Compositions and methods related to ebolavirus vaccines

What is claimed is: 1. A polynucleotide encoding an engineered Ebolavirus glycoprotein (GP) protein that comprises (a) substitution of residue W615 in heptad repeat 2 (HR2) with residue L, A, V, I or F, and (b) one or more proline substitutions in heptad repeat 1 C segment (HR1 C ); wherein the amino acid numbering is based on Zaire Ebolavirus GP sequence with UniProt ID Q05320 (SEQ ID NO:1). 2. The polynucleotide of claim 1 , wherein the Ebolavirus is Zaire Ebolavirus (EBOV), Sudan virus (SUDV), nil forest virus (TAFV), Bundibugyo virus (BDBV), or Reston Ebolavirus (RESTV). 3. The polynucleotide of claim 1 , wherein the proline substitutions comprise T577P or L579P. 4. The polynucleotide of claim 1 , further comprising a truncation at the C-terminus of the membrane proximal external region (MPER). 5. The polynucleotide of claim 4 , further comprising (a) a deletion of the mucin-like domain (MLD) deleted from the GP1 subunit, and/or (b) a deletion of MPER from the GP2 subunit. 6. A polynucleotide encoding an engineered Ebolavirus glycoprotein (GP) protein that comprises (a) a truncated soluble GP of an Ebolavirus that has the mucin-like domain (MLD) deleted from the GP1 subunit and the membrane proximal external region (MPER) deleted from the GP2 subunit, and (b) substitution of residue W615 in heptad repeat 2 (HR2) with residue L, A, V, I or F; wherein the amino acid numbering is based on Zaire Ebolavirus GP sequence corresponding to UniProt ID Q05320 (SEQ ID NO:1). 7. The polynucleotide of claim 6 , further comprising one or more modifications selected from (i) an extension of HR2 at the C terminus, (ii) one or more proline substitutions in heptad repeat 1 C segment (HR1 C ), and (iii) one or more engineered inter-GP disulfide bonds. 8. The polynucleotide of claim 6 , wherein the truncated soluble GP comprises SEQ ID NO:2 or SEQ ID NO:3, or a variant thereof with at least 99% sequence identity. 9. The polynucleotide of claim 6 , comprising the sequence SEQ ID NO:4, or a variant thereof with at least 99% sequence identity. 10. The polynucleotide of claim 6 , further comprising an extension of HR2 at the C-terminus. 11. The polynucleotide of claim 10 , wherein the HR2 extension comprises (a) extending HR2 C terminus with a N-terminal fragment of the adjacent membrane proximal external region (MPER) of the Ebolavirus glycoprotein or (b) replacing a HR2 C-terminal fragment with a longer leucine zipper motif. 12. The polynucleotide of claim 10 , wherein the HR2 extension comprises (a) extending the HR2 C terminus from residue 632 to residue 637 in MPER, (b) extending the HR2 C terminus from residue 632 to residues 643 in MPER, or (c) replacing residues 617-632 with a GCN4 leucine zipper sequence shown in SEQ ID NO:34. 13. The polynucleotide of claim 10 , wherein the W615 substitution comprises W615L substitution or P612G/W615F double mutation. 14. The polynucleotide of claim 10 , comprising (a) W615L substitution and (b) extension of the HR2 C terminus from residue 632 to residue 637 in MPER of the Ebolavirus GP. 15. The polynucleotide of claim 10 , comprising (a) P612G/W615F double mutation in HR2 and (b) replacement of residues 617-632 with a GCN4 leucine zipper sequence shown in SEQ ID NO:34. 16. The polynucleotide of claim 10 , comprising an amino acid sequence as set forth in any one of SEQ ID NOs:5-8, or a variant thereof with at least 99% sequence identity. 17. The polynucleotide of claim 10 , further comprising a C-terminal trimerization motif. 18. The polynucleotide of claim 17 , wherein the C-terminal trimerization motif comprises SEQ ID NO:29 or SEQ ID NO:30, or a variant thereof with at least 99% sequence identity. 19. The polynucleotide of claim 6 , further comprising one or more proline substitutions in the HR1C segment. 20. The polynucleotide of claim 19 , comprising an amino acid sequence as set forth in any one of SEQ ID NOs:9-17 and 20, or a variant thereof with at least 99% sequence identity. 21. The polynucleotide of claim 19 , comprising (a) W615L substitution, (b) proline substitution T577P or L579P, and (c) HR2 extension from residue 632 to residue 637 in MPER. 22. The polynucleotide of claim 19 , further comprising a C-terminal trimerization motif. 23. The polynucleotide of claim 6 , further comprising an engineered disulfide bond between two neighboring GP protomers. 24. The polynucleotide of claim 23 , wherein the engineered disulfide bond is engineered between residues G91/A575 (SS2), F153/Y534 (SS1), T520/A575 (SS3), G1574532 (SS4), D522/A575 (SS5) or K56/G599 (SS6). 25. A pharmaceutical composition, comprising the polynucleotide of claim 6 , and a pharmaceutically acceptable carrier. 26. A polynucleotide encoding a fusion polypeptide that comprises an engineered Ebolavirus glycoprotein (GP) protein and the subunit sequence of a self-assembling nanoparticle, wherein the engineered Ebolavirus GP protein comprises (a) substitution of residue W615 in heptad repeat 2 (HR2) with residue L, A, V, I or F, and (b) one or more proline substitutions in heptad repeat 1 C segment (HR1 C ); wherein the amino acid numbering is based on Zaire Ebolavirus GP sequence with UniProt ID Q05320 (SEQ ID NO:1). 27. The polynucleotide of claim 26 , wherein the engineered Ebolavirus GP protein is fused at its C-terminus to the subunit sequence of the self-assembling nanoparticle. 28. The polynucleotide of claim 26 , wherein the fusion polypeptide comprises from N terminus to C terminus (a) the engineered Ebolavirus GP protein, linker sequence G 4 S (SEQ ID NO:43), nanoparticle sequence ferritin, (b) the engineered Ebolavirus GP protein, linker sequence G 4 S (SEQ ID NO:43), nanoparticle sequence E2p, or (c) the engineered Ebolavirus GP protein, linker sequence (G 4 S) 2 (SEQ ID NO:42), nanoparticle sequence I3-01v9; wherein the engineered Ebolavirus GP protein comprises W615L substitution, proline substitution T577P, and HR2 extension from residue 632 to residue 637 in MPER. 29. The polynucleotide of claim 28 , wherein the fusion polypeptide further comprises a locking domain and/or a T-cell epitope that is fused to the C-terminus of the nanoparticle subunit sequence. 30. The polynucleotide of claim 29 , encoding (1) a fusion polypeptide sequence that comprises from N-terminus to C-terminus (a) the engineered Ebolavirus GP protein shown in SEQ ID NO:17, nanoparticle subunit sequence shown in SEQ ID NO:36 (E2p), locking domain shown in SEQ ID NO:39 (LD4), and T cell epitope shown in SEQ ID NO:31 or (b) the engineered Ebolavirus GP protein shown in SEQ ID NO:17, nanoparticle sequence shown in SEQ ID NO:37 (I3-01v9), locking domain shown in SEQ ID NO:40 (LD7), or (2) a variant of the fusion polypeptide sequence with at least 99% sequence identity.