Engineered transcription activator-like effector (TALE) domains and uses thereof

What is claimed is: 1. A Transcription Activator-Like Effector Nuclease (TALEN), comprising (a) a nuclease cleavage domain; (b) a C-terminal domain conjugated to the nuclease cleavage domain; (c) a TALE repeat array conjugated to the C-terminal domain; and (d) an N-terminal domain conjugated to the TALE repeat array, wherein (i) the N-terminal domain comprises the amino acid sequence of SEQ ID NO: 2, SEQ ID NO: 3, or SEQ ID NO: 4, or a functional truncated version thereof; and/or (ii) the C-terminal domain comprises an amino acid sequence that differs from the canonical C-terminal domain of SEQ ID NO: 22, in that it comprises one or more of the following amino acid replacements: K37Q, K38Q, K48Q, R49Q, R52Q, R53Q, R57Q, and R61Q, or a functional truncated version thereof. 2. The TALEN of claim 1 , wherein the C-terminal domain comprises a Q3 variant sequence of SEQ ID NO: 23. 3. The TALEN of claim 1 , wherein the C-terminal domain comprises a Q7 variant sequence of SEQ ID NO: 24. 4. The TALEN of claim 1 , wherein the nuclease cleavage domain is a FokI nuclease domain. 5. The TALEN of claim 1 , wherein the TALEN is a monomer. 6. The TALEN of claim 5 , wherein the TALEN monomer can dimerize with another TALEN monomer to form a TALEN dimer. 7. The TALEN of claim 6 , wherein the TALEN cleaves the target sequence upon dimerization. 8. The TALEN of claim 1 , wherein the TALEN binds a CCR5 target sequence, an ATM target sequence, or a VEGFA target sequence. 9. The TALEN of claim 1 , wherein the net charge of the C-terminal domain is between +5 and −5. 10. The TALEN of claim 1 , wherein the N-terminal domain comprises an amino acid sequence that differs from the canonical N-terminal domain of SEQ ID NO: 1,in that at least 2 cationic amino acids of SEQ ID NO: 1 are replaced with an amino acid residue that exhibits no charge or a negative charge at physiological pH. 11. The TALEN of claim 1 , wherein the N-terminal domain comprises an amino acid sequence that differs from the canonical N-terminal domain of SEQ ID NO: 1, in that at least 3 cationic amino acids of SEQ ID NO: 1 are replaced with an amino acid residue that exhibits no charge or a negative charge at physiological pH. 12. The TALEN of claim 1 , wherein the N-terminal domain comprises an amino acid sequence that differs from the canonical N-terminal domain of SEQ ID NO: 1, in that at least 5 cationic amino acids of SEQ ID NO: 1 are replaced with an amino acid residue that exhibits no charge or a negative charge at physiological pH. 13. The TALEN of claim 1 , wherein the N-terminal domain comprises an amino acid sequence that differs from the canonical N-terminal domain of SEQ ID NO: 1, in that at least 10 cationic amino acids of SEQ ID NO: 1 are replaced with an amino acid residue that exhibits no charge or a negative charge at physiological pH. 14. The TALEN of claim 1 , wherein the at least one cationic amino acid residue is arginine (R) or lysine (K). 15. The TALEN of claim 1 , wherein each amino acid residue that exhibits no charge or a negative charge at physiological pH is, independently, glutamine (Q) or glycine (G). 16. The TALEN of claim 1 , wherein the N-terminal domain comprises an amino acid sequence that differs from the canonical N-terminal domain of SEQ ID NO: 1, in that at least one lysine or arginine residue is replaced with a glutamine residue. 17. The TALEN of claim 1 , wherein the N-terminal domain comprises an amino acid sequence that differs from the canonical N-terminal domain of SEQ ID NO: 1, in that at least one lysine or arginine residue is replaced with a glycine residue. 18. The TALEN of claim 1 , wherein the N-terminal domain comprises an amino acid sequence that differs from the canonical C-terminal domain of SEQ ID NO: 22, in that at least one lysine or arginine residue is replaced with a glutamine residue. 19. The TALEN of claim 1 , wherein the N-terminal domain comprises an amino acid sequence that differs from the canonical C-terminal domain of SEQ ID NO: 22, in that at least one lysine or arginine residue is replaced with a glycine residue. 20. The TALEN of claim 1 , wherein the C-terminal domain comprises an amino acid sequence that differs from the canonical C-terminal domain of SEQ ID NO: 22, in that it comprises one or more of the following amino acid replacements: K38Q, R52Q, and R61Q. 21. The TALEN of claim 1 , wherein the nuclease cleavage domain comprises a homodimeric FokI domain of SEQ ID NO: 26. 22. The TALEN of claim 1 , wherein the nuclease cleavage domain comprises a FokI-EL domain of SEQ ID NO: 27, a FokI-KK domain of SEQ ID NO: 28, a FokI-ELD domain of SEQ ID NO: 29, or a FokI-KKR domain of SEQ ID NO: 30. 23. A pharmaceutical composition comprising the TALEN of claim 1 and a pharmaceutically acceptable excipient. 24. A method of cleaving a target sequence in a nucleic acid molecule, comprising contacting a nucleic acid molecule comprising the target sequence with the TALEN of claim 1 , wherein the TALEN comprises a TALEN repeat array that binds the target sequence, and wherein the TALEN cleaves the target sequence. 25. The method of claim 24 , wherein the target sequence is comprised in a cell. 26. The method of claim 24 , wherein the target sequence is comprised in a subject. 27. The method of claim 24 , wherein the method comprises administering a pharmaceutical composition comprising the TALEN to the subject in an amount sufficient for the TALEN to bind and cleave the target site. 28. The method of claim 27 , wherein the TALEN binds a CCR5 target sequence, an ATM target sequence, or a VEGFA target sequence.