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1. Modeling of waning immunity after SARS-CoV-2 vaccination and influencing factors

Author

Pérez-Alós, Laura, Armenteros, Jose Juan Almagro, Madsen, Johannes Roth, Hansen, Cecilie Bo, Jarlhelt, Ida, Hamm, Sebastian Rask, Heftdal, Line Dam, Pries-Heje, Mia Marie, Møller, Dina Leth, Fogh, Kamille, Hasselbalch, Rasmus Bo, Rosbjerg, Anne, Brunak, Søren, Sørensen, Erik, Larsen, Margit Anita Hørup, Ostrowski, Sisse Rye, Frikke-Schmidt, Ruth, Bayarri-Olmos, Rafael, Hilsted, Linda Maria, Iversen, Kasper Karmark, Bundgaard, Henning, Nielsen, Susanne Dam, and Garred, Peter

Published
2022
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3. Transient Binding Dynamics of Complement System Pattern Recognition Molecules on Pathogens

Author

Götz, Maximilian Peter, Villegas, Mario Alejandro Duque, Fageräng, Beatrice, Kerfin, Aileen, Skjoedt, Mikkel Ole, Garred, Peter, Rosbjerg, Anne, Götz, Maximilian Peter, Villegas, Mario Alejandro Duque, Fageräng, Beatrice, Kerfin, Aileen, Skjoedt, Mikkel Ole, Garred, Peter, and Rosbjerg, Anne

Abstract

Previous studies of pattern recognition molecules (PRMs) of the complement system have revealed difficulties in observing binding on pathogens such as Aspergillus fumigatus and Escherichia coli, despite complement deposition indicative of classical and lectin pathway activation. Thus, we investigated the binding dynamics of PRMs of the complement system, specifically C1q of the classical pathway and mannose-binding lectin (MBL) of the lectin pathway. We observed consistently increasing deposition of essential complement components such as C4b, C3b, and the terminal complement complex on A. fumigatus and E. coli. However, C1q and MBL binding to the surface rapidly declined during incubation after just 2–4 min in 10% plasma. The detachment of C1q and MBL can be linked to complement cascade activation, as the PRMs remain bound in the absence of plasma. The dissociation and the fate of C1q and MBL seem to have different mechanistic functions. Notably, C1q dynamics were associated with local C1 complex activation. When C1s was inhibited in plasma, C1q binding not only remained high but further increased over time. In contrast, MBL binding was inversely correlated with total and early complement activation due to MBL binding being partially retained by complement inhibition. Results indicate that detached MBL might be able to functionally rebind to A. fumigatus. In conclusion, these results reveal a (to our knowledge) novel “hit-and-run” complement-dependent PRM dynamic mechanism on pathogens. These dynamics may have profound implications for host defense and may help increase the functionality and longevity of complement-dependent PRMs in circulation.

Published
2024

4. CL-11 circulates in serum as functionally distinct isoforms

Author

Sutta, Adrian, Leemans, Nelia Nina, Ploug, Michael, Rosbjerg, Anne, del Agua Villa, Christian, Pérez-Alós, Laura, Cyranka, Leon, Vincek, Adam S., de Garay, Tomás, Rivera, Keith, Bayarri-Olmos, Rafael, Sutta, Adrian, Leemans, Nelia Nina, Ploug, Michael, Rosbjerg, Anne, del Agua Villa, Christian, Pérez-Alós, Laura, Cyranka, Leon, Vincek, Adam S., de Garay, Tomás, Rivera, Keith, and Bayarri-Olmos, Rafael

Abstract

Collectin-11 (CL-11) is a pattern recognition molecule of the lectin pathway capable of interacting with collectin-10 (CL-10) and the MASPs to activate the complement cascade. Alternative splicing of the COLEC11 gene gives rise to two different isoforms found in serum (A and D). These isoforms vary in the length of their collagen-like region, which is involved in the stabilization of the trimeric subunit and the interaction with the MASPs. Here we aim at elucidating the biological differences of naturally occurring CL-11 isoforms A and D. We produced recombinant CL-11 as independent isoforms (CL-11A and CL-11D) and together with CL-10 (CL-10/11A, CL-10/11D). Both CL-11 isoforms associated with CL-10, but CL-11D did so to a lesser extent. CL-10/11 heterocomplexes were composed of trimeric subunits of CL-10 and CL-11, as opposed to CL-10 and CL-11 homotrimers. Heterocomplexes were more stable and migrated with higher apparent molecular weights. Immunoprecipitation of serum CL-11 and subsequent mass spectrometry analysis confirmed that native CL-11 circulates in the form of CL-10/11 heterocomplexes that associate with MASP-1, and MASP-3, but not necessarily MASP-2. Despite a shorter collagen region, CL-11D was capable to bind to the MASPs, suggesting that the missing exon 4 is not required for MASP association CL-11D had a reduced ligand binding compared to full-length CL-11A. Based on its reduced ability to oligomerize, form CL-10/11 heterocomplexes, and bind to ligands, we hypothesize that CL-11D may have a limited complement activation potential compared to full-length CL-11A.

Published
2024

5. Rosbjerg, Anne

Author

Rosbjerg, Anne and Rosbjerg, Anne

Published
2024

6. Complement C7 and clusterin form a complex in circulation

Author

Massri, Mariam, primary, Toonen, Erik J.M., additional, Sarg, Bettina, additional, Kremser, Leopold, additional, Grasse, Marco, additional, Fleischer, Verena, additional, Torres-Quesada, Omar, additional, Hengst, Ludger, additional, Skjoedt, Mikkel-Ole, additional, Bayarri-Olmos, Rafael, additional, Rosbjerg, Anne, additional, Garred, Peter, additional, Orth-Höller, Dorothea, additional, Prohászka, Zoltán, additional, and Würzner, Reinhard, additional

Published
2024
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8. 182 Complement C7 and clusterin form a stable complex in circulation

Author

Massri, Mariam, primary, Toonen, Erik J.M., additional, Sarg, Bettina, additional, Kremser, Leopold, additional, Grasse, Marco, additional, Skjoedt, Mikkel-Ole, additional, Bayarri-Olmos, Raffael, additional, Rosbjerg, Anne, additional, Garred, Peter, additional, Orth, Dorothea, additional, Prohászka, Zoltán, additional, and Würzner, Reinhard, additional

Published
2023
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11. Short-Lived Antibody-Mediated Saliva Immunity against SARS-CoV-2 after Vaccination

Author

Madsen, Johannes Roth, primary, Holm, Bettina Eide, additional, Pérez-Alós, Laura, additional, Bayarri-Olmos, Rafael, additional, Rosbjerg, Anne, additional, Fogh, Kamille, additional, Pries-Heje, Mia Marie, additional, Møller, Dina Leth, additional, Hansen, Cecilie Bo, additional, Heftdal, Line Dam, additional, Hasselbalch, Rasmus Bo, additional, Hamm, Sebastian Rask, additional, Frikke-Schmidt, Ruth, additional, Hilsted, Linda, additional, Nielsen, Susanne Dam, additional, Iversen, Kasper Karmark, additional, Bundgaard, Henning, additional, and Garred, Peter, additional

Published
2023
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12. MAP-2:CD55 chimeric construct effectively modulates complement activation

Author

González-del-Barrio, Lydia, Pérez-Alós, Laura, Cyranka, Leon, Rosbjerg, Anne, Nagy, Simon, Prohászka, Zoltán, Garred, Peter, Bayarri-Olmos, Rafael, González-del-Barrio, Lydia, Pérez-Alós, Laura, Cyranka, Leon, Rosbjerg, Anne, Nagy, Simon, Prohászka, Zoltán, Garred, Peter, and Bayarri-Olmos, Rafael

Abstract

The complement system is a complex, tightly regulated protein cascade involved in pathogen defense and the pathogenesis of several diseases. Thus, the development of complement modulators has risen as a potential treatment for complement-driven inflammatory pathologies. The enzymatically inactive MAP-2 has been reported to inhibit the lectin pathway by competing with its homologous serine protease MASP-2. The membrane-bound complement inhibitor CD55 acts on the C3/C5 convertase level. Here, we fused MAP-2 to the four N-terminal domains of CD55 generating a targeted chimeric inhibitor to modulate complement activation at two different levels of the complement cascade. Its biological properties were compared in vitro with the parent molecules. While MAP-2 and CD55 alone showed a minor inhibition of the three complement pathways when co-incubated with serum (IC50MAP-2+CD551-4 = 60.98, 36.10, and 97.01 nM on the classical, lectin, and alternative pathways, respectively), MAP-2:CD551-4 demonstrated a potent inhibitory activity (IC50MAP-2:CD551-4 = 2.94, 1.76, and 12.86 nM, respectively). This inhibitory activity was substantially enhanced when pre-complexes were formed with the lectin pathway recognition molecule mannose-binding lectin (IC50MAP-2:CD551-4 = 0.14 nM). MAP-2:CD551-4 was also effective at protecting sensitized sheep erythrocytes in a classical hemolytic assay (CH50 = 13.35 nM). Finally, the chimeric inhibitor reduced neutrophil activation in full blood after stimulation with Aspergillus fumigatus conidia, as well as phagocytosis of conidia by isolated activated neutrophils. Our results demonstrate that MAP-2:CD551-4 is a potent complement inhibitor reinforcing the idea that engineered fusion proteins are a promising design strategy for identifying and developing drug candidates to treat complement-mediated diseases., The complement system is a complex, tightly regulated protein cascade involved in pathogen defense and the pathogenesis of several diseases. Thus, the development of complement modulators has risen as a potential treatment for complement-driven inflammatory pathologies. The enzymatically inactive MAP-2 has been reported to inhibit the lectin pathway by competing with its homologous serine protease MASP-2. The membrane-bound complement inhibitor CD55 acts on the C3/C5 convertase level. Here, we fused MAP-2 to the four N-terminal domains of CD55 generating a targeted chimeric inhibitor to modulate complement activation at two different levels of the complement cascade. Its biological properties were compared in vitro with the parent molecules. While MAP-2 and CD55 alone showed a minor inhibition of the three complement pathways when co-incubated with serum (IC50MAP-2+CD551-4 = 60.98, 36.10, and 97.01 nM on the classical, lectin, and alternative pathways, respectively), MAP-2:CD551-4 demonstrated a potent inhibitory activity (IC50MAP-2:CD551-4 = 2.94, 1.76, and 12.86 nM, respectively). This inhibitory activity was substantially enhanced when pre-complexes were formed with the lectin pathway recognition molecule mannose-binding lectin (IC50MAP-2:CD551-4 = 0.14 nM). MAP-2:CD551-4 was also effective at protecting sensitized sheep erythrocytes in a classical hemolytic assay (CH50 = 13.35 nM). Finally, the chimeric inhibitor reduced neutrophil activation in full blood after stimulation with Aspergillus fumigatus conidia, as well as phagocytosis of conidia by isolated activated neutrophils. Our results demonstrate that MAP-2:CD551-4 is a potent complement inhibitor reinforcing the idea that engineered fusion proteins are a promising design strategy for identifying and developing drug candidates to treat complement-mediated diseases.

Published
2023

13. Short-Lived Antibody-Mediated Saliva Immunity against SARS-CoV-2 after Vaccination

Author

Madsen, Johannes Roth, Holm, Bettina Eide, Pérez-Alós, Laura, Bayarri-Olmos, Rafael, Rosbjerg, Anne, Fogh, Kamille, Pries-Heje, Mia Marie, Møller, Dina Leth, Hansen, Cecilie Bo, Heftdal, Line Dam, Hasselbalch, Rasmus Bo, Hamm, Sebastian Rask, Frikke-Schmidt, Ruth, Hilsted, Linda, Nielsen, Susanne Dam, Iversen, Kasper Karmark, Bundgaard, Henning, Garred, Peter, Madsen, Johannes Roth, Holm, Bettina Eide, Pérez-Alós, Laura, Bayarri-Olmos, Rafael, Rosbjerg, Anne, Fogh, Kamille, Pries-Heje, Mia Marie, Møller, Dina Leth, Hansen, Cecilie Bo, Heftdal, Line Dam, Hasselbalch, Rasmus Bo, Hamm, Sebastian Rask, Frikke-Schmidt, Ruth, Hilsted, Linda, Nielsen, Susanne Dam, Iversen, Kasper Karmark, Bundgaard, Henning, and Garred, Peter

Abstract

Knowledge about the effect of vaccination against severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) on immunity reflected in the saliva is sparse. We examined the antibody response in saliva compared to that in serum 2 and 6 months after the first vaccination with the BNT162b2 vaccine. Four hundred fifty-nine health care professionals were included in a prospective observational study measuring antibody levels in saliva and corresponding serum samples at 2 and 6 months after BNT162b2 vaccination. Vaccinated, previously SARS-CoV-2-infected individuals (hybrid immunity) had higher IgG levels in saliva at 2 months than vaccinated, infection-naive individuals (P , 0.001). After 6 months, saliva IgG levels declined in both groups (P , 0.001), with no difference between groups (P = 0.37). Furthermore, serum IgG levels declined from 2 to 6 months in both groups (P , 0.001). IgG antibodies in saliva and serum correlated in individuals with hybrid immunity at 2 and 6 months (r = 0.58, P = 0.001, and r = 0.53, P = 0.052, respectively). In vaccinated, infection-naive individuals, a correlation was observed at 2 months (r = 0.42, P , 0.001) but not after 6 months (r = 0.14, P = 0.055). IgA and IgM antibodies were hardly detectable in saliva at any time point, regardless of previous infection. In serum, IgA was detected at 2 months in previously infected individuals. BNT162b2 vaccination induced a detectable IgG anti-SARS-CoV-2 RBD response in saliva at both 2 and 6 months after vaccination, being more prominent in previously infected than infection-naive individuals. However, a significant decrease in salivary IgG was observed after 6 months, suggesting a rapid decline in antibody-mediated saliva immunity against SARS-CoV-2, after both infection and systemic vaccination. IMPORTANCE Knowledge about the persistence of salivary immunity after SARS-CoV-2 vaccination is limited, and information on this topic could prove important for vaccine strategy and development. W

Published
2023

14. Functional Analysis of a Novel Complement C5a Receptor 1-Blocking Monoclonal Antibody

Author

Cyranka, Leon, Mariegaard, Ida, Skjødt, Mikkel Ole, Bayarri-Olmos, Rafael, Mollnes, Tom Eirik, Garred, Peter, Rosbjerg, Anne, Cyranka, Leon, Mariegaard, Ida, Skjødt, Mikkel Ole, Bayarri-Olmos, Rafael, Mollnes, Tom Eirik, Garred, Peter, and Rosbjerg, Anne

Abstract

Introduction: The complement system anaphylatoxin C5a is a critical player in inflammation. By binding to complement C5a receptor 1 (C5aR1/CD88), C5a regulates many cellular functions, mainly as a potent pro-inflammatory inducer. We describe the generation and selection of a potent antagonistic C5aR1 mouse monoclonal antibody (mAb). Methods: Initial C5aR1 hybridoma clone selection was performed with a cell-binding study in human whole blood. In-house C5aR1 mAb assessment for C5aR1 inhibition was done via the iLite® C5a assay. C5aR1 mAb specificity was investigated on C5aR1his-and C5aR2his-expressing Flp-In™-CHO cells. Physiological C5aR1 inhibition was assessed via a C5a-driven calcium flux assay and stimulation assay based on isolated polymorphonuclear leukocytes (PMNs) and a whole blood model stimulated with Escherichia coli. Results: The supernatant of hybridoma clones targeting the N-Terminal section of C5aR1 displayed efficient binding to C5aR1 in whole blood, which was confirmed for purified mAbs. The C5aR1 mAb 18-41-6 was selected following the assay of in-house C5aR1 mAbs via the iLite® C5a assay. The mAb 18-41-6 was specific for C5aR1. Full-size and/or F(ab')2 preparations of mAb 18-41-6 were found to efficiently abrogate C5a-induced calcium flux in neutrophils and to significantly reduce the upregulation of the activation markers CD11b (neutrophils, monocytes) and CD66b (neutrophils). Conclusion: Our results demonstrate that mAb 18-41-6 is a valuable tool for investigating the C5a-C5aR1 axis and a potential therapeutic candidate for inflammatory disease treatment.

Published
2023

18. The alpha/B.1.1.7 SARS-CoV-2 variant exhibits significantly higher affinity for ACE-2 and requires lower inoculation doses to cause disease in K18-hACE2 mice

Author

Bayarri-Olmos, Rafael, primary, Johnsen, Laust Bruun, additional, Idorn, Manja, additional, Reinert, Line S, additional, Rosbjerg, Anne, additional, Vang, Søren, additional, Hansen, Cecilie Bo, additional, Helgstrand, Charlotte, additional, Bjelke, Jais Rose, additional, Bak-Thomsen, Theresa, additional, Paludan, Søren R, additional, Garred, Peter, additional, and Skjoedt, Mikkel-Ole, additional

Published
2021
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21. Author response: The alpha/B.1.1.7 SARS-CoV-2 variant exhibits significantly higher affinity for ACE-2 and requires lower inoculation doses to cause disease in K18-hACE2 mice

Author

Bayarri-Olmos, Rafael, primary, Johnsen, Laust Bruun, additional, Idorn, Manja, additional, Reinert, Line S, additional, Rosbjerg, Anne, additional, Vang, Søren, additional, Hansen, Cecilie Bo, additional, Helgstrand, Charlotte, additional, Bjelke, Jais Rose, additional, Bak-Thomsen, Theresa, additional, Paludan, Søren R, additional, Garred, Peter, additional, and Skjoedt, Mikkel-Ole, additional

Published
2021
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22. SARS-CoV-2 Neutralizing Antibody Responses towards Full-Length Spike Protein and the Receptor-Binding Domain

Author

Bayarri-Olmos, Rafael, primary, Idorn, Manja, additional, Rosbjerg, Anne, additional, Pérez-Alós, Laura, additional, Hansen, Cecilie Bo, additional, Johnsen, Laust Bruun, additional, Helgstrand, Charlotte, additional, Zosel, Franziska, additional, Bjelke, Jais Rose, additional, Öberg, Fredrik Kryh, additional, Søgaard, Max, additional, Paludan, Søren R., additional, Bak-Thomsen, Theresa, additional, Jardine, Joseph G., additional, Skjoedt, Mikkel-Ole, additional, and Garred, Peter, additional

Published
2021
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23. The SARS-CoV-2 Y453F mink variant displays a pronounced increase in ACE-2 affinity but does not challenge antibody neutralization

Author

Bayarri-Olmos, Rafael, Rosbjerg, Anne, Johnsen, Laust Bruun, Helgstrand, Charlotte, Bak-Thomsen, Theresa, Garred, Peter, Skjoedt, Mikkel Ole, Bayarri-Olmos, Rafael, Rosbjerg, Anne, Johnsen, Laust Bruun, Helgstrand, Charlotte, Bak-Thomsen, Theresa, Garred, Peter, and Skjoedt, Mikkel Ole

Abstract

Transmission of Severe Acute Respiratory Syndrome Coronavirus 2 from humans to animals has been reported for many domesticated species, including farmed minks. The identification of novel spike gene mutations appearing in minks has raised major concerns about potential immune evasion and challenges for the global vaccine strategy. One genetic variant, known as "cluster five,"arose among farmed minks in Denmark and resulted in a complete shutdown of the world's largest mink production. However, the functional properties of this new variant are not established. Here we present functional data on the cluster-five variant, which contains a mutation resulting in a Y453F residue change in the receptor-binding domain (RBD) of the spike protein. Using an ELISA-based angiotensin-converting enzyme-2/RBD inhibition assay, we show that the Y453F variant does not decrease established humoral immunity from previously infected individuals or affect the neutralizing antibody response in a vaccine mouse model based on the original Wuhan strain RBD or spike as antigens. However, biolayer interferometry analysis demonstrates that it binds the human angiotensin-converting enzyme-2 receptor with a 4-fold higher affinity than the original strain, suggesting an enhanced transmission capacity and a possible challenge for viral control. These results also indicate that the rise in the frequency of the clusterfive variant in mink farms might be a result of the fitness advantage conferred by the receptor adaptation rather than evading immune responses.

Published
2021

24. The alpha/B.1.1.7 SARS-CoV-2 variant exhibits significantly higher affinity for ACE-2 and requires lower inoculation doses to cause disease in K18-hACE2 mice

Author

Bayarri-Olmos, Rafael, Johnsen, Laust Bruun, Idorn, Manja, Reinert, Line S., Rosbjerg, Anne, Vang, Søren, Hansen, Cecilie Bo, Helgstrand, Charlotte, Bjelke, Jais Rose, Bak-Thomsen, Theresa, Paludan, Søren R., Garred, Peter, Skjoedt, Mikkel-Ole, Bayarri-Olmos, Rafael, Johnsen, Laust Bruun, Idorn, Manja, Reinert, Line S., Rosbjerg, Anne, Vang, Søren, Hansen, Cecilie Bo, Helgstrand, Charlotte, Bjelke, Jais Rose, Bak-Thomsen, Theresa, Paludan, Søren R., Garred, Peter, and Skjoedt, Mikkel-Ole

Abstract

The alpha/B.1.1.7 SARS-CoV-2 lineage emerged in autumn 2020 in the United Kingdom and transmitted rapidly until winter 2021 when it was responsible for most new COVID-19 cases in many European countries. The incidence domination was likely due to a fitness advantage that could be driven by the RBD residue change (N501Y), which also emerged independently in other Variants of Concern such as the beta/B.1.351 and gamma/P.1 strains. Here we present a functional characterization of the alpha/B.1.1.7 variant and show an eight-fold affinity increase towards human ACE-2. In accordance with this, transgenic hACE-2 mice showed a faster disease progression and severity after infection with a low dose of B.1.1.7, compared to an early 2020 SARS-CoV-2 isolate. When challenged with sera from convalescent individuals or anti-RBD monoclonal antibodies, the N501Y variant showed a minor, but significant elevated evasion potential of ACE-2/RBD antibody neutralization. The data suggest that the single asparagine to tyrosine substitution remarkable rise in affinity may be responsible for the higher transmission rate and severity of the B.1.1.7 variant.

Published
2021

26. MASP-1 and MASP-3 bind directly to aspergillus fumigatus and promote complement activation and phagocytosis

Author

Rosbjerg, Anne, Würzner, Reinhard, Garred, Peter, Skjoedt, Mikkel Ole, Rosbjerg, Anne, Würzner, Reinhard, Garred, Peter, and Skjoedt, Mikkel Ole

Abstract

Activation of the complement system is mediated by the interaction between pathogens and pattern recognition molecules (PRMs); mannose-binding lectin (MBL), ficolins, and collectin-10/-11 from the lectin pathway and C1q from the classical pathway. Lectin pathway activation specifically depends on proteases named MBL-associated serine proteases (MASPs) that are found in complexes with PRMs. In this study, we hypothesize that MASPs can recognize selected pathogens independently of PRMs. Using different clinical strains of opportunistic fungi, we have observed that MASPs directly recognize certain fungal pathogens in a way that can facilitate complement activation. Among these were Aspergillus fumigatus - a dangerous pathogen, especially for immunocompromised patients. In flow cytometry and fluorescence microscopy, we found that MASP-1 and -3 bound to all A. fumigatus growth stages (conidia, germ tubes, and hyphae), whereas rMASP-2 and the nonproteolytic rMAP-1 did not. Bound rMASPs could recruit rMBL and rficolin-3 to A. fumigatus conidia in a nonclassical manner and activate complement via rMASP-2. In experiments using recombinant and purified components, rMASP-1 increased the neutrophilic phagocytosis of conidia. In serum where known complement activation pathways were blocked, phagocytosis could be mediated by rMASP-3. We have encountered an unknown pathway for complement activation and found that MASP-1 and MASP-3 have dual functions as enzymes and as PRMs.

Published
2021

27. SARS-CoV-2 antibody responses are correlated to disease severity in COVID-19 convalescent individuals

Author

Hansen, Cecilie Bo, Jarlhelt, Ida, Pérez-Alós, Laura, Landsy, Lone Hummelshøj, Loftager, Mette, Rosbjerg, Anne, Helgstrand, Charlotte, Bjelke, Jais Rose, Egebjerg, Thomas, Jardine, Joseph G., Jørgensen, Charlotte Sværke, Iversen, Kasper, Bayarri-Olmos, Rafael, Garred, Peter, Skjoedt, Mikkel Ole, Hansen, Cecilie Bo, Jarlhelt, Ida, Pérez-Alós, Laura, Landsy, Lone Hummelshøj, Loftager, Mette, Rosbjerg, Anne, Helgstrand, Charlotte, Bjelke, Jais Rose, Egebjerg, Thomas, Jardine, Joseph G., Jørgensen, Charlotte Sværke, Iversen, Kasper, Bayarri-Olmos, Rafael, Garred, Peter, and Skjoedt, Mikkel Ole

Abstract

Globally, the COVID-19 pandemic has had extreme consequences for the healthcare system and has led to calls for diagnostic tools to monitor and understand the transmission, pathogenesis, and epidemiology, as well as to evaluate future vaccination strategies. In this study, we have developed novel, to our knowledge, flexible ELISA-based assays for specific detection of human SARS-CoV-2 Abs against the receptor-binding domain, including an Ag sandwich ELISA relevant for large population screening and three isotype-specific assays for in-depth diagnostics. Their performance was evaluated in a cohort of 350 convalescent participants with previous COVID-19 infection, ranging from asymptomatic to critical cases. We mapped the Ab responses to different areas on protein N and S and showed that the IgM, A, and G Ab responses against receptor-binding domain are significantly correlated to the disease severity. These assays and the data generated from them are highly relevant for diagnostics and prognostics and contribute to the understanding of long-term COVID-19 immunity.

Published
2021

29. Vaccine monitoring shows that focused immunization with SARS-CoV-2 receptor-binding domain provides a better neutralizing antibody response than full-length spike protein

Author

Bayarri-Olmos, Rafael, primary, Idorn, Manja, additional, Rosbjerg, Anne, additional, Pérez-Alós, Laura, additional, Hansen, Cecilie, additional, Johsen, Laust, additional, Helgstrand, Charlotte, additional, Öberg, Fredrik Kryh, additional, Søgaard, Max, additional, Paludan, Søren, additional, Bak-Thomsen, Theresa, additional, Jardine, Joseph, additional, Skjoedt, Mikkel-Ole, additional, and Garred, Peter, additional

Published
2021
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32. SARS-CoV-2 Antibody Responses Are Correlated to Disease Severity in COVID-19 Convalescent Individuals

Author

Hansen, Cecilie Bo, primary, Jarlhelt, Ida, additional, Pérez-Alós, Laura, additional, Hummelshøj Landsy, Lone, additional, Loftager, Mette, additional, Rosbjerg, Anne, additional, Helgstrand, Charlotte, additional, Bjelke, Jais Rose, additional, Egebjerg, Thomas, additional, Jardine, Joseph G., additional, Sværke Jørgensen, Charlotte, additional, Iversen, Kasper, additional, Bayarri-Olmos, Rafael, additional, Garred, Peter, additional, and Skjoedt, Mikkel-Ole, additional

Published
2021
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33. SARS-CoV-2 antibody responses determine disease severity in COVID-19 infected individuals

Author

Hansen, Cecilie Bo, primary, Jarlhelt, Ida, additional, Pérez-Alós, Laura, additional, Hummelshøj Landsy, Lone, additional, Loftager, Mette, additional, Rosbjerg, Anne, additional, Helgstrand, Charlotte, additional, Bjelke, Jais Rose, additional, Egebjerg, Thomas, additional, Jardine, Joseph G., additional, Sværke Jørgensen, Charlotte, additional, Iversen, Kasper, additional, Bayarri-Olmos, Rafael, additional, Garred, Peter, additional, and Skjoedt, Mikkel-Ole, additional

Published
2020
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35. Functional Analysis of a Novel Complement C5a Receptor 1-Blocking Monoclonal Antibody

Author

Cyranka, Leon, Mariegaard, Ida, Skjødt, Mikkel-Ole, Bayarri-Olmos, Rafael, Mollnes, Tom Eirik, Garred, Peter, and Rosbjerg, Anne

Abstract

Introduction:The complement system anaphylatoxin C5a is a critical player in inflammation. By binding to complement C5a receptor 1 (C5aR1/CD88), C5a regulates many cellular functions, mainly as a potent pro-inflammatory inducer. We describe the generation and selection of a potent antagonistic C5aR1 mouse monoclonal antibody (mAb). Methods:Initial C5aR1 hybridoma clone selection was performed with a cell-binding study in human whole blood. In-house C5aR1 mAb assessment for C5aR1 inhibition was done via the iLite®C5a assay. C5aR1 mAb specificity was investigated on C5aR1his- and C5aR2his-expressing Flp-In™-CHO cells. Physiological C5aR1 inhibition was assessed via a C5a-driven calcium flux assay and stimulation assay based on isolated polymorphonuclear leukocytes (PMNs) and a whole blood model stimulated with Escherichia coli. Results:The supernatant of hybridoma clones targeting the N-terminal section of C5aR1 displayed efficient binding to C5aR1 in whole blood, which was confirmed for purified mAbs. The C5aR1 mAb 18-41-6 was selected following the assay of in-house C5aR1 mAbs via the iLite®C5a assay. The mAb 18-41-6 was specific for C5aR1. Full-size and/or F(ab’)2preparations of mAb 18-41-6 were found to efficiently abrogate C5a-induced calcium flux in neutrophils and to significantly reduce the upregulation of the activation markers CD11b (neutrophils, monocytes) and CD66b (neutrophils). Conclusion:Our results demonstrate that mAb 18-41-6 is a valuable tool for investigating the C5a-C5aR1 axis and a potential therapeutic candidate for inflammatory disease treatment.

Published
2022
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36. The lectin complement pathway is involved in protection against Enteroaggregative Escherichia coli infection

Author

Sørensen, Camilla Adler, Rosbjerg, Anne, Jensen, Betina Hebbelstrup, Krogfelt, Karen Angeliki, Garred, Peter, Sørensen, Camilla Adler, Rosbjerg, Anne, Jensen, Betina Hebbelstrup, Krogfelt, Karen Angeliki, and Garred, Peter

Abstract

Enteroaggregative Escherichia coli (EAEC) causes acute and persistent diarrhea worldwide. Still, the involvement of host factors in EAEC infections is unresolved. Binding of recognition molecules from the lectin pathway of complement to EAEC strains have been observed, but the importance is not known. Our aim was to uncover the involvement of these molecules in innate complement dependent immune protection toward EAEC. Binding of mannose-binding lectin, ficolin-1, -2, and -3 to four prototypic EAEC strains, and ficolin-2 binding to 56 clinical EAEC isolates were screened by a consumption-based ELISA method. Flow cytometry was used to determine deposition of C4b, C3b, and the bactericidal C5b-9 membrane attack complex (MAC) on the bacteria in combination with different complement inhibitors. In addition, the direct serum bactericidal effect was assessed. Screening of the prototypic EAEC strains revealed that ficolin-2 was the major binder among the lectin pathway recognition molecules. However, among the clinical EAEC isolates only a restricted number (n = 5) of the isolates bound ficolin-2. Using the ficolin-2 binding isolate C322-17 as a model, we found that incubation with normal human serum led to deposition of C4b, C3b, and to MAC formation. No inhibition of complement deposition was observed when a C1q inhibitor was added, while partial inhibition was observed when ficolin-2 or factor D inhibitors were used separately. Combining the inhibitors against ficolin-2 and factor D led to virtually complete inhibition of complement deposition and protection against direct bacterial killing. These results demonstrate that ficolin-2 may play an important role in innate immune protection against EAEC when an appropriate ligand is exposed, but many EAEC strains evade lectin pathway recognition and may, therefore, circumvent this strategy of innate host immune protection.

Published
2018

39. Evasion Mechanisms Used by Pathogens to Escape the Lectin Complement Pathway

Author

Rosbjerg, Anne, Genster, Ninette, Pilely, Katrine, Garred, Peter, Rosbjerg, Anne, Genster, Ninette, Pilely, Katrine, and Garred, Peter

Abstract

The complement system is a crucial defensive network that protects the host against invading pathogens. It is part of the innate immune system and can be initiated via three pathways: the lectin, classical and alternative activation pathway. Overall the network compiles a group of recognition molecules that bind specific patterns on microbial surfaces, a group of associated proteases that initiates the complement cascade, and a group of proteins that interact in proteolytic complexes or the terminal pore-forming complex. In addition, various regulatory proteins are important for controlling the level of activity. The result is a pro-inflammatory response meant to combat foreign microbes. Microbial elimination is, however, not a straight forward procedure; pathogens have adapted to their environment by evolving a collection of evasion mechanisms that circumvent the human complement system. Complement evasion strategies features different ways of exploiting human complement proteins and moreover features different pathogen-derived proteins that interfere with the normal processes. Accumulated, these mechanisms target all three complement activation pathways as well as the final common part of the cascade. This review will cover the currently known lectin pathway evasion mechanisms and give examples of pathogens that operate these to increase their chance of invasion, survival and dissemination.

Published
2017

40. C-Reactive Protein Binds to Cholesterol Crystals and Co-Localizes with the Terminal Complement Complex in Human Atherosclerotic Plaques

Author

Pilely, Katrine, Fumagalli, Stefano, Rosbjerg, Anne, Genster, Ninette, Skjoedt, Mikkel-Ole, Perego, Carlo, Ferrante, Angela M R, De Simoni, Maria-Grazia, Garred, Peter, Pilely, Katrine, Fumagalli, Stefano, Rosbjerg, Anne, Genster, Ninette, Skjoedt, Mikkel-Ole, Perego, Carlo, Ferrante, Angela M R, De Simoni, Maria-Grazia, and Garred, Peter

Abstract

Inflammation is a part of the initial process leading to atherosclerosis and cholesterol crystals (CC), found in atherosclerotic plaques, which are known to induce complement activation. The pentraxins C-reactive protein (CRP), long pentraxin 3 (PTX3), and serum amyloid P component (SAP) are serum proteins associated with increased risk of cardiovascular events and these proteins have been shown to interact with the complement system. Whether the pentraxins binds to CC and mediate downstream complement-dependent inflammatory processes remains unknown. Binding of CRP, PTX3, and SAP to CC was investigated in vitro by flow cytometry and fluorescence microscopy. CRP, PTX3, and SAP bound to CC in a concentration-dependent manner. CRP and PTX3 interacted with the complement pattern recognition molecule C1q on CC by increasing the binding of both purified C1q and C1q in plasma. However, CRP was the strongest mediator of C1q binding and also the pentraxin that most potently elevated C1q-mediated complement activation. In a phagocytic assay using whole blood, we confirmed that phagocytosis of CC is complement dependent and initiated by C1q-mediated activation. The pathophysiological relevance of the in vitro observations was examined in vivo in human atherosclerotic plaques. CRP, PTX3, and SAP were all found in atherosclerotic plaques and were located mainly in the cholesterol-rich necrotic core, but co-localization with the terminal C5b-9 complement complex was only found for CRP. In conclusion, this study identifies CRP as a strong C1q recruiter and complement facilitator on CC, which may be highly relevant for the development of atherosclerosis.

Published
2017

41. Ficolin-2 from the lectin pathway of complement recognizes enteroaggregative Escherichia coli and contributes to innate complement dependent immune protection

Author

Sørensen, Camilla Adler, Rosbjerg, Anne, Jensen, Betina Hebbelstrup, Krogfelt, Karen Angeliki, Garred, Peter, Sørensen, Camilla Adler, Rosbjerg, Anne, Jensen, Betina Hebbelstrup, Krogfelt, Karen Angeliki, and Garred, Peter

Abstract

Background: Enteroaggregative Escherichia coli (EAEC) is a cause of acute and persistent diarrhea in adults and children worldwide. The involvement of host factors in EAEC infections is unresolved. Binding of the recognition molecule ficolin-2 from the lectin pathway of complement to certain EAEC strains has been observed, but the importance is not known. Our aim was to uncover the involvement of ficolin-2 in innate complement dependent immune protection towards EAEC. Materials and methods: Ficolin-2 binding was screened by a consumption based ELISA method. Flow cytometry determined the deposition of C4, C3 and formation of the bactericidal C5b-9 membrane attack complex (MAC) on the bacteria in combination with inhibitors against C1q, ficolin-2, and factor D from the classical, lectin, and alternative pathway, respectively. Results and conclusion: Initial screening showed that ficolin-2 bound to three EAEC prototypic laboratory strains. Further screening of 56 EAEC clinical isolates showed that one isolate (E2-1920073) was particularly capable of binding high levels of both recombinant and serum ficolin-2. Thus, we chose to use this isolate to study functional complement deposition. Incubation of the E2-1920073 strain with serum led to deposition of C4, C3 and MAC formation. No inhibition of complement deposition was observed when a C1q inhibitor was added, while partial inhibition was observed when ficolin-2 or factor D inhibitors were used. Combining the inhibitors against ficolin-2 and factor D led to complete inhibition of complement deposition. Our results demonstrate that ficolin-2 is involved in the pathophysiology of EAEC and is crucial in innate complement dependent immune protection against pathogenic EAEC bacteria.

Published
2017

42. MASP-1 and MASP-3 Bind Directly to Aspergillus fumigatusand Promote Complement Activation and Phagocytosis

Author

Rosbjerg, Anne, Würzner, Reinhard, Garred, Peter, and Skjoedt, Mikkel-Ole

Abstract

Activation of the complement system is mediated by the interaction between pathogens and pattern recognition molecules (PRMs); mannose-binding lectin (MBL), ficolins, and collectin-10/-11 from the lectin pathway and C1q from the classical pathway. Lectin pathway activation specifically depends on proteases named MBL-associated serine proteases (MASPs) that are found in complexes with PRMs. In this study, we hypothesize that MASPs can recognize selected pathogens independently of PRMs. Using different clinical strains of opportunistic fungi, we have observed that MASPs directly recognize certain fungal pathogens in a way that can facilitate complement activation. Among these were Aspergillus fumigatus– a dangerous pathogen, especially for immunocompromised patients. In flow cytometry and fluorescence microscopy, we found that MASP-1 and -3 bound to all A. fumigatusgrowth stages (conidia, germ tubes, and hyphae), whereas rMASP-2 and the nonproteolytic rMAP-1 did not. Bound rMASPs could recruit rMBL and rficolin-3 to A. fumigatusconidia in a nonclassical manner and activate complement via rMASP-2. In experiments using recombinant and purified components, rMASP-1 increased the neutrophilic phagocytosis of conidia. In serum where known complement activation pathways were blocked, phagocytosis could be mediated by rMASP-3. We have encountered an unknown pathway for complement activation and found that MASP-1 and MASP-3 have dual functions as enzymes and as PRMs.

Published
2021
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48. Cholesterol Crystals Activate the Lectin Complement Pathway via Ficolin-2 and Mannose-Binding Lectin:Implications for the Progression of Atherosclerosis

Author

Pilely, Katrine, Rosbjerg, Anne, Genster, Ninette, Gál, Péter, Pál, Gábor, Halvorsen, Bente, Holm, Sverre, Aukrust, Pål, Bakke, Siril Skaret, Sporsheim, Bjørnar, Nervik, Ingunn, Niyonzima, Nathalie, Bartels, Emil Daniel, Stahl, Gregory L, Mollnes, Tom Eirik, Espevik, Terje, Garred, Peter, Pilely, Katrine, Rosbjerg, Anne, Genster, Ninette, Gál, Péter, Pál, Gábor, Halvorsen, Bente, Holm, Sverre, Aukrust, Pål, Bakke, Siril Skaret, Sporsheim, Bjørnar, Nervik, Ingunn, Niyonzima, Nathalie, Bartels, Emil Daniel, Stahl, Gregory L, Mollnes, Tom Eirik, Espevik, Terje, and Garred, Peter

Abstract

Cholesterol crystals (CC) play an essential role in the formation of atherosclerotic plaques. CC activate the classical and the alternative complement pathways, but the role of the lectin pathway is unknown. We hypothesized that the pattern recognition molecules (PRMs) from the lectin pathway bind CC and function as an upstream innate inflammatory signal in the pathophysiology of atherosclerosis. We investigated the binding of the PRMs mannose-binding lectin (MBL), ficolin-1, ficolin-2, and ficolin-3, the associated serine proteases, and complement activation products to CC in vitro using recombinant proteins, specific inhibitors, as well as deficient and normal sera. Additionally, we examined the deposition of ficolin-2 and MBL in human carotid plaques by immunohistochemistry and fluorescence microscopy. The results showed that the lectin pathway was activated on CC by binding of ficolin-2 and MBL in vitro, resulting in activation and deposition of complement activation products. MBL bound to CC in a calcium-dependent manner whereas ficolin-2 binding was calcium-independent. No binding was observed for ficolin-1 or ficolin-3. MBL and ficolin-2 were present in human carotid plaques, and binding of MBL to CC was confirmed in vivo by immunohistochemistry, showing localization of MBL around CC clefts. Moreover, we demonstrated that IgM, but not IgG, bound to CC in vitro and that C1q binding was facilitated by IgM. In conclusion, our study demonstrates that PRMs from the lectin pathway recognize CC and provides evidence for an important role for this pathway in the inflammatory response induced by CC in the pathophysiology of atherosclerosis.

Published
2016

49. Complementary Roles of the Classical and Lectin Complement Pathways in the Defense against Aspergillus fumigatus

Author

Rosbjerg, Anne, Genster, Ninette, Pilely, Katrine, Skjoedt, Mikkel-Ole, Stahl, Gregory L, Garred, Peter, Rosbjerg, Anne, Genster, Ninette, Pilely, Katrine, Skjoedt, Mikkel-Ole, Stahl, Gregory L, and Garred, Peter

Abstract

Aspergillus fumigatus infections are associated with a high mortality rate for immunocompromised patients. The complement system is considered to be important in protection against this fungus, yet the course of activation is unclear. The aim of this study was to unravel the role of the classical, lectin, and alternative pathways under both immunocompetent and immunocompromised conditions to provide a relevant dual-perspective on the response against A. fumigatus. Conidia (spores) from a clinical isolate of A. fumigatus were combined with various human serum types (including serum deficient of various complement components and serum from umbilical cord blood). We also combined this with inhibitors against C1q, mannose-binding lectin (MBL), and ficolin-2 before complement activation products and phagocytosis were detected by flow cytometry. Our results showed that alternative pathway amplified complement on A. fumigatus, but required classical and/or lectin pathway for initiation. In normal human serum, this initiation came primarily from the classical pathway. However, with a dysfunctional classical pathway (C1q-deficient serum), lectin pathway activated complement and mediated opsonophagocytosis through MBL. To model the antibody-decline in a compromised immune system, we used serum from normal umbilical cords and found MBL to be the key complement initiator. In another set of experiments, serum from patients with different kinds of immunoglobulin insufficiencies showed that the MBL lectin pathway contribution was highest in the samples with the lowest IgG/IgM binding. In conclusion, lectin pathway appears to be the primary route of complement activation in the absence of anti-A. fumigatus antibodies, whereas in a balanced immune state classical pathway is the main activator. This suggests a crucial role for the lectin pathway in innate immune protection against A. fumigatus in immunocompromised patients.

Published
2016

50. A journey through the lectin pathway of complement-MBL and beyond

Author

Garred, Peter, Genster, Ninette, Pilely, Katrine, Bayarri-Olmos, Rafael, Rosbjerg, Anne, Ma, Ying Jie, Skjoedt, Mikkel-Ole, Garred, Peter, Genster, Ninette, Pilely, Katrine, Bayarri-Olmos, Rafael, Rosbjerg, Anne, Ma, Ying Jie, and Skjoedt, Mikkel-Ole

Abstract

Mannose-binding lectin (MBL), collectin-10, collectin-11, and the ficolins (ficolin-1, ficolin-2, and ficolin-3) are soluble pattern recognition molecules in the lectin complement pathway. These proteins act as mediators of host defense and participate in maintenance of tissue homeostasis. They bind to conserved pathogen-specific structures and altered self-antigens and form complexes with the pentraxins to modulate innate immune functions. All molecules exhibit distinct expression in different tissue compartments, but all are found to a varying degree in the circulation. A common feature of these molecules is their ability to interact with a set of serine proteases named MASPs (MASP-1, MASP-2, and MASP-3). MASP-1 and -2 trigger the activation of the lectin pathway and MASP-3 may be involved in the activation of the alternative pathway of complement. Furthermore, MASPs mediate processes related to coagulation, bradykinin release, and endothelial and platelet activation. Variant alleles affecting expression and structure of the proteins have been associated with a variety of infectious and non-infectious diseases, most commonly as disease modifiers. Notably, the severe 3MC (Malpuech, Michels, Mingarelli, and Carnevale) embryonic development syndrome originates from rare mutations affecting either collectin-11 or MASP-3, indicating a broader functionality of the complement system than previously anticipated. This review summarizes the characteristics of the molecules in the lectin pathway.

Published
2016

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