Fusion proteins and use thereof for preparing vaccines

The invention claimed is: 1. An immunogenic fusion protein comprising at least two peptides: a) on the C-terminal side, a first peptide which consists of: an amino acid sequence of the protein S or the protein M of a human hepatitis B virus (HBV) isolate, wherein the sequence of the protein S is chosen from the group consisting of SEQ ID NO: 1 and 2, and the sequence of the protein M is chosen from the group consisting of SEQ ID NO: 3 and 4, or an amino acid sequence with a percent identity of at least 95% with said amino acid sequence of the protein S or the protein M, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the HBV virus, or, and b) on the N-terminal side, a second peptide which consists of: a sequence of amino acids comprising at least one transmembrane domain and the ectodomain of at least one protein of a Zika virus isolate, or an amino acid sequence with a percent identity of at least 95% with said amino acid sequence of at least one transmembrane domain and the ectodomain of at least one protein of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or immunogenic properties against the Zika virus, said protein of a Zika virus isolate being chosen from among the envelope protein E represented by SEQ ID NO. 15 or a fusion peptide comprising the envelope protein E and the protein prM represented by SEQ ID NO. 50. 2. An immunogenic fusion protein according to claim 1 , wherein the first peptide located on the C-terminal side thereof consists of: the amino acid sequence of the protein S of a human HBV isolate, wherein the sequence of the protein S is represented by of SEQ ID NO: 1, or an amino acid sequence presenting a percent identity of at least 95% with said amino acid sequence of the protein S represented by of SEQ ID NO: 1, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV. 3. An immunogenic fusion protein according to claim 1 , wherein the first peptide located on the C-terminal side thereof consists of: the amino acid sequence of the protein S of a human HBV isolate, wherein the sequence of the protein S is represented by of SEQ ID NO: 2, or an amino acid sequence presenting a percent identity of at least 95% with said amino acid sequence of the protein S represented by of SEQ ID NO: 2, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV. 4. An immunogenic fusion protein according to claim 1 , wherein the first peptide located on the C-terminal side thereof consists of: the amino acid sequence of the protein M of a human HBV isolate, wherein the sequence of the protein M is represented by of SEQ ID NO: 3, or an amino acid sequence presenting a percent identity of at least 95% with said amino acid sequence of the protein M deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV. 5. An immunogenic fusion protein according to claim 1 , wherein the first peptide located on the C-terminal side thereof consists of: the amino acid sequence of the protein M of a human HBV isolate, wherein the sequence of the protein M is represented by of SEQ ID NO: 4, or an amino acid sequence presenting a percent identity of at least 95% with said amino acid sequence of the protein M not deleted from a sequence of 1 to 54 amino acids located at the N-terminal end thereof, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV. 6. An immunogenic fusion protein according to claim 1 , wherein the second peptide located on the N-terminal side thereof consists of: the amino acid sequence of at least one transmembrane domain and the ectodomain of the envelope protein E of a Zika virus isolate, or an amino acid sequence presenting an identity percent of at least 95%, with said amino acid sequence of at least one transmembrane domain and the ectodomain of the envelope protein E of a Zika virus isolate, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus. 7. An immunogenic fusion protein according to claim 1 , wherein the second peptide located on the N-terminal side thereof consists of: the amino acid sequence of a fusion peptide comprising at least one transmembrane domain and the ectodomain of the envelope protein E of a Zika virus isolate and the protein prM of a Zika virus isolate, wherein said amino acid sequence is chosen from among the envelope protein E represented by SEQ ID NO. 15 or a fusion peptide comprising the envelope protein E and the protein prM represented by SEQ ID NO. 50, or an amino acid sequence presenting an identity percent of at 95%, with said amino acid sequence of said fusion peptide, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the Zika virus. 8. An immunogenic fusion protein according to claim 1 , wherein said fusion protein comprises: the amino acid sequence represented by: SEQ ID NO. 7 or SEQ ID NO. 17, or SEQ ID NO. 8 or SEQ ID NO. 18, or SEQ ID NO. 9 or SEQ ID NO. 19, or SEQ ID NO. 10 or SEQ ID NO. 20, or SEQ ID NO. 11 or SEQ ID NO. 21, or SEQ ID NO. 12 or SEQ ID NO. 22, or SEQ ID NO. 13 or SEQ ID NO. 23, or SEQ ID NO. 14 or SEQ ID NO. 24, or an amino acid sequence presenting an identity percent of at least 95% with said SEQ ID NO. 7, SEQ ID NO. 17, SEQ ID NO. 8, SEQ ID NO. 18, SEQ ID NO. 9, SEQ ID NO. 19, SEQ ID NO. 10, SEQ ID NO. 20, SEQ ID NO. 11, SEQ ID NO. 21, SEQ ID NO. 12, SEQ ID NO. 22, SEQ ID NO. 13, SEQ ID NO. 23, SEQ ID NO. 14, SEQ ID NO. 24, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV and/or the Zika virus, or the amino acid sequence of a synthetic variant derived from said SEQ ID NO. 7, SEQ ID NO. 17, SEQ ID NO. 8, SEQ ID NO. 18, SEQ ID NO. 9, SEQ ID NO. 19, SEQ ID NO. 10, SEQ ID NO. 20, SEQ ID NO. 11, SEQ ID NO. 21, SEQ ID NO. 12, SEQ ID NO. 22, SEQ ID NO. 13, SEQ ID NO. 23, SEQ ID NO. 14, SEQ ID NO. 24, provided that said amino acid sequence maintains the ability to form subviral, non-infectious particles and/or the immunogenic properties against the human HBV and/or the Zika virus. 9. Nucleic acid molecules coding a fusion protein according to claim 1 . 10. A subviral, non-infectious and immunogenic particle comprising the following proteins: a protein comprising the wild-type domain S of the surface antigen of a hepatitis B virus isolate, and the fusion protein according to claim 1 . 11. An immunogenic fusion protein according to claim 1 , for its use as a medication, notably as a vaccine. 12. An immunogenic fusion protein according to claim 1 , for its use in preventing and/or treating hepatitis B and/or Zika virus infections. 13. An immunogenic fusion protein according to claim 1 , wherein the second peptide located on the N-terminal side thereof consists of: the sequence of amino acids of at least one transmembrane domain chosen from the group consisting of the amino acid sequences b