The enhanced antitumor-specific immune response with mannose- and CpG-ODN-coated liposomes delivering TRP2 peptide

Purpose: Dendritic cell (DC)-based cancer vaccines is a newly emerging and potent form of immune therapy. As for any new technology, there are still considerable challenges that need to be addressed. Here, we investigate the antitumor potential of a novel liposomal vaccine, M/CpG-ODN-TRP2-Lipo. Meth...

Descripción completa

Detalles Bibliográficos
Autores principales: Lai, Chunhui, Duan, Siliang, Ye, Fang, Hou, Xiaoqiong, Li, Xi, Zhao, Jin, Yu, Xia, Hu, Zixi, Tang, Zhuoran, Mo, Fengzhen, Yang, Xiaomei, Lu, Xiaoling
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2018
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5858178/
https://www.ncbi.nlm.nih.gov/pubmed/29556352
http://dx.doi.org/10.7150/thno.22056
_version_ 1783307606486417408
author Lai, Chunhui
Duan, Siliang
Ye, Fang
Hou, Xiaoqiong
Li, Xi
Zhao, Jin
Yu, Xia
Hu, Zixi
Tang, Zhuoran
Mo, Fengzhen
Yang, Xiaomei
Lu, Xiaoling
author_facet Lai, Chunhui
Duan, Siliang
Ye, Fang
Hou, Xiaoqiong
Li, Xi
Zhao, Jin
Yu, Xia
Hu, Zixi
Tang, Zhuoran
Mo, Fengzhen
Yang, Xiaomei
Lu, Xiaoling
author_sort Lai, Chunhui
collection PubMed
description Purpose: Dendritic cell (DC)-based cancer vaccines is a newly emerging and potent form of immune therapy. As for any new technology, there are still considerable challenges that need to be addressed. Here, we investigate the antitumor potential of a novel liposomal vaccine, M/CpG-ODN-TRP2-Lipo. Methods: We developed a vaccination strategy by assembling the DC-targeting mannose and immune adjuvant CpG-ODN on the surface of liposomes, which were loaded with melanoma-specific TRP2(180-188) peptide as liposomal vaccine. M/CpG-ODN-TRP2-Lipo treatment was used to intendedly induce activation of DCs and antitumor- specific immune response in vivo. Results: Our results demonstrated in vitro that the prepared liposomal particles were efficiently taken up by DCs. This uptake led to an enhanced activation of DCs, as measured by the upregulation of MHC II, CD80, and CD86. Furthermore, M/CpG-ODN-TRP2-Lipo effectively inhibited the growth of implanted B16 melanoma and prolonged the survival of mice. This therapy significantly reduced the number of myeloid-derived suppressor cells (MDSCs) and regulatory T cells, while simultaneously increasing the number of activated T cells, tumor antigen-specific CD8(+) cytotoxic T cells, and interferon-γ-producing cells. At the same time, it was found to suppress tumor angiogenesis and tumor cell proliferation, as well as up-regulate their apoptosis. Interestingly, MyD88-knockout mice had significantly shorter median survival times compared to wild-type mice following the administration of M/CpG-ODN-TRP2-Lipo. Conclusions: The results suggested that the antitumor activities of the vaccine partially rely on the Myd88 signaling pathway. Interestingly, compared to whole tumor cell lysate-based vaccine, M/CpG-ODN-TRP2-Lipo, tumor specific antigen peptide-based vaccine, improved survival of tumor-bearing mice as well as enhanced their antitumor responses. All in all, we describe a novel vaccine formulation, M/CpG-ODN-TRP2-Lipo, with the aim of improving antitumor responses by alleviating the immunosuppressive environment in tumors.
format Online
Article
Text
id pubmed-5858178
institution National Center for Biotechnology Information
language English
publishDate 2018
publisher Ivyspring International Publisher
record_format MEDLINE/PubMed
spelling pubmed-58581782018-03-19 The enhanced antitumor-specific immune response with mannose- and CpG-ODN-coated liposomes delivering TRP2 peptide Lai, Chunhui Duan, Siliang Ye, Fang Hou, Xiaoqiong Li, Xi Zhao, Jin Yu, Xia Hu, Zixi Tang, Zhuoran Mo, Fengzhen Yang, Xiaomei Lu, Xiaoling Theranostics Research Paper Purpose: Dendritic cell (DC)-based cancer vaccines is a newly emerging and potent form of immune therapy. As for any new technology, there are still considerable challenges that need to be addressed. Here, we investigate the antitumor potential of a novel liposomal vaccine, M/CpG-ODN-TRP2-Lipo. Methods: We developed a vaccination strategy by assembling the DC-targeting mannose and immune adjuvant CpG-ODN on the surface of liposomes, which were loaded with melanoma-specific TRP2(180-188) peptide as liposomal vaccine. M/CpG-ODN-TRP2-Lipo treatment was used to intendedly induce activation of DCs and antitumor- specific immune response in vivo. Results: Our results demonstrated in vitro that the prepared liposomal particles were efficiently taken up by DCs. This uptake led to an enhanced activation of DCs, as measured by the upregulation of MHC II, CD80, and CD86. Furthermore, M/CpG-ODN-TRP2-Lipo effectively inhibited the growth of implanted B16 melanoma and prolonged the survival of mice. This therapy significantly reduced the number of myeloid-derived suppressor cells (MDSCs) and regulatory T cells, while simultaneously increasing the number of activated T cells, tumor antigen-specific CD8(+) cytotoxic T cells, and interferon-γ-producing cells. At the same time, it was found to suppress tumor angiogenesis and tumor cell proliferation, as well as up-regulate their apoptosis. Interestingly, MyD88-knockout mice had significantly shorter median survival times compared to wild-type mice following the administration of M/CpG-ODN-TRP2-Lipo. Conclusions: The results suggested that the antitumor activities of the vaccine partially rely on the Myd88 signaling pathway. Interestingly, compared to whole tumor cell lysate-based vaccine, M/CpG-ODN-TRP2-Lipo, tumor specific antigen peptide-based vaccine, improved survival of tumor-bearing mice as well as enhanced their antitumor responses. All in all, we describe a novel vaccine formulation, M/CpG-ODN-TRP2-Lipo, with the aim of improving antitumor responses by alleviating the immunosuppressive environment in tumors. Ivyspring International Publisher 2018-02-12 /pmc/articles/PMC5858178/ /pubmed/29556352 http://dx.doi.org/10.7150/thno.22056 Text en © Ivyspring International Publisher This is an open access article distributed under the terms of the Creative Commons Attribution (CC BY-NC) license (https://creativecommons.org/licenses/by-nc/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Lai, Chunhui
Duan, Siliang
Ye, Fang
Hou, Xiaoqiong
Li, Xi
Zhao, Jin
Yu, Xia
Hu, Zixi
Tang, Zhuoran
Mo, Fengzhen
Yang, Xiaomei
Lu, Xiaoling
The enhanced antitumor-specific immune response with mannose- and CpG-ODN-coated liposomes delivering TRP2 peptide
title The enhanced antitumor-specific immune response with mannose- and CpG-ODN-coated liposomes delivering TRP2 peptide
title_full The enhanced antitumor-specific immune response with mannose- and CpG-ODN-coated liposomes delivering TRP2 peptide
title_fullStr The enhanced antitumor-specific immune response with mannose- and CpG-ODN-coated liposomes delivering TRP2 peptide
title_full_unstemmed The enhanced antitumor-specific immune response with mannose- and CpG-ODN-coated liposomes delivering TRP2 peptide
title_short The enhanced antitumor-specific immune response with mannose- and CpG-ODN-coated liposomes delivering TRP2 peptide
title_sort enhanced antitumor-specific immune response with mannose- and cpg-odn-coated liposomes delivering trp2 peptide
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5858178/
https://www.ncbi.nlm.nih.gov/pubmed/29556352
http://dx.doi.org/10.7150/thno.22056
work_keys_str_mv AT laichunhui theenhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT duansiliang theenhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT yefang theenhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT houxiaoqiong theenhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT lixi theenhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT zhaojin theenhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT yuxia theenhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT huzixi theenhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT tangzhuoran theenhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT mofengzhen theenhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT yangxiaomei theenhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT luxiaoling theenhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT laichunhui enhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT duansiliang enhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT yefang enhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT houxiaoqiong enhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT lixi enhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT zhaojin enhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT yuxia enhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT huzixi enhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT tangzhuoran enhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT mofengzhen enhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT yangxiaomei enhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide
AT luxiaoling enhancedantitumorspecificimmuneresponsewithmannoseandcpgodncoatedliposomesdeliveringtrp2peptide

Ejemplares similares