Complement-Opsonized Nano-Carriers Are Bound by Dendritic Cells (DC) via Complement Receptor (CR)3, and by B Cell Subpopulations via CR-1/2, and Affect the Activation of DC and B-1 Cells

The development of nanocarriers (NC) for biomedical applications has gained large interest due to their potential to co-deliver drugs in a cell-type-targeting manner. However, depending on their surface characteristics, NC accumulate serum factors, termed protein corona, which may affect their cellu...

Descripción completa

Detalles Bibliográficos
Autores principales: Bednarczyk, Monika, Medina-Montano, Carolina, Fittler, Frederic Julien, Stege, Henner, Roskamp, Meike, Kuske, Michael, Langer, Christian, Vahldieck, Marco, Montermann, Evelyn, Tubbe, Ingrid, Röhrig, Nadine, Dzionek, Andrzej, Grabbe, Stephan, Bros, Matthias
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8001596/
https://www.ncbi.nlm.nih.gov/pubmed/33799879
http://dx.doi.org/10.3390/ijms22062869
_version_ 1783671267199549440
author Bednarczyk, Monika
Medina-Montano, Carolina
Fittler, Frederic Julien
Stege, Henner
Roskamp, Meike
Kuske, Michael
Langer, Christian
Vahldieck, Marco
Montermann, Evelyn
Tubbe, Ingrid
Röhrig, Nadine
Dzionek, Andrzej
Grabbe, Stephan
Bros, Matthias
author_facet Bednarczyk, Monika
Medina-Montano, Carolina
Fittler, Frederic Julien
Stege, Henner
Roskamp, Meike
Kuske, Michael
Langer, Christian
Vahldieck, Marco
Montermann, Evelyn
Tubbe, Ingrid
Röhrig, Nadine
Dzionek, Andrzej
Grabbe, Stephan
Bros, Matthias
author_sort Bednarczyk, Monika
collection PubMed
description The development of nanocarriers (NC) for biomedical applications has gained large interest due to their potential to co-deliver drugs in a cell-type-targeting manner. However, depending on their surface characteristics, NC accumulate serum factors, termed protein corona, which may affect their cellular binding. We have previously shown that NC coated with carbohydrates to enable biocompatibility triggered the lectin-dependent complement pathway, resulting in enhanced binding to B cells via complement receptor (CR)1/2. Here we show that such NC also engaged all types of splenic leukocytes known to express CR3 at a high rate when NC were pre-incubated with native mouse serum resulting in complement opsonization. By focusing on dendritic cells (DC) as an important antigen-presenting cell type, we show that CR3 was essential for binding/uptake of complement-opsonized NC, whereas CR4, which in mouse is specifically expressed by DC, played no role. Further, a minor B cell subpopulation (B-1), which is important for first-line pathogen responses, and co-expressed CR1/2 and CR3, in general, engaged NC to a much higher extent than normal B cells. Here, we identified CR-1/2 as necessary for binding of complement-opsonized NC, whereas CR3 was dispensable. Interestingly, the binding of complement-opsonized NC to both DC and B-1 cells affected the expression of activation markers. Our findings may have important implications for the design of nano-vaccines against infectious diseases, which codeliver pathogen-specific protein antigen and adjuvant, aimed to induce a broad adaptive cellular and humoral immune response by inducing cytotoxic T lymphocytes that kill infected cells and pathogen-neutralizing antibodies, respectively. Decoration of nano-vaccines either with carbohydrates to trigger complement activation in vivo or with active complement may result in concomitant targeting of DC and B cells and thereby may strongly enhance the extent of dual cellular/humoral immune responses.
format Online
Article
Text
id pubmed-8001596
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-80015962021-03-28 Complement-Opsonized Nano-Carriers Are Bound by Dendritic Cells (DC) via Complement Receptor (CR)3, and by B Cell Subpopulations via CR-1/2, and Affect the Activation of DC and B-1 Cells Bednarczyk, Monika Medina-Montano, Carolina Fittler, Frederic Julien Stege, Henner Roskamp, Meike Kuske, Michael Langer, Christian Vahldieck, Marco Montermann, Evelyn Tubbe, Ingrid Röhrig, Nadine Dzionek, Andrzej Grabbe, Stephan Bros, Matthias Int J Mol Sci Article The development of nanocarriers (NC) for biomedical applications has gained large interest due to their potential to co-deliver drugs in a cell-type-targeting manner. However, depending on their surface characteristics, NC accumulate serum factors, termed protein corona, which may affect their cellular binding. We have previously shown that NC coated with carbohydrates to enable biocompatibility triggered the lectin-dependent complement pathway, resulting in enhanced binding to B cells via complement receptor (CR)1/2. Here we show that such NC also engaged all types of splenic leukocytes known to express CR3 at a high rate when NC were pre-incubated with native mouse serum resulting in complement opsonization. By focusing on dendritic cells (DC) as an important antigen-presenting cell type, we show that CR3 was essential for binding/uptake of complement-opsonized NC, whereas CR4, which in mouse is specifically expressed by DC, played no role. Further, a minor B cell subpopulation (B-1), which is important for first-line pathogen responses, and co-expressed CR1/2 and CR3, in general, engaged NC to a much higher extent than normal B cells. Here, we identified CR-1/2 as necessary for binding of complement-opsonized NC, whereas CR3 was dispensable. Interestingly, the binding of complement-opsonized NC to both DC and B-1 cells affected the expression of activation markers. Our findings may have important implications for the design of nano-vaccines against infectious diseases, which codeliver pathogen-specific protein antigen and adjuvant, aimed to induce a broad adaptive cellular and humoral immune response by inducing cytotoxic T lymphocytes that kill infected cells and pathogen-neutralizing antibodies, respectively. Decoration of nano-vaccines either with carbohydrates to trigger complement activation in vivo or with active complement may result in concomitant targeting of DC and B cells and thereby may strongly enhance the extent of dual cellular/humoral immune responses. MDPI 2021-03-11 /pmc/articles/PMC8001596/ /pubmed/33799879 http://dx.doi.org/10.3390/ijms22062869 Text en © 2021 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Bednarczyk, Monika
Medina-Montano, Carolina
Fittler, Frederic Julien
Stege, Henner
Roskamp, Meike
Kuske, Michael
Langer, Christian
Vahldieck, Marco
Montermann, Evelyn
Tubbe, Ingrid
Röhrig, Nadine
Dzionek, Andrzej
Grabbe, Stephan
Bros, Matthias
Complement-Opsonized Nano-Carriers Are Bound by Dendritic Cells (DC) via Complement Receptor (CR)3, and by B Cell Subpopulations via CR-1/2, and Affect the Activation of DC and B-1 Cells
title Complement-Opsonized Nano-Carriers Are Bound by Dendritic Cells (DC) via Complement Receptor (CR)3, and by B Cell Subpopulations via CR-1/2, and Affect the Activation of DC and B-1 Cells
title_full Complement-Opsonized Nano-Carriers Are Bound by Dendritic Cells (DC) via Complement Receptor (CR)3, and by B Cell Subpopulations via CR-1/2, and Affect the Activation of DC and B-1 Cells
title_fullStr Complement-Opsonized Nano-Carriers Are Bound by Dendritic Cells (DC) via Complement Receptor (CR)3, and by B Cell Subpopulations via CR-1/2, and Affect the Activation of DC and B-1 Cells
title_full_unstemmed Complement-Opsonized Nano-Carriers Are Bound by Dendritic Cells (DC) via Complement Receptor (CR)3, and by B Cell Subpopulations via CR-1/2, and Affect the Activation of DC and B-1 Cells
title_short Complement-Opsonized Nano-Carriers Are Bound by Dendritic Cells (DC) via Complement Receptor (CR)3, and by B Cell Subpopulations via CR-1/2, and Affect the Activation of DC and B-1 Cells
title_sort complement-opsonized nano-carriers are bound by dendritic cells (dc) via complement receptor (cr)3, and by b cell subpopulations via cr-1/2, and affect the activation of dc and b-1 cells
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8001596/
https://www.ncbi.nlm.nih.gov/pubmed/33799879
http://dx.doi.org/10.3390/ijms22062869
work_keys_str_mv AT bednarczykmonika complementopsonizednanocarriersareboundbydendriticcellsdcviacomplementreceptorcr3andbybcellsubpopulationsviacr12andaffecttheactivationofdcandb1cells
AT medinamontanocarolina complementopsonizednanocarriersareboundbydendriticcellsdcviacomplementreceptorcr3andbybcellsubpopulationsviacr12andaffecttheactivationofdcandb1cells
AT fittlerfredericjulien complementopsonizednanocarriersareboundbydendriticcellsdcviacomplementreceptorcr3andbybcellsubpopulationsviacr12andaffecttheactivationofdcandb1cells
AT stegehenner complementopsonizednanocarriersareboundbydendriticcellsdcviacomplementreceptorcr3andbybcellsubpopulationsviacr12andaffecttheactivationofdcandb1cells
AT roskampmeike complementopsonizednanocarriersareboundbydendriticcellsdcviacomplementreceptorcr3andbybcellsubpopulationsviacr12andaffecttheactivationofdcandb1cells
AT kuskemichael complementopsonizednanocarriersareboundbydendriticcellsdcviacomplementreceptorcr3andbybcellsubpopulationsviacr12andaffecttheactivationofdcandb1cells
AT langerchristian complementopsonizednanocarriersareboundbydendriticcellsdcviacomplementreceptorcr3andbybcellsubpopulationsviacr12andaffecttheactivationofdcandb1cells
AT vahldieckmarco complementopsonizednanocarriersareboundbydendriticcellsdcviacomplementreceptorcr3andbybcellsubpopulationsviacr12andaffecttheactivationofdcandb1cells
AT montermannevelyn complementopsonizednanocarriersareboundbydendriticcellsdcviacomplementreceptorcr3andbybcellsubpopulationsviacr12andaffecttheactivationofdcandb1cells
AT tubbeingrid complementopsonizednanocarriersareboundbydendriticcellsdcviacomplementreceptorcr3andbybcellsubpopulationsviacr12andaffecttheactivationofdcandb1cells
AT rohrignadine complementopsonizednanocarriersareboundbydendriticcellsdcviacomplementreceptorcr3andbybcellsubpopulationsviacr12andaffecttheactivationofdcandb1cells
AT dzionekandrzej complementopsonizednanocarriersareboundbydendriticcellsdcviacomplementreceptorcr3andbybcellsubpopulationsviacr12andaffecttheactivationofdcandb1cells
AT grabbestephan complementopsonizednanocarriersareboundbydendriticcellsdcviacomplementreceptorcr3andbybcellsubpopulationsviacr12andaffecttheactivationofdcandb1cells
AT brosmatthias complementopsonizednanocarriersareboundbydendriticcellsdcviacomplementreceptorcr3andbybcellsubpopulationsviacr12andaffecttheactivationofdcandb1cells

Ejemplares similares