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1. Cellular sources of dysregulated cytokines in relapsing-remitting multiple sclerosis

Author

Romme Christensen Jeppe, Börnsen Lars, Hesse Dan, Krakauer Martin, Sørensen Per, Søndergaard Helle, and Sellebjerg Finn

Subjects
Relapsing-remitting multiple sclerosis, Immunology, Cytokines, Blood, Cerebrospinal fluid cells, Real-time PCR, Neurology. Diseases of the nervous system, RC346-429
Abstract

Abstract Background Numerous cytokines are implicated in the immunopathogenesis of multiple sclerosis (MS), but studies are often limited to whole blood (WB) or peripheral blood mononuclear cells (PBMCs), thereby omitting important information about the cellular origin of the cytokines. Knowledge about the relation between blood and cerebrospinal fluid (CSF) cell expression of cytokines and the cellular source of CSF cytokines is even more scarce. Methods We studied gene expression of a broad panel of cytokines in WB from relapsing-remitting multiple sclerosis (RRMS) patients in remission and healthy controls (HCs). Subsequently we determined the gene expression of the dysregulated cytokines in isolated PBMC subsets (CD4+, CD8+T-cells, NK-cells, B-cells, monocytes and dendritic cells) from RRMS patients and HCs and in CSF-cells from RRMS patients in clinical relapse and non-inflammatory neurological controls (NIND). Results RRMS patients had increased expression of IFN-gamma (IFNG), interleukin (IL) 1-beta (IL1B), IL7, IL10, IL12A, IL15, IL23, IL27, lymphotoxin-alpha (LTA) and lymphotoxin-beta (LTB) in WB. In PBMC subsets the main sources of pro-inflammatory cytokines were T- and B-cells, whereas monocytes were the most prominent source of immunoregulatory cytokines. In CSF-cells, RRMS patients had increased expression of IFNG and CD19 and decreased expression of IL10 and CD14 compared to NINDs. CD19 expression correlated with expression of IFNG, IL7, IL12A, IL15 and LTA whereas CD14 expression correlated with IL10 expression. Conclusions Using a systematic approach, we show that expression of pro-inflammatory cytokines in peripheral blood primarily originates from T- and B-cells, with an important exception of IFNG which is most strongly expressed by NK-cells. In CSF-cell studies, B-cells appear to be enriched in RRMS and associated with expression of pro-inflammatory cytokines; contrarily, monocytes are relatively scarce in CSF from RRMS patients and are associated with IL10 expression. Thus, our findings suggest a pathogenetic role of B-cells and an immunoregulatory role of monocytes in RRMS.

Published
2012
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9. GPR15 + T cells are Th17 like, increased in smokers and associated with multiple sclerosis

Author

Ammitzbøll, Cecilie, von Essen, Marina R., Börnsen, Lars, Petersen, Eva Rosa, McWilliam, Oskar, Ratzer, Rikke, Romme Christensen, Jeppe, Oturai, Annette B., Søndergaard, Helle B., Sellebjerg, Finn, Ammitzbøll, Cecilie, von Essen, Marina R., Börnsen, Lars, Petersen, Eva Rosa, McWilliam, Oskar, Ratzer, Rikke, Romme Christensen, Jeppe, Oturai, Annette B., Søndergaard, Helle B., and Sellebjerg, Finn

Abstract

Smoking is a risk factor for the development and progression of multiple sclerosis (MS); however, the pathogenic effects of smoking are poorly understood. We studied the smoking-associated chemokine receptor-like molecule GPR15 in relation to relapsing-remitting MS (RRMS). Using microarray analyses and qPCR we found elevated GPR15 in blood cells from smokers, and increased GPR15 expression in RRMS. By flow cytometry we detected increased frequencies of GPR15 expressing T and B cells in smokers, but no difference between patients with RRMS and healthy controls. However, after cell culture with the autoantigens myelin basic protein (MBP) and myelin oligodendrocyte glycoprotein, frequencies of MBP-reactive and non-proliferating GPR15 + CD4 + T cells were increased in patients with RRMS compared with healthy controls. GPR15 + CD4 + T cells produced IL-17 and were enriched in the cerebrospinal fluid (CSF). Furthermore, in the CSF of patients with RRMS, GPR15 + T cells were associated with CCR6 + CXCR3 + /CCR6 − CXCR3 + phenotypes and correlated positively with concentrations of the newly identified GPR15-ligand (GPR15L), myelin degradation and disability. In conclusion, we have identified a proinflammatory cell type linking smoking with pathogenic immune cell functions in RRMS.

Published
2019

10. CSF inflammatory biomarkers responsive to treatment in progressive multiple sclerosis capture residual inflammation associated with axonal damage

Author

Romme Christensen, Jeppe, Komori, Mika, von Essen, Marina Rode, Ratzer, Rikke, Börnsen, Lars, Bielekova, Bibi, Sellebjerg, Finn, Romme Christensen, Jeppe, Komori, Mika, von Essen, Marina Rode, Ratzer, Rikke, Börnsen, Lars, Bielekova, Bibi, and Sellebjerg, Finn

Abstract

Background: Development of treatments for progressive multiple sclerosis (MS) is challenged by the lack of sensitive and treatment-responsive biomarkers of intrathecal inflammation. Objective: To validate the responsiveness of cerebrospinal fluid (CSF) inflammatory biomarkers to treatment with natalizumab and methylprednisolone in progressive MS and to examine the relationship between CSF inflammatory and tissue damage biomarkers. Methods: CSF samples from two open-label phase II trials of natalizumab and methylprednisolone in primary and secondary progressive MS. CSF concentrations of 20 inflammatory biomarkers and CSF biomarkers of axonal damage (neurofilament light chain (NFL)) and demyelination were analysed using electrochemiluminescent assay and enzyme-linked immunosorbent assay (ELISA). Results: In all, 17 natalizumab- and 23 methylprednisolone-treated patients had paired CSF samples. CSF sCD27 displayed superior standardised response means and highly significant decreases during both natalizumab and methylprednisolone treatment; however, post-treatment levels remained above healthy donor reference levels. Correlation analyses of CSF inflammatory biomarkers and NFL before, during and after treatment demonstrated that CSF sCD27 consistently correlates with NFL. Conclusion: These findings validate CSF sCD27 as a responsive and sensitive biomarker of intrathecal inflammation in progressive MS, capturing residual inflammation after treatment. Importantly, CSF sCD27 correlates with NFL, consistent with residual inflammation after anti-inflammatory treatment being associated with axonal damage.

Published
2019

11. Smoking is associated with increased disease activity during natalizumab treatment in multiple sclerosis

Author

Petersen, Eva Rosa, Søndergaard, Helle Bach, Laursen, Julie Hejgaard, Olsson, Anna Gabriella, Börnsen, Lars, Soelberg Sørensen, Per, Sellebjerg, Finn, Bang Oturai, Annette, Petersen, Eva Rosa, Søndergaard, Helle Bach, Laursen, Julie Hejgaard, Olsson, Anna Gabriella, Börnsen, Lars, Soelberg Sørensen, Per, Sellebjerg, Finn, and Bang Oturai, Annette

Abstract

Background: Smoking has been associated with increased multiple sclerosis (MS) risk, disease worsening, and progression in MS patients. Furthermore, interactions between smoking and human leukocyte antigen (HLA) genes have been shown for MS risk. Recently, we found that smoking was associated with an increased relapse rate in interferon-beta-treated relapsing-remitting multiple sclerosis (RRMS) patients. Objectives: We examined the association between smoking and relapses in natalizumab-treated RRMS patients. Second, we investigated if an interaction between smoking and HLA-DRB1*15:01 or HLA-A*02:01 affected the number of relapses during treatment. Methods: In this observational cohort study, 355 natalizumab-treated RRMS patients were assessed. Prespecified criteria excluded 62 patients. Clinical data from the starting of treatment to the two-year follow-up visit were collected. Smoking status was obtained by a questionnaire survey. TaqMan allelic discrimination was used for genotyping of tag single-nucleotide polymorphisms (SNPs) for HLA-DRB1*15:01 and HLA-A*02:01. Negative binomial regression analysis was used to analyze the association between relapse rate and smoking intensity and HLA. Results: One pack of cigarettes (20 cigarettes) per day during natalizumab treatment increased the relapse rate during treatment with 38% (incidence rate ratio (IRR) = 1.38, 95% confidence interval (CI): 1.08–1.77, p = 0.01). No association or interaction was found between smoking and HLA-DRB1*15:01 or HLA-A*02:01, respectively. Conclusion: Smoking intensity was significantly associated with the number of relapses during natalizumab treatment.

Published
2019

16. Defining active progressive multiple sclerosis

Author

Sellebjerg, Finn, Börnsen, Lars, Ammitzbøll, Cecilie, Nielsen, Jørgen Erik, Vinther-Jensen, Tua, Hjermind, Lena Elisabeth, von Essen, Marina, Ratzer, Rikke Lenhard, Soelberg Sørensen, Per, Romme Christensen, Jeppe, Sellebjerg, Finn, Börnsen, Lars, Ammitzbøll, Cecilie, Nielsen, Jørgen Erik, Vinther-Jensen, Tua, Hjermind, Lena Elisabeth, von Essen, Marina, Ratzer, Rikke Lenhard, Soelberg Sørensen, Per, and Romme Christensen, Jeppe

Abstract

BACKGROUND: It is unknown whether disease activity according to consensus criteria (magnetic resonance imaging activity or clinical relapses) associate with cerebrospinal fluid (CSF) changes in progressive multiple sclerosis (MS).OBJECTIVE: To compare CSF biomarkers in active and inactive progressive MS according to consensus criteria.METHODS: Neurofilament light chain (NFL), myelin basic protein (MBP), IgG-index, chitinase-3-like-1 (CHI3L1), matrix metalloproteinase-9 (MMP-9), chemokine CXCL13, terminal complement complex, leukocyte counts and nitric oxide metabolites were measured in primary ( n = 26) and secondary progressive MS ( n = 26) and healthy controls ( n = 24).RESULTS: Progressive MS patients had higher CSF cell counts, IgG-index, CHI3L1, MMP-9, CXCL13, NFL and MBP concentrations. Active patients were younger and had higher NFL, CXCL13 and MMP-9 concentrations than inactive patients. Patients with active disease according to consensus criteria or detectable CXCL13 or MMP-9 in CSF were defined as having combined active progressive MS. These patients had increased CSF cell counts, IgG-index and MBP, NFL and CHI3L1 concentrations. Combined inactive patients only had increased IgG-index and MBP concentrations.CONCLUSION: Patients with combined active progressive MS show evidence of inflammation, demyelination and neuronal/axonal damage, whereas the remaining patients mainly show evidence of active demyelination. This challenges the idea that neurodegeneration independent of inflammation is crucial in disease progression.

Published
2017

17. High-dose erythropoietin in patients with progressive multiple sclerosis:A randomized, placebo-controlled, phase 2 trial

Author

Schreiber, Karen, Magyari, Melinda, Sellebjerg, Finn, Iversen, Pernille, Garde, Ellen, Madsen, Camilla Gøbel, Börnsen, Lars, Romme Christensen, Jeppe, Ratzer, Rikke, Siebner, Hartwig Roman, Laursen, Bjarne, Soelberg Sorensen, Per, Schreiber, Karen, Magyari, Melinda, Sellebjerg, Finn, Iversen, Pernille, Garde, Ellen, Madsen, Camilla Gøbel, Börnsen, Lars, Romme Christensen, Jeppe, Ratzer, Rikke, Siebner, Hartwig Roman, Laursen, Bjarne, and Soelberg Sorensen, Per

Abstract

BACKGROUND: Erythropoietin (EPO) is a part of an endogenous neuroprotective system in the brain and may address pathophysiological mechanisms in progressive multiple sclerosis (MS).OBJECTIVE: To evaluate a treatment effect of EPO on progressive MS.METHODS: This was a single-center, randomized, double-blind, placebo-controlled phase 2 trial, in which 52 patients with secondary or primary progressive MS were allocated to treatment with recombinant EPO (48,000 IU) or placebo, administered intravenously 17 times during 24 weeks. Patients had an Expanded Disability Status Score (EDSS) from 4 to 6.5 and clinical progression without relapses in the 2 preceding years. The primary outcome was the change in a composite measure of maximum gait distance, hand dexterity, and cognition from baseline to 24 weeks.RESULTS: A total of 50 patients completed the study. Venesection was performed often but no thromboembolic events occurred. We found no difference in the primary outcome between the EPO and the placebo group using the intention-to-treat principle ( p = 0.22). None of the secondary outcomes, neither clinical nor magnetic resonance imaging (MRI) measures showed any significant differences.CONCLUSION: This study provides class II evidence that treatment with high-dose EPO is not an effective treatment in patients with moderately advanced progressive MS.

Published
2017

18. Smoking reduces circulating CD26hi CD161hi MAIT cells in healthy individuals and patients with multiple sclerosis

Author

Ammitzbøll, Cecilie, Börnsen, Lars, Romme Christensen, Jeppe, Ratzer, Rikke, Romme Nielsen, Birgitte, Søndergaard, Helle B, von Essen, Marina R, Sellebjerg, Finn, Ammitzbøll, Cecilie, Börnsen, Lars, Romme Christensen, Jeppe, Ratzer, Rikke, Romme Nielsen, Birgitte, Søndergaard, Helle B, von Essen, Marina R, and Sellebjerg, Finn

Abstract

Upon chronic cigarette smoke exposure, inhaled antigens and irritants cause altered lung immune homeostasis. Circulating immune cells are affected, and smoking is associated with an increased risk of developing various disorders, including multiple sclerosis (MS). This study was conducted to determine the impact of smoking on circulating immune cell subsets. Furthermore, we determined whether any smoking-associated changes were related to MS. With the use of flow cytometry, CFSE assays, and ELISpot assays, we analyzed circulating immune cell phenotypes and quantified antigen-induced proliferation and cytokine secretion in smokers and nonsmokers in a cohort of 100 healthy individuals (HI). In addition, we analyzed immune cell subsets associated with smoking in 2 independent cohorts of patients with MS. In HI smokers compared with nonsmokers, we found increased blood cell counts of granulocytes, monocytes, and lymphocytes. These cells were not more proinflammatory, autoreactive, or EBV reactive compared with cells from nonsmokers. Phenotypic differences were seen in plasmacytoid dendritic cells (pDCs) and CD8+T cells as higher percentages of ICOS ligand (ICOSL)+pDCs and lower percentages of CD26hiCD161hiCD8+T cells and CCR6+CD8+T cells in smokers compared with nonsmokers. In supplemental analyses, we showed that CD26hiCD161hiCD8+T cells were mainly mucosal-associated invariant T cells (MAITs). Comparable frequencies of ICOSL+pDCs, CCR6+CD8+T cells, and CD26hiCD161hiCD8+T cells were found between HI and MS patients who were nonsmokers. Our findings suggest general proinflammatory effects from smoking combined with skewing of specific cell populations in HI and MS patients. The function of these cell populations needs further investigation.

Published
2017

19. Defining active progressive multiple sclerosis

Author

Sellebjerg, Finn, primary, Börnsen, Lars, additional, Ammitzbøll, Cecilie, additional, Nielsen, Jørgen Erik, additional, Vinther-Jensen, Tua, additional, Hjermind, Lena Elisabeth, additional, von Essen, Marina, additional, Ratzer, Rikke Lenhard, additional, Soelberg Sørensen, Per, additional, and Romme Christensen, Jeppe, additional

Published
2017
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21. Myelin Basic Protein-Induced Production of Tumor Necrosis Factor-α and Interleukin-6, and Presentation of the Immunodominant Peptide MBP85-99 by B Cells from Patients with Relapsing-Remitting Multiple Sclerosis

Author

Nielsen, Claus H, Börnsen, Lars, Sellebjerg, Finn, Brimnes, Marie K, Nielsen, Claus H, Börnsen, Lars, Sellebjerg, Finn, and Brimnes, Marie K

Abstract

B cells are involved in driving relapsing-remitting multiple sclerosis (RRMS), as demonstrated by the positive effect of therapeutic B-cell depletion. Aside from producing antibodies, B cells are efficient antigen-presenting and cytokine-secreting cells. Diverse polyclonal stimuli have been used to study cytokine production by B cells, but here we used the physiologically relevant self-antigen myelin basic protein (MBP) to stimulate B cells from untreated patients with RRMS and healthy donors. Moreover, we took advantage of the unique ability of the monoclonal antibody MK16 to recognize the immunodominant peptide MBP85-99 presented on HLA-DR15, and used it as a probe to directly study B-cell presentation of self-antigenic peptide. The proportions of B cells producing TNF-α or IL-6 after stimulation with MBP were higher in RRMS patients than in healthy donors, indicating a pro-inflammatory profile for self-reactive patient B cells. In contrast, polyclonal stimulation with PMA + ionomycin and MBP revealed no difference in cytokine profile between B cells from RRMS patients and healthy donors. Expanded disability status scale (EDSS) as well as multiple sclerosis severity score (MSSS) correlated with reduced ability of B cells to produce IL-10 after stimulation with MBP, indicative of diminished B-cell immune regulatory function in patients with the most severe disease. Moreover, EDSS correlated positively with the frequencies of TNF-α, IL-6 and IL-10 producing B cells after polyclonal stimulation. Patient-derived, IL-10-producing B cells presented MBP85-99 poorly, as did IL-6-producing B cells, particulary in the healthy donor group. B cells from MS patients thus present antigen to T cells in a pro-inflammatory context. These findings contribute to understanding the therapeutic effects of B-cell depletion in human autoimmune diseases, including MS.

Published
2016

22. Selected CSF biomarkers indicate no evidence of early neuroinflammation in Huntington disease

Author

Vinther-Jensen, Tua, Börnsen, Lars Svend, Budtz-Jorgensen, Esben, Ammitzboll, Cecilie, Larsen, Ida U., Hjermind, Lena E., Sellebjerg, Finn, Nielsen, Jorgen E., Vinther-Jensen, Tua, Börnsen, Lars Svend, Budtz-Jorgensen, Esben, Ammitzboll, Cecilie, Larsen, Ida U., Hjermind, Lena E., Sellebjerg, Finn, and Nielsen, Jorgen E.

Abstract

Objective: To investigate CSF biomarkers of neuroinflammation and neurodegeneration in Huntington disease (HD) gene-expansion carriers compared to controls and to investigate these biomarkers in association with clinical HD rating scales and disease burden score. Methods: We collected CSF from 32 premanifest and 48 manifest HD gene-expansion carriers and 24 gene-expansion negative at-risk controls. We examined biomarkers of neuroinflammation (matrix metalloproteinase 9, C-X-C motif chemokine 13, terminal complement complex, chitinase-3-like-protein 1 [CHI3L1], and osteopontin [OPN]) and neurodegeneration (microtubule-associated protein tau, neurofilament light polypeptide [NFL], and myelin basic protein [MBP]). The study was approved by the Ethics Committee of the Capital Region of Denmark (H2-2011-085) and written informed consent was obtained from each participant before enrollment. Results: NFL was the only biomarker that increased in premanifest stages and no evidence of early involvement of neuroinflammation in HD was found. However, we found that the biomarkers for neurodegeneration, MBP and tau, increased during the disease course in manifest HD gene-expansion carriers and were associated with an increase of the neuroinflammation biomarkers CHI3L1 and OPN. Tau was also increased in all gene-expansion carriers with psychiatric symptoms compared to gene-expansion carriers without psychiatric symptoms. Conclusions: Neuroinflammation, which seems not to be an early event in our cohort, may be secondary to neurodegeneration in late HD. NFL is a possible disease burden correlate in HD, reflecting neuronal loss even before motor symptom onset, and may be useful as a dynamic biomarker in intervention studies.

Published
2016

23. Monthly oral methylprednisolone pulse treatment in progressive multiple sclerosis

Author

Ratzer, Rikke, Iversen, Pernille, Börnsen, Lars, Dyrby, Tim B, Christensen, Jeppe Romme, Ammitzbøll, Cecilie, Madsen, Camilla Gøbel, Garde, Ellen, Lyksborg, Mark, Andersen, Birgit, Hyldstrup, Lars, Sørensen, Per Soelberg, Siebner, Hartwig R, Sellebjerg, Finn, Ratzer, Rikke, Iversen, Pernille, Börnsen, Lars, Dyrby, Tim B, Christensen, Jeppe Romme, Ammitzbøll, Cecilie, Madsen, Camilla Gøbel, Garde, Ellen, Lyksborg, Mark, Andersen, Birgit, Hyldstrup, Lars, Sørensen, Per Soelberg, Siebner, Hartwig R, and Sellebjerg, Finn

Abstract

BACKGROUND: There is a large unmet need for treatments for patients with progressive multiple sclerosis (MS). Phase 2 studies with cerebrospinal fluid (CSF) biomarker outcomes may be well suited for the initial evaluation of efficacious treatments.OBJECTIVE: To evaluate the effect of monthly oral methylprednisolone pulse treatment on intrathecal inflammation in progressive MS.METHODS: In this open-label phase 2A study, 15 primary progressive and 15 secondary progressive MS patients received oral methylprednisolone pulse treatment for 60 weeks. Primary outcome was changes in CSF concentrations of osteopontin. Secondary outcomes were other CSF biomarkers of inflammation, axonal damage and demyelination; clinical scores; magnetic resonance imaging measures of disease activity, magnetization transfer ratio (MTR) and diffusion tensor imaging (DTI); motor evoked potentials; and bone density scans.RESULTS: We found no change in the CSF concentration of osteopontin, but we observed significant improvement in clinical scores, MTR, DTI and some secondary CSF outcome measures. Adverse events were well-known side effects to methylprednisolone.CONCLUSION: Monthly methylprednisolone pulse treatment was safe, but had no effect on the primary outcome. However, improvements in secondary clinical and MRI outcome measures suggest that this treatment regimen may have a beneficial effect in progressive MS.

Published
2016

25. High-dose erythropoietin in patients with progressive multiple sclerosis: A randomized, placebo-controlled, phase 2 trial

Author

Schreiber, Karen, primary, Magyari, Melinda, additional, Sellebjerg, Finn, additional, Iversen, Pernille, additional, Garde, Ellen, additional, Madsen, Camilla Gøbel, additional, Börnsen, Lars, additional, Romme Christensen, Jeppe, additional, Ratzer, Rikke, additional, Siebner, Hartwig Roman, additional, Laursen, Bjarne, additional, and Soelberg Sorensen, Per, additional

Published
2016
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27. Monthly oral methylprednisolone pulse treatment in progressive multiple sclerosis

Author

Ratzer, Rikke, primary, Iversen, Pernille, additional, Börnsen, Lars, additional, Dyrby, Tim B, additional, Romme Christensen, Jeppe, additional, Ammitzbøll, Cecilie, additional, Madsen, Camilla Gøbel, additional, Garde, Ellen, additional, Lyksborg, Mark, additional, Andersen, Birgit, additional, Hyldstrup, Lars, additional, Sørensen, Per Soelberg, additional, Siebner, Hartwig R, additional, and Sellebjerg, Finn, additional

Published
2015
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28. Endogenous Interferon-β-Inducible Gene Expression and Interferon-β-Treatment Are Associated with Reduced T Cell Responses to Myelin Basic Protein in Multiple Sclerosis

Author

Börnsen, Lars, primary, Romme Christensen, Jeppe, additional, Ratzer, Rikke, additional, Hedegaard, Chris, additional, Søndergaard, Helle B., additional, Krakauer, Martin, additional, Hesse, Dan, additional, Nielsen, Claus H., additional, Sorensen, Per S., additional, and Sellebjerg, Finn, additional

Published
2015
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29. Natalizumab in progressive MS:Results of an open-label, phase 2A, proof-of-concept trial

Author

Romme Christensen, Jeppe, Ratzer, Rikke, Börnsen, Lars, Lyksborg, Mark, Garde, Ellen, Dyrby, Tim B, Siebner, Hartwig R, Sorensen, Per S, Sellebjerg, Finn, Romme Christensen, Jeppe, Ratzer, Rikke, Börnsen, Lars, Lyksborg, Mark, Garde, Ellen, Dyrby, Tim B, Siebner, Hartwig R, Sorensen, Per S, and Sellebjerg, Finn

Abstract

OBJECTIVE: Natalizumab inhibits the migration of systemic immune cells to the CNS and may be beneficial in progressive multiple sclerosis (MS). The objective of the study was to examine the effects of natalizumab in progressive MS.METHODS: In an open-label phase 2A study, 24 patients with progressive MS were included to receive natalizumab treatment for 60 weeks. Response to natalizumab was assessed in CSF and MRI studies. The primary endpoint was change in CSF osteopontin, a biomarker of intrathecal inflammation, from baseline to week 60.RESULTS: Seventeen patients completed the study. No new safety issues were encountered. CSF osteopontin decreased by 65 ng/mL (95% confidence interval 34-96 ng/mL; p = 0.0004) from baseline to week 60 in conjunction with decreases in other CSF biomarkers of inflammation, axonal damage, and demyelination. Magnetization transfer ratio increased in both cortical gray and normal-appearing white matter and correlated with decreases in CSF neurofilament light chain.CONCLUSIONS: Natalizumab treatment of progressive MS reduces intrathecal inflammation and tissue damage, supporting a beneficial effect of natalizumab treatment in progressive MS and suggesting that systemic inflammation contributes to the pathogenesis. Moreover, the study establishes the feasibility of using CSF biomarkers in proof-of-concept trials, allowing a low number of participants and short study duration.CLASSIFICATION OF EVIDENCE: This study provides Class IV evidence that in patients with progressive MS, natalizumab reduces biomarkers of intrathecal inflammation.

Published
2014

30. Smoking reduces circulating CD26hiCD161hi MAIT cells in healthy individuals and patients with multiple sclerosis.

Author

Ammitzbøll, Cecilie, Börnsen, Lars, Romme Christensen, Jeppe, Ratzer, Rikke, Romme Nielsen, Birgitte, Søndergaard, Helle B., Essen, Marina R., and Sellebjerg, Finn

Subjects
BLOOD cell count, MULTIPLE sclerosis, T cells, CELL populations, CELL physiology
Abstract

Impact of smoking on circulating immune cells with emphasis on CD26hiCD161hi MAIT cells and ICOSL+ pDCs, in healthy controls and MS patients. Upon chronic cigarette smoke exposure, inhaled antigens and irritants cause altered lung immune homeostasis. Circulating immune cells are affected, and smoking is associated with an increased risk of developing various disorders, including multiple sclerosis (MS). This study was conducted to determine the impact of smoking on circulating immune cell subsets. Furthermore, we determined whether any smoking‐associated changes were related to MS. With the use of flow cytometry, CFSE assays, and ELISpot assays, we analyzed circulating immune cell phenotypes and quantified antigen‐induced proliferation and cytokine secretion in smokers and nonsmokers in a cohort of 100 healthy individuals (HI). In addition, we analyzed immune cell subsets associated with smoking in 2 independent cohorts of patients with MS. In HI smokers compared with nonsmokers, we found increased blood cell counts of granulocytes, monocytes, and lymphocytes. These cells were not more proinflammatory, autoreactive, or EBV reactive compared with cells from nonsmokers. Phenotypic differences were seen in plasmacytoid dendritic cells (pDCs) and CD8+ T cells as higher percentages of ICOS ligand (ICOSL)+ pDCs and lower percentages of CD26hiCD161hi CD8+ T cells and CCR6+ CD8+ T cells in smokers compared with nonsmokers. In supplemental analyses, we showed that CD26hiCD161hi CD8+ T cells were mainly mucosal‐associated invariant T cells (MAITs). Comparable frequencies of ICOSL+ pDCs, CCR6+ CD8+ T cells, and CD26hiCD161hi CD8+ T cells were found between HI and MS patients who were nonsmokers. Our findings suggest general proinflammatory effects from smoking combined with skewing of specific cell populations in HI and MS patients. The function of these cell populations needs further investigation. [ABSTRACT FROM AUTHOR]

Published
2017
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31. High-dose erythropoietin in patients with progressive multiple sclerosis: A randomized, placebo-controlled, phase 2 trial.

Author

Schreiber, Karen, Magyari, Melinda, Sellebjerg, Finn, Iversen, Pernille, Garde, Ellen, Madsen, Camilla Gøbel, Börnsen, Lars, Christensen, Jeppe Romme, Ratzer, Rikke, Siebner, Hartwig Roman, Laursen, Bjarne, and Sorensen, Per Soelberg

Subjects
ERYTHROPOIETIN, MULTIPLE sclerosis treatment, COGNITION, MAGNETIC resonance imaging, RANDOMIZED controlled trials
Abstract

Background: Erythropoietin (EPO) is a part of an endogenous neuroprotective system in the brain and may address pathophysiological mechanisms in progressive multiple sclerosis (MS). Objective: To evaluate a treatment effect of EPO on progressive MS. Methods: This was a single-center, randomized, double-blind, placebo-controlled phase 2 trial, in which 52 patients with secondary or primary progressive MS were allocated to treatment with recombinant EPO (48,000 IU) or placebo, administered intravenously 17 times during 24 weeks. Patients had an Expanded Disability Status Score (EDSS) from 4 to 6.5 and clinical progression without relapses in the 2 preceding years. The primary outcome was the change in a composite measure of maximum gait distance, hand dexterity, and cognition from baseline to 24 weeks. Results: A total of 50 patients completed the study. Venesection was performed often but no thromboembolic events occurred. We found no difference in the primary outcome between the EPO and the placebo group using the intention-to-treat principle (p = 0.22). None of the secondary outcomes, neither clinical nor magnetic resonance imaging (MRI) measures showed any significant differences. Conclusion: This study provides class II evidence that treatment with high-dose EPO is not an effective treatment in patients with moderately advanced progressive MS. [ABSTRACT FROM AUTHOR]

Published
2017
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35. CSF inflammation and axonal damage are increased and correlate in progressive multiple sclerosis

Author

Romme Christensen, Jeppe, Börnsen, Lars, Khademi, Mohsen, Olsson, Tomas, Jensen, Poul Erik, Sørensen, Per Soelberg, Sellebjerg, Finn, Romme Christensen, Jeppe, Börnsen, Lars, Khademi, Mohsen, Olsson, Tomas, Jensen, Poul Erik, Sørensen, Per Soelberg, and Sellebjerg, Finn

Abstract

BACKGROUND: The mechanism underlying disease progression in progressive multiple sclerosis (MS) is uncertain. Pathological studies found widespread inflammation in progressive MS brains correlating with disease progression and axonal damage. OBJECTIVES: To study cerebrospinal fluid (CSF) biomarkers and clarify whether inflammation and axonal damage are associated in progressive MS. METHODS: Using enzyme-linked immunosorbent assay (ELISA), we analysed CSF from 40 secondary progressive (SPMS), 21 primary progressive (PPMS), and 36 relapsing-remitting (RRMS) and 20 non-inflammatory neurological disease (NIND) patients. Twenty-two of the SPMS patients participated in an MBP8298 peptide clinical trial and had CSF follow-up after one year. RESULTS: Compared to NIND patients, inflammatory biomarkers osteopontin and matrix metalloproteinase-9 (MMP9) were increased in all MS patients while CXCL13 was increased in RRMS and SPMS patients. Biomarkers of axonal damage (NFL) and demyelination (MBP) were increased in all MS patients. In progressive MS patients CSF levels of osteopontin and CXCL13 correlated with NFL while osteopontin and MMP9 correlated with MBP. MBP8298 treatment did not affect the levels of the biomarkers after one year of treatment. All biomarkers were continuously increased after one year of follow-up except MBP, which decreased. CONCLUSION: CSF biomarkers of inflammation, axonal damage and demyelination are continuously increased in progressive MS patients and correlate. These findings parallel pathology studies, emphasise a relationship between inflammation, axonal damage and demyelination and support the use of CSF biomarkers in progressive MS clinical trials.

Published
2013

36. Cellular sources of dysregulated cytokines in relapsing-remitting multiple sclerosis

Author

Romme Christensen, Jeppe, Börnsen, Lars, Hesse, Dan, Krakauer, Martin, Sørensen, Per Soelberg, Søndergaard, Helle Bach, Sellebjerg, Finn, Romme Christensen, Jeppe, Börnsen, Lars, Hesse, Dan, Krakauer, Martin, Sørensen, Per Soelberg, Søndergaard, Helle Bach, and Sellebjerg, Finn

Abstract

Numerous cytokines are implicated in the immunopathogenesis of multiple sclerosis (MS), but studies are often limited to whole blood (WB) or peripheral blood mononuclear cells (PBMCs), thereby omitting important information about the cellular origin of the cytokines. Knowledge about the relation between blood and cerebrospinal fluid (CSF) cell expression of cytokines and the cellular source of CSF cytokines is even more scarce.

Published
2012

37. Alterations in KLRB1 gene expression and a Scandinavian multiple sclerosis association study of the KLRB1 SNP rs4763655

Author

Søndergaard, Helle Bach, Sellebjerg, Finn, Hillert, Jan, Olsson, Tomas, Kockum, Ingrid, Lindén, Magdalena, Mero, Inger-Lise, Myhr, Kjell-Morten, Celius, Elisabeth G, Harbo, Hanne F, Christensen, Jeppe Romme, Börnsen, Lars, Sørensen, Per Soelberg, Oturai, Annette Bang, Søndergaard, Helle Bach, Sellebjerg, Finn, Hillert, Jan, Olsson, Tomas, Kockum, Ingrid, Lindén, Magdalena, Mero, Inger-Lise, Myhr, Kjell-Morten, Celius, Elisabeth G, Harbo, Hanne F, Christensen, Jeppe Romme, Börnsen, Lars, Sørensen, Per Soelberg, and Oturai, Annette Bang

Abstract

Multiple sclerosis (MS) is a complex autoimmune disease affecting genetically susceptible individuals. A genome-wide association study performed by the International MS Genetics Consortium identified several putative susceptibility genes; among these, the KLRB1 gene is represented by the single-nucleotide polymorphism rs4763655. We could confirm a marginally significant association between rs4763655 and MS (P=0.046, odds ratio=1.06 (1.00-1.13)) in a large Scandinavian case-control study of 5367 MS patients and 4485 controls. The expression of KLRB1 in blood from MS patients was higher compared with healthy controls (P

Published
2011

43. Smoking reduces circulating CD26hiCD161hiMAIT cells in healthy individuals and patients with multiple sclerosis

Author

Ammitzbøll, Cecilie, Börnsen, Lars, Romme Christensen, Jeppe, Ratzer, Rikke, Romme Nielsen, Birgitte, Søndergaard, Helle B., Essen, Marina R., and Sellebjerg, Finn

Abstract

Impact of smoking on circulating immune cells with emphasis on CD26hiCD161hiMAIT cells and ICOSL+pDCs, in healthy controls and MS patients. Upon chronic cigarette smoke exposure, inhaled antigens and irritants cause altered lung immune homeostasis. Circulating immune cells are affected, and smoking is associated with an increased risk of developing various disorders, including multiple sclerosis (MS). This study was conducted to determine the impact of smoking on circulating immune cell subsets. Furthermore, we determined whether any smoking-associated changes were related to MS. With the use of flow cytometry, CFSE assays, and ELISpot assays, we analyzed circulating immune cell phenotypes and quantified antigen-induced proliferation and cytokine secretion in smokers and nonsmokers in a cohort of 100 healthy individuals (HI). In addition, we analyzed immune cell subsets associated with smoking in 2 independent cohorts of patients with MS. In HI smokers compared with nonsmokers, we found increased blood cell counts of granulocytes, monocytes, and lymphocytes. These cells were not more proinflammatory, autoreactive, or EBV reactive compared with cells from nonsmokers. Phenotypic differences were seen in plasmacytoid dendritic cells (pDCs) and CD8+T cells as higher percentages of ICOS ligand (ICOSL)+pDCs and lower percentages of CD26hiCD161hiCD8+T cells and CCR6+CD8+T cells in smokers compared with nonsmokers. In supplemental analyses, we showed that CD26hiCD161hiCD8+T cells were mainly mucosal-associated invariant T cells (MAITs). Comparable frequencies of ICOSL+pDCs, CCR6+CD8+T cells, and CD26hiCD161hiCD8+T cells were found between HI and MS patients who were nonsmokers. Our findings suggest general proinflammatory effects from smoking combined with skewing of specific cell populations in HI and MS patients. The function of these cell populations needs further investigation.

Published
2017
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44. Alterations in KLRB1 gene expression and a Scandinavian multiple sclerosis association study of the KLRB1 SNP rs4763655

Author

Søndergaard, Helle Bach, primary, Sellebjerg, Finn, additional, Hillert, Jan, additional, Olsson, Tomas, additional, Kockum, Ingrid, additional, Lindén, Magdalena, additional, Mero, Inger-Lise, additional, Myhr, Kjell-Morten, additional, Celius, Elisabeth G, additional, Harbo, Hanne F, additional, Christensen, Jeppe Romme, additional, Börnsen, Lars, additional, Sørensen, Per Soelberg, additional, and Oturai, Annette Bang, additional

Published
2011
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49. Effect of Natalizumab on Circulating CD4+ T-Cells in Multiple Sclerosis.

Author

Börnsen, Lars, Christensen, Jeppe Romme, Ratzer, Rikke, Oturai, Annette Bang, Sørensen, Per Soelberg, Søndergaard, Helle Bach, and Sellebjerg, Finn

Subjects
*AMYLOID beta-protein, *PEPTIDES, *ALZHEIMER'S disease research, *PRESENILINS, *AMYLOID beta-protein precursor, *PROTEOLYSIS
Abstract

In multiple sclerosis (MS), treatment with the monoclonal antibody natalizumab effectively reduces the formation of acute lesions in the central nervous system (CNS). Natalizumab binds the integrin very late antigen (VLA)-4, expressed on the surface of immune cells, and inhibits VLA-4 dependent transmigration of circulating immune-cells across the vascular endothelium into the CNS. Recent studies suggested that natalizumab treated MS patients have an increased T-cell pool in the blood compartment which may be selectively enriched in activated T-cells. Proposed causes are sequestration of activated T-cells due to reduced extravasation of activated and pro-inflammatory T-cells or due to induction of VLA-4 mediated co-stimulatory signals by natalizumab. In this study we examined how natalizumab treatment altered the distribution of effector and memory T-cell subsets in the blood compartment and if T-cells in general or myelin-reactive T- cells in particular showed signs of increased immune activation. Furthermore we examined the effects of natalizumab on CD4+ T-cell responses to myelin in vitro. Natalizumab-treated MS patients had significantly increased numbers of effector- memory T-cells in the blood. In T-cells from natalizumab-treated MS patients, the expression of TNF-α mRNA was increased whereas the expression of fourteen other effector cytokines or transcription factors was unchanged. Natalizumab-treated MS patients had significantly decreased expression of the co-stimulatory molecule CD134 on CD4+ CD26HIGH T-cells, in blood, and natalizumab decreased the expression of CD134 on MBP-reactive CD26HIGH CD4+ T-cells in vitro. Otherwise CD4+ T-cells from natalizumab-treated and untreated MS patients showed similar responses to MBP. In conclusion natalizumab treatment selectively increased the effector memory T-cell pool but not the activation state of T-cells in the blood compartment. Myelin-reactive T-cells were not selectively increased in natalizumab treated MS. [ABSTRACT FROM AUTHOR]

Published
2012
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50. Cellular sources of dysregulated cytokines in relapsing-remitting multiple sclerosis.

Author

Christensen, Jeppe Romme, Börnsen, Lars, Hesse, Dan, Krakauer, Martin, Sørensen, Per Soelberg, Søndergaard, Helle Bach, and Sellebjerg, Finn

Subjects
*CELLULAR immunity, *CYTOKINES, *CEREBROSPINAL fluid, *RETICULO-endothelial system, *VIRUS diseases
Abstract

Background: Numerous cytokines are implicated in the immunopathogenesis of multiple sclerosis (MS), but studies are often limited to whole blood (WB) or peripheral blood mononuclear cells (PBMCs), thereby omitting important information about the cellular origin of the cytokines. Knowledge about the relation between blood and cerebrospinal fluid (CSF) cell expression of cytokines and the cellular source of CSF cytokines is even more scarce. Methods: We studied gene expression of a broad panel of cytokines in WB from relapsing-remitting multiple sclerosis (RRMS) patients in remission and healthy controls (HCs). Subsequently we determined the gene expression of the dysregulated cytokines in isolated PBMC subsets (CD4+, CD8+T-cells, NK-cells, B-cells, monocytes and dendritic cells) from RRMS patients and HCs and in CSF-cells from RRMS patients in clinical relapse and noninflammatory neurological controls (NIND). Results: RRMS patients had increased expression of IFN-gamma (IFNG), interleukin (IL) 1-beta (IL1B), IL7, IL10, IL12A, IL15, IL23, IL27, lymphotoxin-alpha (LTA) and lymphotoxin-beta (LTB) in WB. In PBMC subsets the main sources of pro-inflammatory cytokines were T- and B-cells, whereas monocytes were the most prominent source of immunoregulatory cytokines. In CSF-cells, RRMS patients had increased expression of IFNG and CD19 and decreased expression of IL10 and CD14 compared to NINDs. CD19 expression correlated with expression of IFNG, IL7, IL12A, IL15 and LTA whereas CD14 expression correlated with IL10 expression. Conclusions: Using a systematic approach, we show that expression of pro-inflammatory cytokines in peripheral blood primarily originates from T- and B-cells, with an important exception of IFNG which is most strongly expressed by NK-cells. In CSF-cell studies, B-cells appear to be enriched in RRMS and associated with expression of pro-inflammatory cytokines; contrarily, monocytes are relatively scarce in CSF from RRMS patients and are associated with IL10 expression. Thus, our findings suggest a pathogenetic role of B-cells and an immunoregulatory role of monocytes in RRMS. [ABSTRACT FROM AUTHOR]

Published
2012
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