CD4+ Th1 HER2-Specific T Cells as a Novel Treatment for HER2-Overexpressing Breast Cancer

CD4+ Th1 HER2-Specific T Cells as a Novel Treatment for HER2-Overexpressing Breast Cancer

During the last research period, we have made significant progress in the development of our mouse neu-reactive T cell lines. First, we have confirmed the key CD4+ neu peptides (p101 and p373) most effective at priming T cell responses. Of the peptide-specific T cell lines tested, only p101- and p37...

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1. Verfasser: Lai, Vy P
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Sprache:eng
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ADOPTIVE T CELL THERAPY
BREAST CANCER
CD4+ T CELLS
CELLS(BIOLOGY)
CULTURES(BIOLOGY)
CYTOKINES
EXPANSION
GROWTH(PHYSIOLOGY)
IN VIVO ANALYSIS
INFUSIONS
Medicine and Medical Research
NEOPLASMS
NEU ANTIGEN
NEU-TRANSGENIC MICE
PEPTIDES
PRIMERS
PRODUCTION
REGRESSION ANALYSIS
RESPONSE
T LYMPHOCYTES
VACCINES
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description During the last research period, we have made significant progress in the development of our mouse neu-reactive T cell lines. First, we have confirmed the key CD4+ neu peptides (p101 and p373) most effective at priming T cell responses. Of the peptide-specific T cell lines tested, only p101- and p373- T cells induced both peptide- and protein-specific responses. In preliminary studies involving adjuvants, GMCSF was highly effective for use with our peptide vaccines. Second, we have thoroughly characterized the cytokine production by our ex vivo expanded T cells and observed high levels of secreted Th1 cytokines, primarily IFN and GM-CSF, but also, interestingly, Th2 cytokines, primarily IL-5 and IL-6. Furthermore, IL-17, a pro-inflammatory cytokine, was also found to be secreted by the cultured T cells during ex vivo expansion. Our studies have also demonstrated that the addition of IL-7 (among all the tested cytokines) to IL-2 in the T cell culture regimen is necessary for optimal ex vivo growth. Third, we have clearly demonstrated that our neu specific T cell lines were highly effective at inhibiting tumor growth, particularly MP (multiple peptide)-specific T cells. Three T cell infusions were more effective at inducing tumor regression than a single infusion. Most importantly, the antitumor inhibition was mediated by endogenous CD8+ T cells.
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First, we have confirmed the key CD4+ neu peptides (p101 and p373) most effective at priming T cell responses. Of the peptide-specific T cell lines tested, only p101- and p373- T cells induced both peptide- and protein-specific responses. In preliminary studies involving adjuvants, GMCSF was highly effective for use with our peptide vaccines. Second, we have thoroughly characterized the cytokine production by our ex vivo expanded T cells and observed high levels of secreted Th1 cytokines, primarily IFN and GM-CSF, but also, interestingly, Th2 cytokines, primarily IL-5 and IL-6. Furthermore, IL-17, a pro-inflammatory cytokine, was also found to be secreted by the cultured T cells during ex vivo expansion. Our studies have also demonstrated that the addition of IL-7 (among all the tested cytokines) to IL-2 in the T cell culture regimen is necessary for optimal ex vivo growth. Third, we have clearly demonstrated that our neu specific T cell lines were highly effective at inhibiting tumor growth, particularly MP (multiple peptide)-specific T cells. Three T cell infusions were more effective at inducing tumor regression than a single infusion. Most importantly, the antitumor inhibition was mediated by endogenous CD8+ T cells.</description><language>eng</language><subject>ADOPTIVE T CELL THERAPY ; BREAST CANCER ; CD4+ T CELLS ; CELLS(BIOLOGY) ; CULTURES(BIOLOGY) ; CYTOKINES ; EXPANSION ; GROWTH(PHYSIOLOGY) ; IN VIVO ANALYSIS ; INFUSIONS ; Medicine and Medical Research ; NEOPLASMS ; NEU ANTIGEN ; NEU-TRANSGENIC MICE ; PEPTIDES ; PRIMERS ; PRODUCTION ; REGRESSION ANALYSIS ; RESPONSE ; T LYMPHOCYTES ; VACCINES</subject><creationdate>2007</creationdate><rights>Approved for public release; distribution is unlimited.</rights><oa>free_for_read</oa><woscitedreferencessubscribed>false</woscitedreferencessubscribed></display><links><openurl>$$Topenurl_article</openurl><openurlfulltext>$$Topenurlfull_article</openurlfulltext><thumbnail>$$Tsyndetics_thumb_exl</thumbnail><link.rule.ids>230,780,885,27567,27568</link.rule.ids><linktorsrc>$$Uhttps://apps.dtic.mil/sti/citations/ADA477538$$EView_record_in_DTIC$$FView_record_in_$$GDTIC$$Hfree_for_read</linktorsrc></links><search><creatorcontrib>Lai, Vy P</creatorcontrib><creatorcontrib>WASHINGTON UNIV SEATTLE</creatorcontrib><title>CD4+ Th1 HER2-Specific T Cells as a Novel Treatment for HER2-Overexpressing Breast Cancer</title><description>During the last research period, we have made significant progress in the development of our mouse neu-reactive T cell lines. 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Third, we have clearly demonstrated that our neu specific T cell lines were highly effective at inhibiting tumor growth, particularly MP (multiple peptide)-specific T cells. Three T cell infusions were more effective at inducing tumor regression than a single infusion. Most importantly, the antitumor inhibition was mediated by endogenous CD8+ T cells.</abstract><oa>free_for_read</oa></addata></record>
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subjects ADOPTIVE T CELL THERAPY
BREAST CANCER
CD4+ T CELLS
CELLS(BIOLOGY)
CULTURES(BIOLOGY)
CYTOKINES
EXPANSION
GROWTH(PHYSIOLOGY)
IN VIVO ANALYSIS
INFUSIONS
Medicine and Medical Research
NEOPLASMS
NEU ANTIGEN
NEU-TRANSGENIC MICE
PEPTIDES
PRIMERS
PRODUCTION
REGRESSION ANALYSIS
RESPONSE
T LYMPHOCYTES
VACCINES
title CD4+ Th1 HER2-Specific T Cells as a Novel Treatment for HER2-Overexpressing Breast Cancer
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