C4BP-IgM protein as a therapeutic approach to treat Neisseria gonorrhoeae infections
Serena Bettoni, Jutamas Shaughnessy, Karolina Maziarz, David Ermert, Sunita Gulati, Bo Zheng, Matthias Mörgelin, Susanne Jacobsson, Kristian Riesbeck, Magnus Unemo, Sanjay Ram, Anna M. Blom
Serena Bettoni, Jutamas Shaughnessy, Karolina Maziarz, David Ermert, Sunita Gulati, Bo Zheng, Matthias Mörgelin, Susanne Jacobsson, Kristian Riesbeck, Magnus Unemo, Sanjay Ram, Anna M. Blom
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Research Article Infectious disease Therapeutics

C4BP-IgM protein as a therapeutic approach to treat Neisseria gonorrhoeae infections

Abstract

Gonorrhea is a sexually transmitted infection with 87 million new cases per year globally. Increasing antibiotic resistance has severely limited treatment options. A mechanism that Neisseria gonorrhoeae uses to evade complement attack is binding of the complement inhibitor C4b-binding protein (C4BP). We screened 107 porin B1a (PorB1a) and 83 PorB1b clinical isolates randomly selected from a Swedish strain collection over the last 10 years and noted that 96/107 (89.7%) PorB1a and 16/83 (19.3%) PorB1b bound C4BP; C4BP binding substantially correlated with the ability to evade complement-dependent killing (r = 0.78). We designed 2 chimeric proteins that fused C4BP domains to the backbone of IgG or IgM (C4BP-IgG; C4BP-IgM) with the aim of enhancing complement activation and killing of gonococci. Both proteins bound gonococci (KD C4BP-IgM = 2.4 nM; KD C4BP-IgG 980.7 nM), but only hexameric C4BP-IgM efficiently outcompeted heptameric C4BP from the bacterial surface, resulting in enhanced complement deposition and bacterial killing. Furthermore, C4BP-IgM substantially attenuated the duration and burden of colonization of 2 C4BP-binding gonococcal isolates but not a non–C4BP-binding strain in a mouse vaginal colonization model using human factor H/C4BP–transgenic mice. Our preclinical data present C4BP-IgM as an adjunct to conventional antimicrobials for the treatment of gonorrhea.

Authors

Serena Bettoni, Jutamas Shaughnessy, Karolina Maziarz, David Ermert, Sunita Gulati, Bo Zheng, Matthias Mörgelin, Susanne Jacobsson, Kristian Riesbeck, Magnus Unemo, Sanjay Ram, Anna M. Blom

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Figure 5

C4BP-IgM promotes complement-mediated killing of N. gonorrhoeae.

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C4BP-IgM promotes complement-mediated killing of N. gonorrhoeae. (A–D) C...
(AD) Complement-dependent bactericidal activity of C4BP-IgM on 4 laboratory strains of N. gonorrhoeae. Strains MS11 (A) and 1291 (B) were incubated with 5% NHS, while strains 15253 (C) and FA1090 (D) were tested with 20% NHS. Heat-inactivated NHS (HI NHS) was used as a negative control. One-way ANOVA with Dunnett’s multiple-comparisons test was performed considering NHS as reference. (EG) Complement-mediated bactericidal activity of 20 μg/mL C4BP-IgM in 10% NHS on FA1090, MS11 and F62 in the presence (w SA) or in the absence (w/o SA) of LOS. P values were calculated by 2-way ANOVA with Tukey’s multiple comparison of log10 (CFU/mL). (H) Complement-mediated bactericidal activity of 20 μg/mL C4BP-IgM on 26 clinical isolates of N. gonorrhoeae in the presence of 10% NHS. P values were performed by 2-way ANOVA with Sidak’s multiple-comparisons test. In all graphs horizontal dotted line refers to the starting amount of bacteria used in the assay, and each bar represents the mean ± SD of at least 3 independently performed experiments. *P < 0.05, **P < 0.01, ***P < 0.005, and ****P < 0.0001 as indicated, or compared with NHS.