Immunization against a Saccharide Epitope Accelerates Clearance of Experimental Gonococcal Infection

Gulati, Sunita; Zheng, Bo; Reed, George W.; Su, Xiaohong; Cox, Andrew D.; Michael, Frank St.; Stupak, Jacek; Lewis, Lisa A.; Ram, Sanjay; Rice, Peter A.

doi:10.1371/journal.ppat.1003559

Cited by 66 publications

(105 citation statements)

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“…Expression of LgtG is important for murine infection (14). Passive administration of mAb 2C7, as well as active immunization with a peptide mimic (mimitope) of the 2C7 epitope that was configured as a ‘multi-antigen peptide’ on a poly-lysine ‘backbone’ significantly shortened the duration and burden of infection in the murine vaginal colonization model of gonorrhea (14).…”

Section: Introductionmentioning

confidence: 99%

Phase-Variable Heptose I Glycan Extensions Modulate Efficacy of 2C7 Vaccine Antibody Directed against Neisseria gonorrhoeae Lipooligosaccharide

Chakraborti

Lewis

Cox

et al. 2016

The Journal of Immunology

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Neisseria gonorrhoeae , the causative agent of the sexually transmitted infection, gonorrhea, has developed resistance to most conventional antibiotics. Safe and effective vaccines against gonorrhea are needed urgently. A candidate vaccine that targets a lipooligosaccharide (LOS) epitope recognized by monoclonal (mAb) 2C7 attenuates gonococcal burden in the mouse vaginal colonization model. Glycan extensions from the LOS core heptoses (HepI and HepII) are controlled by phase-variable LOS glycosyltransferase (lgt) genes; we sought to define how HepI glycan extensions affect mAb 2C7 function. Isogenic gonococcal mutants in which the lgt required for mAb 2C7 reactivity (lgtG) was genetically locked ‘ON’ and the lgt loci required for HepI variation (lgtA, lgtC and lgtD) were genetically locked ‘ON’ or ‘OFF’ in different combinations were created. We observed 100% complement-dependent killing by mAb 2C7 of a mutant that expressed lactose (Gal-Glc) from HepI, while a mutant that expressed Gal-Gal-Glc-HepI fully resisted killing (>100% survival). Mutants that elaborated 4- (Gal-GlcNAc-Gal-Glc-HepI) and 5-glycan (GalNAc-Gal-GlcNAc-Gal-Glc-HepI) structures displayed ‘intermediate’ phenotypes (<50% killing with 2 μg/ml and >95% killing with 4 μg/ml of mAb 2C7). The contrasting phenotypes of the lactose-HepI and the Gal-Gal-Glc-HepI LOS structures were recapitulated with phase-variants of a recently isolated clinical strain. Despite lack of killing of the Gal-Gal-Glc-HepI mutants, mAb 2C7 deposited sufficient C3 on these bacteria for opsonophagocytic killing by human neutrophils. In conclusion, mAb 2C7 showed functional activity against all gonococcal HepI LOS structures defined by various lgtA/C/D ‘ON/OFF’ combinations, thereby providing further impetus for use of the 2C7 epitope in a gonococcal vaccine.

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Section: Introductionmentioning

confidence: 99%

Phase-Variable Heptose I Glycan Extensions Modulate Efficacy of 2C7 Vaccine Antibody Directed against Neisseria gonorrhoeae Lipooligosaccharide

Chakraborti

Lewis

Cox

et al. 2016

The Journal of Immunology

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“…The most successful of such single antigens used as vaccines have been bacterial capsular polysaccharides. While these are not present in N. gonorrhoeae, conserved saccharides are present in gonococcal lipooligosaccharides (LOSs) (18) and should be exploited further as vaccine candidates (19).…”

Section: Session 3: Human Studiesmentioning

confidence: 99%

Summary and Recommendations from the National Institute of Allergy and Infectious Diseases (NIAID) Workshop “Gonorrhea Vaccines: the Way Forward”

Wetzler

Feavers

Gray-Owen

et al. 2016

Clin Vaccine Immunol

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There is an urgent need for the development of an antigonococcal vaccine due to the increasing drug resistance found in this pathogen. The U.S. Centers for Disease Control (CDC) have identified multidrug-resistant gonococci (GC) as among 3 "urgent" hazard-level threats to the U.S. population. In light of this, on 29 to 30 June 2015, the National Institute for Allergy and Infectious Diseases (NIAID) sponsored a workshop entitled "Gonorrhea Vaccines: the Way Forward." The goal of the workshop was to gather leaders in the field to discuss several key questions on the current status of gonorrhea vaccine research and the path forward to a licensed gonorrhea vaccine. Representatives from academia, industry, U.S. Government agencies, and a state health department were in attendance. This review summarizes each of the 4 scientific sessions and a series of 4 breakout sessions that occurred during the one and a half days of the workshop. Topics raised as high priority for future development included (i) reinvigoration of basic research to understand gonococcal infection and immunity to allow intervention in processes essential for infection; (ii) clinical infection studies to establish parallels and distinctions between in vitro and animal infection models versus natural human genital and pharyngeal infection and to inform in silico modeling of vaccine impact; and (iii) development of an integrated pipeline for preclinical and early clinical evaluation and direct comparisons of potential vaccine antigens and adjuvants and routes of delivery.

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“…A female mouse model is now available and has been useful for studying N. gonorrhoeae adaptation to the female genital tract , signaling through innate receptors Packiam et al, 2014), and the relationship between antibiotic resistance and fitness (Kunz et al, 2012;Warner et al, 2008). The mouse model has also been used to identify protective and immunosuppressive pathways Liu et al, , 2013Packiam et al, 2014, Zhu et al, 2012 and to accelerate the development of therapeutic and prophylactic products against gonorrhea (Gulati et al, 2013;Plante et al, 2000;Spencer et al, 2004;Zeitlin et al, 2001;Zhu et al, 2011). Known host restrictions that limit the capacity of female mice to mimic gonorrhea in humans include the absence of human-specific receptors for adherence and invasion pathways, human transferrin and lactoferrin glycoproteins, soluble regulators of the complement cascade (factor H, C4b-binding protein), and IgA1, the substrate of gonococcal IgA1 protease (extensively reviewed in Jerse et al (2011)).…”

Section: Animal Models Of Gonococcal Genital Tract Infectionmentioning

confidence: 99%

“…Antibodies against 2C7-OS (Gulati et al, 1996) or a 2C7-OS peptide mimic (Ngampasutadol et al, 2006) are bactericidal and promote opsonophagocytic killing of N. gonorrhoeae. Intraperitoneal immunization of mice with a multiantigenic form of the 2C7-OS peptide mimic protected mice from subsequent challenge, as did passive delivery of 2C7 monoclonal antibody (Gulati et al, 2013). The transferrin receptor is a promising target on the basis of its surface exposure, limited antigenic variability, and importance for experimental urethritis of male subjects (Cornelissen et al, 1992).…”

Section: Gonorrhea Vaccine Developmentmentioning

confidence: 99%

Animal Models of Immunity to Female Genital Tract Infections and Vaccine Development

2015

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Immunization against a Saccharide Epitope Accelerates Clearance of Experimental Gonococcal Infection

Cited by 66 publications

References 50 publications

Phase-Variable Heptose I Glycan Extensions Modulate Efficacy of 2C7 Vaccine Antibody Directed against Neisseria gonorrhoeae Lipooligosaccharide

Phase-Variable Heptose I Glycan Extensions Modulate Efficacy of 2C7 Vaccine Antibody Directed against Neisseria gonorrhoeae Lipooligosaccharide

Summary and Recommendations from the National Institute of Allergy and Infectious Diseases (NIAID) Workshop “Gonorrhea Vaccines: the Way Forward”

Animal Models of Immunity to Female Genital Tract Infections and Vaccine Development

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