Two Host Factors Regulate Persistence of H7 super(a)-Specific T Cells Injected in Tumor-Bearing Mice
Background Injection of CD8 T cells primed against immunodominant minor histocompatibility antigens (MiHA) such as H7 super(a) can eradicate leukemia and solid tumors. To understand why MiHA-targeted T cells have such a potent antitumor effect it is essential to evaluate their in vivo behavior. In t...
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| Veröffentlicht in: | PloS one 2009-01, Vol.4 (1), p.e4116-e4116 |
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| creator | Meunier, Marie-Christine Baron, Chantal Perreault, Claude Unutmaz, Derya |
| description | Background Injection of CD8 T cells primed against immunodominant minor histocompatibility antigens (MiHA) such as H7 super(a) can eradicate leukemia and solid tumors. To understand why MiHA-targeted T cells have such a potent antitumor effect it is essential to evaluate their in vivo behavior. In the present work, we therefore addressed two specific questions: what is the proliferative dynamics of H7 super(a)-specifc T cells in tumors, and do H7 super(a)-specific T cells persist long-term after adoptive transfer? Methodology/Principal Findings By day 3 after adoptive transfer, we observed a selective infiltration of melanomas by anti-H7 super(a) T cells. Over the next five days, anti-H7 super(a) T cells expanded massively in the tumor but not in the spleen. Thus, by day 8 after injection, anti-H7 super(a) T cells in the tumor had undergone more cell divisions than those in the spleen. These data strongly suggest that anti-H7 super(a) T cells proliferate preferentially and extensively in the tumors. We also found that two host factors regulated long-term persistence of anti-H7 super(a) memory T cells: thymic function and expression of H7 super(a) by host cells. On day 100, anti-H7 super(a) memory T cells were abundant in euthymic H7 super(a)-negative (B10.H7 super(b)) mice, present in low numbers in thymectomized H7 super(a)-positive (B10) hosts, and undetectable in euthymic H7 super(a)-positive recipients. Conclusions/Significance Although in general the tumor environment is not propitious to T-cell invasion and expansion, the present work shows that this limitation may be overcome by adoptive transfer of primed CD8 T cells targeted to an immunodominant MiHA (here H7 super(a)). At least in some cases, prolonged persistence of adoptively transferred T cells may be valuable for prevention of late cancer relapse in adoptive hosts. Our findings therefore suggest that it may be advantageous to target MiHAs with a restricted tissue distribution in order to promote persistence of memory T cells and thereby minimize the risk of cancer recurrence. |
| doi_str_mv | 10.1371/journal.pone.0004116 |
| format | Article |
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To understand why MiHA-targeted T cells have such a potent antitumor effect it is essential to evaluate their in vivo behavior. In the present work, we therefore addressed two specific questions: what is the proliferative dynamics of H7 super(a)-specifc T cells in tumors, and do H7 super(a)-specific T cells persist long-term after adoptive transfer? Methodology/Principal Findings By day 3 after adoptive transfer, we observed a selective infiltration of melanomas by anti-H7 super(a) T cells. Over the next five days, anti-H7 super(a) T cells expanded massively in the tumor but not in the spleen. Thus, by day 8 after injection, anti-H7 super(a) T cells in the tumor had undergone more cell divisions than those in the spleen. These data strongly suggest that anti-H7 super(a) T cells proliferate preferentially and extensively in the tumors. We also found that two host factors regulated long-term persistence of anti-H7 super(a) memory T cells: thymic function and expression of H7 super(a) by host cells. On day 100, anti-H7 super(a) memory T cells were abundant in euthymic H7 super(a)-negative (B10.H7 super(b)) mice, present in low numbers in thymectomized H7 super(a)-positive (B10) hosts, and undetectable in euthymic H7 super(a)-positive recipients. Conclusions/Significance Although in general the tumor environment is not propitious to T-cell invasion and expansion, the present work shows that this limitation may be overcome by adoptive transfer of primed CD8 T cells targeted to an immunodominant MiHA (here H7 super(a)). At least in some cases, prolonged persistence of adoptively transferred T cells may be valuable for prevention of late cancer relapse in adoptive hosts. Our findings therefore suggest that it may be advantageous to target MiHAs with a restricted tissue distribution in order to promote persistence of memory T cells and thereby minimize the risk of cancer recurrence.</description><identifier>ISSN: 1932-6203</identifier><identifier>EISSN: 1932-6203</identifier><identifier>DOI: 10.1371/journal.pone.0004116</identifier><language>eng</language><ispartof>PloS one, 2009-01, Vol.4 (1), p.e4116-e4116</ispartof><lds50>peer_reviewed</lds50><woscitedreferencessubscribed>false</woscitedreferencessubscribed></display><links><openurl>$$Topenurl_article</openurl><openurlfulltext>$$Topenurlfull_article</openurlfulltext><thumbnail>$$Tsyndetics_thumb_exl</thumbnail><link.rule.ids>314,776,780,860,27901,27902</link.rule.ids></links><search><creatorcontrib>Meunier, Marie-Christine</creatorcontrib><creatorcontrib>Baron, Chantal</creatorcontrib><creatorcontrib>Perreault, Claude</creatorcontrib><creatorcontrib>Unutmaz, Derya</creatorcontrib><title>Two Host Factors Regulate Persistence of H7 super(a)-Specific T Cells Injected in Tumor-Bearing Mice</title><title>PloS one</title><description>Background Injection of CD8 T cells primed against immunodominant minor histocompatibility antigens (MiHA) such as H7 super(a) can eradicate leukemia and solid tumors. To understand why MiHA-targeted T cells have such a potent antitumor effect it is essential to evaluate their in vivo behavior. In the present work, we therefore addressed two specific questions: what is the proliferative dynamics of H7 super(a)-specifc T cells in tumors, and do H7 super(a)-specific T cells persist long-term after adoptive transfer? Methodology/Principal Findings By day 3 after adoptive transfer, we observed a selective infiltration of melanomas by anti-H7 super(a) T cells. Over the next five days, anti-H7 super(a) T cells expanded massively in the tumor but not in the spleen. Thus, by day 8 after injection, anti-H7 super(a) T cells in the tumor had undergone more cell divisions than those in the spleen. These data strongly suggest that anti-H7 super(a) T cells proliferate preferentially and extensively in the tumors. We also found that two host factors regulated long-term persistence of anti-H7 super(a) memory T cells: thymic function and expression of H7 super(a) by host cells. On day 100, anti-H7 super(a) memory T cells were abundant in euthymic H7 super(a)-negative (B10.H7 super(b)) mice, present in low numbers in thymectomized H7 super(a)-positive (B10) hosts, and undetectable in euthymic H7 super(a)-positive recipients. Conclusions/Significance Although in general the tumor environment is not propitious to T-cell invasion and expansion, the present work shows that this limitation may be overcome by adoptive transfer of primed CD8 T cells targeted to an immunodominant MiHA (here H7 super(a)). At least in some cases, prolonged persistence of adoptively transferred T cells may be valuable for prevention of late cancer relapse in adoptive hosts. 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To understand why MiHA-targeted T cells have such a potent antitumor effect it is essential to evaluate their in vivo behavior. In the present work, we therefore addressed two specific questions: what is the proliferative dynamics of H7 super(a)-specifc T cells in tumors, and do H7 super(a)-specific T cells persist long-term after adoptive transfer? Methodology/Principal Findings By day 3 after adoptive transfer, we observed a selective infiltration of melanomas by anti-H7 super(a) T cells. Over the next five days, anti-H7 super(a) T cells expanded massively in the tumor but not in the spleen. Thus, by day 8 after injection, anti-H7 super(a) T cells in the tumor had undergone more cell divisions than those in the spleen. These data strongly suggest that anti-H7 super(a) T cells proliferate preferentially and extensively in the tumors. We also found that two host factors regulated long-term persistence of anti-H7 super(a) memory T cells: thymic function and expression of H7 super(a) by host cells. On day 100, anti-H7 super(a) memory T cells were abundant in euthymic H7 super(a)-negative (B10.H7 super(b)) mice, present in low numbers in thymectomized H7 super(a)-positive (B10) hosts, and undetectable in euthymic H7 super(a)-positive recipients. Conclusions/Significance Although in general the tumor environment is not propitious to T-cell invasion and expansion, the present work shows that this limitation may be overcome by adoptive transfer of primed CD8 T cells targeted to an immunodominant MiHA (here H7 super(a)). At least in some cases, prolonged persistence of adoptively transferred T cells may be valuable for prevention of late cancer relapse in adoptive hosts. Our findings therefore suggest that it may be advantageous to target MiHAs with a restricted tissue distribution in order to promote persistence of memory T cells and thereby minimize the risk of cancer recurrence.</abstract><doi>10.1371/journal.pone.0004116</doi></addata></record> |
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| title | Two Host Factors Regulate Persistence of H7 super(a)-Specific T Cells Injected in Tumor-Bearing Mice |
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