Peptides conjugated to 2-alkoxy-8-oxo-adenine as potential synthetic vaccines triggering TLR7

Gential, Geoffroy P. P.; Hogervorst, Tim P; Tondini, Elena; Graaff, Michel J. van de; Overkleeft, Herman S.; Codée, Jeroen D. C.; Marel, Gijsbert A. van der; Ossendorp, Ferry; Filippov, Dmitri V.

doi:10.1016/j.bmcl.2019.03.048

Cited by 17 publications

(10 citation statements)

References 23 publications

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“…C-terminal functionalization was achieved by selective removal of the Lys(Mmt) group, and subsequent coupling of an ethylene glycol spacer followed by introduction of the TLR7 agonist (Chan et al, 2009). Using our previously described protocol (Gential et al, 2019), we could introduce Boc protected TLR7-ligand 23 on-resin, resulting in functionalized solid support 25 . Release of the peptide-TLR7 ligand conjugate from the resin and concomitant global deprotection of the side chains under acidic conditions resulted in azido-peptide 26 , which was purified by HPLC.…”

Section: Resultsmentioning

confidence: 99%

“…Synthesis of trifunctional CLR-epitope-TLR conjugates. Reagents and conditions : (a) Fmoc-SPPS; (b) TFA, DCM; (c) Fmoc-SPPS; (d) 23 (Gential et al, 2019), HCTU, DIPEA, DMF; (e) TFA, TIS, H 2 O, octanethiol, phenol; (f) CuI, THPTA, DIPEA, DMSO, H 2 O, (+ NaAsc, Arg, H 2 O), CLR clusters ( 19–22 ).…”

Section: Resultsmentioning

confidence: 99%

“…The high affinity binders were used for conjugation to a model peptide antigen, containing the helper T cell epitope gp100 280−288 and effector T cell epitope gp100 44−59 , to generate conjugates that could be targeted to DCs. To enhance the presentation of the antigens embedded in the conjugates by the DCs, we equipped the conjugates with a previously reported 8-oxo-adenosine analog (Jin et al, 2006; Gential et al, 2019), a ligand for the endosomal TLR7 which resulted in trifunctional conjugates (CLR-antigen-TLR). Using monocyte-derived dendritic cells (moDCs) we showed that the generated trifunctional conjugates represent attractive vaccine modalities that effectively targeted and activated DCs allowing effective antigen presentation.…”

Section: Introductionmentioning

confidence: 99%

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Systematic Dual Targeting of Dendritic Cell C-Type Lectin Receptor DC-SIGN and TLR7 Using a Trifunctional Mannosylated Antigen

Hogervorst

Achilli

et al. 2019

Front. Chem.

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Dendritic cells (DCs) are important initiators of adaptive immunity, and they possess a multitude of Pattern Recognition Receptors (PRR) to generate an adequate T cell mediated immunity against invading pathogens. PRR ligands are frequently conjugated to tumor-associated antigens in a vaccination strategy to enhance the immune response toward such antigens. One of these PPRs, DC-SIGN, a member of the C-type lectin receptor (CLR) family, has been extensively targeted with Lewis structures and mannose glycans, often presented in multivalent fashion. We synthesized a library of well-defined mannosides (mono-, di-, and tri-mannosides), based on known “high mannose” structures, that we presented in a systematically increasing number of copies (n = 1, 2, 3, or 6), allowing us to simultaneously study the effect of mannoside configuration and multivalency on DC-SIGN binding via Surface Plasmon Resonance (SPR) and flow cytometry. Hexavalent presentation of the clusters showed the highest binding affinity, with the hexa-α1,2-di-mannoside being the most potent ligand. The four highest binding hexavalent mannoside structures were conjugated to a model melanoma gp100-peptide antigen and further equipped with a Toll-like receptor 7 (TLR7)-agonist as adjuvant for DC maturation, creating a trifunctional vaccine conjugate. Interestingly, DC-SIGN affinity of the mannoside clusters did not directly correlate with antigen presentation enhancing properties and the α1,2-di-mannoside cluster with the highest binding affinity in our library even hampered T cell activation. Overall, this systematic study has demonstrated that multivalent glycan presentation can improve DC-SIGN binding but enhanced binding cannot be directly translated into enhanced antigen presentation and the sole assessment of binding affinity is thus insufficient to determine further functional biological activity. Furthermore, we show that well-defined antigen conjugates combining two different PRR ligands can be generated in a modular fashion to increase the effectiveness of vaccine constructs.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Systematic Dual Targeting of Dendritic Cell C-Type Lectin Receptor DC-SIGN and TLR7 Using a Trifunctional Mannosylated Antigen

Hogervorst

Achilli

et al. 2019

Front. Chem.

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“…The released amine was subsequently coupled with the spacer 33 and the Boc-protected TLR7 ligand building block 34. [21] After deprotection, release from the resin and RP-HPLC purification peptides 27 and 30 were obtained in a 2 % yield. Coupling of O-M6Po building block 9 to peptides 26, 27, 29 and 30 was performed using a cocktail of CuSO 4 , sodium ascorbate and tris(benzyltriazolylmethyl)amine in DMSO/H 2 O, [31] with the addition of a 20 mM Tris/150 mM NaCl buffer.…”

Section: Synthesis Of M6po-conjugatesmentioning

confidence: 99%

“…Our goal is to enhance the immune response by increasing endosomal trafficking of the peptide vaccine via the MPR which led to the design of bis-conjugates (2, 4, 6, and 8) in which the Toll-like receptor 7 ligand (TLR7L) 2alkoxy-8-oxo-adenine is added at either the N-or the Cterminus of the M6Po-SLP. [20,21] We coupled an α-configured spacer, [12,18,22] carrying an alkyne function to the O-M6Po building block 9 to allow for the copper mediated 1,3-dipolar cycloaddition to azide functions incorporated in the SLP, while C-M6Po building block 10 was used to generate the HAAHAconjugates via solid-phase peptide synthesis (SPPS). This building block is a C-analogue [23] of O-M6Po, in which the anomeric oxygen is replaced with a CH 2 , preventing hydrolysis under the acidic conditions used in SPPS.…”

Section: Introductionmentioning

confidence: 99%

Multivalent, Stabilized Mannose‐6‐Phosphates for the Targeted Delivery of Toll‐Like Receptor Ligands and Peptide Antigens

et al. 2020

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Mannose-6-phosphate (M6P) is recognized by the mannose-6phosphate receptor and plays an important role in the transport of cargo to the endosomes, making it an attractive tool to improve endosomal trafficking of vaccines. We describe herein the assembly of peptide antigen conjugates carrying clusters of mannose-6-C-phosphonates (M6Po). The M6Po's are stable M6P mimics that are resistant to cleavage of the phosphate group by endogenous phosphatases. Two different strategies for the incorporation of the M6Po clusters in the conjugate have been developed: the first relies on a "post-assembly" click approach employing an M6Po bearing an alkyne functionality; the second hinges on an M6Po C-glycoside amino acid building block that can be used in solid-phase peptide synthesis. The generated conjugates were further equipped with a TLR7 ligand to stimulate dendritic cell (DC) maturation. While antigen presentation is hindered by the presence of the M6Po clusters, the incorporation of the M6Po clusters leads to increased activation of DCs, thus demonstrating their potential in improving vaccine adjuvanticity by intraendosomally active TLR ligands.

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Innovative Vaccine Strategy: Self-Adjuvanting Conjugate Vaccines

Manabe

Fukase

2023

Methods in Molecular Biology

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Peptides conjugated to 2-alkoxy-8-oxo-adenine as potential synthetic vaccines triggering TLR7

Cited by 17 publications

References 23 publications

Systematic Dual Targeting of Dendritic Cell C-Type Lectin Receptor DC-SIGN and TLR7 Using a Trifunctional Mannosylated Antigen

Systematic Dual Targeting of Dendritic Cell C-Type Lectin Receptor DC-SIGN and TLR7 Using a Trifunctional Mannosylated Antigen

Multivalent, Stabilized Mannose‐6‐Phosphates for the Targeted Delivery of Toll‐Like Receptor Ligands and Peptide Antigens

Innovative Vaccine Strategy: Self-Adjuvanting Conjugate Vaccines

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