4.8 Article

Chemical synthesis and immunological evaluation of new generation multivalent anticancer vaccines based on a Tn antigen analogue

Journal

CHEMICAL SCIENCE
Volume 11, Issue 17, Pages 4488-4498

Publisher

ROYAL SOC CHEMISTRY
DOI: 10.1039/d0sc00544d

Keywords

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Funding

  1. European Research Council [ERC-2016-STG716878, ERC-2014-COG647938]
  2. Spanish Ministry of Science, Innovation and Universities [CTQ2017-87530-R, RYC-2015-17888, RTI2018-096494-B-100, SAF2015-65327-R, SEV-2016-0644]
  3. CNRS
  4. Universite Grenoble Alpes [ICMG FR 2607]
  5. French ANR project Glyco@Alps [ANR-15-IDEX-02]
  6. Labex ARCANE
  7. CBH-EUR-GS [ANR-17-EURE-0003]

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Tumor associated carbohydrate antigens (TACAs), such as the Tn antigen, have emerged as key targets for the development of synthetic anticancer vaccines. However, the induction of potent and functional immune responses has been challenging and, in most cases, unsuccessful. Herein, we report the design, synthesis and immunological evaluation in mice of Tn-based vaccine candidates with multivalent presentation of the Tn antigen (up to 16 copies), both in its native serine-linked display (Tn-Ser) and as an oxime-linked Tn analogue (Tn-oxime). The high valent vaccine prototypes were synthesized through a late-stage convergent assembly (Tn-Ser construct) and a versatile divergent strategy (Tn-oxime analogue), using chemoselective click-type chemistry. The hexadecavalent Tn-oxime construct induced robust, Tn-specific humoral and CD4(+)/CD8(+) cellular responses, with antibodies able to bind the Tn antigen on the MCF7 cancer cell surface. The superior synthetic accessibility and immunological properties of this fully-synthetic vaccine prototype makes it a compelling candidate for further advancement towards safe and effective synthetic anticancer vaccines.

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