Specific targeting of whole lymphoma cells to dendritic cells <it>ex vivo </it>provides a potent antitumor vaccine

Specific targeting of whole lymphoma cells to dendritic cells <it>ex vivo </it>provides a potent antitumor vaccine

<p>Abstract</p> <p>Background</p> <p>Dendritic cells (DC) pulsed with tumor-derived antigenic material have widely been used in antitumor vaccination protocols. However, the optimal strategy of DC loading has not yet been established. Our aim was to define requirements...

Full description

Bibliographic Details
Main Authors: Mocikat Ralph, Mysliwietz Josef, Adam Christian
Format: Article
Language:English
Published: BMC 2007-03-01
Series:Journal of Translational Medicine
Online Access:http://www.translational-medicine.com/content/5/1/16
id doaj-3c093a6246a74fd489ea39cf9b2edddc
record_format Article
spelling doaj-3c093a6246a74fd489ea39cf9b2edddc2020-11-24T21:30:05ZengBMCJournal of Translational Medicine1479-58762007-03-01511610.1186/1479-5876-5-16Specific targeting of whole lymphoma cells to dendritic cells <it>ex vivo </it>provides a potent antitumor vaccineMocikat RalphMysliwietz JosefAdam Christian<p>Abstract</p> <p>Background</p> <p>Dendritic cells (DC) pulsed with tumor-derived antigenic material have widely been used in antitumor vaccination protocols. However, the optimal strategy of DC loading has not yet been established. Our aim was to define requirements of optimal DC vaccines in terms of <it>in vivo </it>protection in a murine B-cell lymphoma model.</p> <p>Methods</p> <p>We compare various loading reagents including whole parental and modified tumor cells and a single tumor-specific antigen, namely the lymphoma idiotype (Id). Bone marrow-derived DC were pulsed <it>in vitro </it>and used for therapy of established A20 lymphomas.</p> <p>Results</p> <p>We show that a vaccine with superior antitumor efficacy can be generated when DC are loaded with whole modified tumor cells which provide both (i) antigenic polyvalency and (ii) receptor-mediated antigen internalization. Uptake of cellular material was greatly enhanced when the tumor cells used for DC pulsing were engineered to express an anti-Fc receptor immunoglobulin specificity. Upon transfer of these DC, established tumor burdens were eradicated in 50% of mice. By contrast, pulsing DC with unmodified lymphoma cells or with the lymphoma Id, even when it was endowed with the anti-Fc receptor binding arm, was far less effective. A specific humoral anti-Id response could be detected, particularly following delivery of Id protein-pulsed DC, but it was not predictive of tumor protection. Instead a T-cell response was pivotal for successful tumor protection. Interaction of the transferred DC with CD8<sup>+ </sup>T lymphocytes seemed to play a role for induction of the immune response but was dispensable when DC had received an additional maturation stimulus.</p> <p>Conclusion</p> <p>Our analyses show that the advantages of specific antigen redirection and antigenic polyvalency can be combined to generate DC-based vaccines with superior antitumor efficacy. This mouse model may provide information for the standardization of DC-based vaccination protocols.</p> http://www.translational-medicine.com/content/5/1/16
collection DOAJ
language English
format Article
sources DOAJ
author Mocikat Ralph
Mysliwietz Josef
Adam Christian
spellingShingle Mocikat Ralph
Mysliwietz Josef
Adam Christian
Specific targeting of whole lymphoma cells to dendritic cells <it>ex vivo </it>provides a potent antitumor vaccine
Journal of Translational Medicine
author_facet Mocikat Ralph
Mysliwietz Josef
Adam Christian
author_sort Mocikat Ralph
title Specific targeting of whole lymphoma cells to dendritic cells <it>ex vivo </it>provides a potent antitumor vaccine
title_short Specific targeting of whole lymphoma cells to dendritic cells <it>ex vivo </it>provides a potent antitumor vaccine
title_full Specific targeting of whole lymphoma cells to dendritic cells <it>ex vivo </it>provides a potent antitumor vaccine
title_fullStr Specific targeting of whole lymphoma cells to dendritic cells <it>ex vivo </it>provides a potent antitumor vaccine
title_full_unstemmed Specific targeting of whole lymphoma cells to dendritic cells <it>ex vivo </it>provides a potent antitumor vaccine
title_sort specific targeting of whole lymphoma cells to dendritic cells <it>ex vivo </it>provides a potent antitumor vaccine
publisher BMC
series Journal of Translational Medicine
issn 1479-5876
publishDate 2007-03-01
description <p>Abstract</p> <p>Background</p> <p>Dendritic cells (DC) pulsed with tumor-derived antigenic material have widely been used in antitumor vaccination protocols. However, the optimal strategy of DC loading has not yet been established. Our aim was to define requirements of optimal DC vaccines in terms of <it>in vivo </it>protection in a murine B-cell lymphoma model.</p> <p>Methods</p> <p>We compare various loading reagents including whole parental and modified tumor cells and a single tumor-specific antigen, namely the lymphoma idiotype (Id). Bone marrow-derived DC were pulsed <it>in vitro </it>and used for therapy of established A20 lymphomas.</p> <p>Results</p> <p>We show that a vaccine with superior antitumor efficacy can be generated when DC are loaded with whole modified tumor cells which provide both (i) antigenic polyvalency and (ii) receptor-mediated antigen internalization. Uptake of cellular material was greatly enhanced when the tumor cells used for DC pulsing were engineered to express an anti-Fc receptor immunoglobulin specificity. Upon transfer of these DC, established tumor burdens were eradicated in 50% of mice. By contrast, pulsing DC with unmodified lymphoma cells or with the lymphoma Id, even when it was endowed with the anti-Fc receptor binding arm, was far less effective. A specific humoral anti-Id response could be detected, particularly following delivery of Id protein-pulsed DC, but it was not predictive of tumor protection. Instead a T-cell response was pivotal for successful tumor protection. Interaction of the transferred DC with CD8<sup>+ </sup>T lymphocytes seemed to play a role for induction of the immune response but was dispensable when DC had received an additional maturation stimulus.</p> <p>Conclusion</p> <p>Our analyses show that the advantages of specific antigen redirection and antigenic polyvalency can be combined to generate DC-based vaccines with superior antitumor efficacy. This mouse model may provide information for the standardization of DC-based vaccination protocols.</p>
url http://www.translational-medicine.com/content/5/1/16
work_keys_str_mv AT mocikatralph specifictargetingofwholelymphomacellstodendriticcellsitexvivoitprovidesapotentantitumorvaccine
AT mysliwietzjosef specifictargetingofwholelymphomacellstodendriticcellsitexvivoitprovidesapotentantitumorvaccine
AT adamchristian specifictargetingofwholelymphomacellstodendriticcellsitexvivoitprovidesapotentantitumorvaccine
_version_ 1725964044728270848

Similar Items