α/β-peptide mimics of Z-domain peptides

What is claimed is: 1. A method of making peptidomimetic affinity reagents, the method comprising: generating a Z-domain scaffold peptide having affinity recognition and/or binding to a desired target compound substituting at least one β-amino acid residue into at least one helical domain of the Z-domain scaffold peptide, thereby generating an α/β-peptide mimic of a Z-domain scaffold peptide. 2. The method of claim 1 , wherein the at least one β-amino acid residue is cyclically constrained by a ring structure that incorporates alpha-position and beta-position carbon atoms of the β-amino acid residue. 3. The method of claim 1 , wherein the Z-domain scaffold peptide comprises three helical domains designated helix 1, helix 2, and helix 3, and further comprising cleaving helix 3 from the α/β-peptide mimic, and wherein the at least one β-amino acid residue is substituted into helix 1 or helix 2. 4. The method claim 1 , further comprising forming at least one disulfide bond between two residues in the α/β-peptide mimic. 5. The method of claim 1 , wherein the unnatural α/β-peptide mimic of the Z-domain scaffold peptide is labeled. 6. A method of making peptidomimetic affinity reagents, the method comprising: generating an unnatural α/β-peptide mimic of a Z-domain scaffold comprising no more than 60 amino acid residues, and including at least one β-amino acid residue, and having specific affinity recognition and/or binding to a desired target compound. 7. The method of claim 6 , further comprising incorporating into the α/β-peptide mimic of a Z-domain scaffold at least two amino acid residues that are capable of forming a disulfide bridge between them and forming a disulfide bond between the at least two amino acid residues. 8. The method of claim 6 , wherein the at least one β-amino acid residue is cyclically constrained by a ring structure that incorporates alpha-position and beta-position carbon atoms of the β-amino acid residue. 9. The method of claim 6 , wherein the α/β-peptide mimic of a Z-domain scaffold adopts three distinct helical domains in aqueous solution. 10. The method of claim 6 , wherein the α/β-peptide mimic of a Z-domain scaffold has no more than 45 residues and adopts two distinct helical domains in aqueous solution. 11. The method of claim 6 , wherein the unnatural α/β-peptide mimic of the Z-domain scaffold peptide is labeled. 12. A method of inhibiting proteolytic degradation of a Z-domain scaffold peptide, the method comprising providing an unnatural α/β-peptide mimic of the Z-domain scaffold peptide in which at least one α-amino acid residue present in the Z-domain scaffold peptide is replaced with at least one β-amino acid residue. 13. The method of claim 12 , comprising providing an unnatural α/β-peptide mimic having at least three β-amino acid residues. 14. The method of claim 12 , wherein the unnatural α/β-peptide mimic of the Z-domain scaffold peptide is labeled. 15. An unnatural α/β-peptide mimic of a Z-domain scaffold peptide, the α/β-peptide mimic comprising from 25 to 60 amino acid residues, having zero, one, two, or three distinct helical domains in aqueous solution, wherein at least one of the amino acid residues is a β-amino acid residue, and salts thereof. 16. The α/β-peptide mimic of a Z-domain scaffold of claim 15 , wherein the α/β-peptide mimic of the Z-domain scaffold peptide is labeled. 17. The α/β-peptide mimic of a Z-domain scaffold of claim 15 , conjugated, bound, or linked to a therapeutic agent. 18. An unnatural α/β-peptide mimic of a Z-domain scaffold peptide, the α/β-peptide mimic comprising no more than 45 amino acid residues, having no more than two distinct helical domains in aqueous solution, wherein at least one of the amino acid residues is a β-amino acid residue, and including at least one disulfide bond, and salts thereof. 19. The α/β-peptide mimic of a Z-domain scaffold of claim 18 , wherein the α/β-peptide mimic of the Z-domain scaffold peptide is labeled. 20. The α/β-peptide mimic of a Z-domain scaffold of claim 18 , wherein the at least one β-amino acid residue is a cyclically constrained β-amino acid residue. 21. The α/β-peptide mimic of a Z-domain scaffold of claim 18 , conjugated, bound, or linked to a therapeutic agent. 22. A method of selectively delivering a therapeutic agent to a specific cell type or a specific tissue, the method comprising conjugating, binding, or linking the therapeutic agent to an α/β-peptide mimic of a Z-domain scaffold as recited in claim 15 to yield a mimic-agent conjugate, wherein the α/β-peptide mimic selectively binds to the specific cell type or the specific tissue, and then contacting the mimic-agent conjugate with the specific cell type or specific tissue. 23. The method of claim 22 , wherein the α/β-peptide mimic selectively binds to a neoplastic cell.