Therapeutic effects of autologous tumor-derived nanovesicles on melanoma growth and metastasis.

Therapeutic effects of autologous tumor-derived nanovesicles on melanoma growth and metastasis.

Cancer vaccines with optimal tumor-associated antigens show promise for anti-tumor immunotherapy. Recently, nano-sized vesicles, such as exosomes derived from tumors, were suggested as potential antigen candidates, although the total yield of exosomes is not sufficient for clinical applications. In...

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Main Authors: Eun-Young Lee, Kyong-Su Park, Yae Jin Yoon, Jaewook Lee, Hyung-Geun Moon, Su Chul Jang, Kyoung-Ho Choi, Yoon-Keun Kim, Yong Song Gho
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3305328?pdf=render
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spelling doaj-982a3fe8147147e191e726c1cdaf651e2020-11-25T01:47:46ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-0173e3333010.1371/journal.pone.0033330Therapeutic effects of autologous tumor-derived nanovesicles on melanoma growth and metastasis.Eun-Young LeeKyong-Su ParkYae Jin YoonJaewook LeeHyung-Geun MoonSu Chul JangKyoung-Ho ChoiYoon-Keun KimYong Song GhoCancer vaccines with optimal tumor-associated antigens show promise for anti-tumor immunotherapy. Recently, nano-sized vesicles, such as exosomes derived from tumors, were suggested as potential antigen candidates, although the total yield of exosomes is not sufficient for clinical applications. In the present study, we developed a new vaccine strategy based on nano-sized vesicles derived from primary autologous tumors. Through homogenization and sonication of tumor tissues, we achieved high yields of vesicle-bound antigens. These nanovesicles were enriched with antigenic membrane targets but lacked nuclear autoantigens. Furthermore, these nanovesicles together with adjuvant activated dendritic cells in vitro, and induced effective anti-tumor immune responses in both primary and metastatic melanoma mouse models. Therefore, autologous tumor-derived nanovesicles may represent a novel source of antigens with high-level immunogenicity for use in acellular vaccines without compromising safety. Our strategy is cost-effective and can be applied to patient-specific cancer therapeutic vaccination.http://europepmc.org/articles/PMC3305328?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Eun-Young Lee
Kyong-Su Park
Yae Jin Yoon
Jaewook Lee
Hyung-Geun Moon
Su Chul Jang
Kyoung-Ho Choi
Yoon-Keun Kim
Yong Song Gho
spellingShingle Eun-Young Lee
Kyong-Su Park
Yae Jin Yoon
Jaewook Lee
Hyung-Geun Moon
Su Chul Jang
Kyoung-Ho Choi
Yoon-Keun Kim
Yong Song Gho
Therapeutic effects of autologous tumor-derived nanovesicles on melanoma growth and metastasis.
PLoS ONE
author_facet Eun-Young Lee
Kyong-Su Park
Yae Jin Yoon
Jaewook Lee
Hyung-Geun Moon
Su Chul Jang
Kyoung-Ho Choi
Yoon-Keun Kim
Yong Song Gho
author_sort Eun-Young Lee
title Therapeutic effects of autologous tumor-derived nanovesicles on melanoma growth and metastasis.
title_short Therapeutic effects of autologous tumor-derived nanovesicles on melanoma growth and metastasis.
title_full Therapeutic effects of autologous tumor-derived nanovesicles on melanoma growth and metastasis.
title_fullStr Therapeutic effects of autologous tumor-derived nanovesicles on melanoma growth and metastasis.
title_full_unstemmed Therapeutic effects of autologous tumor-derived nanovesicles on melanoma growth and metastasis.
title_sort therapeutic effects of autologous tumor-derived nanovesicles on melanoma growth and metastasis.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description Cancer vaccines with optimal tumor-associated antigens show promise for anti-tumor immunotherapy. Recently, nano-sized vesicles, such as exosomes derived from tumors, were suggested as potential antigen candidates, although the total yield of exosomes is not sufficient for clinical applications. In the present study, we developed a new vaccine strategy based on nano-sized vesicles derived from primary autologous tumors. Through homogenization and sonication of tumor tissues, we achieved high yields of vesicle-bound antigens. These nanovesicles were enriched with antigenic membrane targets but lacked nuclear autoantigens. Furthermore, these nanovesicles together with adjuvant activated dendritic cells in vitro, and induced effective anti-tumor immune responses in both primary and metastatic melanoma mouse models. Therefore, autologous tumor-derived nanovesicles may represent a novel source of antigens with high-level immunogenicity for use in acellular vaccines without compromising safety. Our strategy is cost-effective and can be applied to patient-specific cancer therapeutic vaccination.
url http://europepmc.org/articles/PMC3305328?pdf=render
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