Litcius/Paper detail

Cancer cells educate natural killer cells to a metastasis-promoting cell state

Isaac S. Chan, Hildur Knútsdóttir, Gayathri Ramakrishnan, Veena Padmanaban, Manisha Warrier, Juan Carlos Ramı́rez, Matthew Dunworth, Hao Zhang, Elizabeth M. Jaffee, Joel S. Bader, Andrew J. Ewald

2020The Journal of Cell Biology155 citationsDOIOpen Access PDF

Abstract

Natural killer (NK) cells have potent antitumor and antimetastatic activity. It is incompletely understood how cancer cells escape NK cell surveillance. Using ex vivo and in vivo models of metastasis, we establish that keratin-14+ breast cancer cells are vulnerable to NK cells. We then discovered that exposure to cancer cells causes NK cells to lose their cytotoxic ability and promote metastatic outgrowth. Gene expression comparisons revealed that healthy NK cells have an active NK cell molecular phenotype, whereas tumor-exposed (teNK) cells resemble resting NK cells. Receptor-ligand analysis between teNK cells and tumor cells revealed multiple potential targets. We next showed that treatment with antibodies targeting TIGIT, antibodies targeting KLRG1, or small-molecule inhibitors of DNA methyltransferases (DMNT) each reduced colony formation. Combinations of DNMT inhibitors with anti-TIGIT or anti-KLRG1 antibodies further reduced metastatic potential. We propose that NK-directed therapies targeting these pathways would be effective in the adjuvant setting to prevent metastatic recurrence.

Topics & Concepts

TIGITLymphokine-activated killer cellBiologyCancer researchCytotoxic T cellCancer cellInterleukin 21NK-92MetastasisInterleukin 12AntibodyImmunologyCancerImmunotherapyIn vitroImmune systemBiochemistryGeneticsImmune Cell Function and InteractionCAR-T cell therapy researchT-cell and B-cell Immunology
Cancer cells educate natural killer cells to a metastasis-promoting cell state | Litcius