn, Helene Andersson, Pati, Falguni, Gantelius, Jesper, and Svahn, Helene Andersson

Abstract

Invitro tissue/organ models are useful platforms that can facilitate systematic, repetitive, and quantitative investigations of drugs/chemicals. The primary objective when developing tissue/organ models is to reproduce physiologically relevant functions that typically require complex culture systems. Bioprinting offers exciting prospects for constructing 3D tissue/organ models, as it enables the reproducible, automated production of complex living tissues. Bioprinted tissues/organs may prove useful for screening novel compounds or predicting toxicity, as the spatial and chemical complexity inherent to native tissues/organs can be recreated. In this Review, we highlight the importance of developing 3D invitro tissue/organ models by 3D bioprinting techniques, characterization of these models for evaluating their resemblance to native tissue, and their application in the prioritization of lead candidates, toxicity testing, and as disease/tumor models., QC 20160510

Published

2016

12. A printer-free, vertical flow based, colorimetric planar bead array for point of care applications

Author

Svedberg, Gustav, Gantelius, Jesper, Svahn, Helene Andersson, Svedberg, Gustav, Gantelius, Jesper, and Svahn, Helene Andersson

Abstract

We present a novel planar bead array that utilizes fluorescent colour coding, a convenient and quick bead immobilization technique, rapid pump-driven sample delivery and colorimetric readout enabling analysis of the array using an inexpensive USB microscope or smartphone camera. The array combines high multiplexing potential with a low assay run time and point of care amenability due to low equipment requirements., QC 20161121

Published

2015

13. Micro-droplet based directed evolution outperforms conventional laboratory evolution

Author

Sjostrom, Staffan L., Huang, Mingtao, Nielsen, Jens, Joensson, Haakan N., Svahn, Helene Andersson, Sjostrom, Staffan L., Huang, Mingtao, Nielsen, Jens, Joensson, Haakan N., and Svahn, Helene Andersson

Abstract

We present droplet adaptive laboratory evolution (DrALE), a directed evolution method used to improve industrial enzyme producing microorganisms for e.g. feedstock digestion. DrALE is based linking a desired phenotype to growth rate allowing only desired cells to proliferate. Single cells are confined in microfluidic droplets to prevent the phenotype, e.g. secreted enzymes, from leaking between cells. The method was benchmarked against and found to significantly outperform conventional adaptive laboratory evolution (ALE) in enriching enzyme producing cells. It was furthermore applied to enrich a whole-genome mutated library of yeast cells for α-amylase activity.

Published

2014

14. High-throughput screening for industrial enzyme production hosts by droplet microfluidics

Author

Sjostrom, Staffan L., Bai, Yunpeng, Huang, Mingtao, Liu, Zihe, Nielsen, Jens, Jönsson, Håkan, Svahn, Helene Andersson, Sjostrom, Staffan L., Bai, Yunpeng, Huang, Mingtao, Liu, Zihe, Nielsen, Jens, Jönsson, Håkan, and Svahn, Helene Andersson

Abstract

A high-throughput method for single cell screening by microfluidic droplet sorting is applied to a whole-genome mutated yeast cell library yielding improved production hosts of secreted industrial enzymes. The sorting method is validated by enriching a yeast strain 14 times based on its α-amylase production, close to the theoretical maximum enrichment. Furthermore, a 105 member yeast cell library is screened yielding a clone with a more than 2-fold increase in α-amylase production. The increase in enzyme production results from an improvement of the cellular functions of the production host in contrast to previous droplet-based directed evolution that has focused on improving enzyme protein structure. In the workflow presented, enzyme producing single cells are encapsulated in 20 pL droplets with a fluorogenic reporter substrate. The coupling of a desired phenotype (secreted enzyme concentration) with the genotype (contained in the cell) inside a droplet enables selection of single cells with improved enzyme production capacity by droplet sorting. The platform has a throughput over 300 times higher than that of the current industry standard, an automated microtiter plate screening system. At the same time, reagent consumption for a screening experiment is decreased a million fold, greatly reducing the costs of evolutionary engineering of production strains.

Published

2014

15. Cognitive behavior therapy versus interpersonal psychotherapy for social anxiety disorder delivered via smartphone and computer : A randomized controlled trial

Author

Dagoo, Jesper, Asplund, Robert Persson, Bsenko, Helene Andersson, Hjerling, Sofia, Holmberg, Anna, Westh, Susanne, Oberg, Louise, Ljotsson, Brjann, Carlbring, Per, Furmark, Tomas, Andersson, Gerhard, Dagoo, Jesper, Asplund, Robert Persson, Bsenko, Helene Andersson, Hjerling, Sofia, Holmberg, Anna, Westh, Susanne, Oberg, Louise, Ljotsson, Brjann, Carlbring, Per, Furmark, Tomas, and Andersson, Gerhard

Abstract

In this study, a previously evaluated guided Internet-based cognitive behavior therapy for social anxiety disorder (SAD) was adapted for mobile phone administration (mCBT). The treatment was compared with a guided self-help treatment based on interpersonal psychotherapy (mIPT). The treatment platform could be accessed through smartphones, tablet computers, and standard computers. A total of 52 participants were diagnosed with SAD and randomized to either mCBT (n = 27) or mIPT (n = 25). Measures were collected at pre-treatment, during the treatment, post-treatment and 3-month follow-up. On the primary outcome measure, the Liebowitz Social Anxiety Scale - self-rated, both groups showed statistically significant improvements. However, mCBT performed significantly better than mIPT (between group Cohen's d = 0.64 in favor of mCBT). A larger proportion of the mCBT group was classified as responders at post-treatment (55.6% versus 8.0% in the mIPT group). We conclude that CBT for SAD can be delivered using modern information technology. IPT delivered as a guided self-help treatment may be less effective in this format.

Published

2014

16. Microfluidics for nano-pathophysiology

Author

Sato, Kae, Sasaki, Naoki, Svahn, Helene Andersson, Sato, Kiichi, Sato, Kae, Sasaki, Naoki, Svahn, Helene Andersson, and Sato, Kiichi

Abstract

Nanotechnology-based drug delivery systems hold promise for innovative medical treatment of cancers. While drug materials are constantly under development, there are no practical cell-based models to assess whether these materials can reach the target tissue. Recently developed microfluidic systems have revolutionized cell-based experiments. In these systems, vascular endothelial cells and interstitium are set in microchannels that mimic microvessels. Drug permeability can be assayed in these blood vessel models under fluidic conditions that mimic blood flow. In this review, we describe device fabrication, disease model development, nanoparticle permeability assays, and the potential utility of these systems in the future., QC 20141006

Published

2014

17. Cognitive behavior therapy versus interpersonal psychotherapy for social anxiety disorder delivered via smartphone and computer : A randomized controlled trial

Author

Dagoo, Jesper, Asplund, Robert Persson, Bsenko, Helene Andersson, Hjerling, Sofia, Holmberg, Anna, Westh, Susanne, Oberg, Louise, Ljotsson, Brjann, Carlbring, Per, Furmark, Tomas, Andersson, Gerhard, Dagoo, Jesper, Asplund, Robert Persson, Bsenko, Helene Andersson, Hjerling, Sofia, Holmberg, Anna, Westh, Susanne, Oberg, Louise, Ljotsson, Brjann, Carlbring, Per, Furmark, Tomas, and Andersson, Gerhard

Abstract

In this study, a previously evaluated guided Internet-based cognitive behavior therapy for social anxiety disorder (SAD) was adapted for mobile phone administration (mCBT). The treatment was compared with a guided self-help treatment based on interpersonal psychotherapy (mIPT). The treatment platform could be accessed through smartphones, tablet computers, and standard computers. A total of 52 participants were diagnosed with SAD and randomized to either mCBT (n = 27) or mIPT (n = 25). Measures were collected at pre-treatment, during the treatment, post-treatment and 3-month follow-up. On the primary outcome measure, the Liebowitz Social Anxiety Scale - self-rated, both groups showed statistically significant improvements. However, mCBT performed significantly better than mIPT (between group Cohen's d = 0.64 in favor of mCBT). A larger proportion of the mCBT group was classified as responders at post-treatment (55.6% versus 8.0% in the mIPT group). We conclude that CBT for SAD can be delivered using modern information technology. IPT delivered as a guided self-help treatment may be less effective in this format., AuthorCount:11

Published

2014

18. Microfluidic device for generating a stepwise concentration gradient on a microwell slide for cell analysis

Author

Weibull, Emilie, Matsui, Shunsuke, Sakai, Manabu, Svahn, Helene Andersson, 1000030270812, Ohashi, Toshiro, Weibull, Emilie, Matsui, Shunsuke, Sakai, Manabu, Svahn, Helene Andersson, 1000030270812, and Ohashi, Toshiro

Abstract

Understanding biomolecular gradients and their role in biological processes is essential for fully comprehending the underlying mechanisms of cells in living tissue. Conventional in vitro gradient-generating methods are unpredictable and difficult to characterize, owing to temporal and spatial fluctuations. The field of microfluidics enables complex user-defined gradients to be generated based on a detailed understanding of fluidic behavior at the lm-scale. By using microfluidic gradients created by flow, it is possible to develop rapid and dynamic stepwise concentration gradients. However, cells exposed to stepwise gradients can be perturbed by signals from neighboring cells exposed to another concentration. Hence, there is a need for a device that generates a stepwise gradient at discrete and isolated locations. Here, we present a microfluidic device for generating a stepwise concentration gradient, which utilizes a microwell slide's pre-defined compartmentalized structure to physically separate different reagent concentrations. The gradient was generated due to flow resistance in the microchannel configuration of the device, which was designed using hydraulic analogy and theoretically verified by computational fluidic dynamics simulations. The device had two reagent channels and two dilutant channels, leading to eight chambers, each containing 4 microwells. A dose-dependency assay was performed using bovine aortic endothelial cells treated with saponin. High reproducibility between experiments was confirmed by evaluating the number of living cells in a live-dead assay. Our device generates a fully mixed fluid profile using a simple microchannel configuration and could be used in various gradient studies, e.g., screening for cytostatics or antibiotics. (C) 2013 AIP Publishing LLC.

Published

2013

19. Microfluidic device for generating a stepwise concentration gradient on a microwell slide for cell analysis

Author

Weibull, Emilie, Matsui, Shunsuke, Sakai, Manabu, Svahn, Helene Andersson, Ohashi, Toshiro, Weibull, Emilie, Matsui, Shunsuke, Sakai, Manabu, Svahn, Helene Andersson, and Ohashi, Toshiro

Abstract

Understanding biomolecular gradients and their role in biological processes is essential for fully comprehending the underlying mechanisms of cells in living tissue. Conventional in vitro gradient-generating methods are unpredictable and difficult to characterize, owing to temporal and spatial fluctuations. The field of microfluidics enables complex user-defined gradients to be generated based on a detailed understanding of fluidic behavior at the lm-scale. By using microfluidic gradients created by flow, it is possible to develop rapid and dynamic stepwise concentration gradients. However, cells exposed to stepwise gradients can be perturbed by signals from neighboring cells exposed to another concentration. Hence, there is a need for a device that generates a stepwise gradient at discrete and isolated locations. Here, we present a microfluidic device for generating a stepwise concentration gradient, which utilizes a microwell slide's pre-defined compartmentalized structure to physically separate different reagent concentrations. The gradient was generated due to flow resistance in the microchannel configuration of the device, which was designed using hydraulic analogy and theoretically verified by computational fluidic dynamics simulations. The device had two reagent channels and two dilutant channels, leading to eight chambers, each containing 4 microwells. A dose-dependency assay was performed using bovine aortic endothelial cells treated with saponin. High reproducibility between experiments was confirmed by evaluating the number of living cells in a live-dead assay. Our device generates a fully mixed fluid profile using a simple microchannel configuration and could be used in various gradient studies, e.g., screening for cytostatics or antibiotics. (C) 2013 AIP Publishing LLC.

Published

2013

20. Young researchers to tackle future Grand Challenges

Author

Douagi, Anna Sjöström, Svahn, Helene Andersson, Douagi, Anna Sjöström, and Svahn, Helene Andersson

Abstract

QC 20120308

Published

2012

21. Multiplex analysis of enzyme kinetics and inhibition by droplet microfluidics using picoinjectors

Author

Sjöström, Staffan L., Jönsson, Håkan N., Svahn, Helene Andersson, Sjöström, Staffan L., Jönsson, Håkan N., and Svahn, Helene Andersson

Abstract

We present a novel microdroplet-based device for extensive characterization of the reaction kinetics of enzymeinhibitor systems in a single experiment, for the first time utilizing droplet picoinjectors for bioanalysis. This device enables the scanning of multiple inhibitors, inhibitor concentrations and substrate conditions in a single, highly time resolved experiment yielding the Michaelis constant (Km), the turnover number (Kcat) the mode of inhibition and the inhibitor enzyme binding constants (Ki, Ki). Using this device we determine Km and Kcat for β-galactosidase and the fluorogenic substrate Resorufin β-D-galactopyranoside (RBG) to 252 μM and 477 s-1, respectively. Furthermore, we examine the inhibitory effects of Phenylethyl β-D-thiogalactopyranoside (PETG) on this system., QC 20150604

Published

2012

22. Svahn, Helene Andersson

Author

Svahn, Helene Andersson and Svahn, Helene Andersson

Published

2012

23. Svahn, Helene Andersson

Author

Svahn, Helene Andersson and Svahn, Helene Andersson

Published

2012

24. What determines specific cell functions?

Author

Lundberg, Emma, Svahn, Helene Andersson, Lundberg, Emma, and Svahn, Helene Andersson

Abstract

QC 20110623

Published

2011

25. Lab on a chip technologies for bioenergy and biosustainability research

Author

Uhlén, Mathias, Svahn, Helene Andersson, Uhlén, Mathias, and Svahn, Helene Andersson

Abstract

QC 20111028

Published

2011

26. Towards high-throughput single cell/clone cultivation and analysis

Author

Lindström, Sara, Larsson, Rolf, Svahn, Helene Andersson, Lindström, Sara, Larsson, Rolf, and Svahn, Helene Andersson

Abstract

In order to better understand cellular processes and behavior, a controlled way of studying high numbers of single cells and their clone formation is greatly needed. Numerous ways of ordering single cells into arrays have previously been described, but platforms in which each cell/clone can be addressed to an exact position in the microplate, cultivated for weeks and treated separately in a high-throughput manner have until now been missing. Here, a novel microplate developed for high-throughput single cell/clone cultivation and analysis is presented. Rapid single cell seeding into microwells, using conventional flow cytometry, allows several thousands of single cells to be cultivated, short-term (72 h) or long-term (10-14 days), and analyzed individually. By controlled sorting of individual cells to predefined locations in the microplate, analysis of single cell heterogeneity and clonogenic properties related to drug sensitivity can be accomplished. Additionally, the platform requires remarkably low number of cells, a major advantage when screening limited amounts of patient cell samples. By seeding single cells into the microplate it is possible to analyze the cells for over 14 generations, ending up with more than 10 000 cells in each well. Described here is a proof-of-concept on compartmentalization and cultivation of thousands of individual cells enabling heterogeneity analysis of various cells/clones and their response to different drugs.

Published

2008