Therapeutic agents

The invention claimed is: 1 . An isolated immuno-responsive cell expressing (i) a second generation chimeric antigen receptor comprising: (a) a signalling region at least 95% identical to the amino acid sequence of SEQ ID NO: 1 or SEQ ID NO: 2; (b) a co-stimulatory signalling region; (c) a transmembrane domain; and (d) a binding element that specifically interacts with a first epitope on a target antigen; and (ii) a chimeric costimulatory receptor comprising: (e) a co-stimulatory signalling region which is different to that of (b); (f) a transmembrane domain; and (g) a binding element that specifically interacts with a second epitope on a target antigen. 2 . The immuno-responsive cell of claim 1 which is a T-cell. 3 . The immuno-responsive cell of claim 1 wherein the signalling region is not identical to SEQ ID NO: 1 or SEQ ID NO: 2. 4 . The immuno-responsive cell of claim 1 wherein co-stimulatory signalling regions for (b) and (e) are selected from CD28, CD27, ICOS, 4-1BB, OX40, CD30, GITR, HVEM, DR3 and CD40. 5 . The immuno-responsive cell of claim 4 wherein one of (b) or (e) is CD28 and the other of (b) or (e) is 4-1BB or OX40. 6 . The immuno-responsive cell of claim 5 wherein (b) is CD28. 7 . The immuno-responsive cell of claim 5 wherein (e) is 4-1BB or CD27. 8 . The immuno-responsive cell of claim 1 wherein the transmembrane domains of (c) and (f) are selected from CD8a and CD28 transmembrane domains. 9 . The immuno-responsive cell of claim 1 wherein the first and second epitopes are associated with the same receptor or antigen. 10 . The immuno-responsive cell of claim 1 which co-expresses a chimeric cytokine receptor. 11 . The immuno-responsive cell of claim 10 wherein the chimeric cytokine receptor is 4αβ. 12 . The immuno-responsive cell of claim 1 wherein at least one of binding element (d) or binding element (g) is a ligand for an ErbB dimer, a receptor for colony stimulating factor-1 (CSF-1R) or an α v β 6 integrin-specific binding agent. 13 . The immuno-responsive cell of claim 1 wherein binding element (d) comprises CSF-1 and binding element (g) comprises IL-34. 14 . The immuno-responsive cell of claim 1 , wherein binding element (d) is an α v β 6 integrin-specific binding agent which is a peptide comprising the sequence motif (SEQ ID NO 7) RGDLX 5 X 6 L or (SEQ ID NO 8) RGDLX 5 X 6 I, wherein LX 5 X 6 L or LX 5 X 6 I is contained within an alpha helical structure, wherein X 5 and X 6 are helix promoting residues; and binding element (g) is a TIE peptide. 15 . The immuno-responsive cell of claim 1 wherein binding affinity of binding element (b) is lower than that of binding element (g). 16 . A method for preparing the isolated immuno-responsive cell of claim 1 comprising: transducing an immuno-responsive cell with nucleic acids encoding: (i) a second generation chimeric antigen receptor comprising: (a) a signalling region; (b) a co-stimulatory signalling region; (c) a transmembrane domain; and (d) a binding element that specifically interacts with a first epitope on a target antigen; and (ii) a chimeric costimulatory receptor comprising: (e) a co-stimulatory signalling region which is different to that of (b); (f) a transmembrane domain; and (g) a binding element that specifically interacts with a second epitope on a target antigen; expressing said nucleic acids in said isolated immuno-responsive cell, thereby producing the immuno-responsive cell of claim 1 . 17 . The method of claim 16 wherein the immuno-responsive cell comprises a chimeric cytokine receptor, and wherein an expansion step is carried out in the presence of a cytokine.