The role of Mannose Binding Lectin in the immune response against Borrelia burgdorferi sensu lato
The causative agents of Lyme borreliosis, spirochetes belonging to the Borrelia burgdorferi sensu lato group, have developed several ways to protect themselves against killing by the host complement system. In addition, it has been shown that serum sensitive isolates are (partially) protected by the...
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| Vydáno v: | Scientific reports Ročník 9; číslo 1; s. 1431 |
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| Hlavní autoři: | , , , , , , , , , |
| Médium: | Journal Article |
| Jazyk: | angličtina |
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Nature Publishing Group UK
05.02.2019
Nature Publishing Group |
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| ISSN: | 2045-2322, 2045-2322 |
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| Abstract | The causative agents of Lyme borreliosis, spirochetes belonging to the
Borrelia burgdorferi
sensu lato group, have developed several ways to protect themselves against killing by the host complement system. In addition, it has been shown that serum sensitive isolates are (partially) protected by the
Ixodes
Tick Salivary Lectin Pathway Inhibitor (TSLPI) protein; a salivary gland protein that inhibits the function of Mannose Binding Lectin (MBL). MBL is a C-type lectin that recognizes oligosaccharides on pathogens and activates the complement system via the lectin pathway. MBL deficiency has been linked to a more severe course of several infectious diseases and humans with detectable antibodies against
B. burgdorferi
are significantly more often MBL deficient compared to humans without antibodies against
B. burgdorferi
. Here we set out to investigate the role of MBL in the immune response against
B. burgdorferi
in more detail. We demonstrate that
B. burgdorferi
N40 needle-infected C57BL/6 MBL deficient mice harbored significantly higher
B. burgdorferi
numbers in skin tissue during the early course of infection. In line with these findings they also developed higher anti-
B. burgdorferi
IgG serum antibodies compared to WT controls. In contrast
, B. burgdorferi
loads in distant tissue such as heart, joints or bladder at later time points were similar for both mouse strains. These
in vivo
findings were corroborated using a
B. burgdorferi
N40-infected
I. scapularis
infestation model. We showed that MBL is capable of binding
B. burgdorferi
through its carbohydrate recognition domains, but
in vitro
complement killing assays, peritoneal macrophage and whole blood stimulations, phagocytosis assays and an
in vivo
migration experiment did not reveal the mechanism by which MBL facilitates early clearance of
B. burgdorferi
. To conclude, we show a protective role of MBL in the early stages of
B. burgdorferi
infection, yet the underlying mechanism warrants further investigation. |
|---|---|
| AbstractList | The causative agents of Lyme borreliosis, spirochetes belonging to the Borrelia burgdorferi sensu lato group, have developed several ways to protect themselves against killing by the host complement system. In addition, it has been shown that serum sensitive isolates are (partially) protected by the Ixodes Tick Salivary Lectin Pathway Inhibitor (TSLPI) protein; a salivary gland protein that inhibits the function of Mannose Binding Lectin (MBL). MBL is a C-type lectin that recognizes oligosaccharides on pathogens and activates the complement system via the lectin pathway. MBL deficiency has been linked to a more severe course of several infectious diseases and humans with detectable antibodies against B. burgdorferi are significantly more often MBL deficient compared to humans without antibodies against B. burgdorferi. Here we set out to investigate the role of MBL in the immune response against B. burgdorferi in more detail. We demonstrate that B. burgdorferi N40 needle-infected C57BL/6 MBL deficient mice harbored significantly higher B. burgdorferi numbers in skin tissue during the early course of infection. In line with these findings they also developed higher anti-B. burgdorferi IgG serum antibodies compared to WT controls. In contrast, B. burgdorferi loads in distant tissue such as heart, joints or bladder at later time points were similar for both mouse strains. These in vivo findings were corroborated using a B. burgdorferi N40-infected I. scapularis infestation model. We showed that MBL is capable of binding B. burgdorferi through its carbohydrate recognition domains, but in vitro complement killing assays, peritoneal macrophage and whole blood stimulations, phagocytosis assays and an in vivo migration experiment did not reveal the mechanism by which MBL facilitates early clearance of B. burgdorferi. To conclude, we show a protective role of MBL in the early stages of B. burgdorferi infection, yet the underlying mechanism warrants further investigation.The causative agents of Lyme borreliosis, spirochetes belonging to the Borrelia burgdorferi sensu lato group, have developed several ways to protect themselves against killing by the host complement system. In addition, it has been shown that serum sensitive isolates are (partially) protected by the Ixodes Tick Salivary Lectin Pathway Inhibitor (TSLPI) protein; a salivary gland protein that inhibits the function of Mannose Binding Lectin (MBL). MBL is a C-type lectin that recognizes oligosaccharides on pathogens and activates the complement system via the lectin pathway. MBL deficiency has been linked to a more severe course of several infectious diseases and humans with detectable antibodies against B. burgdorferi are significantly more often MBL deficient compared to humans without antibodies against B. burgdorferi. Here we set out to investigate the role of MBL in the immune response against B. burgdorferi in more detail. We demonstrate that B. burgdorferi N40 needle-infected C57BL/6 MBL deficient mice harbored significantly higher B. burgdorferi numbers in skin tissue during the early course of infection. In line with these findings they also developed higher anti-B. burgdorferi IgG serum antibodies compared to WT controls. In contrast, B. burgdorferi loads in distant tissue such as heart, joints or bladder at later time points were similar for both mouse strains. These in vivo findings were corroborated using a B. burgdorferi N40-infected I. scapularis infestation model. We showed that MBL is capable of binding B. burgdorferi through its carbohydrate recognition domains, but in vitro complement killing assays, peritoneal macrophage and whole blood stimulations, phagocytosis assays and an in vivo migration experiment did not reveal the mechanism by which MBL facilitates early clearance of B. burgdorferi. To conclude, we show a protective role of MBL in the early stages of B. burgdorferi infection, yet the underlying mechanism warrants further investigation. The causative agents of Lyme borreliosis, spirochetes belonging to the Borrelia burgdorferi sensu lato group, have developed several ways to protect themselves against killing by the host complement system. In addition, it has been shown that serum sensitive isolates are (partially) protected by the Ixodes Tick Salivary Lectin Pathway Inhibitor (TSLPI) protein; a salivary gland protein that inhibits the function of Mannose Binding Lectin (MBL). MBL is a C-type lectin that recognizes oligosaccharides on pathogens and activates the complement system via the lectin pathway. MBL deficiency has been linked to a more severe course of several infectious diseases and humans with detectable antibodies against B. burgdorferi are significantly more often MBL deficient compared to humans without antibodies against B. burgdorferi. Here we set out to investigate the role of MBL in the immune response against B. burgdorferi in more detail. We demonstrate that B. burgdorferi N40 needle-infected C57BL/6 MBL deficient mice harbored significantly higher B. burgdorferi numbers in skin tissue during the early course of infection. In line with these findings they also developed higher anti-B. burgdorferi IgG serum antibodies compared to WT controls. In contrast, B. burgdorferi loads in distant tissue such as heart, joints or bladder at later time points were similar for both mouse strains. These in vivo findings were corroborated using a B. burgdorferi N40-infected I. scapularis infestation model. We showed that MBL is capable of binding B. burgdorferi through its carbohydrate recognition domains, but in vitro complement killing assays, peritoneal macrophage and whole blood stimulations, phagocytosis assays and an in vivo migration experiment did not reveal the mechanism by which MBL facilitates early clearance of B. burgdorferi. To conclude, we show a protective role of MBL in the early stages of B. burgdorferi infection, yet the underlying mechanism warrants further investigation. The causative agents of Lyme borreliosis, spirochetes belonging to the Borrelia burgdorferi sensu lato group, have developed several ways to protect themselves against killing by the host complement system. In addition, it has been shown that serum sensitive isolates are (partially) protected by the Ixodes Tick Salivary Lectin Pathway Inhibitor (TSLPI) protein; a salivary gland protein that inhibits the function of Mannose Binding Lectin (MBL). MBL is a C-type lectin that recognizes oligosaccharides on pathogens and activates the complement system via the lectin pathway. MBL deficiency has been linked to a more severe course of several infectious diseases and humans with detectable antibodies against B. burgdorferi are significantly more often MBL deficient compared to humans without antibodies against B. burgdorferi . Here we set out to investigate the role of MBL in the immune response against B. burgdorferi in more detail. We demonstrate that B. burgdorferi N40 needle-infected C57BL/6 MBL deficient mice harbored significantly higher B. burgdorferi numbers in skin tissue during the early course of infection. In line with these findings they also developed higher anti- B. burgdorferi IgG serum antibodies compared to WT controls. In contrast , B. burgdorferi loads in distant tissue such as heart, joints or bladder at later time points were similar for both mouse strains. These in vivo findings were corroborated using a B. burgdorferi N40-infected I. scapularis infestation model. We showed that MBL is capable of binding B. burgdorferi through its carbohydrate recognition domains, but in vitro complement killing assays, peritoneal macrophage and whole blood stimulations, phagocytosis assays and an in vivo migration experiment did not reveal the mechanism by which MBL facilitates early clearance of B. burgdorferi . To conclude, we show a protective role of MBL in the early stages of B. burgdorferi infection, yet the underlying mechanism warrants further investigation. |
| ArticleNumber | 1431 |
| Author | Schuijt, Tim J. Wagemakers, Alex Oei, Anneke Ersoz, Jasmin I. Fikrig, Erol Roelofs, Joris J. T. H. de Boer, Onno J. Hovius, Joppe W. Coumou, Jeroen Narasimhan, Sukanya |
| Author_xml | – sequence: 1 givenname: Jeroen surname: Coumou fullname: Coumou, Jeroen email: lyme@amc.uva.nl organization: Amsterdam UMC, University of Amsterdam, Center for Experimental and Molecular Medicine – sequence: 2 givenname: Alex orcidid: 0000-0001-9632-7830 surname: Wagemakers fullname: Wagemakers, Alex organization: Amsterdam UMC, University of Amsterdam, Center for Experimental and Molecular Medicine – sequence: 3 givenname: Sukanya surname: Narasimhan fullname: Narasimhan, Sukanya organization: Department of Internal Medicine, Yale University School of Medicine – sequence: 4 givenname: Tim J. surname: Schuijt fullname: Schuijt, Tim J. organization: Amsterdam UMC, University of Amsterdam, Center for Experimental and Molecular Medicine – sequence: 5 givenname: Jasmin I. surname: Ersoz fullname: Ersoz, Jasmin I. organization: Amsterdam UMC, University of Amsterdam, Center for Experimental and Molecular Medicine – sequence: 6 givenname: Anneke surname: Oei fullname: Oei, Anneke organization: Amsterdam UMC, University of Amsterdam, Department of Medical Microbiology – sequence: 7 givenname: Onno J. surname: de Boer fullname: de Boer, Onno J. organization: Amsterdam UMC, University of Amsterdam, Department of Pathology, Amsterdam Cardiovascular Sciences, Amsterdam Infection & Immunity – sequence: 8 givenname: Joris J. T. H. surname: Roelofs fullname: Roelofs, Joris J. T. H. organization: Amsterdam UMC, University of Amsterdam, Department of Pathology, Amsterdam Cardiovascular Sciences, Amsterdam Infection & Immunity – sequence: 9 givenname: Erol surname: Fikrig fullname: Fikrig, Erol organization: Department of Internal Medicine, Yale University School of Medicine – sequence: 10 givenname: Joppe W. surname: Hovius fullname: Hovius, Joppe W. organization: Amsterdam UMC, University of Amsterdam, Center for Experimental and Molecular Medicine |
| BackLink | https://www.ncbi.nlm.nih.gov/pubmed/30723261$$D View this record in MEDLINE/PubMed |
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| Snippet | The causative agents of Lyme borreliosis, spirochetes belonging to the
Borrelia burgdorferi
sensu lato group, have developed several ways to protect themselves... The causative agents of Lyme borreliosis, spirochetes belonging to the Borrelia burgdorferi sensu lato group, have developed several ways to protect themselves... |
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| SubjectTerms | 14/34 631/250/262 631/326/421 64/60 692/420/254 82 Borrelia burgdorferi Borreliosis Complement activation Humanities and Social Sciences Immune clearance Immune response Immunoglobulin G Immunoglobulins Infectious diseases Lectins Leukocyte migration Macrophages Mannose multidisciplinary Oligosaccharides Peritoneum Phagocytosis Salivary gland Science Science (multidisciplinary) Skin Spirochetes |
| Title | The role of Mannose Binding Lectin in the immune response against Borrelia burgdorferi sensu lato |
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