Potentiating adoptive cell therapy using synthetic IL-9 receptors

Author:

Kalbasi AnushaORCID,Siurala Mikko,Su Leon L.ORCID,Tariveranmoshabad Mito,Picton Lora K.ORCID,Ravikumar Pranali,Li PengORCID,Lin Jian-Xin,Escuin-Ordinas Helena,Da Tong,Kremer Sarah V.ORCID,Sun Amy L.,Castelli SofiaORCID,Agarwal SangyaORCID,Scholler John,Song Decheng,Rommel Philipp C.ORCID,Radaelli EnricoORCID,Young Regina M.,Leonard Warren J.ORCID,Ribas AntoniORCID,June Carl H.ORCID,Garcia K. ChristopherORCID

Abstract

AbstractSynthetic receptor signalling has the potential to endow adoptively transferred T cells with new functions that overcome major barriers in the treatment of solid tumours, including the need for conditioning chemotherapy1,2. Here we designed chimeric receptors that have an orthogonal IL-2 receptor extracellular domain (ECD) fused with the intracellular domain (ICD) of receptors for common γ-chain (γc) cytokines IL-4, IL-7, IL-9 and IL-21 such that the orthogonal IL-2 cytokine elicits the corresponding γccytokine signal. Of these, T cells that signal through the chimeric orthogonal IL-2Rβ-ECD–IL-9R-ICD (o9R) are distinguished by the concomitant activation of STAT1, STAT3 and STAT5 and assume characteristics of stem cell memory and effector T cells. Compared to o2R T cells, o9R T cells have superior anti-tumour efficacy in two recalcitrant syngeneic mouse solid tumour models of melanoma and pancreatic cancer and are effective even in the absence of conditioning lymphodepletion. Therefore, by repurposing IL-9R signalling using a chimeric orthogonal cytokine receptor, T cells gain new functions, and this results in improved anti-tumour activity for hard-to-treat solid tumours.

Publisher

Springer Science and Business Media LLC

Subject

Multidisciplinary

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