VEGF-A drives TOX-dependent T cell exhaustion in anti-PD-1-resistant microsatellite stable colorectal cancers.
Chang Gon KimMi JangYoungun KimGalam LeemKyung Hwan KimAndrew J LeeTae-Shin KimSeong Jin ChoiHyung-Don KimJi Won HanMinsuk KwonJong Hoon KimAndrew J LeeSu Kyung NamSeok-Joo BaeSat Byol LeeSang Joon ShinSung Ho ParkJoong Bae AhnInkyung JungKang Young LeeSu-Hyung ParkHoguen KimByung Soh MinEui-Cheol ShinPublished in: Science immunology (2020)
Although immune checkpoint blockade therapies have demonstrated clinical efficacy in cancer treatment, harnessing this strategy is largely encumbered by resistance in multiple cancer settings. Here, we show that tumor-infiltrating T cells are severely exhausted in the microsatellite stable (MSS) colorectal cancer (CRC), a representative example of PD-1 blockade-resistant tumors. In MSS CRC, we found wound healing signature to be up-regulated and that T cell exhaustion is driven by vascular endothelial growth factor-A (VEGF-A). We report that VEGF-A induces the expression of transcription factor TOX in T cells to drive exhaustion-specific transcription program in T cells. Using a combination of in vitro, ex vivo, and in vivo mouse studies, we demonstrate that combined blockade of PD-1 and VEGF-A restores the antitumor functions of T cells, resulting in better control of MSS CRC tumors.