Combined tumor-directed recruitment and protection from immune suppression enable CAR T cell efficacy in solid tumors.
- Cadilha, B.L.
- Benmebarek, M.R.
- Dorman, K.
- Oner, A.
- Lorenzini, T.
- Obeck, H.
- Vänttinen, M.
- Pilato, M.D.
- Pruessmann, J.N.
- Stoiber, S.
- Huynh, D.
- Märkl, F.
- Seifert, M.
- Manske, K.
- Suarez-Gosalvez, J.
- Zeng, Y.
- Lesch, S.
- Karches, C.H.
- Heise, C.
- Gottschlich, A.
- Thomas, M.
- Marr, C.
- Zhang, J.
- Pandey, D.
- Feuchtinger, T.
- Subklewe, M.
- Mempel, T.R.
- Endres, S.
- Kobold, S.
DOIAbstract
CAR T cell therapy remains ineffective in solid tumors, due largely to poor infiltration and T cell suppression at the tumor site. T regulatory (Treg) cells suppress the immune response via inhibitory factors such as transforming growth factor–β (TGF-β). Treg cells expressing the C-C chemokine receptor 8 (CCR8) have been associated with poor prognosis in solid tumors. We postulated that CCR8 could be exploited to redirect effector T cells to the tumor site while a dominant-negative TGF-β receptor 2 (DNR) can simultaneously shield them from TGF-β. We identified that CCL1 from activated T cells potentiates a feedback loop for CCR8+ T cell recruitment to the tumor site. This sustained and improved infiltration of engineered T cells synergized ...
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