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Immunosurveillance by antiangiogenesis: tumor growth arrest by T cell-derived thrombospondin-1.


ABSTRACT: Recent advances in cancer immunotherapy suggest that manipulation of the immune system to enhance the antitumor response may be a highly effective treatment modality. One understudied aspect of immunosurveillance is antiangiogenic surveillance, the regulation of tumor angiogenesis by the immune system, independent of tumor cell lysis. CD4(+) T cells can negatively regulate angiogenesis by secreting antiangiogenic factors such as thrombospondin-1 (TSP-1). In tumor-bearing mice, we show that a Th1-directed viral infection that triggers upregulation of TSP-1 in CD4(+) and CD8(+) T cells can inhibit tumor angiogenesis and suppress tumor growth. Using bone marrow chimeras and adoptive T-cell transfers, we demonstrated that TSP-1 expression in the T-cell compartment was necessary and sufficient to inhibit tumor growth by suppressing tumor angiogenesis after the viral infection. Our results establish that tumorigenesis can be stanched by antiangiogenic surveillance triggered by an acute viral infection, suggesting novel immunologic approaches to achieve antiangiogenic therapy.

SUBMITTER: Schadler KL 

PROVIDER: S-EPMC4061618 | biostudies-literature | 2014 Apr

REPOSITORIES: biostudies-literature

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Immunosurveillance by antiangiogenesis: tumor growth arrest by T cell-derived thrombospondin-1.

Schadler Keri L KL   Crosby Erika J EJ   Zhou Alice Yao AY   Bhang Dong Ha DH   Braunstein Lior L   Baek Kwan Hyuck KH   Crawford Danielle D   Crawford Alison A   Angelosanto Jill J   Wherry E John EJ   Ryeom Sandra S  

Cancer research 20140303 8


Recent advances in cancer immunotherapy suggest that manipulation of the immune system to enhance the antitumor response may be a highly effective treatment modality. One understudied aspect of immunosurveillance is antiangiogenic surveillance, the regulation of tumor angiogenesis by the immune system, independent of tumor cell lysis. CD4(+) T cells can negatively regulate angiogenesis by secreting antiangiogenic factors such as thrombospondin-1 (TSP-1). In tumor-bearing mice, we show that a Th1  ...[more]

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