A stabilized glycomimetic conjugate vaccine inducing protective antibodies against Neisseria meningitidis serogroup A

Enotarpi, Jacopo; Tontini, Marta; Balocchi, Cristiana; Es, Daan van der; Auberger, Ludovic; Balducci, Evita; Carboni, Filippo; Proietti, Daniela; Casini, Daniele; Filippov, Dmitri V.; Overkleeft, Hermen S.; Marel, Gijsbert A. van der; Colombo, Cinzia; Romano, Maria; Costantino, Paolo; Codée, Jeroen D. C.; Lay, Luigi; Adamo, Roberto

doi:10.1038/s41467-020-18279-x

Cited by 18 publications

(16 citation statements)

References 59 publications

(78 reference statements)

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“…This finding is consistent with the conclusion that hydrolysis of MPM to PM reduces the amount of available antigen, while MPM-3 is not sensitive to hydrolysis. This favored interpretation is separately supported by plate-bound antigen presentation assays that distinguish responses to PM and MPM ( 12 ), the known susceptibility of this type of glycosyl phosphate diesters to hydrolysis ( 28 ), the demonstrated hydrolysis of MPM, and the overcoming of antigen loss by substituting the link between sugar and phosphate with alternatives that are not subject to hydrolysis.…”

Section: Resultsmentioning

confidence: 99%

Rational design of a hydrolysis-resistant mycobacterial phosphoglycolipid antigen presented by CD1c to T cells

Reijneveld

Marino

Cao

et al. 2021

Journal of Biological Chemistry

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Whereas proteolytic cleavage is crucial for peptide presentation by classical major histocompatibility complex (MHC) proteins to T cells, glycolipids presented by CD1 molecules are typically presented in an unmodified form. However, the mycobacterial lipid antigen mannosyl-β1-phosphomycoketide (MPM) may be processed through hydrolysis in antigen presenting cells, forming mannose and phosphomycoketide (PM). To further test the hypothesis that some lipid antigens are processed, and to generate antigens that lead to defined epitopes for future tuberculosis vaccines or diagnostic tests, we aimed to create hydrolysis-resistant MPM variants that retain their antigenicity. Here, we designed and tested three different, versatile synthetic strategies to chemically stabilize MPM analogs. Crystallographic studies of CD1c complexes with these three new MPM analogs showed anchoring of the lipid tail and phosphate group that is highly comparable to nature-identical MPM, with considerable conformational flexibility for the mannose head group. MPM-3, a difluoromethylene-modified version of MPM that is resistant to hydrolysis, showed altered recognition by cells, but not by CD1c proteins, supporting the cellular antigen processing hypothesis. Furthermore, the synthetic analogs elicited T cell responses that were cross-reactive with nature-identical MPM, fulfilling important requirements for future clinical use.

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Section: Resultsmentioning

confidence: 99%

Rational design of a hydrolysis-resistant mycobacterial phosphoglycolipid antigen presented by CD1c to T cells

Reijneveld

Marino

Cao

et al. 2021

Journal of Biological Chemistry

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“…The resulting conjugates showed induction of antibodies capable of recognizing the native MenA polysaccharide, but with very poor immunogenicity. More recently, oligomers up to 8 repeating units in length were generated [ 77 ]. Particularly, the octamer showed a unique capacity to recognize a bactericidal murine monoclonal antibody that has been mapped by Saturation Transfer NMR and X-ray crystallography, showing that it binds to an O-acetylated trisaccharide epitope [ 78 ].…”

Section: New Approaches Under Preclinical Investigationmentioning

confidence: 99%

“…Particularly, the octamer showed a unique capacity to recognize a bactericidal murine monoclonal antibody that has been mapped by Saturation Transfer NMR and X-ray crystallography, showing that it binds to an O-acetylated trisaccharide epitope [ 78 ]. While initial studies with a conjugate of the non-O-acetylated octamer provided unsatisfactory results, introduction of O-acetylation at a level up to 75 %, similar to the natural polysaccharide, generated an antigen which upon conjugation induced bactericidal antibodies similarly to the MenA polysaccharide vaccine benchmark [ 77 ]. This work represented a proof-of-principle that glycomimetic vaccines can be used as more stable alternatives to polysaccharide-derived ones.…”

Section: New Approaches Under Preclinical Investigationmentioning

confidence: 99%

Carbohydrate based meningococcal vaccines: past and present overview

Romano¹,

Micoli

Adamo³

2021

Glycoconj J

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Neisseria meningitidis is a major cause of bacterial meningitidis worldwide. Children less than five years and adolescents are particularly affected. Nearly all invasive strains are surrounded by a polysaccharide capsule, based on which, 12 N. meningitidis serogroups are differentiated. Six of them, A, B, C, W, X, and Y, cause the vast majority of infections in humans. Mono- and multi-valent carbohydrate-based vaccines against meningococcal infections have been licensed or are currently in clinical development. In this mini-review, an overview of the past and present approaches for producing meningococcal glycoconjugate vaccines is provided.

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“…A rapid and cost-effective chemoenzymatic synthesis of oligosaccharides from N. meningitidis serogroup X produced glycans that elicited functional antibodies in mice ( Figure 7 bottom) [ 63 ]. A vaccine candidate involving glycomimetics that stabilizes the natural CPS of N. meningitis serogroup A after conjugation to CRM 197 elicited in mice high levels of protective antibodies with bactericidal activity [ 64 ], which advanced previous work that had used the synthetic tetrasaccharide conjugate of TT [ 65 ]. The structural epitopes of N. meningitidis serogroup A revealed the importance of acetylation of the respective CPS [ 66 ].…”

Section: Antibacterial Semisynthetic Carbohydrate-based Vaccinesmentioning

confidence: 99%

Semi- and fully synthetic carbohydrate vaccines against pathogenic bacteria: recent developments

Zasłona

Downey

Seeberger

et al. 2021

Biochemical Society Transactions

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The importance of vaccine-induced protection was repeatedly demonstrated over the last three decades and emphasized during the recent COVID-19 pandemic as the safest and most effective way of preventing infectious diseases. Vaccines have controlled, and in some cases, eradicated global viral and bacterial infections with high efficiency and at a relatively low cost. Carbohydrates form the capsular sugar coat that surrounds the outer surface of human pathogenic bacteria. Specific surface-exposed bacterial carbohydrates serve as potent vaccine targets that broadened our toolbox against bacterial infections. Since first approved for commercial use, antibacterial carbohydrate-based vaccines mostly rely on inherently complex and heterogenous naturally derived polysaccharides, challenging to obtain in a pure, safe, and cost-effective manner. The introduction of synthetic fragments identical with bacterial capsular polysaccharides provided well-defined and homogenous structures that resolved many challenges of purified polysaccharides. The success of semisynthetic glycoconjugate vaccines against bacterial infections, now in different phases of clinical trials, opened up new possibilities and encouraged further development towards fully synthetic antibacterial vaccine solutions. In this mini-review, we describe the recent achievements in semi- and fully synthetic carbohydrate vaccines against a range of human pathogenic bacteria, focusing on preclinical and clinical studies.

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A stabilized glycomimetic conjugate vaccine inducing protective antibodies against Neisseria meningitidis serogroup A

Cited by 18 publications

References 59 publications

Rational design of a hydrolysis-resistant mycobacterial phosphoglycolipid antigen presented by CD1c to T cells

Rational design of a hydrolysis-resistant mycobacterial phosphoglycolipid antigen presented by CD1c to T cells

Carbohydrate based meningococcal vaccines: past and present overview

Semi- and fully synthetic carbohydrate vaccines against pathogenic bacteria: recent developments

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