Host type I IFN signals are required for antitumor CD8+ T cell responses through CD8α+ dendritic cells
Despite lack of tumor control in many models, spontaneous T cell priming occurs frequently in response to a growing tumor. However, the innate immune mechanisms that promote natural antitumor T cell responses are undefined. In human metastatic melanoma, there was a correlation between a type I inter...
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| Veröffentlicht in: | The Journal of experimental medicine 2011-09, Vol.208 (10), p.2005-2016 |
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| container_issue | 10 |
| container_start_page | 2005 |
| container_title | The Journal of experimental medicine |
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| creator | Fuertes, Mercedes B. Kacha, Aalok K. Kline, Justin Woo, Seng-Ryong Kranz, David M. Murphy, Kenneth M. Gajewski, Thomas F. |
| description | Despite lack of tumor control in many models, spontaneous T cell priming occurs frequently in response to a growing tumor. However, the innate immune mechanisms that promote natural antitumor T cell responses are undefined. In human metastatic melanoma, there was a correlation between a type I interferon (IFN) transcriptional profile and T cell markers in metastatic tumor tissue. In mice, IFN-β was produced by CD11c+ cells after tumor implantation, and tumor-induced T cell priming was defective in mice lacking IFN-α/βR or Stat1. IFN signaling was required in the hematopoietic compartment at the level of host antigen-presenting cells, and selectively for intratumoral accumulation of CD8α+ dendritic cells, which were demonstrated to be essential using Batf3−/− mice. Thus, host type I IFNs are critical for the innate immune recognition of a growing tumor through signaling on CD8α+ DCs. |
| doi_str_mv | 10.1084/jem.20101159 |
| format | Article |
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However, the innate immune mechanisms that promote natural antitumor T cell responses are undefined. In human metastatic melanoma, there was a correlation between a type I interferon (IFN) transcriptional profile and T cell markers in metastatic tumor tissue. In mice, IFN-β was produced by CD11c+ cells after tumor implantation, and tumor-induced T cell priming was defective in mice lacking IFN-α/βR or Stat1. IFN signaling was required in the hematopoietic compartment at the level of host antigen-presenting cells, and selectively for intratumoral accumulation of CD8α+ dendritic cells, which were demonstrated to be essential using Batf3−/− mice. 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| title | Host type I IFN signals are required for antitumor CD8+ T cell responses through CD8α+ dendritic cells |
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