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1. Dynamically upregulated mast cell CPA3 patterns in chronic obstructive pulmonary disease and idiopathic pulmonary fibrosis

Author

Premkumar Siddhuraj, Jimmie Jönsson, Manar Alyamani, Pavan Prabhala, Mattias Magnusson, Sandra Lindstedt, and Jonas S. Erjefält

Subjects
mast cells, carboxypeptidase A3, lung, COPD, tryptase, Immunologic diseases. Allergy, RC581-607
Abstract

BackgroundThe mast cell-specific metalloprotease CPA3 has been given important roles in lung tissue homeostasis and disease pathogenesis. However, the dynamics and spatial distribution of mast cell CPA3 expression in lung diseases remain unknown.MethodsUsing a histology-based approach for quantitative spatial decoding of mRNA and protein single cell, this study investigates the dynamics of CPA3 expression across mast cells residing in lungs from control subjects and patients with severe chronic obstructive pulmonary disease (COPD) or idiopathic lung fibrosis (IPF).ResultsMast cells in COPD lungs had an anatomically widespread increase of CPA3 mRNA (bronchioles p < 0.001, pulmonary vessels p < 0.01, and alveolar parenchyma p < 0.01) compared to controls, while granule-stored CPA3 protein was unaltered. IPF lungs had a significant upregulation of both mast cell density, CPA3 mRNA (p < 0.001) and protein (p < 0.05), in the fibrotic alveolar tissue. Spatial expression maps revealed altered mast cell mRNA/protein quotients in lung areas subjected to disease-relevant histopathological alterations. Elevated CPA3 mRNA also correlated to lung tissue eosinophils, CD3 T cells, and declined lung function. Single-cell RNA sequencing of bronchial mast cells confirmed CPA3 as a top expressed gene with potential links to both inflammatory and protective markers.ConclusionThis study shows that lung tissue mast cell populations in COPD and IPF lungs have spatially complex and markedly upregulated CPA3 expression profiles that correlate with immunopathological alterations and lung function. Given the proposed roles of CPA3 in tissue homeostasis, remodeling, and inflammation, these alterations are likely to have clinical consequences.

Published
2022
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3. Small Molecule Screening of Primary Human Acute Myeloid Leukemia Using Co-culture and Multiplexed FACS Analysis

Author

Aurelie Baudet, Simon Hultmark, Fredrik Ek, and Mattias Magnusson

Subjects
Biology (General), QH301-705.5
Abstract

Ex vivo culture of primary acute myeloid leukemia (AML) cells is notoriously difficult due to spontaneous differentiation and cell death, which hinders mechanistic and translational studies. To overcome this bottleneck, we have implemented a co-culture system, where the OP9-M2 stromal cells support the growth, but most notably limit the differentiation of primary AML cells, thus allowing for mechanistic studies in vitro. Additionally, the co-culture on OP9-M2 stromal is superior in preserving surface marker expression of primary (adult and pediatric) AML cells in comparison to stroma-free culture. Thus, by combining the co-culture with multicolor, high-throughput FACS, we can evaluate the effect of hundreds of small molecules on multi-parametric processes including: cell survival, stemness (leukemic stem cells), and myeloid differentiation on the primary AML cells at a single-cell level. This method streamlines the identification of potential therapeutic agents, but also facilitates combinatorial screening aiming, for instance, at dissecting the regulatory pathways in a patient-specific manner.Graphic abstract: Schematic representation of the ex vivo small molecule screening of primary human acute myeloid leukemia. Irradiated, sub-confluent OP9-M2 stromal cells are plated in half-area 96 wells plates 4–16 h prior to adding primary AML cells. Compounds are added 36–48 h later and effects on cell number, leukemic stem cell population, and myeloid differentiation are quantifed by FACS after 4 days of treatment.

Published
2022
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4. A validated single-cell-based strategy to identify diagnostic and therapeutic targets in complex diseases

Author

Danuta R. Gawel, Jordi Serra-Musach, Sandra Lilja, Jesper Aagesen, Alex Arenas, Bengt Asking, Malin Bengnér, Janne Björkander, Sophie Biggs, Jan Ernerudh, Henrik Hjortswang, Jan-Erik Karlsson, Mattias Köpsen, Eun Jung Lee, Antonio Lentini, Xinxiu Li, Mattias Magnusson, David Martínez-Enguita, Andreas Matussek, Colm E. Nestor, Samuel Schäfer, Oliver Seifert, Ceylan Sonmez, Henrik Stjernman, Andreas Tjärnberg, Simon Wu, Karin Åkesson, Alex K. Shalek, Margaretha Stenmarker, Huan Zhang, Mika Gustafsson, and Mikael Benson

Subjects
Network tools, scRNA-seq, Biomarker and drug discovery, Medicine, Genetics, QH426-470
Abstract

Abstract Background Genomic medicine has paved the way for identifying biomarkers and therapeutically actionable targets for complex diseases, but is complicated by the involvement of thousands of variably expressed genes across multiple cell types. Single-cell RNA-sequencing study (scRNA-seq) allows the characterization of such complex changes in whole organs. Methods The study is based on applying network tools to organize and analyze scRNA-seq data from a mouse model of arthritis and human rheumatoid arthritis, in order to find diagnostic biomarkers and therapeutic targets. Diagnostic validation studies were performed using expression profiling data and potential protein biomarkers from prospective clinical studies of 13 diseases. A candidate drug was examined by a treatment study of a mouse model of arthritis, using phenotypic, immunohistochemical, and cellular analyses as read-outs. Results We performed the first systematic analysis of pathways, potential biomarkers, and drug targets in scRNA-seq data from a complex disease, starting with inflamed joints and lymph nodes from a mouse model of arthritis. We found the involvement of hundreds of pathways, biomarkers, and drug targets that differed greatly between cell types. Analyses of scRNA-seq and GWAS data from human rheumatoid arthritis (RA) supported a similar dispersion of pathogenic mechanisms in different cell types. Thus, systems-level approaches to prioritize biomarkers and drugs are needed. Here, we present a prioritization strategy that is based on constructing network models of disease-associated cell types and interactions using scRNA-seq data from our mouse model of arthritis, as well as human RA, which we term multicellular disease models (MCDMs). We find that the network centrality of MCDM cell types correlates with the enrichment of genes harboring genetic variants associated with RA and thus could potentially be used to prioritize cell types and genes for diagnostics and therapeutics. We validated this hypothesis in a large-scale study of patients with 13 different autoimmune, allergic, infectious, malignant, endocrine, metabolic, and cardiovascular diseases, as well as a therapeutic study of the mouse arthritis model. Conclusions Overall, our results support that our strategy has the potential to help prioritize diagnostic and therapeutic targets in human disease.

Published
2019
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5. Bone Erosions Detected by Ultrasound Are Prognostic for Clinical Arthritis Development in Patients With ACPA and Musculoskeletal Pain

Author

Michael Ziegelasch, Emma Eloff, Hilde B. Hammer, Jan Cedergren, Klara Martinsson, Åsa Reckner, Thomas Skogh, Mattias Magnusson, and Alf Kastbom

Subjects
anti-citrullinated protein antibodies, rheumatoid arthritis, ultrasound, musculoskeletal pain, erosions, clinical arthritis, Medicine (General), R5-920
Abstract

Anti-citrullinated protein antibodies (ACPA) often precede onset of rheumatoid arthritis (RA) by years, and there is an urgent clinical need for predictors of arthritis development among such at-risk patients. This study assesses the prognostic value of ultrasound for arthritis development among ACPA-positive patients with musculoskeletal pain. We prospectively followed 82 ACPA-positive patients without clinical signs of arthritis at baseline. Ultrasound at baseline assessed synovial hypertrophy, inflammatory activity by power Doppler, and erosions in small joints of hands and feet. We applied Cox regression analyses to examine associations with clinical arthritis development during follow-up (median, 69 months; range, 24–90 months). We also compared the ultrasound findings among the patients to a control group of 100 blood donors without musculoskeletal pain. Clinical arthritis developed in 39/82 patients (48%) after a median of 6 months (range, 1–71 months). One or more ultrasound erosions occurred in 13/82 patients (16%), with none in control subjects (p < 0.001). Clinical arthritis development was more common among patients with baseline ultrasound erosions than those without (77 vs. 42%, p = 0.032), and remained significant in a multivariable Cox regression analysis that included previously described prognostic factors (HR 3.9, 95% CI 1.6–9.4, p = 0.003). Ultrasound-detected tenosynovitis was more frequent among the patients and associated with clinical arthritis development in a univariable analysis (HR 2.5, 95% CI 1.1–5.7, p = 0.031), but did not remain statistically significant in multivariable analysis. Thus, bone erosions detected by ultrasound are independent predictors of clinical arthritis development in an ACPA-positive at-risk population.Trial Registration: Regional Ethics Committee in Linköping, Sweden, Dnr M220-09. Registered 16 December 2009, https://etikprovningsmyndigheten.se/.

Published
2021
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6. Ciliated (FOXJ1+) Cells Display Reduced Ferritin Light Chain in the Airways of Idiopathic Pulmonary Fibrosis Patients

Author

Sofia C. Wijk, Pavan Prabhala, Anna Löfdahl, Annika Nybom, Stefan Lang, Hans Brunnström, Leif Bjermer, Gunilla Westergren-Thorsson, and Mattias Magnusson

Subjects
IPF, ciliated cells, basal cells, single-cell RNA sequencing, immunofluorescence, ferritin light chain, Cytology, QH573-671
Abstract

Cell-based therapies hold great promise in re-establishing organ function for many diseases, including untreatable lung diseases such as idiopathic pulmonary fibrosis (IPF). However, many hurdles still remain, in part due to our lack of knowledge about the disease-driving mechanisms that may affect the cellular niche and thereby possibly hinder the function of any transplanted cells by imposing the disease phenotype onto the newly generated progeny. Recent findings have demonstrated increased ciliation of lung cells from IPF patients, but how this affects ciliated cell function and the airway milieu is not well-known. Here, we performed single-cell RNA sequencing on primary ciliated (FOXJ1+) cells isolated from IPF patients and from healthy control donors. The sequencing identified multiple biological processes, such as cilium morphogenesis and cell signaling, that were significantly changed between IPF and healthy ciliated cells. Ferritin light chain (FTL) was downregulated in IPF, which suggests that iron metabolism may be affected in the IPF ciliated cells. The RNA expression was confirmed at the protein level with histological localization in lung tissue, prompting future functional assays to reveal the potential role of FTL. Taken together, our data demonstrate the importance of careful analyses in pure cell populations to better understand the IPF disease mechanism.

Published
2022
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7. Stem Cells, Cell Therapies, and Bioengineering in Lung Biology and Disease 2019

Author

Darcy E. Wagner, Laertis Ikonomou, Sarah E. Gilpin, Chelsea M. Magin, Fernanda Cruz, Allison Greaney, Mattias Magnusson, Ya-Wen Chen, Brian Davis, Kim Vanuytsel, Sara Rolandsson Enes, Anna Krasnodembskaya, Mareike Lehmann, Gunilla Westergren-Thorsson, John Stegmayr, Hani N. Alsafadi, Evan T. Hoffman, Daniel J. Weiss, and Amy L. Ryan

Subjects
Medicine
Abstract

A workshop entitled “Stem Cells, Cell Therapies and Bioengineering in Lung Biology and Diseases” was hosted by the University of Vermont Larner College of Medicine in collaboration with the National Heart, Lung and Blood Institute, the Alpha-1 Foundation, the Cystic Fibrosis Foundation, the International Society for Cell and Gene Therapy and the Pulmonary Fibrosis Foundation. The event was held from July 15 to 18, 2019 at the University of Vermont, Burlington, Vermont. The objectives of the conference were to review and discuss the current status of the following active areas of research: 1) technological advancements in the analysis and visualisation of lung stem and progenitor cells; 2) evaluation of lung stem and progenitor cells in the context of their interactions with the niche; 3) progress toward the application and delivery of stem and progenitor cells for the treatment of lung diseases such as cystic fibrosis; 4) progress in induced pluripotent stem cell models and application for disease modelling; and 5) the emerging roles of cell therapy and extracellular vesicles in immunomodulation of the lung. This selection of topics represents some of the most dynamic research areas in which incredible progress continues to be made. The workshop also included active discussion on the regulation and commercialisation of regenerative medicine products and concluded with an open discussion to set priorities and recommendations for future research directions in basic and translation lung biology.

Published
2020
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8. Combinatorial molecule screening identified a novel diterpene and the BET inhibitor CPI-203 as differentiation inducers of primary acute myeloid leukemia cells

Author

Simon Hultmark, Aurélie Baudet, Ludwig Schmiderer, Pavan Prabhala, Sara Palma-Tortosa, Carl Sandén, Thoas Fioretos, Rajkumar Sasidharan, Christer Larsson, Sören Lehmann, Gunnar Juliusson, Fredrik Ek, and Mattias Magnusson

Subjects
Diseases of the blood and blood-forming organs, RC633-647.5
Abstract

Combination treatment has proven effective for patients with acute promyelocytic leukemia, exemplifying the importance of therapy targeting multiple components of oncogenic regulation for a successful outcome. However, recent studies have shown that the mutational complexity of acute myeloid leukemia (AML) precludes the translation of molecular targeting into clinical success. Here, as a complement to genetic profiling, we used unbiased, combinatorial in vitro drug screening to identify pathways that drive AML and to develop personalized combinatorial treatments. First, we screened 513 natural compounds on primary AML cells and identified a novel diterpene (H4) that preferentially induced differentiation of FLT3 wild-type AML, while FLT3-ITD/mutations conferred resistance. The samples responding to H4, displayed increased expression of myeloid markers, a clear decrease in the nuclear-cytoplasmic ratio and the potential of re-activation of the monocytic transcriptional program reducing leukemia propagation in vivo. By combinatorial screening using H4 and molecules with defined targets, we demonstrated that H4 induces differentiation by the activation of the protein kinase C (PKC) signaling pathway, and in line with this, activates PKC phosphorylation and translocation of PKC to the cell membrane. Furthermore, the combinatorial screening identified a bromo- and extra-terminal domain (BET) inhibitor that could further improve H4-dependent leukemic differentiation in FLT3 wild-type monocytic AML. These findings illustrate the value of an unbiased, multiplex screening platform for developing combinatorial therapeutic approaches for AML.

Published
2020
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9. Hepatic Leukemia Factor Maintains Quiescence of Hematopoietic Stem Cells and Protects the Stem Cell Pool during Regeneration

Author

Karolina Komorowska, Alexander Doyle, Martin Wahlestedt, Agatheeswaran Subramaniam, Shubhranshu Debnath, Jun Chen, Shamit Soneji, Ben Van Handel, Hanna K.A. Mikkola, Kenichi Miharada, David Bryder, Jonas Larsson, and Mattias Magnusson

Subjects
Biology (General), QH301-705.5
Abstract

Summary: The transcription factor hepatic leukemia factor (HLF) is strongly expressed in hematopoietic stem cells (HSCs) and is thought to influence both HSC self-renewal and leukemogenesis. However, the physiological role of HLF in hematopoiesis and HSC function is unclear. Here, we report that mice lacking Hlf are viable with essentially normal hematopoietic parameters, including an intact HSC pool during steady-state hematopoiesis. In contrast, when challenged through transplantation, Hlf-deficient HSCs showed an impaired ability to reconstitute hematopoiesis and became gradually exhausted upon serial transplantation. Transcriptional profiling of Hlf-deficient HSCs revealed changes associated with enhanced cellular activation, and cell-cycle analysis demonstrated a significant reduction of quiescent HSCs. Accordingly, toxic insults targeting dividing cells completely eradicated the HSC pool in Hlf-deficient mice. In summary, our findings point to HLF as a critical regulator of HSC quiescence and as an essential factor for maintaining the HSC pool during regeneration. : Komorowska et al. report that the transcription factor HLF is required to maintain hematopoietic stem cell (HSC) function during regeneration. Moreover, Hlf-deficient HSCs are less quiescent. In accordance with this, toxic insults targeting dividing cells completely eradicate the HSC pool in Hlf-deficient mice. Keywords: HSC, transcription factor, HLF, quiescence, self-renewal, cell cycle, reconstitution, transplantation, 5FU, stress

Published
2017
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10. Critical Modulation of Hematopoietic Lineage Fate by Hepatic Leukemia Factor

Author

Martin Wahlestedt, Vasileios Ladopoulos, Isabel Hidalgo, Manuel Sanchez Castillo, Rebecca Hannah, Petter Säwén, Haixia Wan, Monika Dudenhöffer-Pfeifer, Mattias Magnusson, Gudmundur L. Norddahl, Berthold Göttgens, and David Bryder

Subjects
hematopoiesis, lineage commitment, gene regulation, transcription factor, lymphopoiesis, myelopoiesis, Biology (General), QH301-705.5
Abstract

A gradual restriction in lineage potential of multipotent stem/progenitor cells is a hallmark of adult hematopoiesis, but the underlying molecular events governing these processes remain incompletely understood. Here, we identified robust expression of the leukemia-associated transcription factor hepatic leukemia factor (Hlf) in normal multipotent hematopoietic progenitors, which was rapidly downregulated upon differentiation. Interference with its normal downregulation revealed Hlf as a strong negative regulator of lymphoid development, while remaining compatible with myeloid fates. Reciprocally, we observed rapid lymphoid commitment upon reduced Hlf activity. The arising phenotypes resulted from Hlf binding to active enhancers of myeloid-competent cells, transcriptional induction of myeloid, and ablation of lymphoid gene programs, with Hlf induction of nuclear factor I C (Nfic) as a functionally relevant target gene. Thereby, our studies establish Hlf as a key regulator of the earliest lineage-commitment events at the transition from multipotency to lineage-restricted progeny, with implications for both normal and malignant hematopoiesis.

Published
2017
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11. Uridine Ameliorates Dextran Sulfate Sodium (DSS)-Induced Colitis in Mice

Author

Manish Kumar Jeengar, Dinesh Thummuri, Mattias Magnusson, V. G. M. Naidu, and Srinivas Uppugunduri

Subjects
Medicine, Science
Abstract

Abstract Uridine, one of the four components that comprise RNA, has attracted attention as a novel therapeutic modulator of inflammation. However, very little is known about its effect on intestinal inflammation. The aim of the present study was to investigate the potential protective effect of intracolonic administered uridine against DSS induced colitis in male C57BL/6 mice. Intracolonic instillation of 3 doses of uridine 1 mg/Kg (lower dose), 5 mg/Kg (medium dose), and 10 mg/Kg (higher dose) in saline was performed daily. Uridine at medium and high dose significantly reduced the severity of colitis (DAI score) and alleviated the macroscopic and microscopic signs of the disease. The levels of proinflammatory cytokines IL-6, IL-1β and TNF in serum as well as mRNA expression in colon were significantly reduced in the uridine treated groups. Moreover, colon tissue myloperoxidase activities, protein expression of IL-6, TNF- α, COX-2, P-NFkB and P-Ikk-βα in the colon tissues were significantly reduced in medium and high dose groups. These findings demonstrated that local administration of uridine alleviated experimental colitis in male C57BL/6 mice accompanied by the inhibition of neutrophil infiltration and NF-κB signaling. Thus, Uridine may be a promising candidate for future use in the treatment of inflammatory bowel disease.

Published
2017
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13. Hypoxia-Induced Alpha-Globin Expression in Syncytiotrophoblasts Mimics the Pattern Observed in Preeclamptic Placentas

Author

Zahra Masoumi, Lena Erlandsson, Eva Hansson, Mattias Magnusson, Eva Mezey, and Stefan R. Hansson

Subjects
preeclampsia, placenta, erythropoiesis, oxidative stress, non-erythroid globin, syncytiotrophoblast, Biology (General), QH301-705.5, Chemistry, QD1-999
Abstract

Preeclampsia (PE) is a pregnancy disorder associated with placental dysfunction and elevated fetal hemoglobin (HbF). Early in pregnancy the placenta harbors hematopoietic stem and progenitor cells (HSPCs) and is an extramedullary source of erythropoiesis. However, globin expression is not unique to erythroid cells and can be triggered by hypoxia. To investigate the role of the placenta in increasing globin levels previously reported in PE, flow cytometry, histological and immunostaining and in situ analyses were used on placenta samples and ex vivo explant cultures. Our results indicated that in PE pregnancies, placental HSPC homing and erythropoiesis were not affected. Non-erythroid alpha-globin mRNA and protein, but not gamma-globin, were detected in syncytiotrophoblasts and stroma of PE placenta samples. Similarly, alpha-globin protein and mRNA were upregulated in normal placenta explants cultured in hypoxia. The upregulation was independent of HIF1 and NRF2, the two main candidates of globin transcription in non-erythroid cells. Our study is the first to demonstrate alpha-globin mRNA expression in syncytiotrophoblasts in PE, induced by hypoxia. However, gamma-globin was only expressed in erythrocytes. We conclude that alpha-globin, but not HbF, is expressed in placental syncytiotrophoblasts in PE and may contribute to the pathology of the disease.

Published
2021
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14. Correction to: A validated single-cell-based strategy to identify diagnostic and therapeutic targets in complex diseases

Author

Danuta R. Gawel, Jordi Serra-Musach, Sandra Lilja, Jesper Aagesen, Alex Arenas, Bengt Asking, Malin Bengnér, Janne Björkander, Sophie Biggs, Jan Ernerudh, Henrik Hjortswang, Jan-Erik Karlsson, Mattias Köpsen, Eun Jung Lee, Antonio Lentini, Xinxiu Li, Mattias Magnusson, David Martínez-Enguita, Andreas Matussek, Colm E. Nestor, Samuel Schäfer, Oliver Seifert, Ceylan Sonmez, Henrik Stjernman, Andreas Tjärnberg, Simon Wu, Karin Åkesson, Alex K. Shalek, Margaretha Stenmarker, Huan Zhang, Mika Gustafsson, and Mikael Benson

Subjects
Medicine, Genetics, QH426-470
Abstract

An amendment to this paper has been published and can be accessed via the original article.

Published
2020
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15. Transient inhibition of NF-κB signaling enhances ex vivo propagation of human hematopoietic stem cells

Author

Mehrnaz Safaee Talkhoncheh, Agatheeswaran Subramaniam, Mattias Magnusson, Praveen Kumar, Jonas Larsson, and Aurélie Baudet

Subjects
Diseases of the blood and blood-forming organs, RC633-647.5
Abstract

Despite extensive studies, defining culture conditions in which hematopoietic stem cells can be expanded ex vivo has been challenging. Here we show that chemical inhibition of the NF-κB signaling pathway leads to a significant improvement of hematopoietic stem cell function from ex vivo cultured human umbilical cord blood derived CD34+ cells. We found a distinct peak of activation of the NF-κB pathway shortly after cells were put in culture, and consequently inhibition of the pathway was both necessary and sufficient during the first 24 hours of culture where it reduced the levels of several pro-inflammatory cytokines. Taken together, NF-κB pathway inhibition facilitates propagation of hematopoietic stem cells in culture and may complement other strategies for hematopoietic stem cell expansion by relieving stress signals that are induced as an immediate response to culture initiation.

Published
2018
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16. Regulatory T-Cells Mediate IFN-α-Induced Resistance against Antigen-Induced Arthritis

Author

Sudeep Chenna Narendra, Jaya Prakash Chalise, Sophie Biggs, Ulrich Kalinke, and Mattias Magnusson

Subjects
interferon-alpha, regulatory T-cells, experimental arthritis, indoleamine 2,3-dioxygenase, kynurenine, Immunologic diseases. Allergy, RC581-607
Abstract

ObjectiveCD4+FoxP3+CD25+ regulatory T-cells (Tregs) are important for preventing tissue destruction. Here, we investigate the role of Tregs for protection against experimental arthritis by IFN-α.MethodsArthritis was triggered by intra-articular injection of methylated bovine serum albumin (mBSA) in wild-type mice, Foxp3DTReGFP+/− mice [allowing selective depletion of Tregs by diphtheria toxin (DT)] and CD4-Cre+/− IFNA1R flox/flox mice (devoid of IFNAR signaling in T-cells) earlier immunized with mBSA, with or without treatment with IFN-α or the indoleamine 2,3-dioxygenase (IDO)-metabolite kynurenine. Tregs were depleted in DT-treated Foxp3DTReGFP+/− mice and enumerated by FoxP3 staining. Suppressive capacity of FACS-sorted CD25+highCD4+ Tregs was tested in vivo by adoptive transfer and ex vivo in cocultures with antigen-stimulated CFSE-stained T-responder (CD25−CD4+) cells. IDO was inhibited by 1-methyl tryptophan.ResultsBoth control mice and mice devoid of IFNAR-signaling in T helper cells were protected from arthritis by IFN-α. Depletion of Tregs in the arthritis phase, but not at immunization, abolished the protective effect of IFN-α and kynurenine against arthritis. IFN-α increased the number of Tregs in ex vivo cultures upon antigen recall stimulation but not in naïve cells. IFN-α also increased the suppressive capacity of Tregs against mBSA-induced T-responder cell proliferation ex vivo and against arthritis when adoptively transferred. The increased suppressive activity against proliferation conferred by IFN-α was clearly reduced by in vivo inhibition of IDO at immunization, which also abolished the protective effect of IFN-α against arthritis.ConclusionBy activating IDO during antigen sensitization, IFN-α activates Tregs, which prevent arthritis triggered by antigen rechallenge. This is one way by which IFN-α suppresses inflammation.

Published
2018
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17. Preeclampsia is Associated with Sex-Specific Transcriptional and Proteomic Changes in Fetal Erythroid Cells

Author

Zahra Masoumi, Gregory E. Maes, Koen Herten, Álvaro Cortés-Calabuig, Abdul Ghani Alattar, Eva Hanson, Lena Erlandsson, Eva Mezey, Mattias Magnusson, Joris R Vermeesch, Mary Familari, and Stefan R Hansson

Subjects
preeclampsia, hematopoietic stem/progenitor cells, umbilical cord blood, erythropoiesis, Biology (General), QH301-705.5, Chemistry, QD1-999
Abstract

Preeclampsia (PE) has been associated with placental dysfunction, resulting in fetal hypoxia, accelerated erythropoiesis, and increased erythroblast count in the umbilical cord blood (UCB). Although the detailed effects remain unknown, placental dysfunction can also cause inflammation, nutritional, and oxidative stress in the fetus that can affect erythropoiesis. Here, we compared the expression of surface adhesion molecules and the erythroid differentiation capacity of UCB hematopoietic stem/progenitor cells (HSPCs), UCB erythroid profiles along with the transcriptome and proteome of these cells between male and female fetuses from PE and normotensive pregnancies. While no significant differences were observed in UCB HSPC migration/homing and in vitro erythroid colony differentiation, the UCB HSPC transcriptome and the proteomic profile of the in vitro differentiated erythroid cells differed between PE vs. normotensive samples. Accordingly, despite the absence of significant differences in the UCB erythroid populations in male or female fetuses from PE or normotensive pregnancies, transcriptional changes were observed during erythropoiesis, particularly affecting male fetuses. Pathway analysis suggested deregulation in the mammalian target of rapamycin complex 1/AMP-activated protein kinase (mTORC1/AMPK) signaling pathways controlling cell cycle, differentiation, and protein synthesis. These results associate PE with transcriptional and proteomic changes in fetal HSPCs and erythroid cells that may underlie the higher erythroblast count in the UCB in PE.

Published
2019
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18. Local but Not Systemic Administration of Uridine Prevents Development of Antigen-Induced Arthritis.

Author

Sudeep Chenna Narendra, Jaya Prakash Chalise, Mattias Magnusson, and Srinivas Uppugunduri

Subjects
Medicine, Science
Abstract

Uridine has earlier been show to down modulate inflammation in models of lung inflammation. The aim of this study was to evaluate the anti-inflammatory effect of uridine in arthritis.Arthritis was induced by intra-articular injection of mBSA in the knee of NMRI mice pre-immunized with mBSA. Uridine was either administered locally by direct injection into the knee joint or systemically. Systemic treatment included repeated injections or implantation of a pellet continuously releasing uridine during the entire experimental procedure. Anti-mBSA specific immune responses were determined by ELISA and cell proliferation and serum cytokine levels were determined by Luminex. Immunohistochemistry was used to identify cells, study expression of cytokines and adhesion molecules in the joint.Local administration of 25-100 mg/kg uridine at the time of arthritis onset clearly prevented development of joint inflammation. In contrast, systemic administration of uridine (max 1.5 mg uridine per day) did not prevent development of arthritis. Protection against arthritis by local administration of uridine did not affect the anti-mBSA specific immune response and did not prevent the rise in serum levels of pro-inflammatory cytokines associated with the triggering of arthritis. In contrast, local uridine treatment efficiently inhibited synovial expression of ICAM-1 and CD18, local cytokine production and recruitment of leukocytes to the synovium.Local, but not systemic administration of uridine efficiently prevented development of antigen-induced arthritis. The protective effect did not involve alteration of systemic immunity to mBSA but clearly involved inhibition of synovial expression of adhesion molecules, decreased TNF and IL-6 production and prevention of leukocyte extravasation. Further, uridine is a small, inexpensive molecule and may thus be a new therapeutic option to treat joint inflammation in RA.

Published
2015
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19. Expansion on stromal cells preserves the undifferentiated state of human hematopoietic stem cells despite compromised reconstitution ability.

Author

Mattias Magnusson, Maria I Sierra, Rajkumar Sasidharan, Sacha L Prashad, Melissa Romero, Pamela Saarikoski, Ben Van Handel, Andy Huang, Xinmin Li, and Hanna K A Mikkola

Subjects
Medicine, Science
Abstract

Lack of HLA-matched hematopoietic stem cells (HSC) limits the number of patients with life-threatening blood disorders that can be treated by HSC transplantation. So far, insufficient understanding of the regulatory mechanisms governing human HSC has precluded the development of effective protocols for culturing HSC for therapeutic use and molecular studies. We defined a culture system using OP9M2 mesenchymal stem cell (MSC) stroma that protects human hematopoietic stem/progenitor cells (HSPC) from differentiation and apoptosis. In addition, it facilitates a dramatic expansion of multipotent progenitors that retain the immunophenotype (CD34+CD38-CD90+) characteristic of human HSPC and proliferative potential over several weeks in culture. In contrast, transplantable HSC could be maintained, but not significantly expanded, during 2-week culture. Temporal analysis of the transcriptome of the ex vivo expanded CD34+CD38-CD90+ cells documented remarkable stability of most transcriptional regulators known to govern the undifferentiated HSC state. Nevertheless, it revealed dynamic fluctuations in transcriptional programs that associate with HSC behavior and may compromise HSC function, such as dysregulation of PBX1 regulated genetic networks. This culture system serves now as a platform for modeling human multilineage hematopoietic stem/progenitor cell hierarchy and studying the complex regulation of HSC identity and function required for successful ex vivo expansion of transplantable HSC.

Published
2013
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20. Intra-articular fms-like tyrosine kinase 3 ligand expression is a driving force in induction and progression of arthritis.

Author

Mats Dehlin, Maria Bokarewa, Robert Rottapel, Simon J Foster, Mattias Magnusson, Leif E Dahlberg, and Andrej Tarkowski

Subjects
Medicine, Science
Abstract

BACKGROUND: One of the hallmarks of rheumatoid arthritis (RA) is hyperplasia and inflammation of the synovial tissue being characterized by in situ occurrence of highly differentiated leukocytes. Fms-like tyrosine kinase 3 (Flt3) has a crucial role in hematopoiesis, regulation of cell proliferation, differentiation and apoptosis. Typically, Flt3 is expressed on early myeloid and lymphoid progenitors and is activated by its soluble ligand (Flt3-L). The highly differentiated cellular pattern in the synovium of the RA patients made us hypothesize that Flt3-L, with its ability to induce proliferation and differentiation, could be of importance in induction and/or progression of arthritis. METHODOLOGY/PRINCIPAL FINDINGS: To investigate occurrence of Flt3-L in RA we have measured its levels in matched serum and synovial fluid samples from 130 patients and 107 controls. To analyse the pro-inflammatory role of Flt3-L, we continuously overexpressed this protein locally in healthy mouse joints using homologous B-cell line transfected with Flt3-L gene. Additionally, recombinant Flt3-L was instillated intra-articularly in combination with peptidoglycans, a Toll Like Receptor 2-ligand with stong arthritogenic properties. Our results show significantly higher levels of Flt3-L in the synovial fluid as compared to serum levels in RA subjects (p = 0.0001). In addition, RA synovial fluid levels of Flt-3-L were significantly higher than these obtained from synovial fluids originating from non-inflammatory joint diseases (p = 0.022). Intra-articular administration of B-cell line transfected with Flt3-L gene resulted in highly erosive arthritis while inoculation of the same B-cell line without hyperexpression of Flt3-L did not induce erosivity and only in a minority of cases caused synovial proliferation! Flt3-ligand potentiated peptidoglycan induced arthritis as compared to mice injected with peptidoglycan alone (p

Published
2008
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21. Stem cells, cell therapies, and bioengineering in lung biology and disease 2021

Author

Laertis Ikonomou, Mattias Magnusson, Ruben Dries, Erica L. Herzog, Robert E. Hynds, Zea Borok, Jin-Ah Park, Steven Skolasinski, Janette K. Burgess, Leigh Turner, Sarah M. Mojarad, John E. Mahoney, Thomas Lynch, Mareike Lehmann, Victor J. Thannickal, Jamie L. Hook, Andrew E. Vaughan, Evan T. Hoffman, Daniel J. Weiss, and Amy L. Ryan

Subjects
Pulmonary and Respiratory Medicine, Physiology, Physiology (medical), Induced Pluripotent Stem Cells, COVID-19, Humans, Bioengineering, Cell Biology, Extracellular Matrix, Lung Regeneration, Pluripotent Stem Cells, Proteomics, Biology, Lung, Pandemics
Abstract

The 9th biennial conference titled “Stem Cells, Cell Therapies, and Bioengineering in Lung Biology and Diseases” was hosted virtually, due to the ongoing COVID-19 pandemic, in collaboration with the University of Vermont Larner College of Medicine, the National Heart, Lung, and Blood Institute, the Alpha-1 Foundation, the Cystic Fibrosis Foundation, and the International Society for Cell & Gene Therapy. The event was held from July 12th through 15th, 2021 with a pre-conference workshop held on July 9th. As in previous years, the objectives remained to review and discuss the status of active research areas involving stem cells (SCs), cellular therapeutics, and bioengineering as they relate to the human lung. Topics included 1) technological advancements in the in situ analysis of lung tissues, 2) new insights into stem cell signaling and plasticity in lung remodeling and regeneration, 3) the impact of extracellular matrix in stem cell regulation and airway engineering in lung regeneration, 4) differentiating and delivering stem cell therapeutics to the lung, 5) regeneration in response to viral infection, and 6) ethical development of cell-based treatments for lung diseases. This selection of topics represents some of the most dynamic and current research areas in lung biology. The virtual workshop included active discussion on state-of-the-art methods relating to the core features of the 2021 conference, including in situ proteomics, lung-on-chip, induced pluripotent stem cell (iPSC)-airway differentiation, and light sheet microscopy. The conference concluded with an open discussion to suggest funding priorities and recommendations for future research directions in basic and translational lung biology.

Published
2022

23. Human Primary Airway Basal Cells Display a Continuum of Molecular Phases from Health to Disease in Chronic Obstructive Pulmonary Disease

Author

Barbora Michaliková, Mikael Sommarin, Leif Bjermer, Sofia C Wijk, Sandra Lindstedt, Gunilla Westergren Thorsson, Nicholas D. Leigh, Karina Kanzenbach, Mattias Magnusson, Alexander Doyle, Stefan Lang, Ellen Tufvesson, Pavan Prabhala, and Göran Karlsson

Subjects
0301 basic medicine, Pulmonary and Respiratory Medicine, education.field_of_study, medicine.diagnostic_test, Clinical Biochemistry, Cell, Population, Cell Biology, Hypoxia (medical), Biology, Cell sorting, Flow cytometry, 03 medical and health sciences, Basal (phylogenetics), 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, 030228 respiratory system, Downregulation and upregulation, medicine, Cancer research, Respiratory epithelium, medicine.symptom, education, Molecular Biology
Abstract

Airway basal cells are crucial for regeneration of the human lung airway epithelium, and are thought to be important contributors to Chronic Obstructive Pulmonary Disease (COPD) and other lung disorders. In order to reveal how basal cells contribute to disease, and to discover novel therapeutic targets, these basal cells need to be further characterized. In this study, we optimized a flow cytometry-based cell sorting protocol for primary human airway basal cells dependent on cell size and Nerve-Growth Factor Receptor (NGFR) expression. The basal cell population was found to be molecularly and functionally heterogeneous in contrast to cultured basal cells. In addition, significant differences were found such as KRT14 expression exclusively existing in cultured cells. Also, colony-forming capacity was significantly increased in cultured cells showing a clonal enrichment in vitro. Next, by single cell RNA sequencing on primary basal cells from healthy donors and GOLD stage IV COPD patients, the gene expression revealed a continuum ranging from healthy basal cell signatures to diseased basal cell phenotypes. We identified several upregulated genes that may indicate COPD, such as stress response related genes GADD45B and AHSA1, along with genes involved in the response to hypoxia such as CITED2 and SOD1. Taken together, the presence of healthy basal cells in stage IV COPD demonstrates the potential for regeneration through the discovery of novel therapeutic targets. In addition, we show the importance of studying primary basal cells when investigating disease mechanisms as well as for developing future cell-based therapies in the human lung.

Published
2021

33. Ciliated (FOXJ1

Author

Sofia C, Wijk, Pavan, Prabhala, Anna, Löfdahl, Annika, Nybom, Stefan, Lang, Hans, Brunnström, Leif, Bjermer, Gunilla, Westergren-Thorsson, and Mattias, Magnusson

Subjects
Gene Expression Profiling, Apoferritins, Humans, Forkhead Transcription Factors, Lung, Idiopathic Pulmonary Fibrosis, Signal Transduction
Abstract

Cell-based therapies hold great promise in re-establishing organ function for many diseases, including untreatable lung diseases such as idiopathic pulmonary fibrosis (IPF). However, many hurdles still remain, in part due to our lack of knowledge about the disease-driving mechanisms that may affect the cellular niche and thereby possibly hinder the function of any transplanted cells by imposing the disease phenotype onto the newly generated progeny. Recent findings have demonstrated increased ciliation of lung cells from IPF patients, but how this affects ciliated cell function and the airway milieu is not well-known. Here, we performed single-cell RNA sequencing on primary ciliated (FOXJ1

Published
2022

34. <P Class='Head'>Multi-Organ Single Cell Analysis Reveals an On/Off Switch System with Potential for Personalized Treatment of Immunological Diseases<O:P></O:P>

Author

Sandra Lilja, Xinxiu Li, Martin Smelik, Eun Jung Lee, Joseph Loscalzo, Pratheek Bellur Marthanda, Lang Hu, Mattias Magnusson, Oleg Sysoev, Huan Zhang, Yelin Zhao, Christopher Sjöwall, Danuta Gawel, Hui Wang, and Mikael Benson

Subjects
History, Polymers and Plastics, Business and International Management, Industrial and Manufacturing Engineering
Published
2022

36. Abstract 3892: High-throughput combination screen for identifying novel therapies against high-risk neuroblastoma

Author

Katarzyna Radke, Karin Hansson, Jani Saarela, Aleksandr Ianevski, Philipp Ianevski, Aurélie Baudet, Mattias Magnusson, and Daniel Bexell

Subjects
Cancer Research, Oncology
Abstract

Neuroblastoma is a childhood solid tumor commonly located in the adrenal gland. High-risk neuroblastoma patients undergo multidrug and multi-interventional treatment but despite these efforts many patients develop resistance to chemotherapy and eventually relapse. Neuroblastoma patients face an urgent need of novel therapeutic strategies that could effectively combat the disease. In a recent study we identified kinesin spindle protein (KSP) as a highly effective target in high-risk neuroblastoma. Pharmacological inhibition of KSP resulted in complete regression of a subset of neuroblastoma subcutaneous PDX tumors and tumor growth delay in orthotopic PDXs (Hansson, Radke et al, Sci. Transl. Med 2020). The purpose of the present study is to identify novel synergistic drug combinations effective against neuroblastoma and investigate their translational potential. We designed, optimized, and performed a high-throughput combination screen using 3D tumor organoids that represent three MYCN-amplified neuroblastoma tumors. KSP inhibition was tested in combination with the FIMM drug set of 527 approved and investigational drugs. Screening was performed stepwise: • Step 1: High-throughput drug screening 527 drug combinations and machine learning prediction (DECREASE tool) of drug combination synergy based on minimal required input. • Step 2: Screening of 6x6 dose-response matrices of top 26 predicted hits in high-risk neuroblastoma models. • Step 3: Screening of 6x6 dose-response matrices of top 26 hits in CD34+ cord blood controls to identify compounds that have low toxicity towards proliferating fraction of hematopoietic cells. Overall, we identified seven drug candidates (P1-P7). They classify as: kinase inhibitors, differentiating modifiers, and one hormone therapy. Screened combinations were chosen based on selective efficacy (difference between anti-neuroblastoma efficacy and efficacy towards CD34+ cord blood controls). Identified drug combinations are common among three high-risk neuroblastoma models and have most synergistic area score (MSA) over five. We further plan to validate seven hits in neuroblastoma models in vitro, investigate MOA of the most promising combination and test it in PDX models in vivo. Citation Format: Katarzyna Radke, Karin Hansson, Jani Saarela, Aleksandr Ianevski, Philipp Ianevski, Aurélie Baudet, Mattias Magnusson, Daniel Bexell. High-throughput combination screen for identifying novel therapies against high-risk neuroblastoma [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2022; 2022 Apr 8-13. Philadelphia (PA): AACR; Cancer Res 2022;82(12_Suppl):Abstract nr 3892.

Published
2022

37. Bone Erosions Detected by Ultrasound Are Prognostic for Clinical Arthritis Development in Patients With ACPA and Musculoskeletal Pain

Author

Mattias Magnusson, Thomas Skogh, Hilde Berner Hammer, Åsa Reckner, Emma Eloff, Michael Ziegelasch, Alf Kastbom, Jan Cedergren, and Klara Martinsson

Subjects
Musculoskeletal pain, rheumatoid arthritis, medicine.medical_specialty, clinical arthritis, Population, Arthritis, Internal medicine, medicine, education, anti-citrullinated protein antibodies, musculoskeletal pain, Rheumatology and Autoimmunity, Original Research, lcsh:R5-920, education.field_of_study, Reumatologi och inflammation, Tenosynovitis, biology, business.industry, Proportional hazards model, ultrasound, erosions, Ultrasound, Anti–citrullinated protein antibody, General Medicine, medicine.disease, Rheumatoid arthritis, biology.protein, Medicine, lcsh:Medicine (General), business
Abstract

Anti-citrullinated protein antibodies (ACPA) often precede onset of rheumatoid arthritis (RA) by years, and there is an urgent clinical need for predictors of arthritis development among such at-risk patients. This study assesses the prognostic value of ultrasound for arthritis development among ACPA-positive patients with musculoskeletal pain. We prospectively followed 82 ACPA-positive patients without clinical signs of arthritis at baseline. Ultrasound at baseline assessed synovial hypertrophy, inflammatory activity by power Doppler, and erosions in small joints of hands and feet. We applied Cox regression analyses to examine associations with clinical arthritis development during follow-up (median, 69 months; range, 24–90 months). We also compared the ultrasound findings among the patients to a control group of 100 blood donors without musculoskeletal pain. Clinical arthritis developed in 39/82 patients (48%) after a median of 6 months (range, 1–71 months). One or more ultrasound erosions occurred in 13/82 patients (16%), with none in control subjects (p < 0.001). Clinical arthritis development was more common among patients with baseline ultrasound erosions than those without (77 vs. 42%, p = 0.032), and remained significant in a multivariable Cox regression analysis that included previously described prognostic factors (HR 3.9, 95% CI 1.6–9.4, p = 0.003). Ultrasound-detected tenosynovitis was more frequent among the patients and associated with clinical arthritis development in a univariable analysis (HR 2.5, 95% CI 1.1–5.7, p = 0.031), but did not remain statistically significant in multivariable analysis. Thus, bone erosions detected by ultrasound are independent predictors of clinical arthritis development in an ACPA-positive at-risk population.Trial Registration: Regional Ethics Committee in Linköping, Sweden, Dnr M220-09. Registered 16 December 2009, https://etikprovningsmyndigheten.se/.

Published
2021

39. Stem cells, cell therapies, and bioengineering in lung biology and disease 2019

Author

Brian R. Davis, Laertis Ikonomou, Sara Rolandsson Enes, Fernanda F. Cruz, Ya-Wen Chen, Chelsea M. Magin, Anna Krasnodembskaya, Gunilla Westergren-Thorsson, Evan T Hoffman, Allison M. Greaney, John Stegmayr, Sarah E. Gilpin, Mareike Lehmann, Daniel J. Weiss, Kim Vanuytsel, Amy L. Ryan, Mattias Magnusson, Hani N. Alsafadi, and Darcy E. Wagner

Subjects
Pulmonary and Respiratory Medicine, 0303 health sciences, medicine.medical_specialty, business.industry, Genetic enhancement, lcsh:R, lcsh:Medicine, Reviews, Context (language use), medicine.disease, Regenerative medicine, Cell therapy, 03 medical and health sciences, 0302 clinical medicine, Pulmonary fibrosis, medicine, Progenitor cell, Stem cell, Intensive care medicine, business, Induced pluripotent stem cell, 030217 neurology & neurosurgery, 030304 developmental biology
Abstract

A workshop entitled “Stem Cells, Cell Therapies and Bioengineering in Lung Biology and Diseases” was hosted by the University of Vermont Larner College of Medicine in collaboration with the National Heart, Lung and Blood Institute, the Alpha-1 Foundation, the Cystic Fibrosis Foundation, the International Society for Cell and Gene Therapy and the Pulmonary Fibrosis Foundation. The event was held from July 15 to 18, 2019 at the University of Vermont, Burlington, Vermont. The objectives of the conference were to review and discuss the current status of the following active areas of research: 1) technological advancements in the analysis and visualisation of lung stem and progenitor cells; 2) evaluation of lung stem and progenitor cells in the context of their interactions with the niche; 3) progress toward the application and delivery of stem and progenitor cells for the treatment of lung diseases such as cystic fibrosis; 4) progress in induced pluripotent stem cell models and application for disease modelling; and 5) the emerging roles of cell therapy and extracellular vesicles in immunomodulation of the lung. This selection of topics represents some of the most dynamic research areas in which incredible progress continues to be made. The workshop also included active discussion on the regulation and commercialisation of regenerative medicine products and concluded with an open discussion to set priorities and recommendations for future research directions in basic and translation lung biology., This workshop report discusses recent advances in cell therapy and bioengineering approaches for repair and regeneration of diseased lungs https://bit.ly/2DqA8eu

Published
2020

40. Correction to: A validated single-cell-based strategy to identify diagnostic and therapeutic targets in complex diseases

Author

Antonio Lentini, Bengt Asking, Mika Gustafsson, Mattias Magnusson, Jesper Aagesen, Jan Ernerudh, Margaretha Stenmarker, Henrik Hjortswang, Huan Zhang, Jordi Serra-Musach, Simon Wu, Sophie Biggs, Malin Bengnér, Xinxiu Li, Ceylan Sonmez, Jan-Erik Karlsson, Karin Åkesson, Alex Arenas, David Martínez-Enguita, Alex K. Shalek, Janne Björkander, Samuel Schäfer, Eunjung Lee, Colm E. Nestor, Mattias Köpsen, Oliver Seifert, Andreas Matussek, Sandra Lilja, Danuta R. Gawel, Mikael Benson, Andreas Tjärnberg, and Henrik Stjernman

Subjects
Multifactorial Inheritance, lcsh:QH426-470, Network tools, Systems biology, lcsh:Medicine, Computational biology, Arthritis, Rheumatoid, Mice, Metabolomics, Drug Discovery, scRNA-seq, Genetics, Biomarker and drug discovery, Medicine, Animals, Humans, Molecular Biology, Biological sciences, Genetics (clinical), business.industry, Gene Expression Profiling, Research, lcsh:R, Correction, Computational Biology, High-Throughput Nucleotide Sequencing, Reproducibility of Results, Genomics, Human genetics, lcsh:Genetics, Disease Models, Animal, Molecular Diagnostic Techniques, Molecular Medicine, Disease Susceptibility, Neural Networks, Computer, Single-Cell Analysis, business, Biomarkers, Cell based
Abstract

Background Genomic medicine has paved the way for identifying biomarkers and therapeutically actionable targets for complex diseases, but is complicated by the involvement of thousands of variably expressed genes across multiple cell types. Single-cell RNA-sequencing study (scRNA-seq) allows the characterization of such complex changes in whole organs. Methods The study is based on applying network tools to organize and analyze scRNA-seq data from a mouse model of arthritis and human rheumatoid arthritis, in order to find diagnostic biomarkers and therapeutic targets. Diagnostic validation studies were performed using expression profiling data and potential protein biomarkers from prospective clinical studies of 13 diseases. A candidate drug was examined by a treatment study of a mouse model of arthritis, using phenotypic, immunohistochemical, and cellular analyses as read-outs. Results We performed the first systematic analysis of pathways, potential biomarkers, and drug targets in scRNA-seq data from a complex disease, starting with inflamed joints and lymph nodes from a mouse model of arthritis. We found the involvement of hundreds of pathways, biomarkers, and drug targets that differed greatly between cell types. Analyses of scRNA-seq and GWAS data from human rheumatoid arthritis (RA) supported a similar dispersion of pathogenic mechanisms in different cell types. Thus, systems-level approaches to prioritize biomarkers and drugs are needed. Here, we present a prioritization strategy that is based on constructing network models of disease-associated cell types and interactions using scRNA-seq data from our mouse model of arthritis, as well as human RA, which we term multicellular disease models (MCDMs). We find that the network centrality of MCDM cell types correlates with the enrichment of genes harboring genetic variants associated with RA and thus could potentially be used to prioritize cell types and genes for diagnostics and therapeutics. We validated this hypothesis in a large-scale study of patients with 13 different autoimmune, allergic, infectious, malignant, endocrine, metabolic, and cardiovascular diseases, as well as a therapeutic study of the mouse arthritis model. Conclusions Overall, our results support that our strategy has the potential to help prioritize diagnostic and therapeutic targets in human disease. Electronic supplementary material The online version of this article (10.1186/s13073-019-0657-3) contains supplementary material, which is available to authorized users.

Published
2020

41. Local administration of 4-Thiouridine, a novel molecule with potent anti-inflammatory properties, protects against experimental colitis and arthritis

Author

Dinesh Thummuri, Manish Kumar Jeengar, Vegi Ganga Modi Naidu, Srinivas Uppugunduri, Sudeep Chenna Narendra, and Mattias Magnusson

Subjects
0301 basic medicine, Male, Knee Joint, medicine.drug_class, Colon, medicine.medical_treatment, Immunology, Thiouridine, Anti-Inflammatory Agents, Arthritis, Inflammation, Pharmacology, Anti-inflammatory, 03 medical and health sciences, 0302 clinical medicine, medicine, Immunology and Allergy, Animals, Colitis, Antigens, biology, business.industry, Dextran Sulfate, NF-kappa B, Serum Albumin, Bovine, medicine.disease, Ulcerative colitis, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Cytokine, Cyclooxygenase 2, 030220 oncology & carcinogenesis, Myeloperoxidase, biology.protein, Cytokines, Tumor necrosis factor alpha, Colitis, Ulcerative, Female, medicine.symptom, business
Abstract

Previous studies in a rat model of Sephadex induced lung inflammation showed that 4-Thiouridine (4SU), a thiol substituted nucleoside, was very effective in reducing edema, leukocyte influx and TNF levels in bronchoalvelolar lavage fluid. However, little is known about the factors and mechanisms underlying these effects. In the present study, we have used two separate mouse models of chronic inflammation, a model of dextran sulphate sodium (DSS) induced colitis and a model of antigen induced arthritis, to evaluate the anti-inflammatory effect of 4-thiouridine. We have analyzed a broad spectrum of inflammatory mediators in order to delineate the mechanisms behind a potential anti-inflammatory effect of 4SU. Colitis was induced in C57BL/6 mice by administration of 3.5% DSS in drinking water for 5 days and the potential anti-colitic effect of 4SU was assessed by monitoring the disease activity index (DAI), measurement of colon length and histopathological analysis of colon tissue. We analyzed tissue myeloperoxidase (MPO) activity, serum pro-inflammatory cytokines (IL-1β, IL-6 and TNF), mRNA and protein expression of pro-inflammatory cytokines, COX-2, and NF-κB activity in colitis tissue. Intracolonic administration of 4SU (5 mg/kg & 10 mg/kg.) significantly inhibited MPO activity and reduced the levels of pro-inflammatory cytokines (IL-1β, IL-6 and TNF) as well as COX-2. Further, NF-κB activation was also blocked by attenuating the phosphorylation of IkB kinase (IKK α/β) in DSS-induced colitis tissues. Arthritis was induced by intra-articular injection of mBSA in the knee of NMRI mice pre-immunized with mBSA and 4SU was administered locally by direct injection into the knee joint. The antiarthritic potential of 4SU was calculated by histopathological scores and histochemical analysis of joint tissue. Further, immunohistochemistry was used to study inflammatory cell infiltration and expression of cytokines and adhesion molecules in the synovium. Local administration of 50–100 mg/kg 4SU at the time of arthritis onset clearly prevented development of joint inflammation and efficiently inhibited synovial expression of CD18, local cytokine production and recruitment of leukocytes to the synovium. Taken together, our data clearly demonstrates a potent anti-inflammatory effect of 4SU in two experimental models. In conclusion 4SU could be a new promising candidate for therapeutic modulation of chronic inflammatory diseases like ulcerative colitis and arthritis.

Published
2020

44. Hepatic Leukemia Factor Maintains Quiescence of Hematopoietic Stem Cells and Protects the Stem Cell Pool during Regeneration

Author

Shubhranshu Debnath, Agatheeswaran Subramaniam, Hanna K. A. Mikkola, David Bryder, Kenichi Miharada, Mattias Magnusson, Karolina Komorowska, Jonas Larsson, Jun Chen, Martin Wahlestedt, Ben Van Handel, Alexander Doyle, and Shamit Soneji

Subjects
0301 basic medicine, Regulator, Apoptosis, Biology, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Mice, Animals, Transcription factor, lcsh:QH301-705.5, Cells, Cultured, Cell Proliferation, Hematopoietic Stem Cell Transplantation, hemic and immune systems, Hematopoietic Stem Cells, Hepatic Leukemia Factor, Cell biology, Hematopoiesis, Transplantation, Mice, Inbred C57BL, Haematopoiesis, 030104 developmental biology, Basic-Leucine Zipper Transcription Factors, lcsh:Biology (General), Stem cell, Transcriptome, DNA Damage
Abstract

Summary: The transcription factor hepatic leukemia factor (HLF) is strongly expressed in hematopoietic stem cells (HSCs) and is thought to influence both HSC self-renewal and leukemogenesis. However, the physiological role of HLF in hematopoiesis and HSC function is unclear. Here, we report that mice lacking Hlf are viable with essentially normal hematopoietic parameters, including an intact HSC pool during steady-state hematopoiesis. In contrast, when challenged through transplantation, Hlf-deficient HSCs showed an impaired ability to reconstitute hematopoiesis and became gradually exhausted upon serial transplantation. Transcriptional profiling of Hlf-deficient HSCs revealed changes associated with enhanced cellular activation, and cell-cycle analysis demonstrated a significant reduction of quiescent HSCs. Accordingly, toxic insults targeting dividing cells completely eradicated the HSC pool in Hlf-deficient mice. In summary, our findings point to HLF as a critical regulator of HSC quiescence and as an essential factor for maintaining the HSC pool during regeneration. : Komorowska et al. report that the transcription factor HLF is required to maintain hematopoietic stem cell (HSC) function during regeneration. Moreover, Hlf-deficient HSCs are less quiescent. In accordance with this, toxic insults targeting dividing cells completely eradicate the HSC pool in Hlf-deficient mice. Keywords: HSC, transcription factor, HLF, quiescence, self-renewal, cell cycle, reconstitution, transplantation, 5FU, stress

Published
2017

45. Critical Modulation of Hematopoietic Lineage Fate by Hepatic Leukemia Factor

Author

David Bryder, Manuel Sánchez Castillo, Martin Wahlestedt, Petter Säwén, Vasileios Ladopoulos, Rebecca Hannah, Isabel Hidalgo, Berthold Göttgens, Monika Dudenhöffer-Pfeifer, Haixia Wan, Gudmundur L. Norddahl, Mattias Magnusson, Hannah, Rebecca [0000-0003-0477-7792], Gottgens, Berthold [0000-0001-6302-5705], and Apollo - University of Cambridge Repository

Subjects
0301 basic medicine, Myeloid, Cellular differentiation, lineage commitment, myelopoiesis, Biology, Article, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Cell Lineage, Myeloid Cells, Lymphopoiesis, lcsh:QH301-705.5, transcription factor, Regulation of gene expression, Leukemia, Multipotent Stem Cells, Cell Differentiation, Hematopoietic Stem Cells, hematopoiesis, Hepatic Leukemia Factor, 3. Good health, Cell biology, Haematopoiesis, Basic-Leucine Zipper Transcription Factors, 030104 developmental biology, NFIC, medicine.anatomical_structure, lcsh:Biology (General), Gene Expression Regulation, Multipotent Stem Cell, 030220 oncology & carcinogenesis, Immunology, gene regulation
Abstract

Summary A gradual restriction in lineage potential of multipotent stem/progenitor cells is a hallmark of adult hematopoiesis, but the underlying molecular events governing these processes remain incompletely understood. Here, we identified robust expression of the leukemia-associated transcription factor hepatic leukemia factor (Hlf) in normal multipotent hematopoietic progenitors, which was rapidly downregulated upon differentiation. Interference with its normal downregulation revealed Hlf as a strong negative regulator of lymphoid development, while remaining compatible with myeloid fates. Reciprocally, we observed rapid lymphoid commitment upon reduced Hlf activity. The arising phenotypes resulted from Hlf binding to active enhancers of myeloid-competent cells, transcriptional induction of myeloid, and ablation of lymphoid gene programs, with Hlf induction of nuclear factor I C (Nfic) as a functionally relevant target gene. Thereby, our studies establish Hlf as a key regulator of the earliest lineage-commitment events at the transition from multipotency to lineage-restricted progeny, with implications for both normal and malignant hematopoiesis., Graphical Abstract, Highlights • During hematopoiesis, Hlf is sharply downregulated upon exit from multipotency • Prolonged Hlf expression instructs GMLPs to adopt myeloid fates • Failure to downregulate Hlf is incompatible with appropriate B and T lymphopoiesis • Hlf governs molecular programs driving myelopoiesis and inhibiting lymphopoiesis, Regulators of early blood cell formation are important in both health and disease. Wahlestedt et al. identify abrupt downregulation of the transcription factor Hlf during hematopoietic differentiation. Failure to downregulate Hlf leads to a drastically skewed output of mature blood cells, positioning Hlf as a critical regulator of hematopoiesis.

Published
2017

46. OP0116 JOINT EROSIONS VISIBLE ON ULTRASOUND PREDICT ARTHRITIS DEVELOPMENT IN PATIENTS WITH ACPA AND MUSCULOSKELETAL PAIN BUT NO SWOLLEN JOINTS

Author

Hilde Berner Hammer, Michael Ziegelasch, Jan Cedergren, Mattias Magnusson, Åsa Reckner, Alf Kastbom, Thomas Skogh, Klara Martinsson, and Emma Eloff

Subjects
musculoskeletal diseases, medicine.medical_specialty, medicine.diagnostic_test, Proportional hazards model, business.industry, Arthritis, Physical examination, medicine.disease, Pharmacotherapy, Rheumatoid arthritis, Erythrocyte sedimentation rate, Internal medicine, Synovitis, medicine, Rheumatoid factor, business
Abstract

Background Anti-citrullinated protein antibodies (ACPA) are associated with an increased risk of developing rheumatoid arthritis (RA), and in particular erosive disease. Detection of joint inflammation prior to clinical synovitis may improve treatment decisions in early disease. Objectives We sought to determine the value of ultrasound (US) to predict arthritis development among ACPA positive patients with musculoskeletal (MSK) pain. Methods We prospectively followed 82 ACPA-positive patients with MSK pain but without arthritis upon baseline clinical examination (mean follow-up 68 months, range 23-91). US at baseline assessed joint erosions, synovial hypertrophy in grey scale (GS), and inflammatory activity judged by power Doppler (PD) in 36 small joints in hands and feet. We used a ProFocus system (BK Medical) with pulse repetition frequency 0.8 kHz for PD grading. The US and PD results were blinded to patients and treating rheumatologists during the initial 3 years. US findings among patients were compared to 100 age-matched healthy blood donors. Arthritis development during follow-up of patients was determined by clinical examination by an experienced rheumatologist. Associations between baseline US findings and arthritis development were tested by Cox regression analysis with adjustment for sex, age, symptom duration, smoking habits, erythrocyte sedimentation rate, C-reactive protein level, rheumatoid factor, and ACPA levels. Results Significantly more patient joints had synovial hypertrophy (GS score >0) compared to control joints in metacarpophalangeal (MCP) (5.2% vs. 2.5%; p 0 compared to patient joints (49% vs. 24%; p 0) occurred significantly more often in patient joints compared to the controls in all joint areas (p Conclusion Arthritis-related US findings are more common among patients at increased risk of RA compared to healthy controls, but with site-specific differences. Erosions detected on US predicted arthritis development. Thus, US assessment of erosions improves risk-stratification of ACPA-positive patients without swollen joints, and potentially identifies patients eligible for very early pharmacotherapy. Disclosure of Interests Michael Ziegelasch Consultant for: AbbVie, MSD, Pfizer, and BK-Medical, Emma Eloff: None declared, Hilde Berner Hammer Speakers bureau: speakers fee from AbbVie, Bristol-Myers Squibb, Roche, UCB Pharma and Pfizer, Jan Cedergren: None declared, Klara Martinsson: None declared, Asa Reckner: None declared, Thomas Skogh: None declared, Mattias Magnusson: None declared, Alf Kastbom Consultant for: Roche and Pfizer, Employee of: Sanofi, Speakers bureau: UCB and BMS

Published
2019

47. Preeclampsia is Associated with Sex-Specific Transcriptional and Proteomic Changes in Fetal Erythroid Cells

Author

Koen Herten, Zahra Masoumi, Mattias Magnusson, Eva Hanson, Mary Familari, Abdul Ghani Alattar, Joris Vermeesch, Stefan R. Hansson, Lena Erlandsson, Álvaro Cortés-Calabuig, Eva Mezey, and Gregory E. Maes

Subjects
0301 basic medicine, Male, Proteomics, Transcription, Genetic, Cellular differentiation, Chemistry, Multidisciplinary, MATERNAL PREECLAMPSIA, mTORC1, Umbilical Cord, Transcriptome, lcsh:Chemistry, RED-BLOOD-CELLS, 0302 clinical medicine, fluids and secretions, Pre-Eclampsia, Cell Movement, Pregnancy, Erythropoiesis, CORD BLOOD, lcsh:QH301-705.5, GESTATIONAL-AGE, Spectroscopy, RIBOSOMAL-PROTEINS, Sex Characteristics, Pregnancy Outcome, Cell Differentiation, General Medicine, progenitor cells, Computer Science Applications, Haematopoiesis, Chemistry, 030220 oncology & carcinogenesis, Cord blood, Physical Sciences, embryonic structures, Female, hematopoietic stem, Life Sciences & Biomedicine, Biochemistry & Molecular Biology, BONE-MARROW, Catalysis, Article, ADHESION MOLECULES, Inorganic Chemistry, Andrology, preeclampsia, 03 medical and health sciences, Fetus, Erythroid Cells, Erythroblast, Humans, Physical and Theoretical Chemistry, Progenitor cell, Molecular Biology, hematopoietic stem/progenitor cells, Science & Technology, Organic Chemistry, HUMAN HEMATOPOIETIC STEM, Hematopoietic Stem Cells, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, Gene Expression Regulation, DIFFERENTIAL EXPRESSION ANALYSIS, Protein Biosynthesis, umbilical cord blood, erythropoiesis
Abstract

Preeclampsia (PE) has been associated with placental dysfunction, resulting in fetal hypoxia, accelerated erythropoiesis, and increased erythroblast count in the umbilical cord blood (UCB). Although the detailed effects remain unknown, placental dysfunction can also cause inflammation, nutritional, and oxidative stress in the fetus that can affect erythropoiesis. Here, we compared the expression of surface adhesion molecules and the erythroid differentiation capacity of UCB hematopoietic stem/progenitor cells (HSPCs), UCB erythroid profiles along with the transcriptome and proteome of these cells between male and female fetuses from PE and normotensive pregnancies. While no significant differences were observed in UCB HSPC migration/homing and in vitro erythroid colony differentiation, the UCB HSPC transcriptome and the proteomic profile of the in vitro differentiated erythroid cells differed between PE vs. normotensive samples. Accordingly, despite the absence of significant differences in the UCB erythroid populations in male or female fetuses from PE or normotensive pregnancies, transcriptional changes were observed during erythropoiesis, particularly affecting male fetuses. Pathway analysis suggested deregulation in the mammalian target of rapamycin complex 1/AMP-activated protein kinase (mTORC1/AMPK) signaling pathways controlling cell cycle, differentiation, and protein synthesis. These results associate PE with transcriptional and proteomic changes in fetal HSPCs and erythroid cells that may underlie the higher erythroblast count in the UCB in PE. ispartof: INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES vol:20 issue:8 ispartof: location:Switzerland status: published

Published
2019

48. MLLT3 governs human haematopoietic stem-cell self-renewal and engraftment

Author

Vincenzo Calvanese, Andrew T. Nguyen, Timothy J. Bolan, Anastasia Vavilina, Trent Su, Lydia K. Lee, Yanling Wang, Fides D. Lay, Mattias Magnusson, Gay M. Crooks, Siavash K. Kurdistani, and Hanna K. A. Mikkola

Subjects
General Science & Technology, Cells, 1.1 Normal biological development and functioning, Biology, Regenerative Medicine, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Underpinning research, Cell Self Renewal, Animals, Humans, Progenitor cell, Cells, Cultured, 030304 developmental biology, Regulation of gene expression, Transplantation, 0303 health sciences, Cultured, Multidisciplinary, Hematopoietic Stem Cell Transplantation, Nuclear Proteins, hemic and immune systems, Hematology, Stem Cell Research, Hematopoietic Stem Cells, Stem Cell Self-Renewal, Chromatin, Cell biology, Haematopoiesis, Gene Expression Regulation, 030220 oncology & carcinogenesis, Stem Cell Research - Nonembryonic - Non-Human, Stem cell, Biotechnology, Protein Binding
Abstract

Limited knowledge of the mechanisms that govern the self-renewal of human haematopoietic stem cells (HSCs), and why this fails in culture, have impeded the expansion of HSCs for transplantation1. Here we identify MLLT3 (also known as AF9) as a crucial regulator of HSCs that is highly enriched in human fetal, neonatal and adult HSCs, but downregulated in culture. Depletion of MLLT3 prevented the maintenance of transplantable human haematopoietic stem or progenitor cells (HSPCs) in culture, whereas stabilizing MLLT3 expression in culture enabled more than 12-fold expansion of transplantable HSCs that provided balanced multilineage reconstitution in primary and secondary mouse recipients. Similar to endogenous MLLT3, overexpressed MLLT3 localized to active promoters in HSPCs, sustained levels of H3K79me2 and protected the HSC transcriptional program in culture. MLLT3 thus acts as HSC maintenance factor that links histone reader and modifying activities to modulate HSC gene expression, and may provide a promising approach to expand HSCs for transplantation. MLLT3 is identified as a crucial regulator of the self-renewal of human haematopoietic stem cells, and helps to maintain an active chromatin state in haematopoietic stem-cell regulatory genes during culture.

Published
2018

50. Small molecule screen identifies differentiation-promoting compounds targeting genetically diverse acute myeloid leukaemia

Author

Shamit Soneji, Mattias Magnusson, Aurélie Baudet, Josef Davidsson, Jörg Cammenga, Gunnar Juliusson, Roger Olsson, and Fredrik Ek

Subjects
0301 basic medicine, medicine.medical_specialty, Indoles, Myeloid, Biology, Small Molecule Libraries, 03 medical and health sciences, Cell Line, Tumor, hemic and lymphatic diseases, Internal medicine, medicine, Humans, Early Detection of Cancer, Hematology, Genetic Variation, Cell Differentiation, respiratory system, medicine.disease, Small molecule, Coculture Techniques, Leukemia, Myeloid, Acute, Leukemia, 030104 developmental biology, medicine.anatomical_structure, Cell culture, Immunology, Cancer research, Coculture Technique, Myeloid leukaemia, human activities
Abstract

Small molecule screen identifies differentiation-promoting compounds targeting genetically diverse acute myeloid leukaemia

Published
2015

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