Pseudomonas exotoxin a with less immunogenic T cell and/or B cell epitopes

The invention claimed is: 1. A Pseudomonas exotoxin A (PE) comprising a PE amino acid sequence having a substitution of one or more of amino acid residues selected from the group consisting of D463, Y481, and L516 as defined by reference to SEQ ID NO: 1, with the proviso that when the amino acid residue at position 516 is substituted with alanine, at least one of amino acid residues D463 and Y481 is also substituted, wherein the PE optionally has a further substitution of one or more amino acid residues within one or more B cell epitopes, and/or a further substitution of one or more amino acid residues within one or more T-cell epitopes, and/or a deletion of one or more continuous amino acid residues of residues 1-273 and 285-394 as defined by SEQ ID NO: 1. 2. The PE of claim 1 , wherein the PE has the further substitution of an amino acid within one or more B-cell epitopes, and the further substitution of an amino acid within one or more B-cell epitopes is a substitution of one or more of amino acid residues selected from the group consisting of E282, E285, P290, R313, N314, P319, D324, E327, E331, Q332, D403, D406, R412, R427, E431, R432, R458, D461, R467, R490, R505, R513, E522, R538, E548, R551, R576, K590, Q592, and L597, as defined by reference to SEQ ID NO: 1. 3. The PE of claim 2 , wherein the substitution of one or more of amino acid residues D463, Y481, and L516 is a substitution of, independently, alanine, glycine, serine, or glutamine in place of one or more of amino acid residues D463, Y481, and L516. 4. The PE of claim 2 , wherein the further substitution of an amino acid within one or more B-cell epitopes is a substitution of, independently, alanine, glycine, or serine in place of one or more of amino acid residues R427, R458, R467, R490, R505, and R538. 5. The PE of claim 4 , wherein the substitution of one or more of amino acid residues D463, Y481, and L516 is a substitution of alanine in place of amino acid residue D463, and the further substitution of one or more amino acid residues within one or more B-cell epitopes is selected from the group consisting of: (a) a substitution of alanine for amino acid residue R427; (b) a substitution of alanine for amino acid residue R458; (c) a substitution of alanine for amino acid residue R467; (d) a substitution of alanine for amino acid residue R490; (e) a substitution of alanine for amino acid residue R505; and (f) a substitution of alanine for amino acid residue R538, as defined by reference to SEQ ID NO: 1. 6. The PE of claim 1 , wherein the substitution of one or more amino acid residues within one or more T-cell epitopes is a substitution of alanine, glycine, serine, or glutamine in place of one or more of amino acid residues selected from the group consisting of I493, R494, N495, G496, L498, L499, R500, V501 and Y502. 7. A chimeric molecule comprising (a) a targeting moiety conjugated or fused to (b) the PE of claim 1 . 8. The chimeric molecule of claim 7 , wherein the targeting moiety is a monoclonal antibody. 9. The chimeric molecule of claim 8 , wherein the monoclonal antibody specifically binds to a cell surface marker selected from the group consisting of CD19, CD21, CD22, CD25, CD30, CD33, CD79b, transferrin receptor, epidermal growth factor (EGF) receptor, mesothelin, cadherin, and Lewis Y. 10. The chimeric molecule of claim 8 , wherein the targeting moiety is an antibody selected from the group consisting of B3, RFB4, SS, SS1, MN, MB, HN1, HN2, HB21, MORAb-009, HA22, and antigen binding portions thereof. 11. The chimeric molecule of claim 8 , wherein the targeting moiety is the antigen binding portion of HA22. 12. A pharmaceutical composition comprising (a) the PE of claim 1 and (b) a pharmaceutically acceptable carrier. 13. A method of inhibiting the growth of a target cell, wherein the method comprises contacting the cell with the PE of claim 1 , in an amount effective to inhibit growth of the target cell. 14. The method of claim 13 , wherein the target cell is a cancer cell.