Avirulent, immunogenic flavivirus chimeras

We claim: 1. An immunogenic composition comprising one or more live, attenuated flaviviruses comprising: (a) a nucleic acid chimera encoding: (i) a flavivirus structural protein, wherein the flavivirus structural protein is selected from the group consisting of: a C protein of Zika virus, a prM protein of Zika virus, and an E protein of Zika virus; and (ii) non-structural proteins from a second different flavivirus wherein the second different flavivirus comprises: a live, attenuated dengue-2 virus containing non-conservative amino acid substitutions; or other flavivirus genomes containing analogous mutations at the same loci as the dengue-2 virus, wherein the chimera is avirulent; and (b) a pharmaceutically acceptable carrier or excipient. 2. The immunogenic composition of claim 1 , further comprising a live, attenuated dengue-2 virus or other dengue-2 chimera. 3. The immunogenic composition of claim 1 , further comprising a chimeric dengue-2/dengue-1 virus comprising a nucleic acid sequence encoding at least one nonstructural protein from dengue-2 and a nucleic acid sequence encoding at least one of a C, prM, or E structural protein from dengue-1 virus. 4. The immunogenic composition of claim 2 , further comprising an additional flavivirus chimera. 5. The immunogenic composition of claim 1 , wherein the immunogenic composition comprises a dengue chimera, wherein the backbone of the dengue chimera comprises at least one non-structural protein of dengue-2 and a structural protein of dengue-2. 6. The immunogenic composition of claim 5 , wherein the structural protein of dengue-2 comprises a C (capsid) protein. 7. The immunogenic composition of claim 2 , wherein the live, attenuated dengue-2 virus comprises at least one of: a) a mutation at position 2579 which results in the presence of an aspartate at amino acid residue 53 of the NS1 protein of the live, attenuated dengue-2 virus; b) a mutation at position 57 which disrupts the function of the 5′ noncoding region protein of the live, attenuated dengue-2 virus; and c) a mutation at position 5270 which results in the presence of a valine at amino acid residue 250 of the NS3 protein of the live, attenuated dengue-2 virus. 8. The immunogenic composition of claim 2 , wherein the live, attenuated dengue-2 virus is vaccine strain PDK-53. 9. The immunogenic composition according to claim 2 , wherein the live, attenuated dengue-2 virus comprises the amino acid sequence of SEQ ID NO: 16. 10. The immunogenic composition of claim 2 , wherein the live, attenuated dengue-2 virus comprises the nucleic acid sequence of SEQ ID NO: 15. 11. The immunogenic composition of claim 1 , wherein the composition comprises nucleic acid sequences from at least three dengue virus serotypes. 12. The immunogenic composition of claim 1 , further comprising a dengue-2/dengue-1 chimera. 13. The immunogenic of claim 12 , wherein the dengue-2/dengue-1 chimera comprises the amino acid sequence of SEQ ID NO: 28 or the nucleic acid sequence of SEQ ID NO: 27. 14. The immunogenic composition of claim 1 , further comprising a dengue-2/dengue-3 chimera. 15. The immunogenic composition of claim 14 , wherein the dengue-2/dengue-3 chimera comprises the amino acid sequence of SEQ ID NO: 10 or the nucleic acid sequence of SEQ ID NO: 9. 16. The immunogenic composition of claim 1 , further comprising a dengue-2/dengue-4 chimera. 17. The immunogenic composition of claim 16 , wherein the dengue-2/dengue-4 chimera comprises the amino acid sequence of SEQ ID NO: 12 or the nucleic acid sequence of SEQ ID NO: 11. 18. The immunogenic composition of claim 1 , wherein the nucleic acid chimera comprises a dengue-2/Zika virus chimera and the nucleic acid chimera encodes at least one Zika virus structural protein. 19. The immunogenic composition of claim 1 , further comprising an immunogenic composition against a different flavivirus selected from the group consisting of West Nile virus, Japanese encephalitis virus, St. Louis encephalitis virus, tick-borne encephalitis virus, yellow fever virus, and a combination thereof. 20. The immunogenic composition of claim 1 , wherein the immunogenic composition is formulated for intramuscular, subcutaneous, or inhalation administration to a subject. 21. A method of inducing an immune response to Zika virus in a subject, comprising administering to the subject the immunogenic composition of claim 1 . 22. The method of claim 21 , wherein the composition is formulated for subcutaneous administration to the subject. 23. A kit comprising the immunogenic composition of claim 1 and a container. 24. A nucleic acid construct comprising a nucleic acid chimera encoding: (i) a flavivirus structural protein, wherein the flavivirus structural protein is selected from the group consisting of: a C protein of Zika virus, a prM protein of Zika virus, and an E protein of Zika virus; and (ii) a non-structural proteins from a second different flavivirus wherein the second different flavivirus comprises a live, attenuated dengue-2 virus containing non-conservative amino acid substitutions or other flavivirus genomes containing analogous mutations at the same loci as the dengue-2 virus, wherein the chimera is avirulent. 25. The nucleic acid construct of claim 24 , wherein the nucleic acid construct encodes a polypeptide sequence that is part of a live, attenuated virus. 26. A vector encoding the nucleic acid construct of claim 25 . 27. An isolated cell comprising the nucleic acid construct of claim 25 . 28. The immunogenic composition of claim 1 , wherein the flavivirus structural protein is the prM protein of Zika virus and further comprising an E protein of Zika virus. 29. The immunogenic composition of claim 28 , further comprising a C protein of Zika virus.