Mannosylated Polycations Target CD206+Antigen-Presenting Cells and Mediate T-Cell-Specific Activation in Cancer Vaccination

Federica Bellato; Sara Feola; Gloria Dalla Verde; Greta Bellio; Marco Pirazzini; Stefano Salmaso; Paolo Caliceti; Vincenzo Cerullo; Francesca Mastrotto

doi:10.1021/acs.biomac.2c00993

Mannosylated Polycations Target CD206+Antigen-Presenting Cells and Mediate T-Cell-Specific Activation in Cancer Vaccination

Federica Bellato, Sara Feola, Gloria Dalla Verde, Greta Bellio, Marco Pirazzini, Stefano Salmaso, Paolo Caliceti, Vincenzo Cerullo, Francesca Mastrotto

Tutkimustuotos: Artikkelijulkaisu › Artikkeli › Tieteellinen › vertaisarvioitu

Abstrakti

Immunotherapy is deemed one of the most powerful therapeutic approaches to treat cancer. However, limited response and tumor specificity are still major challenges to address. Herein, mannosylated polycations targeting mannose receptor are developed as vectors for plasmid DNA (pDNA)-based vaccines to improve selective delivery of genetic material to antigen presenting cells and enhance immune cell activation. Three diblock glycopolycations (M15A12, M29A25, and M58A45) and two triblock copolymers (M29A29B9 and M62A52B32) are generated by using mannose (M), agmatine (A), and butyl (B) derivatives to target CD206, complex nucleic acids, and favor the endosomal escape, respectively. All glycopolycations efficiently complex pDNA at N/P ratios

Alkuperäiskieli	englanti
Lehti	Biomacromolecules
Vuosikerta	23
Numero	12
Sivut	5148-5163
Sivumäärä	16
ISSN	1525-7797
DOI - pysyväislinkit	https://doi.org/10.1021/acs.biomac.2c00993
Tila	Julkaistu - 17 marrask. 2022
OKM-julkaisutyyppi	A1 Alkuperäisartikkeli tieteellisessä aikakauslehdessä, vertaisarvioitu

Tieteenalat

317 Farmasia

Pääsy asiakirjaan

10.1021/acs.biomac.2c00993Lisenssi: CC BY

acs.biomac.2c00993Lopullinen julkaistu versio, 10,2 MBLisenssi: CC BY

Siteeraa tätä

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title = "Mannosylated Polycations Target CD206+Antigen-Presenting Cells and Mediate T-Cell-Specific Activation in Cancer Vaccination",

abstract = "Immunotherapy is deemed one of the most powerful therapeutic approaches to treat cancer. However, limited response and tumor specificity are still major challenges to address. Herein, mannosylated polycations targeting mannose receptor are developed as vectors for plasmid DNA (pDNA)-based vaccines to improve selective delivery of genetic material to antigen presenting cells and enhance immune cell activation. Three diblock glycopolycations (M15A12, M29A25, and M58A45) and two triblock copolymers (M29A29B9 and M62A52B32) are generated by using mannose (M), agmatine (A), and butyl (B) derivatives to target CD206, complex nucleic acids, and favor the endosomal escape, respectively. All glycopolycations efficiently complex pDNA at N/P ratios ",

keywords = "Gene delivery, Diblock copolymers, Dna vaccine, In-vivo, Polymers, Raft, Immunotherapy, Nanoparticles, Adjuvants, Antigens, 317 Pharmacy",

author = "Federica Bellato and Sara Feola and {Dalla Verde}, Gloria and Greta Bellio and Marco Pirazzini and Stefano Salmaso and Paolo Caliceti and Vincenzo Cerullo and Francesca Mastrotto",

year = "2022",

month = nov,

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doi = "10.1021/acs.biomac.2c00993",

language = "English",

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T1 - Mannosylated Polycations Target CD206+Antigen-Presenting Cells and Mediate T-Cell-Specific Activation in Cancer Vaccination

AU - Bellato, Federica

AU - Feola, Sara

AU - Dalla Verde, Gloria

AU - Bellio, Greta

AU - Pirazzini, Marco

AU - Salmaso, Stefano

AU - Caliceti, Paolo

AU - Cerullo, Vincenzo

AU - Mastrotto, Francesca

PY - 2022/11/17

Y1 - 2022/11/17

N2 - Immunotherapy is deemed one of the most powerful therapeutic approaches to treat cancer. However, limited response and tumor specificity are still major challenges to address. Herein, mannosylated polycations targeting mannose receptor are developed as vectors for plasmid DNA (pDNA)-based vaccines to improve selective delivery of genetic material to antigen presenting cells and enhance immune cell activation. Three diblock glycopolycations (M15A12, M29A25, and M58A45) and two triblock copolymers (M29A29B9 and M62A52B32) are generated by using mannose (M), agmatine (A), and butyl (B) derivatives to target CD206, complex nucleic acids, and favor the endosomal escape, respectively. All glycopolycations efficiently complex pDNA at N/P ratios

AB - Immunotherapy is deemed one of the most powerful therapeutic approaches to treat cancer. However, limited response and tumor specificity are still major challenges to address. Herein, mannosylated polycations targeting mannose receptor are developed as vectors for plasmid DNA (pDNA)-based vaccines to improve selective delivery of genetic material to antigen presenting cells and enhance immune cell activation. Three diblock glycopolycations (M15A12, M29A25, and M58A45) and two triblock copolymers (M29A29B9 and M62A52B32) are generated by using mannose (M), agmatine (A), and butyl (B) derivatives to target CD206, complex nucleic acids, and favor the endosomal escape, respectively. All glycopolycations efficiently complex pDNA at N/P ratios

KW - Gene delivery

KW - Diblock copolymers

KW - Dna vaccine

KW - In-vivo

KW - Polymers

KW - Raft

KW - Immunotherapy

KW - Nanoparticles

KW - Adjuvants

KW - Antigens

KW - 317 Pharmacy

U2 - 10.1021/acs.biomac.2c00993

DO - 10.1021/acs.biomac.2c00993

M3 - Article

C2 - 36394394

VL - 23

SP - 5148

EP - 5163

JO - Biomacromolecules

JF - Biomacromolecules

SN - 1525-7797

IS - 12

ER -